Isoniazid preventive therapy and risk for resistant tuberculosis.In the context of tuberculosis tuberculosis (TB), contagious, wasting disease caused by any of several mycobacteria. The most common form of the disease is tuberculosis of the lungs (pulmonary consumption, or phthisis), but the intestines, bones and joints, the skin, and the genitourinary, (TB) resurgence re·sur·gence n. 1. A continuing after interruption; a renewal. 2. A restoration to use, acceptance, activity, or vigor; a revival. , isoniazid isoniazid (ī'sōnī`əzĭd), drug used to treat tuberculosis. Also known as isonicotinic acid hydrazide, isoniazid is the most effective antituberculosis drug currently available. preventive therapy (IPT IPT - IP Telephony ) is increasingly promoted, but concerns about the risk for development of isoniazid-resistant tuberculosis may hinder hin·der 1 v. hin·dered, hin·der·ing, hin·ders v.tr. 1. To be or get in the way of. 2. To obstruct or delay the progress of. v.intr. its widespread implementation. We conducted a systematic review of data published since 1951 to assess the effect of primary IPT on the risk for isoniazid-resistant TB. Different definitions of isoniazid resistance were used, which affected summary effect estimates; we report the most consistent results. When all 13 studies (N = 18,095 persons in isoniazid groups and N = 17,985 persons in control groups) were combined, the summary relative risk for resistance was 1.45 (95% confidence interval confidence interval, n a statistical device used to determine the range within which an acceptable datum would fall. Confidence intervals are usually expressed in percentages, typically 95% or 99%. 0.85-2.47). Results were similar when studies of HIV-uninfected and HIV-infected persons were considered separately. Analyses were limited by small numbers and incomplete testing of isolates, but findings do not exclude an increased risk for isoniazid-resistant TB after IPT. The diagnosis of active TB should be excluded before IPT. Continued surveillance for isoniazid resistance is essential. ********** Tuberculosis (TB) has reemerged as a major threat to global public health. Its incidence is rising, particularly in countries with a high HIV HIV (Human Immunodeficiency Virus), either of two closely related retroviruses that invade T-helper lymphocytes and are responsible for AIDS. There are two types of HIV: HIV-1 and HIV-2. HIV-1 is responsible for the vast majority of AIDS in the United States. prevalence (1). HIV-infected persons have an increased risk for reactivated latent Hidden; concealed; that which does not appear upon the face of an item. For example, a latent defect in the title to a parcel of real property is one that is not discoverable by an inspection of the title made with ordinary care. TB infection (2), of having new TB infection progress rapidly to active disease (3,4), and of dying during a TB episode (5). Since current TB control methods appear inadequate to prevent the rise in TB incidence among HIV-infected persons in settings with high TB prevalence (6), additional measures are required. Studies in the late 1980s and 1990s found that TB "preventive therapy" (treatment of latent TB infection) reduced TB incidence among HIV-infected persons, at least among those with positive tuberculin skin test Tuberculin Skin Test Definition Tuberculosis (TB) is an airborne infectious disease caused by the bacteria Mycobacterium tuberculosis. Besides culturing in the laboratory, the two most common types of tests to screen for exposure to this disease results (7). However, despite recommendations from the World Health Organization (WHO) and the Joint United Nations Programme on HIV/AIDS HIV/AIDS Human Immunodeficiency Virus/Acquired Immune Deficiency Syndrome in 1998 (8), TB preventive therapy has not been widely adopted. One obstacle to more widespread use is the concern that using isoniazid monotherapy monotherapy /mono·ther·a·py/ (-ther´ah-pe) treatment of a condition by means of a single drug. mon·o·ther·a·py n. Treatment of a disorder with a single drug. to treat latent TB infection could promote isoniazid-resistant TB; a literature review in 1970 concluded that, since the introduction of isoniazid in 1952, no evidence existed to support this conclusion (9). Since then, a number of placebo-controlled trials of isoniazid preventive therapy (IPT) have been conducted, mostly among HIV-infected persons. We carried out a systematic review of studies (in both the pre-HIV and the HIV era) that compared those who received IPT to an untreated group and reported data on resistance to isoniazid, aiming to assess the effect of primary IPT on the risk of developing isoniazid-resistant TB. Methods Identification and Selection of Studies We searched 5 electronic databases (PubMed, Embase, Popline, National Library of Medicine Gateway, Cochrane Library The Cochrane Library is a collection of databases in medicine and other healthcare specialties provided by the Cochrane Collaboration. At its core is a database of systematic reviews and meta-analyses which summarise and interpret the results of high-quality medical research. ) to identify studies of IPT published in English, French, or Spanish from 1951 to October 2003. Thesaurus and free-text terms were used in various combinations, depending on the requirements of each database (details available on request). We also searched by hand the reference lists in all identified publications and recent systematic reviews (7,10-12). We reviewed the full text of all studies evaluating the effectiveness of primary IPT (given to persons with no history of TB), applying the following inclusion criteria
Inclusion criteria are a set of conditions that must be met in order to participate in a clinical trial. : 1) compared incidence of TB in persons receiving isoniazid monotherapy versus those receiving no preventive therapy; 2) randomized controlled trial A randomized controlled trial (RCT) is a scientific procedure most commonly used in testing medicines or medical procedures. RCTs are considered the most reliable form of scientific evidence because it eliminates all forms of spurious causality. (RCT RCT Randomized Controlled Trial RCT Regimental Combat Team (infantry regiment with their own artillery, engineers, medical and tanks) RCT Rollercoaster Tycoon RCT Randomized Clinical Trial RCT Rhondda Cynon Taff ) or cohort study A cohort study is a form of longitudinal study used in medicine and social science. It is one type of study design. In medicine, it is usually undertaken to obtain evidence to try to refute the existence of a suspected association between cause and disease; failure to refute designs; and 3) results of susceptibility testing susceptibility test Antimicrobial susceptibility test, see there of positive cultures presented for both isoniazid and control groups, so the proportion of resistant strains could be ascertained in each group. We excluded studies conducted only in children (among whom microbiologic confirmation is less common), studies of secondary preventive therapy, and studies, or subgroups within studies, of persons with "recently active disease," many of whom had previously received isoniazid. Data were extracted in duplicate by 2 investigators independently, using a standardized standardized pertaining to data that have been submitted to standardization procedures. standardized morbidity rate see morbidity rate. standardized mortality rate see mortality rate. data-collection form. Data included study details (study population and size, design, intervention drug regimen regimen /reg·i·men/ (rej´i-men) a strictly regulated scheme of diet, exercise, or other activity designed to achieve certain ends. reg·i·men n. 1. , outcomes recorded) and quality measures (e.g., generation and concealment of allocation sequences, blinding, duration of and loss to follow-up). Statistical Analysis We estimated the incidence of TB caused by isoniazid-resistant strains separately for the isoniazid and control group of each study by dividing the number of persons with isoniazid-resistant TB by the total number of persons in that group. We chose the incidence of isoniazid-resistant TB in preference to the proportion of culture-positive TB cases that were isoniazid resistant because incidence better represents the impact (and risk for transmission) of resistant disease at the population level. Also, comparison of the proportion of resistant isolates between groups is complicated if the study population includes persons who have latent TB infection with an isoniazid-resistant organism. In the group receiving isoniazid, preventive therapy will decrease the number of reactivated TB cases attributable to isoniazid-susceptible strains but will have less effect on resistant strains, which will increase the proportion of resistant strains among subsequent cases of active TB. As a result, the proportion of isoniazid-resistant active TB cases will be higher in the isoniazid group than in the control group, even if isoniazid does not promote new resistance. The analysis involved a number of assumptions, summarized in Table 1. In studies in which not all TB patients underwent resistance testing, we assumed that isolates tested were a random sample of all TB cases and multiplied the total number of TB cases by the proportion of isoniazid-resistant cases in the sample to estimate the total number of isoniazid-resistant cases. For example, if 1,000 persons were randomly assigned to isoniazid therapy, active TB developed in 50, 40 of these were tested, and 8 (20%) of 40 had isoniazid-resistant isolates, we then estimated a total of 10 (50 x 0.2) resistant TB cases and an incidence of isoniazid-resistant TB of 10 per 1,000 persons. Relative risks (RR) for resistant TB in the isoniazid group compared to the control group were calculated for each study. The extra variation incurred by sampling isolates for resistance was incorporated into the 95% confidence intervals (CIs) of each RR. The RR could be written as the product of 2 ratios (the ratio of TB incidence in exposed/unexposed multiplied by the ratio of the proportion of resistant cases in the sample tested for the exposed/unexposed). Thus, the log RR could be expressed as the sum of the logs of these ratios, and the variance of the log RR could be calculated by a double application of a standard formula (details available on request). When no resistant cases were found in 1 of the 2 groups, we added 0.5 to the numerator numerator the upper part of a fraction. numerator relationship see additive genetic relationship. numerator Epidemiology The upper part of a fraction and denominator denominator the bottom line of a fraction; the base population on which population rates such as birth and death rates are calculated. denominator of both groups when estimating the risk, and 0.1 to the numerators and denominators when calculating the variance of the ratio of proportions (13). Tests of between-study heterogeneity het·er·o·ge·ne·i·ty n. The quality or state of being heterogeneous. heterogeneity the state of being heterogeneous. were performed, and meta-analyses were carried out to derive summary RRs, by using a random-effects model when evidence of heterogeneity was found (14). In the meta-analysis, we first considered all studies as a single group, then considered separately studies from the pre-HIV era and studies of HIV-infected persons; we hypothesized that HIV-infected persons could be at higher risk of having resistance develop. When latent TB infection is treated, few organisms are exposed to the drug (15). The risk for selection pressure favoring a drug-resistant organism is therefore low (16) unless persons have undiagnosed active TB and thus inadvertently receive monotherapy for active disease. Active TB may be more difficult to detect among HIV-infected persons, which could lead to a higher risk for undiagnosed active disease. Sensitivity analyses primarily consisted of excluding from meta-analyses studies a) that had zero resistant cases in a group and b) that were not RCTs. Publication bias was investigated by using funnel plots and adjusted rank correlation In statistics, rank correlation is the study of relationships between different rankings on the same set of items. It deals with measuring correspondence between two rankings, and assessing the significance of this correspondence. tests (17). All analyses were carried out in Stata version 8.0 (Stata Corp., College Station, TX, USA). Results We identified 19 studies comparing primary IPT with no treatment that reported isoniazid resistance among adults (9,18-35). Of the 11 studies from the pre-HIV era, 4 (23-26) were excluded because resistance data from the control group were incomplete or not reported. In 2 studies (9,19), we excluded subgroups of persons with previously active disease, for which many had received isoniazid. Of the 8 studies among HIV-infected persons, 2 (28, 29) were excluded because the total number of isolates tested in the relevant groups could not be determined. For 1 study (33), unpublished resistance data were obtained from the authors (E Godfrey-Faussett, pers. comm.). Characteristics of Included Studies Thirteen studies were included in the analysis (Tables 2, 3), 12 RCTs and 1 retrospective cohort study. The 7 pre-HIV era studies (N = 32,179) were mostly conducted in the late 1950s or early 1960s in populations of persons with radiologically-inactive TB lesions (9,19,22), persons in communities with high TB incidence (20,21), and household contacts of TB cases (18); 1 study was of persons with silicosis in Hong Kong Hong Kong (hŏng kŏng), Mandarin Xianggang, special administrative region of China, formerly a British crown colony (2005 est. pop. 6,899,000), land area 422 sq mi (1,092 sq km), adjacent to Guangdong prov. in the 1980s (27). Study population size ranged from 225 to 15,751 patients. In most studies, isoniazid 300 mg (or 5 mg/kg) was given daily, although in the Greenland study (20), 400 mg was given on 2 consecutive days each week. Duration of treatment was 24 weeks to 2 years. All 6 studies among HIV-infected persons (N = 3,901) recruited participants from HIV clinics or voluntary counseling and testing Voluntary Counseling and Testing (VCT) for HIV usually involves two counseling sessions: one prior to taking the test known as "pre-test counseling" and one following the HIV test when the results are given, often referred to as "post-test counseling". centers. Study population size was 121-1,718. RCTs administered isoniazid for 6 months at 300 mg daily (30,31,34,35) or 900 mg twice weekly (33); in the cohort study, an unspecified Adj. 1. unspecified - not stated explicitly or in detail; "threatened unspecified reprisals" specified - clearly and explicitly stated; "meals are at specified times" dose was given for 9 to 12 months (32). We could assess the method of assigning the treatment allocation in 5 of the 12 RCTs: 2 studies (31,33) used computer-generated random numbers, 2 (20,21) used random number tables, and 1 (19) assigned by odd or even hospital number. Three RCTs reported that the treatment was concealed: 2 used sealed envelopes (33,34), and 1 used numbered packages containing isoniazid or matching placebo (27). Eight RCTs were double-blinded (18,20,21,27,30,31,33,34), although in 1 study, isoniazid and placebo groups may have received different numbers of tablets (34); 2 were not blinded (19,35), and 2 did not report blinding (9,22). Loss to follow-up was reported in 11 studies: in 6, this loss was <20% in both groups (see unabridged, online versions of Tables 2 and 3, available at http://www.cdc.gov/ncidod/eid/vol12no05/05-0681.htm# table2). Tuberculosis Cases and the Proportion of Isoniazid-resistant Isolates The total number of TB cases within a study ranged from 7 to 561. In all studies combined, 564 TB cases occurred among persons who received isoniazid, and 1,034 occurred among controls. In the 7 studies that reported this information, 55%-100% of TB cases were sputum-culture positive (20,22,27,31,32,34,35). In 4 of these studies, [greater than or equal to] 90% of culture-positive isolates underwent resistance testing (22,27,31,35). In total, 158 persons in the isoniazid groups and 328 in control groups had isolates tested for resistance to isoniazid. Definitions of isoniazid resistance varied, and the proportion of tested isolates that were resistant ranged from 0% to 100% (Tables 2, 3, and unabridged online versions). A total of 31 resistant isolates were obtained from the isoniazid groups and 28 or 24 (depending on the definition of resistance) from control groups. Of the 6 studies among HIV-infected persons, 1 found no resistant isolates in the isoniazid group (33), 2 found no resistant isolates in the control group (31,32), and 1 found no resistance in either group (30) (Table 3). Relative Risk for Isoniazid Resistance and Meta-analyses In 8 of the 12 studies in which a single definition of resistance was used, the point estimate of RR for isoniazid resistance in the isoniazid group compared to that of controls was >1, although this result was not statistically significant in any study (Tables 2, 3). Two alternative (and substantially different) definitions of resistance were used in the Greenland study, which resulted in different estimates of the effect of IPT on isoniazid resistance (Table 2). We therefore conducted 2 analyses, using each definition of resistance for this study. By using definition (a) from the Greenland study, the summary RR for all 13 studies combined was 1.25 (95% CI 0.75-2.10) in either a random or fixed effects model (Figure 1A) with little evidence of heterogeneity ([P.sub.het] = 0.789). By using definition (b) from the Greenland study, the summary RR was 1.45 (95% CI 0.85-2.47, Figure 1B), again with little evidence of heterogeneity ([P.sub.het] = 0.923). Summary estimates were virtually unaltered when analyses were restricted to RCTs without zero cells (Figure 1). We also excluded the Greenland study from the meta-analysis to assess its overall effect on the summary estimate. The summary RR using the remaining 12 studies was similar to that obtained by using definition (b) for resistance (RR 1.43, 95% CI 0.83-2.46). [FIGURE 1 OMITTED] Among the 7 studies from the pre-HIV era, the summary RR for isoniazid resistance was 1.24 (95% CI 0.69-2.21) when the definition (a) from the Greenland study (a) was used and 1.50 (95% CI 0.82-2.73) with definition (b). The summary RR was 1.30 (95% CI 0.42-4.02) for the 6 studies of HIV-infected persons. Little evidence of between-study heterogeneity was found in any of these analyses ([P.sub.het] >0.5 for all). When meta-analysis of the studies of HIV-infected persons was restricted to the 2 RCTs without zero cells (34,35), the summary RR rose slightly to 1.42 (95% CI 0.26-7.69) in a random-effects model, with slightly stronger evidence of heterogeneity ([P.sub.het] = 0.179). Funnel plots (Figure 2) suggested little evidence of publication bias (p = 0.625 and p = 0.542 by using definition [a] and definition [b], respectively, for the Greenland study). [FIGURE 2 OMITTED] Discussion Our summary RR for isoniazid-resistant TB after IPT is not statistically significant, but the point estimate and upper boundary of the 95% CI are consistent with an increased risk. Our review highlights the limitations of existing data; however, since further individually randomized ran·dom·ize tr.v. ran·dom·ized, ran·dom·iz·ing, ran·dom·iz·es To make random in arrangement, especially in order to control the variables in an experiment. , controlled trials controlled trial Clinical research A clinical study in which one group of participants receives an experimental drug while the other receives either a placebo or an approved–'gold standard' therapy. See Blinding, Double-blinded. of IPT would be inappropriate, additional data of this type are unlikely to become available. The numbers of TB cases in the individual studies were often small, and in 4 studies, no resistant TB cases occurred in at least 1 of the comparison groups. Comparison of summary estimates with and without these 4 studies suggests that adding a small number to the numerators and denominators so they could contribute to summary estimates did not in itself affect the result. The 95% CIs for RRs in these studies were very wide, and so their contribution to the summary RR estimate was limited. The summary estimate of effect was similar in HIV-infected and HIV-uninfected persons. Screening for active TB before enrollment could have been more rigorous in studies among HIV-infected persons; the screening procedures were not always clearly described. The proportion of positive cultures tested for resistance varied from 37% to 100%; why all isolates were not tested was not clear. The most important assumption made in the analysis was that the proportion of resistant cases among the isolates tested was representative of all TB cases in that group. If investigators were not blinded to the treatment allocation, and if persons receiving isoniazid were more likely to have positive cultures tested for resistance, ascertainment of resistance in the isoniazid group could have increased, and thus RR could have been overestimated. However, in 10 of the 13 studies, a placebo was used; 8 studies specified that the trial was double blinded, and (for studies for which information was available) similar proportions of culture-positive TB cases were tested from each group. Therefore, differential ascertainment of resistance is unlikely. Our estimate of the total number of isoniazid-resistant cases disregarded whether case-patients were sputum-culture positive. Persons with isoniazid-resistant isolates that are sputum-culture negative are less likely to transmit disease and present less of a public health concern. This situation is unlikely to affect our estimate of the effect of isoniazid on the incidence of resistant disease, but our estimate may exaggerate the public health risk. Study quality and review methods may have affected the results in other ways. For example, inadequate random assignment of HIV-infected persons could result in more advanced immunosuppression immunosuppression Suppression of immunity with drugs, usually to prevent rejection of an organ transplant. Its aim is to allow the recipient to accept the organ permanently with no unpleasant side effects. among those in the isoniazid group and thus a higher probability of resistance. However, when reported, the method of randomization randomization (ranˈ·d  ·m in trials of
HIV-infected persons appeared adequate. Differences in loss to follow-up
between comparison groups could affect results if those who were lost to
follow-up had a different probability of resistance than those not lost.
In 6 of the 11 RCTs with information, <20% were lost to follow-up in
both groups, but the loss was noticeably higher in the isoniazid group
than for controls in 2 studies of HIV-infected persons (34,35).
Publication bias could affect the results if studies finding increased
resistance among persons receiving isoniazid were more likely to be
published. However, the aim of all the studies was to investigate
effectiveness of IPT, not to ascertain development of resistance, and
our analyses suggest that publication bias did not affect the summary
estimate.The methods used to test for isoniazid resistance are now relatively standardized and based on the proportion method in which resistance is defined as growth on medium containing 0.2 [micro]g/mL isoniazid that exceeds 1% of the growth on control medium (36). In older studies, methods were less standardized and were based on absolute numbers of colonies growing on media with various concentrations of antituberculous drugs. In the Greenland study, results for resistance were presented by using 2 divergent di·ver·gent adj. 1. Drawing apart from a common point; diverging. 2. Departing from convention. 3. Differing from another: a divergent opinion. 4. definitions (neither corresponding to modern methods), and these gave quite different estimates of effect. Definition (a) is likely to have led to an overestimation o·ver·es·ti·mate tr.v. o·ver·es·ti·mat·ed, o·ver·es·ti·mat·ing, o·ver·es·ti·mates 1. To estimate too highly. 2. To esteem too greatly. of resistance in both groups; definition (b) is likely to have led to an underestimation of resistance in both groups. When this study was excluded from the analysis, the summary estimate was similar to that using definition (b), which suggests that the estimates using definition (a) were more anomalous a·nom·a·lous adj. 1. Deviating from the normal or common order, form, or rule. 2. Equivocal, as in classification or nature. . Studies using DNA fingerprinting DNA fingerprinting or DNA profiling, any of several similar techniques for analyzing and comparing DNA from separate sources, used especially in law enforcement to identify suspects from hair, blood, semen, or other biological materials found at illustrate that in settings with a high prevalence of TB, newly acquired infection is an important cause of active TB (37,38). Thus, isoniazid-resistant TB may be newly acquired rather than attributable to any previous IPT. However, any such effect should be equally distributed between randomized groups (Table 1). IPT is a safe, low-cost intervention that has the potential to reduce illness and death caused by TB, especially among HIV-infected persons. The main cause of antituberculous drug resistance is inadequate treatment of active TB. Therefore, any risk for a small increase in the incidence of isoniazid resistance attributable to wider use of IPT needs to be weighed against its benefit in reducing TB incidence. If IPT does increase the risk for isoniazid-resistant TB, one might argue that combination regimens should be used. Combination regimens have similar efficacy to isoniazid alone among HIV-infected persons and are shorter, but these regimens generally have more adverse effects (7,39), are more expensive, and risk promoting resistance to rifampin rifampin (rĭfăm`pĭn), antibiotic used in the treatment of tuberculosis. It is also used to eliminate the meningococcus microorganism from carriers and to treat leprosy, or Hansen's disease. . We did not compare the risk for antituberculous drug resistance with IPT versus combination regimens. Our review highlights the paucity pau·ci·ty n. 1. Smallness of number; fewness. 2. Scarcity; dearth: a paucity of natural resources. of available data and does not exclude an increased risk for isoniazid-resistant TB after IPT. IPT substantially reduces the risk for active TB disease in persons whose tuberculin skin test is positive, and we support the expansion of its use, in line with recent recommendations from the HIV/TB working group of the Stop TB partnership (40). If the main reason for the development of resistance among persons receiving IPT is failure to diagnose failure to diagnose, n a failure to assess a patient's condition. Harm may be inflicted by the failure to administer treatment to a potentially treatable condition. active TB, our results underscore The underscore character (_) is often used to make file, field and variable names more readable when blank spaces are not allowed. For example, NOVEL_1A.DOC, FIRST_NAME and Start_Routine. (character) underscore - _, ASCII 95. the need for effective diagnostic strategies and tests. In accordance with WHO policy, ongoing surveillance for isoniazid resistance is required among populations in which this intervention is widely implemented. Acknowledgments We thank Neal Alexander, Tim Clayton, and Laura Rodrigues for valuable discussions concerning methodology. Dr Balcells is an infectious diseases infectious diseases: see communicable diseases. resident at the Pontificia Universidad Cato1ica in Santiago, Chile Santiago, officially Santiago de Chile (Spanish: (helpinfo)), is the capital of Chile, and the center of its largest conurbation (Greater Santiago). . Her research interests include the epidemiology epidemiology, field of medicine concerned with the study of epidemics, outbreaks of disease that affect large numbers of people. Epidemiologists, using sophisticated statistical analyses, field investigations, and complex laboratory techniques, investigate the cause and prevention of HIV infection and TB. She carried out this study as a master's degree master's degree n. An academic degree conferred by a college or university upon those who complete at least one year of prescribed study beyond the bachelor's degree. Noun 1. candidate at the London School of Hygiene and Tropical Medicine tropical medicine, study, diagnosis, treatment, and prevention of certain diseases prevalent in the tropics. The warmth and humidity of the tropics and the often unsanitary conditions under which so many people in those areas live contribute to the development and . References (1.) Corbett EL, Watt C J, Walker N, Maher D, Williams BG, Raviglione MC, et al. The growing burden of tuberculosis: global trends and interactions with the HIV epidemic. Arch Intern intern /in·tern/ (in´tern) a medical graduate serving in a hospital preparatory to being licensed to practice medicine. in·tern or in·terne n. Med. 2003;163:1009-21. (2.) Selwyn PA, Hartel D, Lewis VA, Schoenbaum EE, Vermund SH, Klein RS, et al. A prospective study of the risk of tuberculosis among intravenous drug users with human immunodeficiency virus human immunodeficiency virus n. HIV. Human immunodeficiency virus (HIV) A transmissible retrovirus that causes AIDS in humans. infection. N Engl J Med. 1989;320:545-50. (3.) Daley CL, Small PM, Schecter GF, Schoolnik GK, McAdam RA, Jacobs WR Jr, et al. An outbreak of tuberculosis with accelerated progression among persons infected in·fect tr.v. in·fect·ed, in·fect·ing, in·fects 1. To contaminate with a pathogenic microorganism or agent. 2. To communicate a pathogen or disease to. 3. To invade and produce infection in. with the human immunodeficiency virus. An analysis using restriction-fragment-length polymorphisms. N Engl J Med. 1992;326:231-5. (4.) Di Perri G, Cruciani M, Danzi MC, Luzzati R, De CG, Malena M, et al. Nosocomial nosocomial /noso·co·mi·al/ (nos?o-ko´me-il) pertaining to or originating in a hospital. nos·o·co·mi·al adj. 1. Of or relating to a hospital. 2. epidemic of active tuberculosis among HIV-infected patients. Lancet lancet /lan·cet/ (lan´set) a small, pointed, two-edged surgical knife. lan·cet n. . 1989;2:1502-4. (5.) Mukadi YD, Maher D, Harries A. Tuberculosis case fatality rates case fatality rate n. The proportion of individuals contracting a disease who die of that disease. in high HIV prevalence populations in sub-Saharan Africa. AIDS. 2001;15:143-52. (6.) De Cock cock watchful church-tower sitter. [Christian Symbolism: Appleton, 21] See : Guardianship cock its crowing reminded Peter of his betrayal. [N.T. KM, Chaisson RE. Will DOTS do it? A reappraisal of tuberculosis control in countries with high rates of HIV infection. Int J Tuberc Lung Dis. 1999;3:457-65. (7.) Woldehanna S, Volmink J. Treatment of latent tuberculosis latent tuberculosis Infectious disease Infection with M tuberculosis that has been contained by the host's immune system and thus does not infect others Diagnosis Tuberculin skin test; release of IFN-γ in blood after PPD stimulation. See Tuberculosis. infection in HIV infected persons (Cochrane Review). The Cochrane Library, Issue 3. Chichester (UK): John Wiley John Wiley may refer to:
(8.) World Health Organization Global Tuberculosis Programme, Joint United Nations Programme on HIV/AIDS. Policy statement on preventive therapy against tuberculosis in people living with HIV [cited 2006 Mar 20]. Geneva Geneva, canton and city, Switzerland Geneva (jənē`və), Fr. Genève, canton (1990 pop. 373,019), 109 sq mi (282 sq km), SW Switzerland, surrounding the southwest tip of the Lake of Geneva. : The Organization; 1998. WHO/TB/98.255. Available from http://www.who.int/docstore/gtb/ publications/ TB_HIV_polstmnt/index.html (9.) Ferebee S. Controlled chemoprophylaxis chemoprophylaxis /che·mo·pro·phy·lax·is/ (-pro?fi-lak´sis) prevention of disease by means of a chemotherapeutic agent. che·mo·pro·phy·lax·is n. Disease prevention by use of chemicals or drugs. trials in tuberculosis: a general review. Adv Tuberc Res. 1970;17:28-106. (10.) Smieja MJ, Marchetti CA, Cook DJ, Smaill FM. Isoniazid for preventing tuberculosis in non-HIV infected persons (Cochrane Review). The Cochrane Library, Issue 4. Chichester (UK): John Wiley & Sons; 2003. (11.) Wilkinson D, Squire SB, Garner P. Effect of preventive treatment preventive treatment n. See prophylactic treatment. for tuberculosis in adults infected with HIV: systematic review of randomised Adj. 1. randomised - set up or distributed in a deliberately random way randomized irregular - contrary to rule or accepted order or general practice; "irregular hiring practices" placebo controlled trials. BMJ BMJ n abbr (= British Medical Journal) → vom BMA herausgegebene Zeitschrift . 1998;317:625-9. (12.) Bucher HC, Griffith LE, Guyatt GH, Sudre P, Naef M, Sendi P, et al. Isoniazid prophylaxis prophylaxis (prō'fĭlăk`sĭs), measures designed to prevent the occurrence of disease or its dissemination. Some examples of prophylaxis are immunization against serious diseases such as smallpox or diphtheria; quarantine to confine for tuberculosis in HIV infection: a meta-analysis of randomized controlled trials. AIDS. 1999; 13:501-7. (13.) Sankey SS, Weissfeld LA, Fine MJ, Kapoor WN. An assessment of the use of the continuity correction In probability theory, if a random variable X has a binomial distribution with parameters n and p, i.e., X is distributed as the number of "successes" in n independent Bernoulli trials with probability p for sparse sparse - A sparse matrix (or vector, or array) is one in which most of the elements are zero. If storage space is more important than access speed, it may be preferable to store a sparse matrix as a list of (index, value) pairs or use some kind of hash scheme or associative memory. data in meta-analysis. Commun Stat Simul simul /sim·ul/ (sim´ul) [L.] at the same time as. Comput. 1996;25:1031-56. (14.) DerSimonian R, Laird laird n. Scots The owner of a landed estate. [Scots, from Middle English lard, variant of lord, owner, master; see lord. N. Meta-analysis in clinical trials. Control Clin Trials. 1986;7:177-88. (15.) Gomez JE, McKinney JD. M. tuberculosis M. tuberculosis, n the bacterium responsible for tuberculosis, generally a respiratory infection in man; nonrespiratory tuberculosis is considered an indicator disease for AIDS. See also tuberculosis. persistence, latency (1) The time between initiating a request in the computer and receiving the answer. Data latency may refer to the time between a query and the results arriving at the screen or the time between initiating a transaction that modifies one or more databases and its completion. , and drug tolerance drug tolerance Psychiatry Repeated use of some substance or drug, often narcotics, so that ever larger doses are required to produce the same physiologic and/or psychologic effect obtained previously by a smaller dose. . Tuberculosis. 2004;84:29-44. (16.) David HL. Probability distribution Probability distribution A function that describes all the values a random variable can take and the probability associated with each. Also called a probability function. probability distribution of drug-resistant mutants in unselected populations of Mycobacterium tuberculosis Mycobacterium tuberculosis n. Tubercic bacillus. Mycobacterium tuberculosis . Appl Microbiol. 1970;20:810-4. (17.) Begg CB, Mazumdar M. Operating characteristics of a rank correlation test for publication bias. Biometrics. 1994;50:1088-101. (18.) Ferebee SH, Mount FW. Tuberculosis morbidity morbidity /mor·bid·i·ty/ (mor-bid´it-e) 1. a diseased condition or state. 2. the incidence or prevalence of a disease or of all diseases in a population. mor·bid·i·ty n. in a controlled trial of the prophylactic prophylactic /pro·phy·lac·tic/ (pro?-fi-lak´tik) 1. tending to ward off disease; pertaining to prophylaxis. 2. an agent that tends to ward off disease. pro·phy·lac·tic n. use of isoniazid among household contacts. Am Rev Respir Dis. 1962;85:490-510. (19.) Katz J, Kunofsky S, Damijonaitis V, Lafleur A, Caron T. Effect of isoniazid upon the reactivation reactivation to become active after a period of quiescence or, as in bacterial and viral infections, latency. cross reactivation of inactive in·ac·tive adj. 1. Not active or tending to be active. 2. a. Not functioning or operating; out of use: inactive machinery. b. tuberculosis; final report. Am Rev Respir Dis. 1965;91:345-50. (20.) Horwitz O, Payne PG, Wilbek E. Epidemiological epidemiological emanating from or pertaining to epidemiology. epidemiological associations the associative relationships between the frequency of occurrence of a disease and its determinants, its predisposing and precipitating basis of tuberculosis eradication eradication extermination of an infectious agent so that no further cases of the related disease can occur. virtual eradication . 4. The isoniazid trial in Greenland. Bull World Health Organ. 1966;35:509-26. (21.) Comstock GW, Ferebee SH, Hammes LM. A controlled trial of community-wide isoniazid prophylaxis in Alaska. Am Rev Respir Dis. 1967;95:935-43. (22.) Pamra SP, Mathur GP. Effects of chemoprophylaxis on minimal pulmonary tuberculosis pulmonary tuberculosis n. Tuberculosis of the lungs. pulmonary tuberculosis Infectious disease Infection by Mycobacterium tuberculosis lesions of doubtful activity. Bull World Health Organ. 1971;45:593-602. (23.) Debre R, Perdrizet S, Lotte A, Naveau M, Lert F. Isoniazid chemoprophylaxis of latent primary tuberculosis primary tuberculosis n. Tuberculosis caused by infection with tubercle bacilli and characterized by the formation of a primary complex in the lungs consisting of a small peripheral pulmonary focus and hilar or paratracheal lymph node involvement; it : in five trial centres in France from 1959 to 1969. Int J Epidemiol. 1973;2:153-60. (24.) Grzybowski S, Ashley MJ, Pinkus G. Chemoprophylaxis in inactive tuberculosis: long-term evaluation of a Canadian trial. Can Med Assoc J. 1976;114:607-11. (25.) Krebs A. The IUAT trial on isoniazid preventive treatment in persons with fibrotic Fibrotic Pertaining to or characterized by fibrosis. In dermatological description, "fibrotic" would be used to describe leathery, bound-down, or thickened, scarred skin. Mentioned in: Lymphedema lung lesions. Bull Int Union Tuberc. 1976;51:193-201. (26.) Nolan CM, Aitken ML, Elarth AM, Anderson KM, Miller WT. Active tuberculosis after isoniazid chemoprophylaxis of Southeast Asian refugees. Am Rev Respir Dis. 1986; 133:431-6. (27.) British Medical Research Council. A double-blind placebo-controlled clinical trial of three antituberculosis chemoprophylaxis regimens in patients with silicosis silicosis (sĭlĭkō`sĭs), occupational disease of the lungs caused by inhalation of free silica (quartz) dust over a prolonged period of time. in Hong Kong. Am Rev Respir Dis. 1992;145:36-41. (28.) Pape JW, Jean SS, Ho JL, Hafner A, Johnson WD Jr. Effect of isoniazid prophylaxis on incidence of active tuberculosis and progression of HIV infection. Lancet. 1993;342:268-72. (29.) Guelar A, Gatell JM, Verdejo J, Podzamczer D, Lozano L, Aznar E, et al. A prospective study of the risk of tuberculosis among HIV-infected patients. AIDS. 1993;7:1345-9. (30.) Gordin FM, Matts JP, Miller C, Brown LS, Hafner R, John SL, et al. A controlled trial of isoniazid in persons with anergy anergy /an·er·gy/ (an´er-je) 1. extreme lack of energy. 2. diminished reactivity to one or more specific antigens.aner´gic an·er·gy n. and human immunodeficiency virus infection who are at high risk for tuberculosis. N Engl J Med. 1997;337:315-20. (31.) Hawken MP, Meme HK, Elliott LC, Chakaya JM, Morris JS, Githui WA, et al. Isoniazid preventive therapy for tuberculosis in HIV-1-infected adults: results of a randomized controlled trial. AIDS. 1997;11:875-82. (32.) Moreno S Moreno, city (1991 pop. 287,188), Buenos Aires prov., E Argentina. It is a residential and district administrative center in the Greater Buenos Aires area. The district was the scene of several major battles during the Argentine War of Independence and the , Miralles P, Diaz MD, Baraia J, Padilla B, Berenguer J, et al. Isoniazid preventive therapy in human immunodeficiency immunodeficiency Defect in immunity that impairs the body's ability to resist infection. The immune system may fail to function for many reasons. Immune disorders caused by a genetic defect are usually evident early in life. virus-infected persons. Long-term effect on development of tuberculosis and survival. Arch Intern Med. 1997;157:1729-34. (33.) Mwinga A, Hosp M, Godfrey-Faussett P, Quigley M, Mwaba P, Mugala BN, et al. Twice weekly tuberculosis preventive therapy in HIV infection in Zambia. AIDS. 1998;12:2447-57. (34.) Johnson JL, Okwera A, Hom DL, Mayanja H, Kityo CM, Nsubuga P, et al. Duration of efficacy of treatment of latent tuberculosis infection in HIV-infected adults. AIDS. 2001;15:2137-47. (35.) Rivero A, Lopez-Cortes L, Castillo R, Lozano F, Garcia MA, Diez F, et al. Randomized trial of three regimens to prevent tuberculosis in HIV-infected patients with anergy [in Spanish]. Enferm Infect infect /in·fect/ (in-fekt´) 1. to invade and produce infection in. 2. to transmit a pathogen or disease to. in·fect v. 1. Microbiol Clin. 2003;21:287-92. (36.) Rieder HL, Chonde MT, Myking H, Urbaniczik R, Laszlo A, Kim SJ, et al. The public health service national tuberculosis reference laboratory and the national laboratory network: minimum requirements, role and operation in a low-income country. Paris: International Union against Tuberculosis and Lung Disease lung disease Pulmonary disease Pulmonology Any condition causing or indicating impaired lung function Types of LD Obstructive lung disease–↓ in air flow caused by a narrowing or blockage of airways–eg, asthma, emphysema, chronic bronchitis; ; 1998. (37.) Sonnenberg P, Murray J, Glynn JR, Shearer S, Kambashi B, Godfrey-Faussett P. HIV-1 and recurrence recurrence /re·cur·rence/ (-ker´ens) the return of symptoms after a remission.recur´rent re·cur·rence n. 1. , relapse and reinfection reinfection /re·in·fec·tion/ (-in-fek´shun) a second infection by the same agent or a second infection of an organ with a different agent. re·in·fec·tion n. of tuberculosis after cure: a cohort study in South African mineworkers. Lancet. 2001;358:1687-93. (38.) van Rie A, Warren R, Richardson M, Victor TC, Gie RP, Enarson DA, et al. Exogenous Exogenous Describes facts outside the control of the firm. Converse of endogenous. reinfection as a cause of recurrent tuberculosis after curative curative /cur·a·tive/ (kur´ah-tiv) tending to overcome disease and promote recovery. cu·ra·tive adj. 1. Serving or tending to cure. 2. treatment. N Engl J Med. 1999;341:1174-9. (39.) Centers for Disease Control and Prevention Centers for Disease Control and Prevention (CDC), agency of the U.S. Public Health Service since 1973, with headquarters in Atlanta; it was established in 1946 as the Communicable Disease Center. . Update: adverse event data and revised American Thoracic thoracic /tho·rac·ic/ (thah-ras´ik) pectoral; pertaining to the thorax (chest). tho·rac·ic adj. Of, relating to, or situated in or near the thorax. Society/CDC recommendations against the use of rifampin and pyrazinamide for treatment of latent tuberculosis infection--United States, 2003. MMWR MMWR Morbidity & Mortality Weekly Report Epidemiology A news bulletin published by the CDC, which provides epidemiologic data–eg, statistics on the incidence of AIDS, rabies, rubella, STDs and other communicable diseases, causes of mortality–eg, Morb Mortal mortal /mor·tal/ (mor´t'l) 1. subject to death, or destined to die. 2. fatal. mor·tal adj. 1. Liable or subject to death. 2. Wkly Rep. 2003;52:735-9. (40.) World Health Organization. Interim policy on collaborative TB/HIV activities. Geneva: The Organization; 2004. WHO/HTM/TB/ 2004.330. Available at http://www.who.int/hiv/pub/tb/tbhiv/en/ index.html Address for correspondence: Alison D. Grant, Clinical Research Unit, Department of Infectious and Tropical Diseases Tropical diseases are infectious diseases that either occur uniquely in tropical and subtropical regions (which is rare) or, more commonly, are either more widespread in the tropics or more difficult to prevent or control. , London School of Hygiene and Tropical Medicine, Keppel St, London WC1E 7HT, UK; email: alison.grant@lshtm.ac.uk Maria Elvira Balcells, * (1) Sara L. Thomas, * Peter Godfrey-Faussett, * and Alison D. Grant * * London School of Hygiene and Tropical Medicine, London, United Kingdom (1) Current affiliation: Pontificia Universidad Catolica de Chile, Santiago, Chile
Table 1. Assumptions underlying the anaylsis
Assumption Comment
When a sample of Additional variation incurred by
culture positive isolates sampling tuberculosis (TB) cases for
underwent resistance resistance was incorporated into 95%
testing, this was a random confidence interval estimates and
sample of all cases, thus the weighting of studies in
meta-analyses. Differential
ascertainment of resistance is
unlikely because most of included
studies were double-blinded and
(for studies in which information was
available) similar proportions of
culture-positive TB cases from each
group were tested.
Latent infection with 12 of 13 studies were comparisons
isoniazid-resistant TB was of randomized groups; any latent
equally distributed between infection with a resistant organism
comparison groups. would likely be equally distributed
between comparison groups. Any
imbalance due to random error
would be bidirectional
and so would result in summary
estimate of relative risk tending
towards 1 (i.e., being underestimated).
Risk for isoniazid- Similarly, any new infection with an
resistant TB resulting from isoniazid-resistant organism would
recent infection was likely be equally distributed between
equally distributed between randomized groups. Any imbalance
comparison groups. would similarly result in summary
estimate of relative risk being
underestimated.
Table 2. Studies comparing isoniazid treatment with no treatment
in HIV-uninfected populations *.
Author, Intervention/ Enrolled (n)
country, comparison; INH/
dates Population blinding control
Ferebee, Household 12 mo INH 4-7 7,755/7,996
USA, 1957- contacts of mg/kg/day/placebo;
NS (18) TB patients double blind
Katz, USA, Mental 2 y INH, 300 mg 118/107
1958-1964 hospital daily/no treatment;
(19) patients not blind
with
inactive
lesions
Horwitz, 76 villages 2 X 13 wk INH, 400 4,174/3,907
Greenland, mg twice weekly/0.1
1956-1963 mg INH; double
(20) blind
Comstock, Residents 12 mo INH, 3,047/3,017
USA of 28 300 mg [section]
(Alaska), villages daily/placebo;
1957-1964 and 2 double blind
(21) boarding
schools
Ferebee, Persons 12 mo INH, 701/714
USA, 1960- with 5 mg/kg/day/
1967 inactive placebo; NS
lesions
Pamra, X-ray 12 mo INH, 139/178
India, screening 3-4 mg/kg/day/
1958-1968 attendees placebo; NS
(22) with
inactive TB
Hong Kong Men with 24 wk INH, 300 mg 167/159
Chest silicosis daily/placebo;
Service, double blind
Hong Kong,
1981-1987
(27)
TB cases:
culture
positive/
total (%)
Author, Controls
country,
dates INH Controls
Ferebee, NS/86 NS/215
USA, 1957-
NS (18)
Katz, USA, N S/9 NS/10
1958-1964
(19)
Horwitz, 123/238 186/323
Greenland, -51.70 -57.60
1956-1963
(20)
Comstock, NS/58 NS/141
USA
(Alaska),
1957-1964
(21)
Ferebee, NS/18 NS/49
USA, 1960-
1967
Pamra, 10/18 57/76
India, (55.6) (75)
1958-1968
(22)
Hong Kong 19/25 29/36
Chest (76) (80.6)
Service,
Hong Kong,
1981-1987
(27)
Resistant
cases/total
tested (%
culture
positive
Author, tested)
country,
dates INH Controls
Ferebee, 2/10 2/31
USA, 1957- NS NS
NS (18)
Katz, USA, 1/1 2/5
1958-1964 NS NS
(19)
Horwitz, (a) 2/461 (a) 5/661
Greenland,
1956-1963 (b) 2/46 (b) 1/66
(20) (37) (36)
([double ([double
dagger]) dagger])
Comstock, 4/20 1/50
USA NS NS
(Alaska),
1957-1964
(21)
Ferebee, 2/5 2/25
USA, 1960- NS NS
1967
Pamra, 3/9 6/52
India, (90) (91)
1958-1968
(22)
Hong Kong 5/19 4/28
Chest (100) (97)
Service,
Hong Kong,
1981-1987
(27)
Risk for
resistant
Author, TB/1,000 RR
country, (95%
dates INH Controls CI)
Ferebee, 2.22 1.73 1.28
USA, 1957- (0.20-
NS (18) 8.07)
Katz, USA, 76.27 37.38 2.04
1958-1964 (0.52-
(19) 8.08)
Horwitz, (a) 2.481 (a) 6.261 (a) 0.40
Greenland, (0.08-
1956-1963 1.97)
(20) ([dagger])
(b) 2.48 (b) 1.25 (b) 1.98
([double ([double (0.18-
dagger]) dagger]) 21.31)
([double
dagger])
Comstock, 3.81 0.93 4.07
USA (0.47-
(Alaska), 34.98)
1957-1964
(21)
Ferebee, 10.27 5.49 1.87
USA, 1960- (0.31-
1967 11.19)
Pamra, 43.17 49.27 0.88
India, (0.24-
1958-1968 3.15)
(22)
Hong Kong 39.39 32.35 1.22
Chest (0.34-
Service, 4.32)
Hong Kong,
1981-1987
(27)
* INH, isoniazid; TB, tuberculosis; RR, relative risk;
CI, confidence interval; NS, not stated; med., median;
Rx, reatment. Because of space limitations,
some data have been removed; see online version
for complete table.
([dagger]) (a), definition of resistance as [greater than
or equal to] 1 colony growth at [greater than
or equal to] 0.32 wg/mL INH.
([double dagger]) (b), definition of resistance as growth
equal to control tube at [greater than or
equal to] 0.32 pg/mL INH.
([section]) Children were given
5 mg/kg/day INH.
Table 3. Studies comparing isoniazid treatment with no
treatment in HIV-infected populations *
Author, Intervention/ Enrolled
country, comparison; (n)
dates Population blinding INH/control
Randomized
controlled
trials
Gordin, USA, Clinic 6 mo INH 300 mg 260/257
1991-1996 attendees; daily vs. placebo;
(30) med. CD4 double blind
233/247
Hawken, Clinic or VCT 6 mo INH 300 mg 342/342
Kenya, 1992- attendees; daily/placebo;
1997 (31) med. CD4 double blind
321.5/346
Mwinga, VCT 6 mo INH 900 mg 350/352
Zambia, 1992- attendees twice
1996 (33) weekly/placebo;
double blind
Johnson, Clinic or 6 mo INH 300 mg 931/787
Uganda, counseling daily/placebo;
1993-NS (34) attendees partially double
blind ([double
dagger])
Rivero, Spain, Clinic 6 mo INH 300 mg 82/77
1994-2000 attendees; daily/no treatment,
(35) med. CD4 not blind
193/215
Cohort study
Moreno, Clinic 9-12 mo INH (dose 29/92
Spain, 1985- attendees; NS)/no treatment;
1994 (32) med. CD4 not blind
689/648
TB cases;
culture
positive/
Author, total (%)
country,
dates INH Controls
Randomized
controlled
trials
Gordin, USA, NS/3 NS/6
1991-1996
(30)
Hawken, 19/25 22/23
Kenya, 1992- (76) (95.7)
1997 (31)
Mwinga, NS/27 NS/44
Zambia, 1992-
1996 (33)
Johnson, 36/51 46/64
Uganda, (70.6) (71.9)
1993-NS (34)
Rivero, Spain, 3/3 4/4
1994-2000 (100) (100)
(35)
Cohort study
Moreno, 3/3 39/43
Spain, 1985- (100) (90.7)
1994 (32)
Resistant
cases/total
tested (%
culture
positive
Author, tested)
country,
dates INH Controls
Randomized
controlled
trials
Gordin, USA, 0/3 0/5
1991-1996 (NS) (NS)
(30)
Hawken, 2/17 0/21
Kenya, 1992- (90) (96)
1997 (31)
Mwinga, 0/3 1/5
Zambia, 1992- (NS) (NS)
1996 (33)
Johnson, 5/20 1/24
Uganda, (56) (52)
1993-NS (34)
Rivero, Spain, 3/3 4/4
1994-2000 (100) (100)
(35)
Cohort study
Moreno, 2/2 0/12
Spain, 1985- (67) (31)
1994 (32)
Risk for
resistant
Author, TB/1,000
country,
dates INH Controls RR (95% CI)
Randomized
controlled
trials
Gordin, USA, 1.921 1.94 0.99 (0.06-
1991-1996 ([dagger]) 6,298.19)
(30)
Hawken, 10.051 1.46 6.88 (0.01-
Kenya, 1992- ([dagger]) 3,882.85)
1997 (31)
Mwinga, 1.431 26.38 0.05 (0.00-
Zambia, 1992- ([dagger]) 30.47)
1996 (33)
Johnson, 13.69 3.39 4.04(0.50-
Uganda, 32.80)
1993-NS (34)
Rivero, Spain, 36.59 51.95 0.70 (0.16-
1994-2000 3.05)
(35)
Cohort study
Moreno, 118.64 5.41 21.95
Spain, 1985- ([dagger]) ([dagger]) (0.04-
1994 (32) 11,582.31)
* INH, isoniazid; TB, tuberculosis; RR, relative risk; CI,
confidence interval; med., median; NS, not stated; Rx,
treatment; VCT, voluntary counseling and testing; PPD, purified
protein derivative. Because of space limitations, some data
have been removed; see online version for complete table.
([dagger]) Calculated by adding 0.5 to numerator and
denominator of both groups.
([double dagger]) Unclear whether isoniazid and placebo
group received the same number of tablets.
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