ANTITUBERCULOSIS DRUGS
Outline
Copyright, Purdue Research Foundation, 1996
| BMS 445 Intro |
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The Therapeutic Problem
Therapeutic Goals
- Prevention or prophylaxis
- Cure of clinical disease
- Prolonged therapy
- Combined therapy
- Compliance
- Development of drug resistance
- Cures, ideally, 95-100%
The Disease
- Mycobacterium tuberculosis
- Cell wall -- high lipid (60% dry weight) content
- Mycolic acid a major component
- Slow growth
- Survive within phagocytes
- resistance to chemical disinfectants
- Atypical Mycobacteria
Members
- Isoniazid, (INH) [Dow-Isoniazid, Nydrazid]
- Rifampin [Rifadin, Rimactane]
- Rafabutin [Mycobutin] AMADE93, 1:33
- pyrazinamide (PZA)
- Capreomycin Sulfate [Capastat Sulfate]
- Cycloserine [Seromycin]
- Ethambutol Hydrochloride [Myambutol]
- Ethionamide [Trecator-SC]
- Streptomycin Sulfate
ISONIAZID [INH, NYDRAZID]
General comments
- Prophylaxis as single agent
- Cure -- ALWAYS in combination
- Slows development of resistance
Chemistry / structure
- Resembles the B-vitamin, nicotinic acid
- Need supplementation with the vitamin during Rx
Antibacterial activity
- Bacteriostatic at most concentrations
Resistance
- Increasing
- Easy to create by culture techniques
Mechanism of action
- Inhibits mycolic acid synthesis
Pharmacokinetics
- IM and PO
- Well absorbed
- Widely distributed
- intracellular
- CSF
- Necrotic material
- Elimination mainly acetylation
- Bimodal distribution in human population
- Fast and slow acetylators
- Elimination half-life:
- Fast = 70 min
- Slow = 180 min
- Fast/Slow = 50:50 Western countries (whites and blacks)
- Fast/Slow = 90/10 Eskimos and Japanese
- Slow dominant most Scandinavians, Jews, and North African Caucasians.
Adverse Effects
- Most notable -- peripheral neuritis
- Supplement with pyridoxine
- Others - see reference
RIFAMPIN (RifadinR, RimactaneR)
Source/Structure
- Macrocyclic antibiotic
- Streptomyces mediterranei
Antibacterial Spectrum
- M. tuberculosis
- cidal
- Broad spectrum of bacteria
- Many Gram(-)
- Many chlamydiae
Resistance
- Develops quickly
- Not use drug alone for TB or other bacteria
Mechanism of Action
- Binds to DNA-dependent RNA polymerase
- Inhibits initiation -- not elongation
Pharmacokinetics
- PO -- Well absorbed
- Broadly distributed -- even CSF
- Orange-red color stains tissues / secrections / urine
- Half-life of rifampin is 1.5 to 5 h and is increased by hepatic
dysfunction.
- Autoinduction of metabolism
- Half-life shortens 40% first 14 days of Rx
- Hepatic microsomal induction
Adverse reactions
- Relatively safe
- Jaundice
- rare if liver normal
- Increases if chronic liver disease, old age, alcoholism
- Drug interaction
- Hepatic microsomal induction
- Shortens half-life of many drugs, eg.,
- prednisone, digitoxin,
quinidine, ketoconazole, propranolol, metoprolol, clofibrate,
and sulfonylureas, oral contraceptives, and oral anticoagulants.
It has precipitated methadone withdrawal.
- Redman syndrome
- Marked overdosage
- Severe liver damange
- bright red urine, tears, saliva
- skin resembles broiled lobster
- Other effects -- see reference
Recent applications
- Never used alone -- resistance development
- Tuberculosis
- Leprosy
- Fungi/yeasts -- additive or synergistic with amphotericin B
- Various bacterial infections, e.g., with a beta-lactam
or vancomycin for staphylococcal endocarditis.
RIFABUTIN (MycobutinR)
- New -- resembles rifampicin
- Indication: prevention of disseminated MAC disease in advanced
AIDS
REFERENCES
See Antileprosy drugs handout
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Gordon L. Coppoc, DVM, PhD
Professor of Veterinary Pharmacology
Head, Department of Basic Medical Sciences
School of Veterinary Medicine
Purdue University
West Lafayette, IN 47907-1246
Tel: 317-494-8633Fax: 317-494-0781
Email: coppoc@vet.purdue.edu
Last modified 11:10 PM on 4/16/96
GLC