BANGABANDHU SHEIKH MUJIB MEDICAL UNIVERSITY Dhaka, Bangladesh October 2005
Antibiotic Guidelines
BANGABANDHU SHEIKH M...
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BANGABANDHU SHEIKH MUJIB MEDICAL UNIVERSITY Dhaka, Bangladesh October 2005
Antibiotic Guidelines
BANGABANDHU SHEIKH MUJIB MEDICAL UNIVERSITY Dhaka, Bangladesh October 2005
ISBN
:
984-32-2715-8
Published by : Bangabandhu Sheikh Mujib Medical University Shahbag, Dhaka, Bangladesh
© All rights reserved by the BSMMU
First Edition: October, 2005 ,
Price: T k. 50.00
Printed by: Asian Colour Printing 130, DIT Extension Road Fakirerpool, Dhaka-1000 Tel: 9357726, 8362258
Acknowledgement All teachers of BSMMU who actively participate in preparing this guidelines.
Committee to prepare the manual I.
Prof. M . A. Mannan
Chairman
Pro-Vice Chancellor (Hospital)
2.
Prof. Md. Salehuddin
Member
Department of Ophthalmology
3.
Prof. Md. Ruhul Amin Miah
Member
Department of Microbiology
4.
Prof. M. J alilur Rahman
Member
Department of Hematology
5.
Prof. M. Anwar Hussain
Member
Department of Obstetrics & Gynecology
6.
Prof. Motiur Rahman Molla
PREFACE Member
Department of Maxillofacial Surgery
7.
Prof. Zahidul Haq
Member
Department of Surgery
8.
Prof. Nasim Akhter Chowdhury
Antibiotics are an expensive sector of modem medicine.
In
Bangladesh, we spend about forty percent of our pharmacy budget of more than Taka four thousand crores on antibiotics alone. No doubt antibiotics are essential medicines. They selectively kill organisms that are sensitive to them. As a result, if used for Member
prolonged periods, not only such use is uneconomic, but they also produce unwanted side effects and may encourage the overgrowth of
Department of Medicine
resistant organisms. As antibiotic resistance is increasing, antibiotic
9.
Dr. Hossain Imam Al Hadi
Member
Department of Otolaryngology
10.
Prof. Mir Misbahuddin Department of Pharmacology
abuse carries collective penalties for the individual patient and for the community. Therefore, antibiotics should be used carefully.
Member Secretary
Owing to geographical differences in bacterial sensitivity, each hospital has its own antibiotic guideline. Therefore, this booklet is published on treatment
guideline
that may help our doctors
overcome the above mentioned problems and thereby improve the quality of treatment. Our antibiotic guideline is mainly based on empirical treatment that we are using in BSMMU Hospital. This guideline will be reviewed and updated periodically because of continuing changes in the pattern
of bacterial resistance to antibiotic. In this booklet common diseases
Contents
are highlighted and their appropriate therapeutic recommendations are mentioned. Microbiological statistics of our hospital is presented, though inadequate, may be helpful for our doctors for proper selection of the antibiotic. Constructive criticism and useful suggestions for improving the quality and contents of this booklet are welcomed from its users.
I thank the chairman and members of the committee and contributing faculty members for their active support and help without which this publication on the safe use of antibiotics would not have been seen the light of the day.
� (Prof. M.A. Hadi) Vice Chancellor
Principles of antimicrobial therapy in infectious disease Collection of sample for culture
4
Microbiological statistics
10
Desirable serum antibiotic levels
24
Treatment of specific diseases
25
Acne vulgaris
26
Alveolar abscess
27
Alveolar osteitis (dry socket)
27
Amoebiasis
28
Bite wounds
29
Breast abscess/mastitis
30
Bronchiectasis
31
Bronchitis
32
Chancroid
33
Cellulitis
34
Cerebral abscess
35
Cholecystitis (acute)
36
Cholera
36
Conjunctivitis
37
Corneal ulcer
38
Cystitis (acute uncomplicated)
39
Dysentery (bacillary)
39
Eczema (infected)
40
Enteric fever
40
Febrile neutropenia
41
Genital herpes
42
Giardiasis
43
Gingivitis
44
Pyogenic liver abscess
44
Mastoiditis
44
ANTIBIOTIC GUIDELINE Meningitis
45
Neonatal sepsis
47
Otitis externa
47
Otitis media (acute suppurative)
48
Selection of antimicrobial agent depends on the following factors:
Oral thrush (candidiasis)
49
Agent:
PRINCIPLES OF ANTIMICROBIAL THERAPY IN INFECTIOUS DISEASE
Peptic ulcer (due to helicobacter pylori)
49
Pericoronitis
50
knowledge on possible organism in particular situation
Periodontal abscess
50
aware about situation possible load and virulence
Spontaneous bacterial peritonitis
51
Pharyngitis
51
Pneumonia
52
Prostatitis
55
Pyelonephritis (acute)
55
Sepsis in neuropathic foot in diabetes mellitus
56
Sinusitis
56
Syphilis
57
Tonsillitis
58
Tuberculosis
58
Urethritis (acute, for males)
62
identification of possible agent- identify/suspect
sampling to identify agent
Host and environment: identification of host and environmental factors site of infection immunological status nutritional status precondition affecting susceptibility- congenital heart disease, presence of foreign body, steroid, susceptible disease, liver/renal impairment, heart/respiratory failure
Choice of antibiotic:
Urinary tract infections
62
Vaginal candidiasis
63
Vaginal trichomoniasis
64
which drug to choose- pharmacokinetic properties
Vaginosis (bacterial)
64
choosing combination preparation
Wounds (infected)
65
Guideline for use of antibiotics in renal failure
66
Use of antibiotics in liver disease
67
Antibiotics in pregnancy
78
Drug present in breast milk
70
Management of anaphylactic shock
71
Antibiotic prophylaxis in surgery
72
Antibiotic prophylaxis for nonsurgical conditions
80
Antimicrobial agents associated with photosensitivity
84
Hospital infection control team
85
Index
89
empiric and specific
Monitoring response: clinical estimation of drug level development of resistance/ superinfection
Representative specimen collection before starting therapy It is important to obtain adequate and representative specimens from all potentially infected sites prior to the initiation of antimicrobial therapy. Appropriate antimicrobial therapy is based on definitive identification of pathogenic organisms,
which usually requires
culture. Once antimicrobial therapy has been started, cultures often are rendered sterile, even though viable organisms may remain in the host. It is also important to avoid or minimize contamination by surface contaminants and commensals when collecting specimens.
ANTIBIOTIC GUIDELINE
ANTIBIOTIC GUIDELINE
Initial empirical choice based on the most likely pathogens and susceptibilities In most cases, it may be impossible to determine the exact nature of the infecting organisms before institution of antimicrobial therapy. Initial therapy must therefore be empirical - to make a rational choice
Assays for drugs with narrow therapeutic:toxic ratio For antibiotics such as the aminoglycosides and vancomycin, the measurement of their concentrations in serum/plasma or other body fluids is often useful to avoid excessive levels which are associated
from the many currently available antimicrobial agents, the clinician
with toxicity, yet ensure that adequate (therapeutic) levels are
must be able to predict or "guess" infecting microorganism(s) and the
achieved.
antimicrobial susceptibility thereof.
In these cases, the use of
"bacteriological statistics" i.e. an awareness of those microorganisms most likely to cause infection in a given clinical
setting, in
conjunction with the local antibiotic resistance patterns, may be particularly helpful in choosing an empiric antimicrobial agent.
Pharmacokinetic properties of antibiotics Knowledge of the pharmacodynamic and kinetic properties of antibiotics is imperative in choosing the correct antibiotic and correct dose.
Subsequent need to adjust antimicrobial therapy in light of the sensitivity results
Time dependant killing: (penicillins, cephalosporins, macrolides).
Since different organisms vary in their susceptibility to antimicrobial
concentration (MIC) is crucial in predicting clinical outcome and
agents, it is imperative that we have some means for determining the
cure. Concentrations of members of this group of antibiotics are
antimicrobial susceptibility of the infecting organism(s). Once the
required to be above the MIC for at least 50% of the dosing interval.
pathogen has been isolated, susceptibility testing to be done.
Monitoring therapeutic response In many patients, it is possible to monitor the therapeutic response on clinical grounds alone. Thus the subsidence of fever, the return of well-being, and the disappearance of both local and systemic signs of infection in the patient, all signify an appropriate response. No further formal monitoring is necessary in most cases. An apparent failure to respond clinically may be due to either ineffectiveness of antimicrobial agent(s) (due to resistance or inappropriate route of administration) or to other reasons e.g. a localised infection that requires surgical drainage, or a superinfection
The time that the antibiotic exceeds the mimi mal inhibitory
If the bacterium is more resistant, the MIC is higher with subsequent reduction in time that the antibiotic concentration exceeds the MIC and therefore higher dosages of the drug may be required.
Concentration dependant antibiotics: (quinolones, aminoglyco sides). The more the antibiotic concentration exceeds the MIC, the more killing will take place (irrespective and independent of the time the concentration exceeds the MIC). For this group of antibiotics a ratio of concentration: MIC 10 is required. This implies that a dose regimen should be chosen which results in a serum or tissue concentration of at least 10 times the MIC. Failure to achieve this
etc. Careful reassessment is recommended when considering changes
concentration at the site of infection will lead to clinical and
of antimicrobial therapy.
bacteriological failure, and is likely to induce resistance to the entire
In certain situations, measurement of antimicrobial activity may be
class of antibiotic.
useful in predicting clinical response, e.g. determination of serum bactericidal activity (Schlichter test) in cases of infective endocarditis.
2
3
ANTIBIOTIC GUIDELINE
ANTIBIOTIC GUIDELINE
COLLECTION OF SAMPLE FOR CULTURE
Transport: All specimens should be processed in the laboratory within
URINE SAMPLE
following. a)
Collection:
b)
1. Male: Cleaning the urethral meatus with plain tap water (free skin retracted), allow to dry and at least 30 ml of mid stream urine
2 hours of
collection; if delay is unavoidable more than 2 hours use one of the Refrigerate the urine at
° 4 C in the same container.
Collect and transport in a container with boric acid (O.lg/
10 ml of urine). Any way delay should not be longer than 18 hours after collection.
(MSU) should be collected in sterile container. It is better to collect the first MSU passed at the beginning of the day.
2.
�
Labia is separated and morning mid stream urine (MSU)
should be collected in a wide mouth sterile container.
3.
Children:
Administration of drugs or antidiarrheal substances (mineral oil, barium, bismith, magnesium, antibiotics) should be terminated at least one week before stool collection. - Stool container should be a)
(a) Sterile adhesive bag: · (b) Suprapubic tap: Tap by fingers on the suprapubic region 1 hour after feed (one tap per second) for 10 seconds; 1 minute interval repeat the proced�re.
4.
STOOL SAMPLE
Female: The vulva is cleaned by cotton plug soaked with water
Clean, dry, leak proof, disinfectant free and wide necked container.
b)
A light plastic box or a especially designed glass jar attached spoon with the stopper.
- Amount of stool that is to be collected
Suprapubic aspiration: Occasionally necessary in acute
a)
About a spoonful specimen is sufficient
retention of urine or unconscious patient.
b)
Transfer a portion of stool that contain mucous, pus, blood, if present.
5. Urethral catheterization: Rarely used in children or unconscious patients. Fresh sterile catheter should be used. Urine sample should be collected directly from the catheter, never from collecting bag.
- Send the specimen to the lab as early as possible. - If transport delay is unavoidable Transport medium
a)
surgery/ examination, when necessary.
7. Genito-urinary tuberculosis : 3 consecutive early· morning 1 % boric acid. 4
place specimen in
Cary - Blair media.
Procedure of transport:
6. Ureteric cathelerization: In operation theatre during urological
urine specimen (EMU) or
�
�
24 hours urine in a container containing
With the help of cotton swab, a portion of stool is taken.
b)
Insert the swab in the container of sterile Cary-Blair transpoi\ medium.
c)
Breaking off the swab stick to allow the bottle top to be replaced lightly.
5
ANTIBIOTIC GUIDELINE
ANTIBIOTIC GUIDELINE
- For infants or other patients if necessary 'Rectal Swab' may be collected. a)
W OUND SWAB
Moisten the swab with normal saline & introduce the swab
Sample should be collected from the base of the ulcer or nodule
into rectum (one inch into the anal canal) and kept for 10
following removal of overlying debris or by surgical biopsy of deep
seconds, tum the swab several times with a circular movement. Care should be taken to avoid unnecessary contamination of the specimen with bacteria from anal skin. - Precaution a)
Avoid contaminating the faeces with urine or water
b)
Never store in the incubator
c)
Never store in the refrigerator
ENDOMETRIUM
tissues without contact with the superficial layer of the lesion. If possible two swabs should be collected. Specimens should be placed in sterile container capped properly and send to the laboratory as easily as possible.
SPUTUM COLLECTION Patient instruction -
Collect early morning specimen before breakfast or mouthwash.
-
Rinse mouth with water before collection.
-
Remember that saliva and naso pharyngeal discharge are not sputum. Collect only the exudative material brought up from lungs after a
- Curetting / scrapings / small tissue samples of endometrium should collected aseptically, avoiding lower genital tract contamination and transported in sterile saline. - Send immediately to laboratory.
deep production cough in a dry wide necked leak-proof container. -
Send the container as early as possible. Never refrigerate such sample.
If pulmonary tuberculosis is suspected -
Collect a series of three to six single early morning sputum on successive days.
THROAT SWAB
-
If not possible the 151 sample at spot and 2nd early morning sample.
Swab should be collected in the morning before any mouthwash, food
-
If a patient produces very little sputum,
or drink. Mouth of the patient should be widely opened, neck flexed.
24-48 hours pooled
specimen is needed to yield a positive culture.
Hold the head fixed. Keep the tongue down with a tongue depressor. Oral cavity should be properly illuminated with good light source. A sterile cotton swab (supplied from dept.) is rubbed vigorously over one tonsil, then uvula, other tonsil, the posterior wall of the pharynx and over any other inflamed area. Care should be taken not to touch the tongue, buccal surface or lips. Place the swab stick in the sterile
CONJUNCTIVAL SWAB The conjunctival swab should be taken with a thin sterile cotton swab moistened with sterile trypticase soy !broth sterile normal saline. Conjunctival swab is collected across the lower tarsal conjunctiva and fornix from medial to lateral canthus-taking care not to touch the lid margin.
container tube. It is preferable to take two swabs from the same
Chlamydial infections: Specimen includes scrapings from conjunctiva.
patient. Specimen should be dispatched to the laboratory as soon as
Mycotic infections: Specimen consists of scrapings from the base of
possible.
edge of corneal ulcer.
6
7
ANTIBIOTIC GUIDELINE
ANTIBIOTIC GUIDELINE
CSF Collection and transport - Approximately 5- 10 ml of CSF (in adult patient) should be collected in two sterile tubes (Screw-Capped). Collect about I ml of CSF in tube No. I (for culture) and rest of the portion in tube no. 2 (for other tests). - The specimen should be delivered to the laboratory immediately as early as possible. Do not refrigerate the sample. - If tuberculus meningitis is suspected, 3rd tube is kept in the refrigeration undisturbed to see whether a pellicle or coagulum forms.
METHODS OF COLLECTION OF BLOOD FOR CULTURE - Asepsis of blood culture bottle top Timing of sample collection: a) At spike of febrile illness b) Before antibiotic use c) If antibiotic already started blood should be collected just before next dose of antibiotic. Optimal volume of blood culture: a) For adult minimum 5-1 0 ml b) For children 1-3 ml. c) For neonate I m!.
ASPIRATED FLUIDS Exudates from pleural, peritoneal, pericardial or synovial spaces must be
After collection immediately inoculate blood into culture bottle (Bed side inoculation) and send to laboratory within one hour.
aspirated with aseptic technique. Specimen should be placed in a sterile screw cap tube and sealed properly and transferred to the laboratory within 20 minutes of collection (syringe transport not recommended).
CERVICAL SWAB/ HVS Genital specimen from women - All specimens should be collected during pelvic examination using a speculum. - The speculum should be moistened with warm water before use, but antiseptics or gynecological exploration should not be used. - After inserting the speculum, cervical mucus should be wiped off with a cotton wool ball. -
A sampling swab should be then be introduced into the cervical canal and rotated for at least 10 seconds before withdrawal.
- Specimen should be transported in Amies and Stuart transport media. For urethral discharge and genital ulcer the patient should be referred to Microbiology Department.
8
9
ANTIBIOTIC G U I D ELINE
"DESIRABLE" SERUM ANTIBIOTIC LEVELS (MG/L) Peak
Trough
Increased risk of toxicity
Gentamicin
6
-
12
<
1.5
Trough> 2
Tobramycin
6
-
12
<
1.5
Trough> 2
Netilmicin
6
-
12
<
1.5
Trough> 2
Amikacin
15 - 30
<
1.5
Trough> 5
Vancomycin
20 - 40
5 - 10
Trough> 1 0
TREATMENT OF SPECIFIC DISEASES
24
ANTIBIOTIC GUIDELINE
ANTIBIOTIC GUIDELINE
In case of inflammatory acne, comedones, papules or pustules
ACNE VU LGARIS In case of comedonal, blackheads, whiteheads, earliest form with no inflammation
There is proliferation of P
acnes and desquamation of follicular cells.
Drug of choice
There is excessive sebum production and gland obstruction. Goal is
Erythromycin plus
Apply cream (3%) locally twice daily
prevention, reduction in the number of new comedones and creates an
Benzoyl peroxide plus
Apply cream (5%) locally twice daily
Doxycycline
100 mg orally in empty stomach twice daily for 4-5 months
environment unfavorable to
Propionibacterium acnes.
Drug of choice Tretinoin
Apply cream (0.05% ) locally once daily
Tretinoin is an acid form of retinal. It is a keratolytic agent that reduces follicular hyperkeratosis by stimulating the turnover of epithelial cells. Benefit is seen after 2 months. It has initant activity and may promote UV -induced skin cancer. The drug should be avoided in sunny weather and in pregnancy. Tretinoin may initially be applied for short intervals of time and the strength and duration gradually increased. It should not be used in combination with other keratolytics. Topical corticosteroid should not be used to treat acne.
In case of mild inflammatory acne, small papules or pustules There is proliferation of P
acnes and desquamation of follicular cells.
Drug of choice Azelaic acid
Apply cream (20%) locally twice daily for up to 6 moni hs
or Erythromycin
Apply cream (3%) locally twice daily
500 mg orally after taking meal daily for 4 days a week for 6 weeks
Azelaic acid inhibits the growth of Propiollibacterium spp. And reduces keratinization. Improvement usually occurs within 4 weeks. Topical application of azelaic acid may produce a transient skin irritation that disappears on continued treatment. It should not be applied to the eys, mouth, or other mucous membranes. Erythromycin and azithromycin are macrolid antibiotics with wide spectrum of activity. Oral administration of azithromycin is preferred over erythromycin due to its less gastrointestinal adverse effects though there may be diarrhea, nausea and abdominal pain. Azithromycin should be avoided in patient of liver disease due to high hepatic excretion.
26
Administration of doxycycline in empty stomach ensures better absorption. Oral erythromycin may be used as an alternative to doxycycline. However, resistance to erythromycin is increasing so it is usually reserved for those patients in whom other antimicrobials are unsuitable.
ALVEOLAR ABSCESS Alveolar abscess is the continuation of periapical abscess. It is caused by
Streptococcus, Peptococcus, Bacteroides and Fusobacterium.
Drug of choice Amoxycillin
500 mg orally 8 hourly for 5 - 7 days
or Flucloxacillin
250-500 mg orally 6 hourly for 5 - 7 days
plus Metronidazole
plus Azithromycin
Banzoyl peroxide has mild keratolytic properties. Topical application of benzoyl peroxide may produce skin irritation, particularly on beginning treatment. Caution is required when applying it near the eyes, the mouth and other sensitive areas.
200-400 mg orally 8 hourly for 5 - 7 days
Drainage of pus is important.
ALVEOLAR OSTEITIS (Dry socket) Alveolar osteitis is the most frequent painful complication of extraction. Pathogens are mainly anaerobes. Drug of choice Cefradine
500 mg orally 8 hourly for 5-7 days
plus Metronidazole
200-400 mg orally thrice daily for 5 days
Warm saline mouth rinses. Socket dressing is required.
27
ANTIBIOTIC GU I D ELINE
ANTIBIOTIC GU I DELI NE
BITE WOU N DS
AMOEBIASIS Amoebiasis (amoebic dysentery) is a protozoan parasite infection
Bites may be by cat, dog, rat, snake, bee, hornet, insect, bat, monkey.
Entamoeba histolytica. It exists in two forms: the hardy
Pasteurella multocida (cats and dogs), Eikenella corrodens (humans), Staphylococcus aureus, Streptococcus spp., and/or oral anaerobes.
caused by
infective cyst and the more fragile potentially pathogenic tropozoite. The disease spreads between humans by its cysts. The parasite is now
E. dispar (non-pathogenic) histolytica (pathogenic). Cysts of these two species are
known to consist of two separate species: and E.
morphologically
identical,
distinguishable only
by
molecular
techniques, isoenzyme studies or monoclonal antibody typing. Only
E. histolytica can give rise to amoebic dysentery or extraintestinal amoebiasis (amoebic liver abscess).
daily for 5-1 0 days
plus Co-amoxiclav
2 g once daily orally for 3 days
plus Rabies vaccine
or Secnidazole
2 g (30 mg/kg in children) single dose orally
Drug of choice 500 m g orally 1 2 hourly for 1 0- 1 4 days
plus 80 mg intravenously 8 hourly for 1 0- 1 4 days
plus Metronidazole
28
375 / 625 mg orally after meal 8 hourly. Duration of treatment depends on the clinical condition 1 ml intramuscularly at the deltoid region, one each on days
plus Human rabies
20 I U/kg body weight given once on day O. If a natomically
immune globulin feasible, the half dose should be infiltrated around the wound(s), the rest should be administered intramuscularly in the gluteal area There are several types of rabies vaccine available in the drug store. The dosage schedule of each vaccine varies. So, please check the dose schedule of rabies vaccine from the supplied patient information leaflet and administer accordingly. Corticosteroid should not be used because in mouse model, it increases the mortality rate and shorten the incubation period. Rabies postexposure prophylaxis , which is highly effective if given prompt/yo Combination therapy may be superior to therapy with a single agent. Because immunization by the intramuscular route may take a week or more to produce detectable immune response, multiple sites (e.g., 8 or 4 sites) intradermal immunization may be considered to accelerate the response.
BI LIARY SEPSIS
Gentamicin
All post-exposure treatment should begun with immediate, thorough cleaning of all wounds with soap and water. Then treat with 70% ethanol or an iodine tincture. Where possible, wounds should be kept open or only sutured to secure apposition
0, 3, 7, 1 4 and 28
Both metronidazole and tinidazole are effective against tropozoites. Tinidazole has longer duration of action over metronidazole. In both the cases the patient may complain nausea, vomiting, diarrhea, furred tongue and an unpleasant metallic taste in the mouth. Rashes, urticaria and angioedema may occur. Peripheral neuropathy occurs if treatment is prolonged and epileptiform seizures if the dose is high. Follow-up stool examination is always necessary because no regimen is completely effective in eradicating intestinal infection. Use of chemoprophylactic agent is not advised.
Ciprofloxacin
Drug of choice
400-800 mg (35 mg/kg/day in children) orally thrice
or Tinidazole
In case of dog bites Only 5% of the dog bites become infected. Prophylaxis may be worthwhile.
Local wound cleaning
Drug of choice Metronidazole
Microorganisms involved are
200-400 mg orally thrice daily for 5 days
Rabies vaccine is the inactivated rabies virus in chick embryo ceil culture. Its potency is equal to or more than 2.5 IU. The immunization schedule must be followed exactly, even if considerable time has elapsed since exposure. The vaccine should be stored at 0 to 4° C . It should not be used after the expiry date. The vaccine should be used immediately after reconstitution. Intravas-cular administration may cause anaphy l actic shock Human rabies immune globulin neutralizes the virus before its invasion of the
29
ANTIBIOTIC GUIDELI N E
ANTIBIOTIC GUIDELINE
nervous system. I t should not b e administered i n the same syringe, o r into the same anatomical site as vaccine, or more than 7 days after the initiation of vaccine. Because Human rabies immune globulin may partially suppress active production of antibody, no more than the recommended dose should be given. Amoxycillin is a 4-hydroxy analogue of ampicillin and is better absorbed from the "ut especially after food. Diarrhoea is less frequent with amoxycillin than with ampicillin. Amoxycillin is preferred because of its greater bioavailability and fewer side effects. Clavulanic acid is a beta-Iactam compound which has little intrinsic antibacterial acitivity but is important because it binds competitively to beta lactarnases. Thereby competitively penicillin protects it against bacteria which owe their resistance to production of beta-Iactamase, i.e., clavulanic acid acts as a "suicide" inhibitor. Combination of amoxycillin and c1avulanic acid is known as co-amoxiclav.
In case of snake bite (treatment within the hospital) Drug of choice
Cloxacillin is narrow spectrum penicillin that resists degradation by gastric acid and is absorbed from the gut. Food markedly interferes with absorption. Cefradine is a first-generation cephalosphorin antibiotic. It is available in oral and parenteral preparation.
In case of nonlactating woman It is usually due to anaerobes and/or
Staphylococcus aureus.
Drug of choice Flucloxacillin
500 mg orally 6 hourly
or Cloxacillin
Polyvalent
5-20 vials should be diluted ( 1 0 ml each) and then added to
or
antiserum
500 ml of intravenous fluid and infused slowly over a period
Cefradine
of about 4 hours
500 mg orally 6 hourly 500 mg intravenously or deep intramuscularly 6 hourly. I ntravenous administration should be done in 5 min
plus
plus
tetanus
250-500 units deep intramuscularly or tetanus toxoid (primary
immunoglobulin
immunization) intramuscularly depending on the immunization status of the victim
Tetanus toxoid should be given at the same time but at a separate site. Any antibiotic (preferable penicillin) may be prescribed if there is any sign of infection.
Metronidazole
7.5 mg/kg intravenously 6 hourly
Flucloxacillin is better absorbed and gives higher concentration than does cloxacillin. It may cause cholestatic jaundice, particularly when used for more than 2 weeks or to patients >55 years.
BREAST ABSCESSIMASTITIS
Metronidazole is one of the azoles and is bacteriostatic. In anaerobic microorganisms metronidazole is converted into an active form by reduction of its nitro group. This binds to DNA and prevents nucleic acid formation.
In case of lactating woman
Pretreatment aerobic culture is required. Surgical drainage for abscess may be done.
Mastitis is usually due to
Staphylococcus aureus. There is no
contraindication of breast feeding, rather continuing breast feeding helps response to antibiotic therapy. Drug of choice Flucloxacillin
Drug of choice 500 mg orally 6 hourly
or Cloxacillin
500 mg orally 6 hourly
or Cefradine
30
BRONCHIECTASIS
Ampicillin or
500 mg orally 6 hourly for 1 4 days
Amoxycillin
500 mg orally 8 hourly for 1 4 days
or 500 mg orally 6 hourly
Co-trimoxazole
1 DS tablet twice daily orally for 1 4 days
31
ANTIBIOTIC GUIDELINE
In case ofpseudomonas aeroginossa
ANTIBIOTIC GUI DELINE
Very rarely, an infection caused by a fungus can cause acute bronchitis. If severe, secondary bacterial infection may be assumed,
Drug of choice C iprofloxacin or
500 mg orally 1 2 hourly for 1 4 days
Cefotaxime
1 9 intravenously 8 hourly for 1 4 days
usually due to
Streptococcus pneumoniae or Haemophilus injluenzae
Drug of choice Amoxycillin
500 mg orally 8 hourly for 7 days
or Erythromycin
In chronic case Drug of choice Amoxycillin
Tetracycline 500 mg orally 8 hourly for 4 weeks
or Polymyxin B
500 mg orally 8 hourly for 7 days
or
1 -2 mega units inhaled twice daily
500 mg orally 6 hourly for 7 days
Dose of amoxicillin should be reduced in severe renal impairment. If the patient is a smoker, then cut down on the number of cigarette smoke, or stop smoking altogether. This will help the bronchial tree heal faster. Erythromycin is an effective alternative choice for penicillin-allergic patients.
Or Amoxycillin followed by Co-trimoxazole
500 mg orally 8 hourly for 1 4 days 1 OS tablet orally twice daily for 1 4 days
followed by Tetracycline
500 mg orally 6 hourly for 1 4 days
B RONCHITIS
In case acute exacerbation of chronic form Viruses are often implicated, at least initially. Secondary infections by bacteria such as Streptococcus pneumoniae, Moraxella catarrhalis and Haemophilus injluenzae may be involved when sputum becomes purulent and increases in volume. Although most clinicians treat patients in this setting with antibiotics, most studies comparing antibiotics with placebo have shown little difference in the rate of resolution of symptoms. If antibiotics are prescribed, these should be based on the culture and sensitivity results and should be given for 7-10 days. Amoxycillin may be considered initially for empiric antibiotic therapy.
In case of acute attack (viral cause) Acute bronchitis is almost always caused by viruses (influenza viruses, adenoviruses). Drug of choice
CHANCROID Chancroid ulcer is due to the Ducrey bacillus, Antibiotic therapy eliminates
Haemophilus ducreyi. H. ducreyi and lesions heal in 1-2
weeks. No antibiotic
In case of acute attack (bacterial cause) Bacterial infection is much less common in bronchitis than we used to think. In the immunocompetent host, acute bronchitis, even when bacterial in etiology, is self-limiting condition. Antibiotic therapy is not required. 32
Drug of choice Co-trimoxazole
1 OS tablet twice daily orally for 7 days
or Cefixime
400 mg orally as a single dose
Co-trimoxazole is a sulfonamide-trimethoprim combination (5: I). Each drug is well absorbed from the gut and is mainly excreted by the kidney. The dose of co-trimoxazole should be reduced when renal function is impaired. 33
ANTIBIOT I C GUI DELINE
ANTIBIOTIC GUIDELIN E
Cefixime is a third-generation cephalosphorin antibiotic and is stable to hydrolysis by many beta-Iactamases. Cefixime is better absorbed from oral suspension than from tablet. Absorption is fairly slow. The most frequent adverse effects are gastrointestinal disturbances especially diarrhea. It should be discontinued if diarrhea is severe.
Caution should b e exercised when gatifloxacin i s used with drugs such as astemizole, terfenadine, cisapride, erythromycin, pentamidine, phenothiazines or tricyclic antidepressants. The dose of gatifloxacin should be reduced in patient with renal im airment. p . ImtIal dose of 400 mg should be followed by maintenance dose of 200 rna ., daily in those with a creatinine clearance less than 40 mllmin.
CELLU LITIS Cellulitis is usually due to
Streptococcus pyogenes, but Staphylo coccus aureus is often also involved. When cellulitis is associated with an open wound, there is usually an exudate that can be obtained for culture. In the setting of cellulitis with unbroken skin, a needle aspiration from the advancing edge can sometimes yield a positive diagnosis. Blood cultures are also of diagnostic value. Ludwig's angina is a severe form of cellulitis which usually arise from the lower second or third molar. It involves the sublingual and
CEREBRAL ABSCESS Bacteria may enter the cerebral substance through penetrating injury, by direct spread from paranasal sinuses or the middle ear or by hematogenous spread from septicemia. Antimicrobial therapy is indicated once the diagnosis is made. Surgical treatment by burrhole aspiration or excision may be necessary. Drug of choice
submandibular spaces bilaterally and it readily spreads into the lateral
Ceftriaxone
pharyngeal and pterygoid spaces and can extend up to mediastinum.
plus
Pathogens involves are mainly Fus iform (bacilli and spiral form), Staphylococcus, Streptococcus, Bacterides, E. coli and Pseudomonas.
Gentamicin
In diabetics and debilitated patients, consider
Metronidazole
Staphylococcus aureus,
followed by
Drug of choice
Cefixime 375/ 62 5 mg orally half an hour before meal 8 hourly for 7 days
or F lucloxacillin
500 mg orally 6 hourly for 7 days
plus phenoxymethyl 2 50 -500 mg 6 hourly half an hour before meal for 7 days penicillin or Gatifloxacin or Ceftriaxone
2 9 intravenously daily in single or divided doses
Crystalline penicilline
200 mg orally twice daily for 6 weeks
10 lac unit intravenously 6 hourly for 1 5 days
plus 80 mg intravenously 8 hourly for 1 5 days
plus Metronidazole
Ceftriaxone is a third-generation cephalosphorin antibiotic. It is highly protein-bound and is able to displace bilirubin from albumin binding sites, causing hyperbilirubinemia.
followed by
Gatifloxacin is a fluoroquinolone antibacterial with actions and uses similar to those of ciprofloxacin. Gatifloxacin may have the potential to prolong the QT interval and should be avoided in patients with existing QT prolongation.
or
34
400 mg intravenously 8 hourly for 1 5 days
or
Gentamicin 400 mg once daily orally for 7 days
80 mg intravenously 8 hourly for 1 5 days
plus
Enterobactericeae and anaerobes.
Co-amoxiclav
1 9 intra muscularly or intravenously
Amoxycillin
Co-amoxiclav
400 mg intravenously 8 hourly for 1 5 days
500 mg orally 8 hourly for 6 weeks
37 5/ 62 5 mg orally after meal 8 hourly for 6 weeks
35
ANTIBIOTIC GUIDELINE
ANTIBIOTIC GUIDELINE
CHOLECYSTITIS (ACUTE)
CONJUNCTIVITIS
The pathogenesis of acute choleystitis is unclear, but the initial
In case of viral conjunctivitis (pink eye)
inflammation is possibly chemically induced. At the time of surgcn-y approximately 50% of cultures of the gall bladder contents are sterile. Infection occurs eventually and in elderly patients or those with diabetes mellitus a severe infection with gas-forming organism can
Viral conjunctivitis is usually unilateral and highly contagious. It is usually self-limited, but there i s evidence that treatment with a topical antibiotic shortens its course and prevent bacterial superinfection. Children are generally kept out of the school for up to
2 weeks after
cause emphysematous cholecystitis.
the onset of infection. Topical antiviral drugs are not administered.
Drug of choice
The use of topical corticosteroid therapy is controversial. Onset of ocular pain and photophobia in an adult suggests associated keratitis
Gentamicin or Ceftriaxone
80 mg intravenously 8 hourly 1 9 intravenously 12 hourly depend ing on the body weight
10 days, the patient should
be referred to an ophthalmologist.
and severity of infection
In case of bacterial conjunctivitis
500 mg intravenously 8 hourly ( 1 5 mg/kg in children)
staphylococci and/or streptococci.
Acute bacterial conjunctivitis in the adult is most often due to
plus Metronidazole
(rare). If there is no improvement in 7 to
Gentamicin is an aminoglycoside antibiotic and has adverse effects like ototoxicity and nephrotoxicity. This drug should not generally be mixed with other drugs in syringes or infusion solutions nor given through the same intravenous line. When gentamicin is given with a beta-lactam administration should generally be at separate sites.
Haemophilus inJluenzae is more
common in children. Treatment
consists
of
a
broad-spectrum
topical
antibiotic
administered 4 times daily. This empirical approach is highly effective, and adverse consequences are infrequent. Drug of choice
.
CHOLERA
Chloramphenicol
Cholera is caused by
or
Vibrio cholerae serotype 01. A new classical toxigenic strain, serotype 0139, established itself in Bangladesh in 1992 and started a new pandemic.
Ciprofloxacin (0.3%)
Antibiotic treatment in adult reduces the duration of excretion of
Ofloxacin (0.3%)
Vibrio and the total volume of fluid needed for replacement.
or
Drug of choice
Tobramycin (0.3%)
Tetracycline
40 mg/kg/day orally for 3 days
or Doxycycline
300 mg (6 mg/kg in children) single dose orally
or Erythromycin or Ciprofloxacin
1
9 single dose orally
There is no risk of staining teeth with such short courses of tetracyclines in case of children. 36
1 -2 drops 4 times daily for 7-1 0 days 1 -2 drops 4 times daily for 7-1 0 days
or 1 -2 drops 4 times daily for 7-10 days 1 -2 drops 4 times daily for 7-1 0 days
Tobramycin is an aminoglycoside antibiotic with actions and uses similar to those of gentamicin. Though highly effective and topical chloramphenicol (0.5 %) has been associated with a rare but devastating aplastic anemia. The topical ciprofloxacin (0.3 %) and ofloxacin (0.3%) are also highly effective but should be reserved for severe infections. Bacitracin (500 units/g) and erythromycin (0.5%). which are effective against Gram-positive bacteria. are available only in the form of ointments that are difficult to install and cause blurred vision. Oral antibiotics alone may be insufficient to treat bacterial conjunctivitis in adults. If the disorder does not improve in one week. the patient should be referred to an ophthalmologist. 37
ANTIBIOTIC G UI D ELINE
ANTIBIOTIC G UIDELINE
In case of conjunctivitis in the newborn It is due to Chlamydia trachomatis or Neisseria gonorrhoeae. The best form of prophylaxis is 2.5% aqueous povidone-iodine solution. In case of conjunctivitis (Chlamydia trachomatis)
CYSTITIS (ACUTE UNCOMPLICATED) This includes patients with asymptomatic bacteriuria. It is usually caused by
Escherichia coli (90%), Staphylococcus saprophyticus (5%), or other Enterobactericeae (5%). Mixed infections are rare. In view of the high prevalence of resistance to ampicillin and co
Drug of choice
trimoxazole, an oral first generation cephalosporin (e.g. cephalexin),
Tetracycline or Erythromycin
O intment twice daily in the eye for 2 weeks 2 5 m g!kg orally twice daily for 2 weeks
or a quinolone (ciprofloxacin, ofloxacin etc) is recommended empiric agents of choice.
as
the
However, some advocate the use of co
trimoxazole for uncomplicated UTI since these antibiotics frequently. achieve concentrations in urine in excess of the MICs of resistant
Investigate and treat parents for genital infection.
strains. This may explain why an uncomplicated UTI may apparently respond to an antibiotic even when the pathogen is judged resistant by
In case of conjunctivitis (Neisseria gonorrhoeae)
laboratory tests.
Drug of choice Ceftriaxone
2 5-50 m g!kg intram uscularly as a single dose
or Gentam icin!
Drug of choice Amoxycillin
S hould be given topically
2 50 mg 8 hourly orally for 3 days ( 50 m g/ kg/day in children)
or
bacitracin
Investigations and treatment of parents needed for genital infection.
Co-trim oxazole Ciprofloxacin
CORN EAL ULCER In case of bacterial cause Bacterial infection is a common sight threatening condition of cornea (keratitis), if untreated often leads to progessive tissue destruction with perforation. Common causes are trauma, contact lens wear and infection from ocular adnexa. Common organism is Staphyllococcus
aureus. Staph epidermis, aeruginosa etc.
Strep pneumoniae,
1 DS tablet 1 2 hourly for 3 days
or 2 50 mg orally 1 2 hourly for 3 days
Single dose therapy is no longer favored. In pregnancy, consider a 7-day regimen of amoxycillin, co-trimoxazole (not in 3rd trimester) or cephalexin. Quinolones should be avoided during pregnancy. A 3-day regimen achieves the best results in patients with uncomplicated UTI. This is considered as effective, costs less, and causes fewer side effects than 7-day regimens. One day regimens are associated with higher recurrence rates.
Pseudomonous
In case of fungal cause Fungal keratitis is common among agriculture workers.
Candida albicans (yeast) and Fusarium solani (filamentous), Aspergillous spp. are common pathogens.
5% for filamentary fungal keratitis and 0.15% solution is recommended for Aspergillous Spp.
DYSENTERY (BACILLARY) Bacillary dysenter (shigellosis) is an enteric infection caused by the Shigella spp.
S. dysentery, S. flexneri, S. boydii, or S. sonnei. Disease S. sonnei infections that may escape detection to more severe S. flexneri infections, while those due to S. dysenteriae may be fulminating and cause death within 48 hours. severity varies from mild
Topical drops of natamycin
Shigella gastroenteritis is essentially self-limiting and antibiotics are
amphotericin B
probably only indicated for severely ill patients, those with dysentery,
and yeast keratitis. 38
and the very young or old. 39
ANTIBIOTIC G UI DELI N E
ANTIBIOTIC G UI DELIN E
Drug of choice 500 mg orally 1 2 hourly for 5-7 days
Ciprofloxacin pius
A single oral dose of 200,000 I U
V itamin A (in case of children)
I n case o f severe case o f enteric fever with delirium, obtundation, stupor; coma, shock Drug of choice 15 mg/kg/day by intravenous infusion (O.2% solution) over 30 min for 1 0- 1 4 days
Ofloxacin plus Dexamethasone
ECZEMA (IN FECTED) Drug of choice Apply thrice daily for u p t o 2 weeks
Combination of gentamicin and hydrocortisone or Combination of neomycin and betamethasone
Apply thrice daily for up to 2 weeks
Use of drug after removal of crusts ensure better access of drug. Topical neomycin is preferred as it is not ordinarily used for systemic infection and therefore, development of drug resistance is less likely. Absorption of neomycin may cause serious injury to eight cranial nerve. Hydrocortisone or betamethasone is used to suppress inflammation.
3 mg/kg by slow intravenous infusion followed by 1 mg/kg every 6 hourly for eight additional doses
The mortality rate was reduced from over 50 % to 10 % in Indonesian adults and children who were given dexamethasone at an initial dose of 3 mg/kg by slow intravenous infusion over a period of 30 minutes, followed by I mg of dexamethasone per kg given at the same rate every 6 hours for 8 additional doses. Hydrocortisone at a lower dose is not effective. There are fe'w data on the treatment of pregnant women with typhoid. The beta-Iactam antibiotics are considered safe. In addition, there have been several case reports of the successful use of fluoroquino lones. Although these drugs have generally been avoided because of concern about safety, the general consensus is that they are also safe
ENTERIC FEVER Enteric fever is caused by
Salmonella typhi and paratyphi.
In case of uncomplicated enteric fever Drug of choice Co-trimoxazole
DS 1 tablet orally 1 2 hourly for 1 4 days
or P-floxacillin
400 mg 1 2 hourly for 1 0- 1 4 days
FEBRILE NEUTROPENIA Patients of febrile neutropeni a are treated at the Ward. Drug of choice Ceftazidime
1 00 mg/kg/day ( 1 .5 g/m2 /dose, maximum dose of 2 g) intravenously 8 hourly for 7 days
or Aminoglycoside
8 mg/m2/dose ever y 8 hourly
or Ciprofloxacin
500-750 mg orally 1 2 hourly for 1 0-1 4 days
No intramuscular injection
60 mg/kg/day (maximal dose- 4 g) intravenously for 7
If any of the following conditions are present, add vancomycin 400 mg/m2/dose every 8 hourly infused over I hour. First dose stat
or Ceftriaxone
days
a)
or Azithromycin
500 mg orally once daily for 7 days
Carrier state should be treated for
40
4
weeks
recent history of receiving intensive chemotherapy that produces substantial mucosal damage (defined as confluent fibrinous mucositis, ulceration, pain, superficial ulceration, necrosis, hemorrhage). 41
ANTIBIOTIC GUI DEL INE
ANTIBIOTIC G UI DEL INE b)
evidence of sepsis. including shock. hypotension. rigors. septic
emboli.
unexplained
respiratory
distress
or
III case of recurrence
hypoxemia. or poor peripheral perfusion c) If
any
proven or suspected meningitis (including eNS shunt infection) of
the
following
conditions
are
present.
substitute
imipenemlmeropenem for ceftazidime/cetriaxone: a)
b)
Topical acyclovir provides no benefit in the episodic treatment of genital herpes and is not recommended.
Drug of choice Acyclovir or
severe abdominal pain or radiographic findings suggesting
Famciclovir
typhlitis
or
severe abdominal pain with evidence of sepsis. including shock.
hypotension. rigors.
septic
400 mg orally 8 hourly for 5 days
Valacyclovir
250 mg orally 8 hourly for 1 0 days
1 g orally 1 2 hourly for 1 0 days
emboli. unexplained
respiratory distress or hypoxemia or poor peripheral perfusion
In case of prophylaxis
After 2 days careful reassessment of the patient via physical examination and
Drug of choice
review of culture results. If culture report is positive. then antibiotic
Acyclovir
should be changed accordingly. If culture is negative. then continue
or
ceftazidime/cefriaxone for minimum 7 days and reevaluate criteria
Famciclovir
for using vancomycin andlor imipenemlmeropenem.
or
If the patient does not respond after 7 days of using antibiotics
Valacyclovir
Begin ampotericin B empirically at 1 mg/kg/day (maximum dose of
400 mg orally 1 2 hourly 250 mg orally 1 2 hourly 0 .5-1 g orally daily
50 mg) along with antibiotics.
GIARDIASIS
If afebrile. then discontinue intravenous antibiotic therapy and change
Giardiasis is caused by a flagellate protozoan
to suitable oral antibiotic.
(also known as
Giardia intestinalis
G. lamblia).
Drug of choice
GENITAL HERPES Infection is caused by herpes simplex type 1 or type
M etronidazole
2.
400 mg orally twice daily ( 1 5 mg /k g/day in 3 divided doses children) for 7 -1 0 days
III case offirst episode or
Drug of choice Acyclovir
Tinidazole 400 mg orally 8 hourly for 7 -1 0 days
or F amciclovir or
250 mg orally 8 hourly for 7 -1 0 days
Valacyclovir
1 g orally 1 2 hourly for 7 ·1 0 days
42
2 g orally as a single dose or
2 g orally as a single dose
or Secnidazole
2 g (30 mglkg in children) single dose orally
Paromomycin can be used during pregnancy. but when disease is mild. delay of treatment till after delivery is recommended. Drug resistance and relapses may occur with any drug.
43
ANTIBIOTIC G U I DELI NE
ANTIBIOTI C G U I DELI N E
GINGIVITIS
In case of chronic mastoiditis
The vast majority of cases of gingivitis are caused by the collection of
Treatment will be surgical intervention with antibiotics.
highly infected debris on the tooth surface in the ledge formed by the
Drug of choice
gingival margin. The microorganisms present in the debris are
Ceftriaxone
500 mg intravenously 1 2 hourly for 1 0 days
or Ciprofloxacin
500 mg intravenously 1 2 hourly for 1 0 days
Streptococcus, Actinomyces, Veillonella, Treponema, Fusobacterium., .. nucleatum, Prevotella intermedia. Among gingivitis, acute ulcerative type is a purely infectous type where the causative microorganisms are mainly
Treponema and Fusobacterium nucleatum.
Drug of choice Metronidazole plus Tetracycline or Doxycycline or Amoxycillin
200-400 mg orally 8 hourly for 5-7 days 250 mg orally 6 hourly for 5-7 days 200 mg orally stat and 1 00 m g daily for 5-7 days 250-500 mg orally 8 hourly for 5-7 days
MENINGITIS
In case of bacterial meningitis S. Pneumoniae is the Commonest cause of meningitis in adult (almost
50% of all cases). N. meningitides accounts for
25% of all cases. The presence of
petechial or purpuric skin lesions can provide an important clue. Enteric gram-negative bacilli are increasingly common causes of
PYOGENIC LIVER ABSCESS
meningitis in individuals with chronic and debilitating diseases such
Drug of choice
as diabetes mellitus, cirrhosis of liver, alcoholism or those with UTI or craniotomy.
Ciprofloxacin
500 mg orally 1 2 hourly for 1 0-1 4 days
plus Gentam icin
80 mg intravenously 8 hourly for 1 0- 1 4 days
plus Metronidazole
N L. monocytogenes in neonate, pregnant women & >
200-400 mg orally thrice daily for 1 0-1 4 days
age. N H. influenzae is another important cause in our country
Group B Streptococcus or S. agalactiae in patient>
50 years of age. 60 years of
although its incidence is declining in western world due to
MASTOIDITIS
vaccination.
In case of acute mastoiditis
S. aureus & coagulase negative staphylococci are important causes in
Acute mastoiditis is due to S. pneumoniae, S. pyogens, S. aureus, H. injluenzae and P. aeruginosa. An urgent specialist opinion i s advisable, a s surgery may b e necessary.
invasive neurosurgical procedures. Treatment : Bacterial meningitis is a medical emergency. Treatment
Drug of choice
should be started within
Cefotaxim e or Ceftriaxone
1 -2 9 intravenously 4-8 hourly (depends on severity) 2 9 intravenously daily in single or divided doses on adult. The dose may be m odified in case of children according to the age
44
60 minutes of patient's arrival.
Empirical treatment should be started in suspected cases o f bacterial meningitis before doing CSF study. S . Pneumoniae and N . meningitides are the commonest organisms in adult. Due to emergence
of
penicillin
and
cep�losporin
r e s i s ta n t
S. 45
ANTIBIOTIC GUI DELINE
ANTIBIOTIC GUIDELINE
pneumoniae, empirical therapy of community acquired bacterial
NEONATAL SEPSIS
meningitis
Drug of choice
in
children
and
adult
should
include
a
third
generation cephalosporin (e.g. ceftriaxone or cefotaxime) and vancomycin.
Ampici l lin
100 mglkg body weight/day
plus
Antibiotics used in empirical therapy of bacterial meningitis and focal
eNS infections
Gentamicin If the
patient's condition is not improved, then-
Drug of choice
Indication
Antibiotics
Pre-term infants to infants <1 month
Ampicillin
+
cefotaxime
Ceftazidime
Infants 1 -3 months
Ampicillin
+
cefotaxime or ceftriaxone
plus
Immunocompetent children > 3 months
Cefotaxime or ceftriaxone
+
vancomycin
100 mglkg/day intravenously every 8 h ourly for 7 days
Amikacin
and adult < 55 years Adult > 55 years and adults of any age
Ampicillin + cefotaxime or ceftriaxone +
OTITIS EXTERNA
w�h Alcoholism or other debitlitating
vancomycin
Most are due to so-called "swimmer's ear" and the pathogens
disease Hospital-acquired meningitis,
Ampicillin + Ceftazidime + vancomycin
involved are usually
Pseudomonas aeruginosa, Poteus mirabilis
or
other gram negative bacteria. Treatment of otitis extema varies
post-traumatic or postneurosurgery
according to the disease condition, In all cases meticulous cleaning of
meningitis, cases patients with impaired
the ear if necessary by micro suction is essential for effective
immunity neu1ropenic
treatment and prevention of further recurrence. Drug of choice Gentamicin or ciprofloxacin
2-4 drops topically 6-8 hourly
Antimicrobial agent
Child «1 month)
Adult
AmpiCillin
200 mglkg/d, q 4h
12 9 mid, q 4h
Cefotaxime
200 mglkg/d, q 6h
12 9 mid, q 4h
Ceftriaxone
100 mglkg/d, q12 h
4 grnld, q 12h
Ceftazidime
150 mglkg/d, q 8h
6 grnld, q 8h
Drug of choice
Gentamicin
7,5 mg/kg/d, q 8h
7,5 mg/kg/d, q 8h
Topical antifungal cream with
Apply on a cotton bud twice daily
Vancomycin
60 mg/kgld, 16h
2g,d, q 12h
Steroid e,g, Econazole nitrate 1%
for 10-14 days
with hydrocortisone ear drop
In case of otomycosis
+ Triamcinolone
46
acetonide
47
ANTIBIOTIC GU I DELINE
ANTIBIOTIC GUIDELINE
In case of furunculosis
Drug of choice
Drug of choice Flucloxacin
250-500 mg daily 6 hourly for 7-1 0 days
In case of otitis externa with cellulitis of the auricle or periauricular structure Systemic antibiotics are necessary along with ear drop and ear wick (eg. Pope wick)
Co-amoxiclav
375 mg or 625 mg 8 hourly for 7 days
or Ciprofloxacin
500 mg twice daily for 7-1 0 days
or Ceftriaxone
1 9 invervenously once daily ,
Dose should be reduced in patient with severe renal impairment.
Drug of choice Gentamicin or ciprofloxacin
2-4 drops 6 - 8 hourly
with hydrocortisone ear drop plus Co-amoxiclav
Oral thrush is caused by the yeast 375/625 mg orally 8 hourly for 7-1 0 day
Candida albicans.
It is a normal
mouth commensal but it may proliferate to cause thrush. Drug of choice
Or Ciprofloxacin
ORAL THRUSH (CANDIDIASIS)
500 mg twice daily for 7-1 0 days
Nystatin
Wash with 5-10 ml of suspension (1 00,000 u nits/ml) thrice daily
In case of malignant otitis externa
or
for minimum 14 days
Drug of choice
Fluconazole
1 00 mg orally daily for 7 -1 4 days
Ciprofloxacin
500-750 mg twice daily for prolonged
or
period (up to 6-8 weeks) if there is
Itraconazole
200 mg (oral solution) orally once daily.
radiological evidence of osteomyelitis Surgical debridement may necessary if medical therapy is unsuccessful.
PEPTIC ULCER (DUE TO HELICOBACTER PYLORI)
Certain general skin conditions may cause otitis extema e.g. psoriasis,
All patients with peptic ulceration who are also infected with H.
seborrhoeic dermatitis and eczema. Treatment of any underlying
pylori should receive antibiotic therapy. Effective treatment regimens
eczema in the canal, e.g. with 1 % hydrocortisone cream introduced on
include a proton pump inhibitor plus at least two antibiotics.
a cotton bud is important when the inflammation has settled.
Drug of choice
OTITIS MEDIA (ACUTE SUPPURATIVE) Otitis media is usually caused by Streptococcus pneul11oniae, Haemophilus injluenZQe and Moraxella catarrhalis. Occa sional pathogens include Streptococcus pyogenes and Staphylococcus au reus. 48
Omeprazole
20 mg orally twice daily for 7-14 days
plus Amoxycillin
1 9 orally 12 hourly for 7-1 4 days
plus Metronidazole
400 mg orally twice daily for 7-14 days
49
ANTIBIOTIC GUIDELINE
ANTIBIOTIC GUIDELIN E
or
SPONTANEOUS BACTERIAL PERITONITIS
Drug o f choice
Drug of choice 30 mg orally 12 hourly for 14 days
Lansoprazole plus Amoxycillin plus Clarithromycin
1 g orally 12 hourly for 14 days 500 mg orally 12 hourly for 14 days
Lansoprazole is a proton pump inhibitor with actions and uses similar to those of omeprazole. Glossitis associated with black t?ngue or. .stomatltls may de velop. Antacids and sucralfate may reduce the blOavailabthty of lansopra zole. Treatment with lansoprazole may cause false-negatIve results III the urea breath test for H. pylori. Clarithromycin is a macrolide derived from erythromycin. It should not be used during pregnancy if po ssible. Dose should be reduced III patIents With renallhepatic impairment.
Ceftriaxone
1 g intravenously 12 hourly
or Cefotaxime
1 g intravenously 8-12 hourly (depends on severity)
or Ceftipime
1 g i ntravenously 12 hourly
Till the patient improves then switch over to 500 mg orally 12 hourly for 14 days
Ciprofloxacin
For prophylaxis of spontaneous bacterial peritonitis, tablet n orfl oxacin 400
mg 1-2 times daily for indefinite perio d PHARYNGITIS
PERICORONITIS Incomplete eruption of a wisdom tooth produces a large stagnation area under the gum flap. It can easily become infected, causing acute pericoronitis. It is caused by various microorganisms (both .aerobic and anaerobic) like
Staphylococcus, Streptococcus, Fusobacterium and Bacteroids. Drug of choice
The commonest causes are viral. Drug of choice No antibiotic.
The most important bacterial cause is
Streptococcus pyogenes. Other Corynebacterium haemoly-ticum, Corynebacterium diphtheriae, Neisseria
Amoxicillin or Cefradine plus
250-500 mg orally 8 hourly for 7 days
bacterial causes of pharyngitis inClude
250-500 mg orally 6-8 hourly for 7 days
chlamydia pneumoniae, gonorrhoeae, group C beta-haemolytica Streptococci and anaerobic bacteria.
Metronidazole
200-400 mg orally thrice daily for 5-7 days
Penicillin is the only agent conclusively shown to prevent rheumatic fever. The expense of the new macrolides and the cephalosporins do not warrant their use as first line agents.
PERIODONTAL ABSCESS Periodrullal abscess may occur as
a
sequele of chronic periodontitis.
It is caused by Fusobacterium nucleatum, Prevotella intermedia and Eikpnl"Ua corrodens. Drug of choice A!tJ oxyciliin
500 mg orally 8 hourly for 5-7 days
or Cefradine
500 mg orally 8 hourly for 5-7 days
plus Metronidazole
50
200-400 mg orally thrice daily for 5-7 days
Drug of choice Benzathine benzylpenic illin or Phenoxyme thylpenicillin or Erythromycin or Clarithromycin
600,000 unit as Single intramuscu lar dose «30 kg body weight) 1200,000 unit as single intramuscular dose (>30 kg body weight) 250-500 mg (50 mg/kg/day in children) orally 6 hourly for 10 days
250-500 mg orally 8 hourly for 10 days (in case of penicillin
allergic patient) 500 mg by mouth 12 hourly for 10 days (in case of hypersensitivity)
51
ANTIBIOT I C GUI DELINE
ANT IBIOTIC GUIDELINE
Benzathine benzylpenicillin is given by deep intramuscular injection, it forms a depot from which it is slowly released and hydrolyzed to penicillin. Depending on the dose, benzylpenicillin is usually detectable in plasma for up to 4 weeks.
In case of community acquired severe pneumonia (age above 60 years or pre-existing lung disease)
PNEUMONIA
Cefotaxime
Drug of choice 1 9 intravenously 8 hourly for 1 4 days
plus 500 mg intravenously 1 2 hourly for 14 days
In case of community acquired less-severe pneumonia (below the age of 60 years)
Clarithromycin
Drug of choice
In case of hospital acquired less-severe pneumonia
Benzylpenicillin or
1 . 2 9 intravenously 6 hourly for 14 days
Ampicillin
500 mg intravenously 6 hourly for 14 days
or Clarithromycin
500 mg intravenously 12 hourly for 14 days
or Co-amoxiclav
375 / 625 mg orally after meal 8 hourly. Duration of treatment
depends on the clinical condition
Drug of choice Cefuroxime Cefotaxime
1 9 intravenously 8 hourly for 1 4 days
or Co-amoxiclav
1.2 9 intravenously 8 hourly for 14 days
or Ciprofloxacin
In case ofcommunity acquired severe pneumonia (below the age of 60 years and presence of co-existing lung disease) Drug of choice Co-amoxiclav
1.2 9 intravenously 8 hourly for 14 days
plus Clarithromycin
500 mg intravenously 12 hourly for 14 days
Cefuroxime
1 .5 9 intravenously 8 hourly for 1 4 days
Clindamycin
500 mg intravenously 12 hourly for 14 days
Drug of choice Cefuroxime
Ciprofloxacin
400 mg intravenously 12 hourly for 1 4 days
plus Vancomycin
1 9 intravenously 12 hourly for 1 4 days
80 mg intravenously 8 hourly for 14 days
or
Cefotaxime
1 9 intravenously 8 hourly for 1 4 days
plus 80 mg intravenously 8 hourly for 14 days
or
Imipenem
1 9 intravenously 8 hourly for 14 days
plus Gentamicin
52
1.5 9 intravenously 8 hourly for 1 4 days
plus
Gentamicin
or
300 mg intravenously 8 hourly for 14 days
In case of hospital acquired severe pneumonia
plus Clarithromycin
400 mg intravenously 12 hourly for 1 4 days
or
Gentamicin
or
1 .5 9 intravenously 8 hourly for 1 4 days
or
80 mg intravenously 8 hourly for 14 days
53
ANTIBIOT I C GU I DELI NE
ANT IBIOTIC GUIDELINE
In case of lung abscess/suppurative pneumonia/aspiration pneumonia Drug of choice Benzylpenicillin
Drug of choice 1.2 9 intravenously
6 hourly for 4-6 weeks
plus Metronidazole
200 mg intravenously 8 hourly for 4-6 weeks
plus Gentamicin
PROSTATITIS In acute case
80 mg intravenously 8 hourly for 4-6 weeks
Ciprofloxacin
500 mg 1 2 hourly for 2-4 weeks
or Co-trimoxazole
1 double strength tablet 1 2 hourly for 2-4 weeks
Urine culture is necessary in the initial work up. and 1 0- 1 4 days after completion of treatment.
In case of mycoplasma pneumonae In chronic case
Drug of choice Ery1hromycin
Drug of choice 500 mg orally
6 hourly for 2-3 weeks
or Tetracycline
500 mg orally
6 hourly for 2-3 weeks
or Doxycycline
1 00 mg orally 12 hourly for 2-3 weeks
or Ciprofloxacin
500 mg orally 12 hourly for 2-3 weeks
Ciprofloxacin
500 mg 12 hourly for
4 weeks
or Co-trimoxazole If there
1 DS tablet 12 hourly for 4 weeks
is no response after 4 weeks. the same antibiotic should be given for
12 weeks.
PYELONEPHRITIS (ACUTE) In case of empyma thoracis
This is caused by the same range of pathogens as uncomplicated cystitis.
Drug of choice
except that Staphylococcus saprophyticus is a rare cause of pyelonephritis.
Benzylpenicillin plus
1.2 9 intravenously
Metronidazole
200 mg intravenously 8 hourly for
6 hourly for 4-6 weeks 4-6 weeks
or Clindamycin
600 mg intravenously 8 hourly for 4-6 weeks
In case of mild-to-moderate illness Drug of choice. Ciprofloxacin
250 mg orally 1 2 hourly for 1 4 days
Change the antibiotic that depends on culture and sensitivity
In case of acute severe illness and possible urosepsis Drug of choice
54
9 intravenously 12 hourly for 7 days
Ceftriaxone or
1
Imepenum
1 9 intravenously 12 hourly for 7 days
55
ANTIBIOTIC GUI DELINE
ANTIBIOTIC GUI DELI N E
SEPSIS IN NEUROPATHIC FOOT IN DIABETES MELLITUS
SYPHI LIS
Antibiotic should be used for general cover or specific if organism is
Syphilis is a sexually transmitted disease caused by the spirochaete
known .
Treponema pallidum. In case of early congenital syphilis
For general cover regimen
Drug of choice Benzylpenicillin
Drug of choice Cefuroxime
1 .5 g intravenously for 1 0- 1 4 days
plus Flucloxacillin
500 mg intravenously 6 hourly for 1 0- 1 4 days
plus Metronidazole
500 mg intravenously 6 hourly for 1 0- 1 4 days or
50,000 U/kg intravenously 1 2 hourly for 1 0- 1 4 days
or Procaine benzylpenicillin or Benzathine
50,000 U/kg intramuscularly once daily for 1 0 days for symptomatic infant or those with neurosyphilis 50,000 U/kg intramuscularly as a single injection for asymptomatic infant without neurosyphilis
benzylpenicillin
Benzylpenicillin or procaine benzylpenicillin is preferred to benzathine benzylpnicillin for infants with congenital syphylis. The pharmacokinetics of benzathine penicillin appear to be altered in late pregnancy (only
400-800 mg orally for 1 0- 1 4 days
40% achieved adequate
serum concentration
for 7 days).
In case of primary or secondary syphilis Drug of choice
SINUSITIS Sinusitis
is
caused
by
Haemophilus injl.uenzae, Streptococcus
pneumoniae and Moraxella catarrhalis. Anaerobes play a significant role in adult sinusitis especially if persistent - so-called "chronic sinusitis".
Benzathine
2.4 million U intramuscularly once per week for 1 4 days
benzylpenicillin or Doxycycline
If the patient responds poorly to first choice of therapy, consider
or
treatment which includes anaerobes in its spectrum of activity.
Tetracycline
1 00 mg orally 12 hourly for 1 4 days 500 mg orally 6 hourly for 1 4 days
If a patient is allergic to penicillin, then doxycycline/tetracycline is administered.
Drug of choice
In case of latent or tertiary syphilis Co-amoxiclav
375/625 mg orally after meal 8 hourly for 1 0- 1 4 days
Drug of choice
500 mg 1 2 hourly ( 1 25 mg 1 2 hourly in children
Tetracycline
or Ciprofloxacin
<
2 years,
and 250 mg in children 2-1 2 years) for 1 0- 1 4 days or Levofloxacin
Doxycycline 500 mg once daily for 1 0- 1 4 days.
Topical decongestant for 5 days
56
500 mg orally 6 hourly for 1 4 days
or 200 mg orally 12 hourly for 14 days, for penicillin-allergic patient
or Benzathine
2.4 million unit intramuscularly weekly for 3 successive weeks
benzylpenicillin
57
ANTIBIOTIC G U I DELINE
ANTIBIOTIC GUIDELI NE
In case of neurosyphilis The disease is very difficult to treat. Follow sequential serum and CSF titres Drug of choice Benzylpenicillin
extrapulmonary tuberculosis (e.g. meningeal, miliary, pericardial, peritoneal, massive unilateral! bilateral pleural effusion, spinal, intestinal, genitourinary and multi-organ tuberculosis)] Drug of choice
2.4 million U intravenously 4 hourly for 1 4 days
or 2.4 million U intramuscularly once \;laily for 1 4-21 days
Procaine
Patient weight (kg)
Dosage
30-37
2 tablets (4Fixed-dose combination) daily for first
benzylpenicillin
2 months followed by 2 tablets (2Fixed-dose combination) thrice-weekly
Benzathine benzylpenicillin is not recommended due to its poor penetration to the CSF.
for another 4 months 3 tablets (4Fixed-dose combination) daily for first 2 months
TONSILLITIS The most common and important bacterial cause is
followed by
Streptococcus
pyogenes.
3 tablets (2Fixed-dose combination) thrice-weekly for another
Penicillin is the only agent conclusively shown to prevent rheumatic fever. The expense of the new macrolides and the cephalosporins do not warrant their use as first line agents.
4 months 55-70
Drug of choice Co-amoxiclav
followed by 375 / 625 mg orally after meal 8 hourly for 1 0 days
or Ery1hromycin
4 tablets
(2Fixed-dose combination) thrice-weekly for another 4 months
250-500 mg orally 8 hourly for 1 0 days >70
or Cefalaxin
4 tablets (4Fixed-dose combination) daily for first 2 months
1 -2 g daily orally in 2-3 divided doses
4 tablets (4Fixed-dose combination) daily for first 2 months followed by
For the penicillin-allergic patient, erythromycin may be used.
4 tablets
Cefalexin is a first-generation cephalosporin antibiotic. If it is taken with food, absorption may be delayed, but the total amount absorbed is not appreciably altered. Doses may need to be reduced in severe renal impairment.
4Fixed-dose combination contains 150 mg of rifampicin + 75 mg of isoniazid + 400 mg of pyrazinamide + 275 mg of ethambutol
TUBERCULOSIS In case of category-I tuberculosis [new smear-positive, new smear-negative pulmonary tuberculosis with extensive parenchymal involvement or severe forms of 58
(2Fixed-dose combination) thrice-weekly for another 4 months
2Fixed-dose combination contains 150 mg of rifampicin + 75 mg of isoniazid
In case of category-II tuberculosis (previously treated for more than I month with sputum smear-positive pulmonary tuberculosis with relapse/treatment after interruption! treatment failure). 59
ANTIBIOTIC G U I DELINE
ANTIBIOTIC GUIDELINE
Drug of choice
Drug of choice Patient
Patient
Dosage
weight (kg) 30-37
Dosage
weight (kg) 2 tablets (4Fixed-dose combination) daily for first 3 months plus
30-37
2 tablets (3Fixed-dose combination) daily for first 2 months followed by
Streptomycin injection 500 mg daily for first 2 months followed by
2 tablets (2Fixed-dose combination) thrice-weekly for another
2 tablets (2Fixed-dose combination)
4 months
+
2 tablets of ethumbutol
(400 mg) thrice-weekly for another 5 months
38-54
3 tablets (3Fixed-dose combination) daily for 2 first months followed by
38-54
2 tablets (4Fixed-dose combination) daily for first 3 months plus
3 tablets (2Fixed-dose combination) thrice-weekly for another
Streptomycin injection 750 mg daily for first 2 months followed by
4 months
3 tablets (2Fixed-dose combination)
+
3 tablets of ethumbutol
55-70
4 tablets (3Fixed-dose combination) daily for first 2 months
(400 mg) thrice-weekly for another 5 months
followed by
2 tablets (4Fixed-dose combination) daily for first 3 months plus
4 months
4 tablets (2Fixed-dose combination) thrice-weekly for another 55-70
Streptomycin injection 1 000 mg daily for first 2 months followed by 4 tablets (2Fixed-dose combination)
+
>70
4 tablets of ethumbutol
4 tablets (2Fixed-dose combination) thrice-weekly for another
(400 mg) thrice-weekly for another 5 months >70
2 tablets (4Fixed-dose combination) daily for first 3 months plus Streptomycin injection 1 000 mg daily for first 2 months followed by 4 tablets (2Fixed-dose combination)
+
5 tablets of ethumbutol
(400 mg) thrice-weekly for another 5 months The dose of streptomycin should not exceed years
750 mg daily after the age of 50
In case of category-Ill tuberculosis [new smear-negative pulmonary tuberculosis (other than category l), less severe form of extrapulmonary tuberculosis (e.g., lymph node, pleural effusion {unilateral}, bone {excluding spine}, peripheral joint, skin tuberculosis)) 60
4 tablets (3Fixed-dose combination) daily for first 2 months followed by 4 months
3Fixed-dose combination contains 400 mg of pyrazinamide
1 5 0 mg of rifampicin
2Fixed-dose combination contains
ISO mg of rifampicin + 75 mg of isoniazid
+
75 mg of isoniazid
+
In case of tuberculosis with pregnancy Most antitubercular drugs are safe in pregnancy with the exception of streptomycin, which is ototoxic to the fetus.
In case of tuberculosis with lactation A women with tuberculosis which is breast-feeding should receive a full course of antitubercular drugs.
Regular and full course
chemotherapy is the best way to prevent transmission of tuberculi bacilli to her baby. The mother and baby should stay together and breast-feeding should be continued. 61
ANTIBIOTIC GUIDELI N E
ANTIBIOTIC GUIDELINE
In case of tubercuLosis woman taking oraL contraceptive
Drug of choice
A women taking oral contraceptive and antitubercular drugs has
Nitrofurantoin or
1 00 mg orally after dinner for 2-3 months
Ciprofloxacin
250 mg orally at bed time for 2-3 months
increased risk of pregnancy. Rifampicin reduces the efficacy of estrogen. So, a higher dose of estrogen with rifampicin or another form of contraception can be used.
or Ofloxacin
200 mg at bed time for 2-3 months
or
U R ETHRITIS (ACUTE, FOR MALES)
Co-trimoxazole
In case of gonococcaL or chLamydiaL infection
Duration of treatment varies according to age and clinical condition of patient.
Drug of choice
Prevention of catheter-associated UTI
Azithromycin
Administration of antimicrobials is
1 g orally as a single dose
480 mg orally at bed time for 2-3 months
not of value in preventing
colonisation/i nfection in patients with indwelling catheters. Furthermore, Gastrointestinal adverse effects are usually mild and less frequent than with erythromycin. Absorption frm the capsule formulation, but not the tablet
this has been shown to promote the selection of resistance.
formulation, is reduced by food. Capsule formulation should be given at least an hour before, or
2 hour after, meal. Concurrent administration of antacids
VAGINAL CANDIDIASIS
containing aluminium or magnesium salts can reduce the rate, but not the extent of absorption of azithromycin.
In case of non-pregnant woman Drug of choice
U RINARY TRACT IN FECTIONS
Clotrimazole
500 mg vaginal tab once
Initial management will be the use of an antibiotic that depends on
or
culture and sensitivity and general condition of patient.
two 1 00 mg vaginal tab nocte for 3 nights
Drug of choice
vaginal ( 1 %) cream nocte for 6 nights
Co-trimoxazole
1 DS tablet twice daily orally for 1 0- 1 4 days
or Fluconazole
500 mg orally 12 hourly for 7-14 days
Clotrimazole is an imidazole antifungal agent. Intravaginal preparation may
or
Ciprofloxacin
1 50 mg orally as a Single dose
damage latex contraceptives and additional contraceptive measures are
or Nitrofurantoin
or
1 00 mg 6 hourly for 7-1 4 days
therefore necessary during local administration. Fluconazole is a triazole antifungal agent. Concentration of fluconazole in
In case of recurrent infection Continuous prophylactic antibiotic therapy should be considered in
breast milk, joint fluid, saliva, sputum, vaginal fluids and peritoneal fluids are .
simi lar to those achieved in plasma.
women with more than 3 UTI' s/year.
62
63
ANTIBIOTIC G U I DELI N E
ANTIBIOTIC GUIDELINE
In case ofpregnant woman
WOUNDS (INFECTED)
Drug of choice
Treat according to the clinical condition and the results of culture and sensitivity tests from representative specimens. It is important to
Clotrimazole
500 mg vaginal tab for 7 days
or two 1 00 mg vaginal tab nocte for 7 nights or vaginal ( 1 %) cream nocte for 7 nights
The need for tetanus prophylaxis should be evaluated in the case of
5 g of intravaginal cream (2%) to be inserted into the vagina once
Drug of choice
or Miconazole
distinguish between superficial wound colonization and true infection. as antimicrobial therapy is generally not indicated for
daily for 1 0- 1 4 days or twice daily for 7 days Clotrimazole is not contraindicated in pregnancy but one should be cautious
colonization. traumatic wounds.
Gentamicin
about its use as there may be systemic absorption.
Fusidic acid
Miconazole is an imidazole antifungal agent. Intravaginal preparation may
or
damage latex contraceptives and additional contraceptive measures are
Mupirocin
therefore necessary during local administration.
or
VAG INAL TRICHOMONIASIS Drug of choice Metronidazole or Tinidazole or Secnidazole
Apply the cream locally 2-3 times daily
or Apply the cream/ointment locally 2-3 times daily Apply the cream/ointment locally 2-3 times daily
Combination
Apply the cream locally 2-3 times daily Fusidic acid is
of Bacitracin
a steroid antimicrobial agent which is used almost
and Neomycin
exclusively against �-lactamase-producing staphylococci.
2 g as a single oral dose or 400 mg 1 2 hourly for 7 days 2 g orally as a single dose
Fusidic acid is a steroid antimicrobial agent which is used almost exclusively against �-lactarnase-producing staphylococci.
2 g single dose for both partners
Metronidazole has been used extensively in pregnancy for the treatment of trichomoniasis. The teratogenic effect appears to be minimal and if present. greatest during the first trimester. when the drug should not be used. If therapy cannot be avoided. then it can probably be used safely in the last two trimesters of pregnancy. The sexual partner(s) should also be treated to prevent reinfection.
VAGINOSIS (BACTERIAL) Drug of choice Clindamycin
One applicatorful intravaginally at night for 7 days
or Metronidazole
64
One applicator/ul intravaginally once daily for 5 days
65
ANTIBIOTIC GUIDELINE ANTIBIOTIC GUIDELIN E
GUIDELINE FOR USE OF ANTIBIOTICS IN RENAL FAI LURE Drugs
Acyclovir
Creatinine level
Dosage recommendation
Drugs
Comment
Increase dosing interval (IV) I ncrease dosing interval (oral)
Azithromycin
Avoid; jaundice reported
Ceftriaxone
Reduce dose and monitor plasma concentration if associated renal impairment
Chloramphenicol
Avoid- increased risk of bone marrow depression
Ciprofloxacin
Hepatitis with necrosis may occur
Clarithromycin
H'i!patic dysfunction including jaundice reported
Co-amoxiclav
Cholestatic jaundice reported, mon�or liver function in liver disease
(mmolll)
1 50-350 >500
USE OF ANTIBIOTICS IN LIVER DISEASE
Aminoglycosides
1 50-300
I ncrease dosing interval; avoid if possible
Amoxicillin
>500
I ncrease dosing interval
Azathioprine
>500
Decrease dose/ increase dosing interval
Benzylpenicillin
>500
Halve the dose
Ceftazidine
>1 50-300
Increase dosing interval
Cefuroxime
>500
Increase dosing interval
Cefalexin
>500
Increase dosing interval
Ceftriaxone
>500
No adjustment if hepatic function is normal
Chloramphenicol
>700
Avoid
Co-trimoxazole
Avoid in severe liver disease
Chloroquine
1 50-300 300-500
Maximum 75 mg/day Maximum 50 mg/day
Doxycycline
Use with caution
Ciprofloxacin
150-300
Halve the dose
Erythromycin
May cause idiosyncratic hepatotoxicity
Cisplatin
150-300
I ncrease dosing interval
Co-trimoxazole
>500
Maximum 960 mg/day
Flucloxacillin
Cholestatic jaundice
Cyclophosphamide
300-500
Fluconazole
Monitor liver function, discontinue if liver function impaired
Fusidic acid
Impair biliary excretion; increased risk of hepatotoxicity; avoid or reduce dose
Griseofulvin
Avoid in sevEll'e liver disease
Isoniazid
Avoid if possible; idiosyncratic hepatotoxicity more common; monitor liver function regularly
Itraconazole
Half-life prolonged; dose reduction may be necessary
Ketoconaiole
Avoid
Mefloquine
Avoid for prophylaxis in severe liver disease
Metronidazole
Reduce the dose in severe liver disease
Norfloxacin
Hepatitis with necrosis; use in spontaneous bacterial peritonitis
Ofloxacin
Reduce dose
Rifampicin
Avoid in liver disease
Decrease dose Decrease dose if GFR falls
Cyclosporine Doxycycline
1 50-300
I ncrease dosing interval
Ethumbutol
150-300
Increase dosing interval
Fluconazole
1 50-300
Increase dosing interval
Isoniazid
>500
Maximum 200 mg/day
Ketoconazole
1 50-300
Unchanged
Methotrexate
300-500
I ncrease dosing interval
Nalidixic acid
300-500
Avoid
Neomycin
150-300
Avoid
Nitrofurantoin
1 50-300
Avoid
Sulfadiazine
>500
Avoid
Sulfasalazine
>500
Ensure increase fluid intake
Tetracycline
150-300
Avoid
Vancomycin
1 50-300
Avoid
Vincristine
1 50-300
Unchanged
66 67
ANTIBIOTIC GUIDELINE
ANTIBIOTIC G U IDELI N E Drugs
ANTIBIOTICS IN PREGNANCY Drugs
Amikacin
Use only when potential benefit outweighs risk
2, 3
alternatives are not available
least 1 month after administration Use only i n life-threatening situations (toxicity at
Ceftriaxone
Not known to be harmful
Chloramphenicol
Neonatal 'Grey syndrome'
1 , 2, 3
Avoid- arthropathy in alternatives available
animal
studies;
safer
Not known to be harmful but use only if adequate alternatives are not available
Clindamycin
Not known to be harmful
Co-amoxiclav
3
menstrual period
3
Mefloquine
1 1
Fansidar
3
Metronidazole
Nitrofurantoin
3
Theoretical teratogenic risk (trimethoprim a folate antagonist)
Norfloxacin
1 , 2, 3
Neonatal hemolysis and methemoglobinemia; fear of increased risk of kernicterus in neonates
Ofloxacin
1 , 2, 3
Effects on skeletal development in animal studies
Pentamidine
Dental discoloration; maternal hepatotoxicity with
Primaquine
3
Pyrimethamine
1
large parenteral doses
Gentamicin
68
arthropathy
in
animal
studies;
safer
alternatives available May produce neonatal hemolysis if use at term Avoid-
arthropathy
in
animal
studies;
safer
in
animal
studies;
safer
alternatives available Avoid-
arthropathy
alternatives available Avoid unless essential Neonatal hemolysis and methemoglobinemia
antagonist); adequate folate supplements should be given to mother
Possible teratogenic risk (trimethoprim a folate antagonist)
Neonatal hemolysis and methemoglobinemi a; fear of increased risk of kernicterus in neonates appears to be unfounded
Quinine Streptomycin
Tetracyclines
Teratogenic in animal studies; use only when potential benefit outweighs risk
2, 3
Avoid-
Theoretical teratogenic risk (trimethoprim a folate
May be teratogenic
with long-term high doses
Flucytosine
Teratogenic in animal studies Avoid high-dose regimen
essential
Avoid- multiple congenital abnormalities reported Fluconazole
Toxicity in animal studies
1
1 , 2, 3
Not known to be harmful
Erythromycin
warning to avoid in pregnancy
Mebendazole
appears to be unfounded
1
Teratogenic in animal studies; packs carry a
Nalidixic acid
No evidence of teratogenicity but avoid unless
1
Ethionamide
contraception during treatment and until the next
Ketoconazole
Clarithromycin
Doxycycline
high doses in animal studies); ensure effective
Itraconazole
Not known to be harmful but use only if adequate alternatives are not available
Co-trimoxazole
effective contraception required during and for at
Auditory or vestibular nerve damage
Azithromycin
Ciprofloxacin
Griseofulvin
Not known to be harmful but use only if adequate
Amphotericin B
Co mment
Avoid (fetotoxicity and teratogenicity in animals);
Comment
Trimester
Acyclovir
Trimester
Auditory or vestibular nerve damage
Zidovudine
1 2, 3 1 3
Teratogenic at high doses; but in malaria benefit of treatment outweighs risk Auditory or vestibular nerve damage Effects on skeletal development in animal studies Dental discoloration; maternal hepatotoxicity with large parenteral doses Limited information available; use only if clearly indicated
69
ANTIBIOTIC G U I DELI N E
ANTIBIOTIC GUI DELINE
DRUGS PRESENT IN BREAST MILK Comment
Drugs
MANAGEMENT OF ANAPHYLACTIC SHOCK Management consists of stopping the offending drug, treating the acute reaction, and making a determination concerning futures use of
Aciclovir
Significant amount is found in milk after systemic administration
the drug. A detailed medical history, knowledge of the signs and
Azithromycin
Prescribe with caution; no harmful effect is known; use only if there is no alternative
syndrome, anaphylaxis and asthma are helpful.
Chloramphenicol
Use alternative, if possible; may cause bone marrow depression; concentration in milk is insufficient to cause Grey baby syndrome
Chloroquine
Amount too small to be harmful; inadequate for reliable protection against malaria
2.
remove the cause; raising the foot end may help restore the
Ciprofloxacin
High concentration in milk; avoid
3.
give adrenaline intramuscularly (0.5 mI of 1: 1 000); repeat every
Clarithromycin
Avoid; excreted in milk
Co-trimoxazole
Small risk of kernicterus in jaundiced infant and of hemolysis in G6PD-deficient infant
Doxycycline
Avoid; if necessary discontinue breast feeding
Fluconazole
Avoid; present in milk
Gentamicin
Avoid
Interferon
Avoid; no information available
Isotretinoin
Avoid
Itraconazole
Small amount found in milk; not harmful
Metronidazole
Significant amount in milk; do not take single large dose
Ofloxacin
Avoid
Penicillamine
Trace amount in milk; use with caution
Rifampicin
Amount to small to be harmful
Tetracycline
Avoid; deformity and dental decolorization in infant
Tretinoin
Avoid
70
symptoms which often include rashes, angio-edema, serum sickness Management of acute reaction includes :
I.
secure the airway- give 1 00% oxygen. Intubate i f respiratory obstruction imminent
circulation
5 mins, if needed as guided by blood pressure, pulse, respiratory function 4.
5.
secure intravenous access chlorpheniramine 1 0 mg intravenously and hydrocortisone 200 mg intravenously
6.
intravenous infusion (0.9% saline, eg., 500 mI over 1 5 minutes; up to 2 I may be needed). Titrate against blood pressure
7.
if wheeze, nebulize salmeterol, 20 min interval. Intubate if necessary for ventilatory support
8.
if still hypotensive admission to ICU and an intravenous infusion of adrenaline may be needed
±
aminophylline and nebulized
salbutamol; get expert help
Further management: •
Admit to ward; monitor ECG
•
Continue chiorpheniramine 4 mg orally 8 hourly if itching
•
Skin-prick tests showing specific IgE help identify which allergens to avoid
71
ANTIBIOTIC G UI DELI N E
ANTIBIOTIC GUI DELIN E
ANTIBIOTIC PROPHYLAXIS IN SURGERY Fundamental principles of Surgical Prophylaxis •
The antibiotic must be in the tissue before the bacteria are introduced i . e . antibiotic must be given intravenously shortly
Operations for acute cholecystitis , empyema of the gallbladder, ascending cholangitis or liver abscess require antibiotic treatment
given too early. The half-life of the particular antibiotic is therefore important. There is no data to support more than a single dose. Further doses generally constitute treatment.
Note the waste of
resources, the increased risk of complications and the fact that mUltiple doses are not associated with increased efficiency (not to be continued after •
72 hours if not otherwise indicated).
The chosen antibiotics must be active against the most common expected pathogens.
•
High risk patients, e.g. patients with j aundice or diabetes, or
identified at the time of the operation. Timing of antibiotic prophylaxis Current recommendations are that the parenteral antibiotics used in prophylaxis should be given in sufficient dosage (according to weight of the patient) within 30 minutes preceding incision. This results in near maximum drug levels in the wound and the surrounding tissues during the operation. This can be facilitated by administer the
bile, ets for culture and sensitivity).
For which type of operations? Antibiotic prophylaxis is generally indicated for patients undergoing the following types of operations: All clean-contaminated procedures; these include penetration of the gastrointestinal tract (especially colo-rectal), whether by penetrating trauma or related to a pathological organ event (e.g. ruptured appendix, perforated colonic diverticulum) prior to the development of clinical peritoniti s. Clean operations with foreign body implant (e.g. vascular, cardiac and orthopaedic operations), and those without foreign body implants especially hernia repair, breast surgery, median
72
and/or intra-abdominal abscess, and penetrating abdominal trauma where significant gastrointestinal leakage with peritoneal soiling is
devices, generally warrant antibiotic prophylaxis. For all practical purpose suitable antibiotic to be prescribed on the basis of
•
rather than prophylaxis. The same applies to operations for a perforated appendix with evidence of local or generalized peritonitis
patients who undergo any procedures to insert prosthetic
bacteriological culture and sensitivity whenever possible (e.g., blood, pus,
•
dirtylinfected should be considered as therapeutic and is clearly not prophylactic i.e. treatment should be given for a longer duration.
before surgery to ensure high blood / tissue levels. Prophylaxis failure may be due to antibiotics given too late or more often,
•
The u s e o f antibiotics i n operations classified a s contaminated or
antibiotic in the operating room when the intravenous lines are inserted shortly before operative incision. A single preoperative dose of antibiotic has the same efficacy as multiple doses and the current recommendation is to administer a second dose only if the operation lasts for longer than
2 - 3 hours. With the oral preoperative antibiotic
preparation commonly used before elective colonic resection, the chosen agents should be given during the
24 hours before the
operation in order to attain significant intraluminal (local) and serum (systemic) levels. Route of administration of prophylactic antibiotics Intravenous administration of the prophylactic antibiotic is preferred for most patients undergoing an operative procedure. Oral antibiotics currently play a major role only in the preparation of patients before
sternotomy, vascular surgery involving the aorta and the lower
elective colon surgery.
extremities, and craniotomy.
Antibiotic prophylaxis for common surgical operations 73
ANTIBIOTIC GUI DELINE
ANTIBIOTIC G U I DELINE
1 . Cardiovascular surgery
2. Orthopaedic surgery
Antibiotic prophylaxis in cardiovascular surgery has proven
In case of arthroplasty ofjoints. and/or joint replacement
beneficial only in the following procedures: •
Reconstruction of the abdominal aorta
•
Procedures on the leg which involve a groin incision
•
Any vascular procedure with insertion of a prosthesis I foreign body
•
Lower extremity amputation for ischaemia
•
Cardiac surgery
In case of prosthetic valve insertion. coronary a rtery bypass graft. other open heart surgery and pacemaker implant Drug of choice Ceftriaxone
1 9 intravenously daily for 5-7 days
plus Gentamicin
80 mg intravenously 8 hourly for 5-7 days
Ceftriaxone should be started 24 hours before operation. Gentamicin should be gi ven after operation
In case of superficial infection following cardiovascular surgery Drug of choice Flucloxacillin
500 mg orally 6 hourly for 1 0-1 5 days
In case of aortic resection Drug of choice Ceftriaxone
1 9 intravenously daily for 5-7 days
plus Gentamicin
In case of open reduction of fracture. laminectomy. spinal fusion, lower limb amputation Any 3rd generation cephalosporin I
-
2 g IV pre-operatively.
Compound (open) fractures are considered contaminated. so antibiotics are essentially therapeutic in such situations. 3. Gastroduodenal surgery
Antibiotics are indicated in high risk patients only, i.e. patients with bleeding ulcer, obstructive duodenal ulcer, gastric ulcer, low gastric acidity, decreased or motility, malignancy or morbid obesity. a.
1 st generation cephalosporins e.g. cefazolin I g IV pre-operatively.
b.
For beta-Iactam allergy, gentamicin 1 20 mg plus clindamicin 600 mg IV preoperatively.
4. Biliary tract surgery
Most studies show that achieving adequate drainage will prevent post-procedural cholangitis or sepsis and there is no further benefit from prophylactic antibiotics. With inadequate drainage, antibiotics may be of value. The American Society for GI Endoscopy recommends prophylaxis for known or suspected biliary obstruction. The value of prophylaxis for ERCP is controversial. Note that cephalosporins are not active against the enterococci, yet' are clinically effective as prophylaxis in biliary surgery. With cholangitis, treat as infection, not prophylaxis. High risk patients include those >70 years of age, acute cholecystitis, non-functioning gall-bladder, obstructive jaundice or common duct stones. a.
500 mg intravenously 8 hourly for 3 days. After 3 days oral
OR
preparation of the drug should be administered
74
-
80 mg intravenously 8 hourly for 5-7 days
plus Metronidazole
Any 3rd generation cephalosporins I 2 g pre-operatively. If the operation is longer than 3 hours, give a second dose or for up to 48 hours after the procedure.
b.
1 st generation cephalosporins e.g. cefazolin 2 g pre-operatively as a single dose cefoxitin 2 g pre-operatively as a single dose. 75
ANTIBIOTIC GUI DELINE
ANTIBIOTIC GUI DELINE
5.
Inguinal hernia repair
recommended. For a mesh Available data is limited , routine use is not cephalosporin as a single tion genera implant, give prophy laxis e.g. I st
Prostatectomy Drug of choice 1 9 intravenously stat and daily for 3 days or till the catheter
Ceftriaxone
is removed
dose. or
6.
Appendicectomy
Ciprofloxacin
500 mg intravenously stat and then 500 mg of tablet given orally for 3-5 days
Drug of choice 2 9 intravenously preoperatively and 2 more doses.
Ceftriaxone
If perforated, continued for 3-5 days
Transrectal prostate biopsy Drug of choice
or 500 mg intravenously pre-operatively or use
Metronidazole
metronidazole in the form of suppository with beta-lactam allergy Metronidazole should be given for patients
Ceftriaxone
1 9 intravenously pre-operatively (1 5 minutes prior to operation)
followed by Cefalexine
500 mg orally 6 hourly for 5 days
plus
7.
Penetrating abdominal trauma
as treatment and not as Any antibiotic cover can be considered
prophylaxis.
pius Ceftriaxone
400 mg orally thrice daily for 5 days.
Kidney transplantation
Drug of choice Gentamicin
Metronidazole
In case of donar 80 mg intravenously 8 hourly for 1 0 days 2 9 intravenously on admission and then 1 9 twice daily for
Drug of choice 1 9 intravenously pre-operatively (1 5 minutes prior to
Ceftriaxone
3-5 days or
supplemented by
Cefuroxime
8.
operation) stat and then for 3 days
750 mg intravenously 8 hourly for 5-7 days
Urological surgery
Amoxycillin
250 mg of amoxycillin plus 1 25 mg of
plus Clavulanic
Clavulanic acid orally after meal 8 hourly.
acid
Cystoscopy
In case of recipient
Drug of choice Gentamicin
80 mg intravenously prior to anesthesia
Ceftriaxone
or Ceftriaxone
76
Drug of choice
1
9 intravenously prior to anesthesia
1 9 intravenously pre-operatively ( 1 5 minutes prior to operation) stat and then for 3 days
77
ANTIBIOTIC G U I DELI N E
9.
Head and neck surgery
Major head, neck and oral surgery
10.
Maxillofacial surgery
Cleft lip/palate surgery, condylectomy, segmental resection of
Drug of choice 1 9 intravenously pre-operatively ( 1 5 minutes prior to operation)
Ceftriaxone
ANTIBIOTIC GUIDELINE
maxilla/mandible, post·excisional bone grafting, malignancy, jaw fracture.
or Gentamicin plus 80 mg of gentamicin and 600 mg of clindamycin Clindamycin
intramuscularly as single dose
Drug of choice Ceitriaxone
or 1 9 intravenously as single dose
Cefradine
1 9 intravenously pre-operatively ( 1 5 minutes prior to operation) and next 2-4 days
or
10.
Obstetrics & Gynecology
Cefradine
500 mg intravenously 8 hourly for 5-7 days
Cesarean section Drug of choice Ceftriaxone
1 9 intravenously pre-operatively (1 5 minutes prior to operation)
plus Metronidazole
500 mg intravenously pre-ope�atively (within 60 minutes prior to operation)
Maintenance dose: Ceftriaxone 1 9 intravenously till the patient is nothing by mouth followed by oral dose of cephalosporin 500 mg 6 hourly up to 5-7 days of operation Hysterectomy (abdominal and vaginal) Drug of choice Ceftriaxone
1 9 intravenously pre-operatively ( 1 5 minutes prior to operation)
plus Metronidazole
500 mg intravenously pre-operatively (within 60 minutes prior to operation)
Maintenance dose: Ceftriaxone 1 9 intravenously till the patient is noth ing by mouth followed by oral dose of cephalosporin 500 mg 6 hourly up to 5-7 days of operation. 78 79
ANTIBIOTIC GUIDELINE
ANTIBIOTIC PROPHYLAXIS FOR NONSURGICAL CONDITIONS Bacterial endocarditis
Prevention of infective endocarditis in persons with certain underlying cardiac conditions is important since this infection continues to cause serious morbidity and mortality despite advances in diagnosis and treatment.
Procedures for which Endocarditis Prophylaxis is necessary, include:
ANTIBIOTIC GUI DELINE
Genitourinary and gastrointestinal procedures
The relevant organisms are usually enterococci, and rarely Gram negative bacilli. Ampicillin 2 g intravenously (50 mg/kg in children) PLUS gentamicin 1 .5 mg/kg intravenously ( 1 .5 mg/kg in children) 30 minutes before the procedure followed by one dose of amoxycillin 1 g orally (25 mg/kg in children) 6 hours after the
Dental procedures known to cause mucosal or gingival bleeding e.g.extractions, dental implant placement and reimplantation of avulsed teeth, root canal instrumentation or surgery, professional cleaning
or
•
Tonsillectomy and/or adenoidectomy Surgical conditions that involve penetration of intestinal or respiratory mucosa
8 hours after the initial dose.
•
•
Bronchoscopy with a rigid bronchoscope
Vancomycin I g intravenously (20 mg/kg in children) PLUS
•
Sclerotherapy for oesophageal varices
gentamicin 1 . 5 mg/kg intravenously (2 mg/kg in children) 30
•
Biliary tract surgery
minutes before the procedure, as single dose only.
•
Cystoscopy
Contacts
•
Urethral dilatation
meningococcal infections
•
Urethral catheterisation, if infection is present
•
Prostatic surgery
•
Incision and drainage of infected tissue
•
Prophylactic regimens
In case of tooth extraction or minor oral surgery Streptococcus viridans is the most common cause of endocarditis following dental, oral, respiratory tract, or oesophageal procedures. Drug of choice Amoxicillin
80
If allergic to ampicillin/penicillin or unable to take oral medication:
of
invasive
Haemophilus influenza
type
b
and
The purpose of chemoprophylaxis in contacts is to eradicate nasopharyngeal
colonization by Neisseria meningitidis or Haemophilus influenzae type b and thus reduce both the risk of disease in contacts and the transmission to nonimmune susceptible people. Meningococcus contacts
Household contacts, day-care contacts, and only health-care workers with direct exposure to oral secretions (e.g. mouth-to infection, require prophylaxis. The index case also requires an agent to eradicate nasopharyngeal carriage, prior to discharge
For 5-7 days
plus Metronidazole
one dose of ampicillin 1 g intravenously (25 mg/kg in children)
mouth resuscitation) of patients with invasive meningococcal 500 mg orally 8 hourly for 5-7 days
or Any cephalosporin
initial dose
400 mg three times daily for 5-7 days
from hospital (unless treated with ceftriaxone or cefotaxime) since therapy with penicillin may not eliminate nasopharyngeal carriage of the organism. 81
ANTIBIOTIC GUI DELINE
ANTIBIOTIC GUI DELINE
The recommended chemoprophylactic agents include: Rifampicin for 4 doses or Ceftriaxone
20 mglkg (to a maximum of 600 mg) given 1 2 hourly orally
250 mg (in adults) or 1 25 mg (in children) intramuscularly as a single dose
or Ciprofloxacin
500 mg orally as a single dose in adults and older children
In case of rhehmatic fever with carditis but no residual valvular lesion Chemoprophylaxis is usually started after the first episode of rheumatic fever and continued for 1 0 years, or up to the age of 30 years, which ever is the longer. Drug of choice Benzathine
1 .2 million U intramuscularly every 3-weekly (600,000 U for children less than 30 kg body weight)
or
Contact with chicken pox
Acyclovir orally 20 mg/kg/day for 5 days
Phenoxymethylpenicillin or Erythromycin
Contact with measles
250 mg orally 1 2 hourly ( 1 25 mg orally 1 2 hourly in children less than 5 years) 250 mg orally 1 2 hourly ( 1 0 mg/kglday if less than 40 kg) In case of sensitivity to penicillin
Hyperimmune gamma globulin 1 .5 g/m2 single dose (if not available, then polyvalent globulin)
In case of rhehmatic fever with carditis and residual valvular lesion
Pertussis
Erythromycin may be given to household contacts in doses of 50 mg/kg/day in 4 divided doses for 14 days. Rheumatic fever
Chemoprophylaxis is usually started after the first episode of rheumatic fever and continued for lifelong. Drug of choice Benzathine
In case of rhehmatic fever without carditis
1 .2 million U intramuscularly every 3-weekly (600,000 U
benzylpenicillin
for children less than 30 kg body weight)
Chemoprophylaxis is usually started after the first episode of rheumatic
or
fever and continued for 5 years, or up to the age of 22 years, which ever
Phenoxymethylpenicillin
is the longer. The aim is to maintain antibiotic levels sufficient to prevent pharyngeal infection with Streptococcus pyogenes.
Benzathine benzylpenicillin or Phenoxymethylpenicillin or Erythromycin
or Erythromycin
Drug of choice 1 .2 million IU deep intramuscularly every 3-weekly
250 mg orally 1 2 hourly ( 1 25 mg orally 1 2 hourly in children less than 5 years) 250 mg orally 12 hourly (10 mglkg/day if less than 40 kg) In case of sensitivity to penicillin
(600,000 IU for children less than 30 kg body weight) 250 mg orally 1 2 hourly (1 25 mg orally 1 2 hourly in children less than 5 years) 250 mg orally 12 hourly ( 1 0 mg/kglday if less than 40 kg) I n case of sensitivity to penicillin
82
83
ANTIBIOTIC G U I D EL I N E
ANTIBIOTIC G U I DELI N E
ANTIMICROBIAL AGENTS ASSOCIATED WITH PHOTOSENSITIVITY
HOSPITAL INFECTION CONTROL
The fol lowing drugs are known to cause photosensitivity in
An infection within the hospital, you can take the help of infection control team. To whom you have to contact:
some individuals:
Azithromycin, ciprofloxacin, dapsone, doxycycline, erythromycin. flucytosine, gancic\ovir, griseofulvin, interferons, levofloxacin, lomeflozacin, norfloxacin, ofloxacin, pefloxacin, pyrazinamide, saquinavir, sparfloxacin, sulfonamides, tetracyclines, tretinions, trovafloxacin, trimethoprim
Dr. Sharmin Ahmed
Associate Professor Department of Microbiology and Immunology Telephone 4424 44 1 8
84
85
» z --i
Susceptibil ity of some bacteria to certain antibiotics
co (j)
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1
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R
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1
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1
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1
0
2
0
2
0
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0
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0
0
R
2
R
R
R
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2
0
Listeria monocytogenes
0
0
1
0
R
R
R
R
2
R
R
0
0
0
2
0
R
0
0
H influenzae
R
R
1R
0
2
1R
1
2
0
2
Ecoli
R
R
2R
2
2
1 R 2R
Klebsiella species
R
R
R
2R
2
1R
Serratia/Enterobacter species
R
R
R
2R
2
1R
Posteus species
R
R
1R
2R
2
1 R 2R
Pseudomonas aeruginosa
R
R
R
1R
R
Bacteroides frogilis
R
R
R
R
R
R
R
R
2
R
2
0
2R
R
R
R
1
R
2
Other Bacteroides species
2
R
R
R
R
R
R
R
2
R
2
0
2R
R
R
R
1
R
2
0
0
0
0
0
0
0
0
0
0
0
0
0
2
1
0
0
0
Clostridium difficule 1= susceptible, first choice. 2
=
2nd choice, R
=
Resistance likely. 0
=
2
0
2
R
R
2R
0
R
R
2
R
2
R
R
R
R
1 R 1 R*
R
R
2
2
2R
2R
2
R
R
R
R
1 R 1 R*
R
R
2
2
2R
2R
2
R
R
R
R
1 R 1 R*
R
R
2
2R
R
2
R
R
R
R
1 R 1 R*
R
R
2
2
1R
2
R
R
R
R
R
R
1
R
R
Usually inappropriate. R'
0 =
R
1 R*
o
G
0
2
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0
R
0
>-_ c -g. C>Q) o
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2
2
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resistance is rare in most areas.
NB : This table is a guide only, and different populations will exhibit their own (changing) patterns of resistance. .. In practice, the best thing is often to talk to a microbiologist
Classification of medically important bacteria Characteristics
I.
A.
Representative Diseases
Free-living (extracellular bacteria) 1. Gram-positive a. b.
c.
Cocci
(2) Anaerobic Non-spore-forming rods
(2) 2.
Streptococcus
Spore-forming rods ( 1 ) Aerobic Bacillus
(1 )
Nonfilamentous Filamentous
G ram-negative a. Cocci b.
Rods ( 1 ) Facultative (a) Straight (i)
(ii) co -.,J
Genus
Rigid, thick-walled cells
Staphylococcus
Pneumonia, pharyngitis, cellulites Abscess of skin and other organs
Anthrax Clostridium
Tetanus, gas gangrene, botulism
Corynebacterium
Diphtheria
Listeria
Meningitis
Actinomyces Nocardia
ActinomYCOSis
Neisseria
Gonorrhea, meningitis
Nocardiosis
» z
Respiratory organisms
Haemophilus
Zoonotic organisms
Bordetella Legionella Brucella
Whooping cough Pneumonia
Francisella
Tularemioa
Yersinia
Plagus
Meningitis
Brucellosis
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a m
r
Z m
ANTIBIOTIC G U I D ELINE
I N DEX A
B
Abdominal trauma 76
Bacitracin 38, 65
Abscess alveolar 27
Bacterial endocarditis 80 Benzylpen icillin 35,52,54, 57,58 Benzathine 5 1 , 57
breast 30 cerebral 35
Benzoyl peroxide 27
liver (pyogenic) 44
Betamethasone 40
periodontal 50
Biopsy
Acne vulgaris 26 Acyclovir 42, 43 Alveolar osteitis 27 Amikacin 47 Amoebiasis 28
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Cefalaxin 58
39, 44, 49, 50
Cefixime 33, 35 Cefotaxime 32, 44, 46, 5 1 , 53 Cefradine 27, 30, 3 1 , 50
:2 a; 0 �
lower limb 75 Antibiotic liver disease 67
2 ca
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U III III
Ceftazidime 4 1 , 46, 47 Ceftipime 5 1 Cefuroxime 52, 53, 56 Cellulitis 34
pregnancy 68
Cesarean section 78
renal failure 66
Ceftriaxone 34, 35, 36, 38,
Antim icrobial therapy 1
Ql (j) Gi .c :is 0 ";C e
88
Amoxycillin 27, 3 1 , 32, 33,
Ampicillin 3 1 , 46, 47, 52
"2'
c
Amputation
.'§
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Bronchitis 32
a.
(ij
�
trans rectal p rostate 77 Bronchiectasis 3 1
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Procaine 57, 58
Antiserum 30 Aortic resection 74
�
Appendicectomy 76
�
Azelaic acid 26
--'
=
Azithromycin 26, 40, 62
40, 44, 45, 46, 49, 5 1 , 55
Chicken pox 82 Chancroid 33 Chloramphenicol 37 Cholecystitis acute 36 Cholera 36 89
ANTIBIOTIC GUI DELINE
Ciprofloxacin 28, 32, 36, 37,
ANTIBIOTIC GUIDELINE
F
39, 40, 44, 45, 47 , 48, 49, 5 1 , 52, 53, 54, 55, 56, 62, 63
Famciciovir 42, 43
Clarithromycin 50, 5 1 , 52, 53
Fever enteric 40 rheumatic 82 Febrile neutropenia 4 1 Flucloxacillin 2 7 , 3 0 , 3 1 , 34,
Cleft lip 79 Clindamycin 53, 54, 64 Clotrimazole 63, 64 Cloxacillin 30, 3 1 Co-amoxiclav 2 9 , 34, 3 5 , 49, 52, 53, 56, 58
Conjunctivitis 37 Co-trimoxazole 3 1 , 32, 33, 39, 40, 55, 62, 63
Cystoscopy 76
o Dexamethasone 4 1 Doxycycline 27, 36, 44, 54, 57
Fluconazole 49, 63 F racture open reduction 75 Fusidic acid 65
breast m i l k 70 amoebic 28 bacillary 39
Joints
Omeprazole 49
replacement 75
Oral thrush (candidiasis) 49 Otitis
Gatifloxacin 34 Gentamicin 28, 35, 36, 40, 44, 46, 47, 48, 53, 54, 65 Giardiasis 43 Ging ivitis 44
Lansoprazole 50 Levofloxacin 56
M Mastitis 30
Erythromycin 26, 27, 33, 36, Ethambutol 59
Peptic ulcer 49 Pericoronitis 50 Peritonitis 5 1
Mastoiditis 44
Pertussis 82 P-floxacillin 40
H
Meningitis 45
Pharyngitis 5 1
Helicobacter pylori 49 Herpes genital 42
Meningococcus contact 81
Phenoxymethylpenicillin 34, 51
Metronidazole 27, 28, 3 1 , 35,
Photosensitivity 84
36, 43, 44, 49, 50, 54, 56, 64
Polymyxin B 32
Miconazole 64
Pneumonia 52
Mupirocin 65
P rostate biopsy transrectal 77
Eczema (infected) 40
38, 5 1 , 54, 58 .
p Pacemaker implant 74
Econazole 47
Enteric fever 40
media (acute suppurative) 48
Measles 82
E
bacterial 80
externa 47
L
G
Hydrocortisone 40, 47, 48 Hysterectomy 78
Endocarditis
Ofloxacin 37, 4 1 , 63
arthroplasty 75
Liver abscess (pyogenic) 44
Drugs i n Dysentery
o
48, 56
Cystitis acute uncomplicated 39
J
I mepenum 53, 55 Infection urinary tract 62 Inguinal hernia repair 76 Isoniazid 59, 60, 6 1 Itraconazole 49
N
P rostatectomy 77 P rostatitis 55
Neomycin 40, 65
P rosthetic valve insertion 74
Nitrofurantoin 62, 63
Pyelonephritis (acute) 55
Nystatin 49
Pyrazinamide 59, 60, 6 1
90 91
ANTIBIOTIC GUIDELINE
R
Surgery biliary tract 75 cardiovascular 74
Rabies immune globulin 29
gastroduodenal 75
vaccine 29
open heart 74
Rheumatic fever 82
orthopaedic 75 u rolog ical 76
Rifampicin 59, 60, 6 1 T
Syphilis 57
Tetanus immunogiobulin 30 Tetracycline 32, 33, 36 , 38, 44, 54, 57
u
Tinidazole 28, 43, 64 Tobramycin 37
Ulcer
Tonsillitis 58
corneal 38
Tooth extraction 80
U rethritis (acute, for males) 62
Transplantation
U rinary tract infection 62
Kidney 77
v
Tretinoin 26 Triamcinolone 47
Vaccine
Tuberculosis 58
rabies 29 Vaginal candidiasis 63
s
trichomoniasis 64 Vaginosis (bacterial) 64
Secnidazole 28, 43, 64
Valacyclovir 42 , 43
Sepsis
Vancomycin 46,52
bil iary 28
Vitamin A 40
neonatal 47 neuropathic
foot
diabetes mellitus 56 Shock anaphylactic 7 1
in
W Wounds
Sinusitis 56
bite 29
Streptomycin 60
infected 65