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Side Effects of Antituberculosis Therapy

In an article by Yee and colleagues (1), the authors found a high incidence of major side effects for pyrazinamide. Although this might be in line with clinical impression, there could have been a major methodologic pitfall.

Individual susceptibility is a key factor for drug reactions. Patients tolerating the drugs initially are much less likely to develop side effects afterward. Indeed, in the article (1), 98% of major side effects occurred within the first 2 months of drug administration. Similarly, in a previous controlled trial of 2, 4, and 6 months of pyrazinamide in short-course regimens, 83% of side effects of any kind occurred within the first 2 months (2). As pyrazinamide is regularly given for 2 months, whereas isoniazid and rifampin are given for 6 months, the use of incidence rate per person-month of treatment would have introduced up to a threefold bias against pyrazinamide.

Consider the following hypothetical situation: the three drugs produced an equal number of major side effects within the first 2 months, and no major side effects occurred afterward among those not experiencing side effects initially. The calculated relative risk for pyrazinamide versus isoniazid or rifampin would be 3 by person-month of treatment, but only 1 by intention-to-treat analysis on per-person basis.

The Cox analysis cannot eliminate the systematic bias that was introduced. The complex statistical calculation is no more robust than a simple comparison among groups, as consistently used in all the randomized controlled trials quoted by the authors (3–5). Indeed, the nature of the data might not have allowed the authors to draw any firm conclusion about drug-induced hepatitis. All the quoted hepatitis events occurred when the drugs were used together, and two or more drugs were subsequently withdrawn, making it difficult to pinpoint the offending agent. It is also possible that the drug combination, rather than pyrazinamide alone, caused the hepatitis. As patients' safety often precludes actual rechallenge, one can never exclude the possibility that all the original drugs might be successfully put back as reported previously (6). Simple apportioning of the blame, although intuitively appealing, might not be most appropriate.

The currently used 6-month short-course regimen has been established through meticulous research. However, much remains unknown about pyrazinamide, including its optimal dosage and frequency of administration among different age groups. Carefully designed research is necessary to address these critical issues for the benefit of the vast number worldwide of patients with tuberculosis.

Chi Chiu Leung^a, Chi Kuen Chan^a and Wing Wai Yew^b

^a Department of Health Hong Kong, China
^b Grantham Hospital Hong Kong, China

FOOTNOTES

Conflict of Interest Statement: C.C.L., C.K.C., and W.W.Y. have no declared conflict of interest.

REFERENCES

1. Yee D, Valiquette C, Pelletier M, Parisien I, Rocher I, Menzies D. Incidence of serious side effects from first-line antituberculosis drugs among patients treated for active tuberculosis. Am J Respir Crit Care Med 2003;167:1472–1477.[Abstract/Free Full Text]
2. Hong Kong Chest Service/British Medical Research Council. Controlled trial of 2, 4, and 6 months of PZA in 6-month, three-times-weekly regimens for smear-positive pulmonary tuberculosis, including an assessment of a combined preparation of isoniazid, rifampin, and pyrazinamide: results at 30 months. Am Rev Respir Dis 1991;143:700–706.[Medline]
3. Combs DL, O'Brien RJ, Geiter LJ. USPHS tuberculosis short course chemotherapy trial 21: effectiveness, toxicity and acceptability. Ann Intern Med 1990;112:397–406.
4. British Thoracic Association. A controlled trial of 6-months isoniazid and rifampin therapy for pulmonary tuberculosis: first report: results during drug therapy. Br J Dis Chest 1981;75:141–153.[CrossRef][Medline]
5. Zierski M, Bek E. Side-effects of drug regimens used in short-course chemotherapy for pulmonary tuberculosis: a controlled clinical study. Tubercle 1980;61:41–49.[CrossRef][Medline]
6. Dossing M, Wilcke JT, Askgaard DS, et al. Liver injury during antituberculous treatment: an 11-year study. Tuber Lung Dis 1996;77:335–340.[CrossRef][Medline]

From the Authors:

We thank Dr. Leung and colleagues for their comments regarding our study (1). We used the incidence density method to account for the variable duration of exposure of pyrazinamide, isoniazid, and rifampin. This could have exaggerated differences among drugs, if adverse events occurred only in the first 2 months; but in one large-scale trial, isoniazid hepatoxicity continued to occur in the seventh to twelfth month of therapy (2). Given this, person-time estimates will be more accurate and particularly useful for comparison of risks, benefits, and costs of regimens of different duration, such as 2 months of rifampin–pyrazinamide versus 9 months of isoniazid for latent tuberculosis (TB) infection.

Attribution of adverse events to individual drugs can be difficult in an observational study. However, in our study, pyrazinamide was the most commonly responsible drug for hepatitis and overall adverse events when a single drug was identified unequivocally in 36 out of 46 serious adverse events. Even if all the events of hepatitis that we divided between isoniazid and pyrazinamide had been attributed entirely to isoniazid, the incidence of isoniazid- and pyrazinamide-related hepatotoxicity would have been equal, and overall adverse events in pyrazinamide would have been twice as high as any other drug (1).

We agree with Dr. Leung that carefully conducted randomized trials have established the use of pyrazinamide for therapy of active TB, but we do not agree that these trials accurately estimated the incidence of adverse events. In randomized trials of therapy for tuberculosis infection and disease, incidence of adverse events has been considerably less than observed later in routine clinical practice (3). In initial randomized, placebo-controlled trials involving more than 100,000 individuals, isoniazid hepatotoxicity caused by isoniazid was uncommon (0.1–0.3%), and no deaths were reported (4). However, after widespread use in routine practice, isoniazid hepatotoxicity was 10 times higher with associated mortality (5). Similarly, in randomized trials, occurrence of adverse effects with 2 months of rifampin–pyrazinamide was similar to that with 6 to 12 months of isoniazid; but after more widespread use, much higher rates of serious and even fatal hepatotoxicity were reported (6).

The differences between the incidence of adverse events in randomized trials and routine clinical practice remain unexplained. However, they underscore the importance of careful surveillance to estimate adverse events from new regimens whose utility has been demonstrated in randomized trials, after their introduction into routine clinical use.

Daphne P. Yee and Dick Menzies

McGill University Montreal, Quebec, Canada

REFERENCES

1. Yee D, Valiquette C, Pelletier M, Parisien I, Rocher I, Menzies D. Incidence of serious side effects from first-line antituberculosis drugs among patients treated for active tuberculosis. Am J Respir Crit Care Med 2003;167:1472–1477.
2. International Union Against Tuberculosis Committee on Prophylaxis. Efficacy of various durations of isoniazid preventive therapy for tuberculosis: five years of follow-up in the IUAT trial. Bull World Health Organ 1982;60:555–564.[Medline]
3. Schaberg T, Rebhan K, Lode H. Risk factors for side-effects of isoniazid, rifampin and pyrazinamide in patients hospitalized for pulmonary tuberculosis. Eur Respir J 1996;9:2026–2030.[Abstract]
4. Ferebee SH. Controlled chemoprophylaxis trials in tuberculosis. Adv Tuberc Res 1969;17:28–106.
5. Kopanoff DE, Snider D, Caras GJ. Isoniazid-related hepatitis. Am Rev Respir Dis 1978;117:991–1001.[Medline]
6. Update: fatal and severe liver injuries associated with rifampin and pyrazinamide for latent tuberculosis infection, and revisions in the American Thoracic Society/CDC recommendations—United States, 2001. MMWR Morb Mortal Wkly Rep 2001;50:733–735.

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