Isoniazid-related Hepatitis: a U.S. Public Health Service Cooperative Surveillance Study

Overview

Journal Am Rev Respir Dis

Specialty Pulmonary Medicine

Date 1978 Jun 1

PMID 666111

Citations 107

Authors

D E Kopanoff

D E Snider Jr

G J Caras

Affiliations

Soon will be listed here.

Abstract

After an outbreak of hepatitis in Washington, D.C. in 1970 among a group of persons taking isoniazid to prevent tuberculosis, an isoniazid surveillance study was conducted among 13,838 persons in 21 participating health departments. Age appeared to be the predominant factor influencing the risk of developing isoniazid-related hepatitis, i.e., increasing age was associated with an increasing risk. Drinking alcohol, especially on a daily basis, also seemed to enhance the risk of hepatitis among persons concurrently taking isoniazid. In general, case rates among males and females of the same race, and rates among different races, were not markedly different; however, there were striking differences in the case rates among males of different races. The incidence of hepatitis varied greatly among the 21 cities, but was not unique to any geographic region, nor was it related to a specific manufacturer of isoniazid. The onset, in most cases, occurred within the first few months of treatment. Eight fatalities were reported by the 21 participating health departments, 7 occurring in one city. Black females accounted for 5 of the 8 deaths. This information provides a basis for weighing the benefits of isoniazid in preventing tuberculosis against the risk of its causing hepatitis. Close monitoring for overt signs or symptoms of hepatitis among persons receiving isoniazid preventive therapy is indicated, especially for persons greater than or equal to 35 years of age and those who drink alcoholic beverages on a daily basis.

Citing Articles

Clinical perspectives of isoniazid-induced liver injury.

Lei S, Gu R, Ma X Liver Res. 2025; 5(2):45-52.

PMID: 39959342 PMC: 11791842. DOI: 10.1016/j.livres.2021.02.001.

Polymorphism of is associated with anti-tuberculosis drug-induced hepatotoxicity.

Lee S, Chen P, Liu C, Li Y, Wu L Pharmacogenomics. 2024; 25(5-6):241-247.

PMID: 38884784 PMC: 11388135. DOI: 10.1080/14622416.2024.2346069.

Predictive Model of Oxaliplatin-induced Liver Injury Based on Artificial Neural Network and Logistic Regression.

Huang R, Cai Y, He Y, Yu Z, Zhao L, Wang T J Clin Transl Hepatol. 2024; 11(7):1455-1464.

PMID: 38161498 PMC: 10752815. DOI: 10.14218/JCTH.2023.00399.

Cost-effectiveness of 3-months isoniazid and rifapentine compared to 9-months isoniazid for latent tuberculosis infection: a systematic review.

Lai W, Brethour K, DSilva O, Chaisson R, Zwerling A BMC Public Health. 2022; 22(1):2292.

PMID: 36476206 PMC: 9727859. DOI: 10.1186/s12889-022-14766-6.

Comparative Efficacy of Rifapentine Alone and in Combination with Isoniazid for Latent Tuberculosis Infection: a Translational Pharmacokinetic-Pharmacodynamic Modeling Study.

Radtke K, Ernest J, Zhang N, Ammerman N, Nuermberger E, Belknap R Antimicrob Agents Chemother. 2021; 65(12):e0170521.

PMID: 34606336 PMC: 8597776. DOI: 10.1128/AAC.01705-21.