Antiretroviral therapy during tuberculosis treatment and marked reduction in death rate of HIV-infected patients, Thailand (1).Antiretroviral antiretroviral /an·ti·ret·ro·vi·ral/ (-ret´ro-vi?ral) effective against retroviruses, or an agent with this quality. an·ti·ret·ro·vi·ral adj. therapy (ART) is lifesaving in patients with advanced 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. infection, but the magnitude of benefit in HIV-infected patients receiving tuberculosis (TB) treatment remains uncertain, and population-based data from developing countries are limited. We prospectively collected data about HIV-infected TB patients from February 2003 through January 2004 in Ubon-ratchathani, Thailand. During 12 months, HIV was diagnosed in 329 (14%) of 2,342 patients registered for TB treatment. Of patients with known outcomes, death during TB treatment occurred in 5 (7%) of 71 who received ART and 94 (43%) of 219 who did not. Using multivariate analysis multivariate analysis, n a statistical approach used to evaluate multiple variables. multivariate analysis, n a set of techniques used when variation in several variables has to be studied simultaneously. , we found a large reduction in the odds of death for patients receiving ART before or during TB treatment (odds ratio, 0.2; 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%. , 0.1-0.5), adjusting for CD4 count CD4 count n. A measure of the number of helper T cells per cubic millimeter of blood, used to analyze the prognosis of patients infected with HIV. , smear smear (smer) a specimen for microscopic study prepared by spreading the material across the slide. Pap smear , Papanicolaou smear see under test. status, co-trimoxazole use, and treatment facility. ART is associated with a substantial reduction in deaths during TB treatment for HIV-infected TB patients in Thailand. ********** Tuberculosis (TB) is one of the most common opportunistic infections Opportunistic infections Infections that cause a disease only when the host's immune system is impaired. The classic opportunistic infection never leads to disease in the normal host. and causes of death in HIV-infected persons (1). In developing countries, many HIV-infected persons frequently receive the diagnosis of HIV infection or AIDS after first having TB diagnosed at a health facility (1). The proportion of HIV-infected TB patients who die during TB treatment is high: an estimated 6%-39% die during TB treatment in sub-Saharan Africa (2,3). Deaths occurring in the first few months after TB diagnosis are more likely TB related, whereas deaths occurring later are more likely to be attributable to other HIV-related illnesses (4-7). Thailand has experienced a severe TB/HIV syndemic, i.e., 2 diseases acting synergistically syn·er·gis·tic adj. 1. Of or relating to synergy: a synergistic effect. 2. Producing or capable of producing synergy: synergistic drugs. 3. to cause excess illness and death (8). Almost 600,000 persons are currently HIV 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. , and >90,000 TB cases are estimated to occur annually (2,9). One fourth of persons in whom AIDS was diagnosed first have TB, and an estimated 12% of TB cases in Thailand are HIV associated, although the proportion is as high as 40% in some provinces (10). Antitretroviral therapy (ART), which uses highly active combinations of drugs, improves survival in HIV-infected persons (11,12). HIV-infected persons in Thailand now have widespread access to ART, but physicians often do not prescribe it to HIV-infected TB patients because of concerns about drug-drug interactions, overlapping toxicities, immune reconstitution syndrome, and pill burden Pill burden is a term that refers to the number of tablets, capsules or other dosage forms that a patient takes on a regular schedule. Higher pill burden decreases compliance with drug therapy, due to the need to take a large quantity of pills on a regular basis. . Expert groups and the World Health Organization (WHO) also recommend that public health programs make treatment of TB the first priority and ideally begin ART after TB treatment is tolerated and CD[4.sup.+] T-lymphocyte (CD4) count is measured (13). Several studies have now documented that ART reduces the likelihood of death during TB treatment of HIV-infected TB patients, but these studies relied on retrospective data collection, occurred outside routine public health programs, or involved resource-rich countries without large TB or HIV epidemics (14-18). In this study, we analyzed data from a prospective, population-based surveillance system to estimate the benefit of ART on reducing mortality during TB treatment in HIV-infected TB patients living in rural Thailand. Methods Setting Ubon-ratchathani is a large, predominantly rural province in northeastern Thailand with a population of 1.7 million persons. The rate of reported TB cases is 145/100,000 persons, and HIV prevalence in women attending public antenatal clinics antenatal clinic n → clínica prenatal antenatal clinic n → service m de consultation prénatale antenatal clinic antenatal n was 0.6% (in 2004). Treatment of TB or HIV is offered by 25 health facilities, including 20 Ministry of Public Health (MOPH MOPH Ministry of Public Health MOPH Military Order of the Purple Heart ) hospitals, 3 private hospitals, 1 military hospital, and 1 MOPH outpatient TB and HIV referral clinic. Except for those who are seriously ill A patient is seriously ill when his or her illness is of such severity that there is cause for immediate concern but there is no imminent danger to life. See also very seriously ill. , TB and HIV patients are managed in outpatient specialty clinics at these facilities. Data Collection In 2003, the US 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. (CDC See Control Data, century date change and Back Orifice. CDC - Control Data Corporation ) began collaborating with the MOPH and Ubon-ratchathani Province on a special project to enhance surveillance, monitoring, evaluation, and treatment of TB, HIV-associated TB, and multidrug-resistant TB (MDR MDR, n See multidrug resistance. MDR, n the abbreviation for minimum daily requirement, specifically the Minimum Daily Requirements for Specific Nutrients compiled by the United States Food and Drug Administration. TB) in a project known as the Thailand TB Active Surveillance Network. For all patients with a diagnosis of TB in any of the 25 participating healthcare facilities, public health staff recorded standardized standardized pertaining to data that have been submitted to standardization procedures. standardized morbidity rate see morbidity rate. standardized mortality rate see mortality rate. epidemiologic data, collected sputum sputum /spu·tum/ (spu´tum) [L.] expectoration; matter ejected from the trachea, bronchi, and lungs through the mouth. sputum cruen´tum bloody sputum. specimens for laboratory testing (including staining for acid-fast bacilli bacilli /ba·cil·li/ (bah-sil´i) plural of bacillus. bacilli see bacillus. [AFB AFB abbr. acid-fast bacillus AFB Acid-fast bacillus, also 1. Aflatoxin B 2. Aorto-femoral bypass ], mycobacterial mycobacterial emanating from or pertaining to mycobacterium. mycobacterial granuloma may be caused by Mycobacterium tuberculosis (see cutaneous tuberculosis), M. culture, species identification, and drug-susceptibility testing), and offered HIV counseling and testing. Sputum specimens were collected for AFB staining and culture at the beginning of TB treatment. Specimens were cultured at an MOPH laboratory in the province on Ogawa (February-March 2003) or Lowenstein-Jensen agar (April 2003-January 2004) by using standard methods, and isolates were sent to the MOPH national reference laboratory for drug-susceptibility testing. Public health staff from the TB program collected patient data prospectively from routine medical and laboratory records, recorded data in a modified version of the standard national TB register, and entered data into an electronic database. Patient Population All persons registered for TB treatment, regardless of their final diagnosis, were considered TB patients, consistent with WHO guidelines (19). We restricted our analysis to TB patients who had laboratory confirmation of HIV infection and who were registered for TB treatment from February 2003 through January 2004. Patient outcomes were only recorded through the end of TB treatment, which was usually 6 months after treatment initiation; no data about outcomes were recorded after the end of TB treatment. For TB treatment, patients received standardized regimens, consistent with WHO guidelines; new (not previously treated) patients received 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. , 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. , ethambutol ethambutol /etham·bu·tol/ (e-tham´bu-tol) an antibacterial, specifically effective against Mycobacterium; used with one or more other antituberculous drugs in the treatment of pulmonary tuberculosis, administered as the , and pyrazinamide (18). HIV-infected TB patients were referred to HIV-related care and treatment, but individual physicians used their own clinical judgment about measuring CD4 count, providing opportunistic infection opportunistic infection n. An infection by a microorganism that normally does not cause disease but becomes pathogenic when the body's immune system is impaired and unable to fight off infection, as in AIDS and certain other diseases. 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 or ART, and managing other clinical conditions. When measured, CD4 counts were usually checked within the first month of TB treatment. Thai MOPH guidelines recommend that HIV-infected patients with CD4 <200 cells/[mm.sup.3] receive co-trimoxazole and stavudine, lamivudine, and nevirapine nevirapine /ne·vir·a·pine/ (ne-vir´ah-pen) a nonnucleoside inhibitor of HIV-1reverse transcriptase, used in combination with other antiretroviral agents in the treatment of HIV infection. (known as "GPO-vir"); in patients with TB, efavirenz efavirenz /ef·a·vi·renz/ (ef´ah-vi?renz) an antiretroviral, inhibiting reverse transcriptase; used in the treatment of HIV infection. e·fa·vir·enz n. is recommended instead of nevirapine. Definitions Standard WHO definitions were used to categorize cat·e·go·rize tr.v. cat·e·go·rized, cat·e·go·riz·ing, cat·e·go·riz·es To put into a category or categories; classify. cat patients according to according to prep. 1. As stated or indicated by; on the authority of: according to historians. 2. In keeping with: according to instructions. 3. previous TB treatment history, type of TB (sputum smear Noun 1. sputum smear - any of several cytologic smears obtained from different parts of the lower respiratory tract; used for cytologic study of cancer and other diseases of the lungs bronchoscopic smear, lower respiratory tract smear positive, pulmonary; sputum smear-negative, pulmonary; extrapulmonary), and treatment outcome. Consistent with WHO guidelines, we classified all deaths occurring during TB treatment, whether the cause was known or not, as a TB death (18). We classified ART use according to whether ART was begun before TB treatment, begun during TB treatment, or not taken during TB treatment. We classified co-trimoxazole use as either taken or not taken during TB treatment. No data on interruptions of ART or co-trimoxazole treatment were collected; for the purposes of surveillance, any patient already taking or started on ART or co-trimoxazole was considered to be taking it throughout TB treatment. We stratified stratified /strat·i·fied/ (strat´i-fid) formed or arranged in layers. strat·i·fied adj. Arranged in the form of layers or strata. CD4 count (cells/[mm.sup.3]) as <50, 50-99, 100199, and [greater than or equal to] 200. Data Analysis For descriptive analysis, all patients were included. For univariate and multivariate analysis of risk factors for death, we restricted our analysis to TB patients with an outcome of cured, completed, failed, or died; we excluded patients who defaulted on treatment or transferred out, because their final treatment outcome was not known. Patients with an outcome of failure were combined with those who were cured or completed treatment, since all 3 groups were known to have survived the first 6 months of TB treatment. We calculated relative risk (RR) for factors associated with death in patients with all forms of TB and in the subset of patients with pulmonary, sputum smear--positive TB. For multivariate analysis, we calculated adjusted odds ratios (OR) for factors associated with death by using logistic regression In statistics, logistic regression is a regression model for binomially distributed response/dependent variables. It is useful for modeling the probability of an event occurring as a function of other factors. . Variables were chosen based on [greater than or equal to] 1 of the following: statistical significance (p<0.05) in univariate analysis, biologic plausibility, or previously published evidence. Because 41% of patients had data missing for CD4 count, we performed several analyses to explore the impact of missing CD4 count on our final model estimates, including the following: 1) classifying patients with unknown CD4 as a separate strata in analysis; 2) recoding Noun 1. recoding - converting from one code to another coding, steganography, cryptography, secret writing - act of writing in code or cipher patients with unknown CD4 as having CD4 <50 cells/[mm.sup.3]; 3) recoding patients with unknown CD4 as CD4 >200 cells/[mm.sup.3]; and 4) excluding all patients with unknown CD4 from the analysis. Because rates of default were high and cases of default may actually be deaths, we also recoded cases of default as death and repeated all multivariate The use of multiple variables in a forecasting model. analyses. In analyses for which there were no outcomes in some CD4 strata, we log-transformed the CD4 count and modeled it as a continuous variable (20). The protocol for this project was reviewed by the Thailand MOPH and CDC and the study was found to be surveillance and public health program implementation and not human subjects research requiring oversight by an institutional review board. Results From February 2003 through January 2004, 2,342 patients were registered for TB treatment in Ubon-ratchathani Province. Of these, 225 (10%) were known to be HIV infected before their TB diagnosis. Of the remaining 2,117 patients, 1,626 (77%) received HIV pretest pre·test n. 1. a. A preliminary test administered to determine a student's baseline knowledge or preparedness for an educational experience or course of study. b. A test taken for practice. 2. counseling, 680/1,626 (42%) agreed to HIV testing HIV test Various tests have been used to detect HIV and production of antibodies thereto; some HTs shown below are no longer actively used, but are listed for completeness and context. See HIV, Immunoblot. , and 104/680 (15%) were found to be HIV infected. In all, 329 (14%) of the 2,342 total TB patients were either known to be HIV infected before TB diagnosis (225; 68% of all TB/HIV patients) or were identified as HIV infected after testing through the TB program (104; 32% of all TB/HIV patients). The median age of the 329 HIV-infected TB patients was 32 years (range 10 months-68 years), 112 (34%) were female, and 307 (93%) had new TB cases (Table 1). TB was classified as sputum smear--positive in 120 (36%), sputum smear--negative in 107 (33%), and extrapulmonary in 102 (31%). CD4 count was unavailable or not performed in 134 (41%). Of the 195 patients with CD4 results available, the median CD4 count was 53 cells/[mm.sup.3] (range 1-873); 93% had CD4 <200 cells/[mm.sup.3]. Sputum cultures Sputum Culture Definition Sputum is material coughed up from the lungs and expectorated (spit out) through the mouth. A sputum culture is done to find and identify the microorganism causing an infection of the lower respiratory tract such as pneumonia were performed in 145 (64%) of 227 patients with pulmonary TB pulmonary TB Pulmonary tuberculosis, see there , including 93 (78%) of 120 with sputum smear-positive TB and 52 (49%) of 107 with sputum smear--negative TB (Table 2). Of the 93 patients whose sputum smears were positive and who had a culture performed, 65 (70%) grew Mycobacterium tuberculosis Mycobacterium tuberculosis n. Tubercic bacillus. Mycobacterium tuberculosis (MTB MTB Mountain Bike MTB Mycobacterium Tuberculosis MTB Marshall Tucker Band MTB Motor Torpedo Boat MTB Making The Band (TV show) MTB Minus The Bear (band) MTB Mozilla Thunderbird ); of these, 4 (6%) isolates were resistant to at least isoniazid and rifampin, i.e., MDR TB. Of the 52 sputum smear-negative patients with a culture performed, only 3 (6%) were culture positive, and none exhibited MDR TB. Before TB treatment, 30 (9%) patients were receiving ART; an additional 45 (14%) patients began ART during TB treatment; and the remaining 254 (77%) patients did not receive ART before or during TB treatment. In 40 of the 45 patients who began ART during TB treatment and in whom a date of starting ART was available, the median time between TB diagnosis and ART initiation was 93 days (range 0-170 days). Among all patients receiving ART, 38 (51%) received a combination regimen of stavudine, lamivudine, and nevirapine; 35 (47%) received efavirenz instead of nevirapine; and 2 (2%) were on other regimens. During TB treatment, 225 (68%) received co-trimoxazole. Of all 329 patients, 187 (57%) were cured or completed TB treatment; 99 (30%) died during TB treatment. In the remaining 43 patients, treatment failed (for 4 patients) or the patient defaulted (a WHO term defined as missing at least 2 continuous months of treatment) (31 patients), transferred out (4 patients), or received a final diagnosis other than TB (4 patients). Of the 4 patients with MDR TB, 3 died and 1 was recorded as having failed treatment with final outcome not recorded. In univariate analysis restricted to the 290 patients with an outcome of cured, completed treatment, failed treatment, or died, we analyzed several factors associated with death during TB treatment. For all TB patients, having an unknown CD4 count was associated with increased likelihood of death, and receiving co-trimoxazole or ART was associated with reduced mortality (Table 3). For ART, 5 (7%) of 71 patients who received ART died compared with 94 (43%) of 219 patients who did not receive ART (RR 0.2; 95% confidence interval [CI] 0.1-0.4; absolute risk reduction 36; number-needed-to-treat 2.8). For sputum smear-positive TB patients, results were similar; additionally, male patients were at higher risk for death than female patients (RR 2.3, 95% CI 1.1-4.7). In multivariate analysis adjusted for CD4 count, smear status, hospital providing treatment, and co-trimoxazole use, ART remained strongly associated with reduced mortality during TB treatment (Table 4). The adjusted OR (aOR) for death in patients who received ART before or during TB treatment was 0.2 (95% CI 0.1-0.5) compared with that in patients who did not receive ART. Receiving co-trimoxazole was no longer significantly associated with reduced mortality. We found virtually identical results when we did the following: 1) restricted our analysis to only those patients who received ART during TB treatment compared with patients who did not receive ART during TB treatment; 2) restricted our analysis to previously untreated, non-MDR patients without nontuberculous mycobacteria Nontuberculous mycobacteria (NTM), or atypical mycobacteria or mycobacteria other than tuberculosis (MOTT), are mycobacteria which do not cause tuberculosis or Hansen's disease (leprosy). ; 3) coded patients with unknown CD4 as having CD4 >200 cells/[mm.sup.3], as having CD4 <50 cells/[mm.sup.3], or as missing (i.e., removed from the analysis). All analyses also produced essentially identical results when we reclassified cases of default as death. When we restricted our analysis to sputum smear-positive patients, we found a similarly strong beneficial effect for ART. Because no deaths occurred in the group of smear-positive patients with CD4 >200 cells/[mm.sup.3], we modeled CD4 as a continuous variable. The aOR was 0.1 (95% CI 0.0-0.9). Results were similar when we recoded patients with unknown CD4 count as having CD4 equal to 50 cells/[mm.sup.3] (indicative of profound 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. and imminent risk of death) or 250 cells/[mm.sup.3] (not eligible for antiretroviral treatment in many country guidelines because they are relatively immune competent). Because of small sample size, we were only able to perform univariate, not multivariate, analysis for the 57 culture-positive patients who had an outcome of cured, completed, failed, or died. One (8%) of 13 culture-positive patients receiving ART died compared with 17 (36%) of 47 culture-positive patients not receiving ART (RR 0.2, 95% CI 0.0-1.5; absolute risk reduction 28; number-needed-to-treat 3.6). Because patients who died soon after TB diagnosis were also unlikely to have begun ART, we modeled the effect of ART after excluding 32 patients who died in the first month of beginning TB treatment (aOR 0.1, 95% CI 0.0-0.8) and the additional 16 patients who died in the second month (aOR 0.1, 95% CI 0.0-1.2). Results were similar when we recoded patients with unknown CD4 count as having CD4 equal to 50 cells/[mm.sup.3] or 250 cells/[mm.sup.3], except that the effect of ART was now statistically significant for the analysis excluding deaths within the first and second months (aOR 0.1, 95% CI 0.0-0.7 for unknown CD4 recoded as 50 cells/[mm.sup.3]; aOR 0.1; 95% CI 0.0-0.9 for unknown CD4 recoded as 250 cells/[mm.sup.3]). We explored the effect of co-trimoxazole on mortality for the 218 patients who did not receive ART: 52 (38%) of 137 patients receiving co-trimoxazole died compared with 42 (51%) of 82 patients not receiving co-trimoxazole (RR 0.7, CI 0.6-1.0; absolute risk reduction 13; number-needed-to-treat 7.7). The association between co-trimoxazole and survival was not statistically significant when we excluded patients who died in the first month (RR 0.9, CI 0.5-1.5) or in the first 2 months (RR 1.2, CI 0.5-3.0) and when we limited the analysis to smear-positive patients (RR 0.8, CI 0.5-1.3). In multivariate analysis of patients who did not receive ART and adjusting for CD4 count, smear status, and hospital providing treatment, co-trimoxazole was not associated with survival (aOR 0.9, CI 0.5-1.9). Discussion In this prospective, population-based study from a rural province in northeastern Thailand, we documented a high rate of death in HIV-infected TB patients and a substantial reduction in the risk for death during TB treatment for patients receiving ART. In this population, TB occurred predominantly in persons with preexisting pre·ex·ist or pre-ex·ist v. pre·ex·ist·ed, pre·ex·ist·ing, pre·ex·ists v.tr. To exist before (something); precede: Dinosaurs preexisted humans. v.intr. HIV diagnoses and low CD4 counts, and, as expected, the CD4 count was inversely related to death. These findings are more consistent with the epidemiology of TB in high-income countries, such as the United States United States, officially United States of America, republic (2005 est. pop. 295,734,000), 3,539,227 sq mi (9,166,598 sq km), North America. The United States is the world's third largest country in population and the fourth largest country in area. , than that in sub-Saharan Africa, where studies have found that most TB and HIV have not previously been diagnosed in patients with HIV infection and that TB occurs across a broad spectrum of immune suppression (21-26). Although CD4 counts were not recorded for many patients in this study, we can infer from the high mortality in these patients that their CD4 counts were probably low. Research would be needed to document whether data from this evaluation are representative of other settings in Thailand or Southeast Asia Southeast Asia, region of Asia (1990 est. pop. 442,500,000), c.1,740,000 sq mi (4,506,600 sq km), bounded roughly by the Indian subcontinent on the west, China on the north, and the Pacific Ocean on the east. . That TB occurred predominantly in persons with advanced, diagnosed HIV infection suggests that interventions targeted specifically at HIV-infected patients--such as early ART, treatment of latent TB infection, and earlier screening for and treatment of TB disease in household contacts of TB patients and during routine HIV care--are also needed to reduce incidence and mortality of HIV-associated TB. Given the advanced immune suppression in this population, that ART improved survival during TB treatment is not surprising. The magnitude of benefit, however, was substantial. Treating 3 HIV-infected TB patients with ART in this population would translate into 1 life saved during TB treatment. In fact, co-trimoxazole, which is known to save lives during TB treatment in Africa (27), was not significantly associated with survival after adjusting for ART use. Co-trimoxazole protects AIDS patients against a wide range of infections that commonly occur in Thailand, including Pneumocystis Pneumocystis /Pneu·mo·cys·tis/ (-sis´tis) a genus of yeastlike fungi. P. cari´nii is the causative agent of interstitial plasma cell pneumonia. pneu·mo·cys·tis n. jirovecii and Toxoplasma Toxoplasma /Toxo·plas·ma/ (tok?so-plaz´mah) a genus of sporozoa that are intracellular parasites of many organs and tissues of birds and mammals, including humans. T. gon´dii is the etiologic agent of toxoplasmosis. sp. (28). We were not able to demonstrate a survival benefit of co-trimoxazole in patients receiving ART or those not receiving ART. We do not know whether this is a true phenomenon or attributable to bias, misclassification, or small sample size. Further studies are needed to evaluate the survival benefit of co-trimoxazole in HIV-infected TB patients in Thailand. Our sample size was too small to compare outcomes between patients receiving regimens with efavirenz versus nevirapine or to compare outcomes between patients who received ART during the first 2 months of TB treatment compared with those who received ART later. Our evaluation reinforces the importance of providing TB patients with early access to HIV diagnosis and treatment, as recommended in WHO's Interim Policy on TB/HIV Collaborative Activities (1). In this project, we found several missed opportunities, including HIV testing of TB patients, measurement of CD4 count, and initiation of co-trimoxazole and ART. Educating providers about the life-saving benefits of ART in HIV-infected TB patients is a major priority, but more data from observational studies observational studies, n.pl an investigational method involving description of the associations be-tween interventions and outcomes. Outcomes research and practice audits are examples of this investigational method. and clinical trials are needed to provide evidence-based guidance about the optimum timing of ART and the incidence and management of overlapping toxicities and immune-reconstitution syndrome. This study has several major limitations. First, we do not know the reasons why patients did not receive ART. Many patients who did not receive ART were likely deemed too ill and, therefore, unlikely to benefit from ART. This bias would exaggerate the benefit of ART; survival would determine ART use, not the reverse. To address this issue, we controlled for 2 factors likely to predict when a patient would receive ART, such as CD4 count and hospital of care (a surrogate surrogate n. 1) a person acting on behalf of another or a substitute, including a woman who gives birth to a baby of a mother who is unable to carry the child. 2) a judge in some states (notably New York) responsible only for probates, estates, and adoptions. for physician preference or resources). Moreover, after excluding persons who died within the first 2 months of TB treatment, i.e., persons likely to receive minimal benefit from ART and likely to have been deemed too ill to receive ART, we still identified a substantial benefit for ART. Another limitation is that not all TB patients underwent HIV testing, which could skew (1) The misalignment of a document or punch card in the feed tray or hopper that prohibits it from being scanned or read properly. (2) In facsimile, the difference in rectangularity between the received and transmitted page. our population toward those patients most likely to have advanced immune suppression and, therefore, most likely to benefit from ART. Since these data were collected, rates of HIV testing of TB patients have increased substantially in Ubon-ratchathani, but the proportion identified as HIV infected remains similar to what it was in this study, suggesting that the number of HIV infections missed in this study population was small. This study was also based on surveillance and monitoring data from a public health program, which, though prospectively collected, necessarily relied on incomplete data, such as from routine medical records. Core data elements, such as CD4 count, were missing for many patients, and data about adverse events and causes of death, which are critical to assessing the risks of combined ART and TB treatment, were not collected. Low rates of culture positivity, particularly in smear-negative patients, leave open the possibility that some patients did not, in fact, have TB. Since this study, we have identified several reasons for the low yield of culture, including delayed transport times for specimens and inadequate specimen collection; efforts to improve these procedures have since been implemented. Even though many patients were not culture confirmed in this study, sputum smear positive patients benefited strongly from ART, which suggests that misdiagnosis mis·di·ag·no·sis n. pl. mis·di·ag·no·ses An incorrect diagnosis. mis·di  ag·nose of TB is an unlikely explanation for
our findings.
Major strides have been made in enhancing access to HIV treatment in the developing world. Nevertheless, as this study shows, deaths of patients with both TB and HIV remain high, and, even in a country such as Thailand with high rates of access to ART, few HIV-infected TB patients receive ART. Globally, measures to save lives of patients with both diseases have focused on making TB and HIV programs collaborate more closely. To that end, more data from these settings are urgently needed to convince policymakers in countries affected by this syndemic about the critical importance of rapidly expanding access to ART, particularly for HIV-infected TB patients. Funding for this project was received from the Thailand Ministry of Public Health and CDC. References (1.) World Health Organization. Interim policy on collaborative TB/ HIV activities. 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; 2004. WHO/HTM/ TB/2004.330. [cited 30 Apr 2007]. Available from http://whqlibdoc.who.int/hq/2004/who_htm_tb_2004.330.pdf (2.) World Health Organization. Global tuberculosis control: surveillance, planning, financing. WHO report 2005. Geneva: The Organization; 2005. WHO/HTM/TB/2005.349. (3.) 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. (4.) Chaisson RE, Schecter GF, Theuer CP, Rutherford GW, Echenberg DF, Hopewell PC. Tuberculosis in patients with acquired immunodeficiency syndrome acquired immunodeficiency syndrome, see AIDS. : clinical features, response to therapy, and survival. Am Rev Respir Dis. 1987;136:5704. (5.) 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Human immunodeficiency virus (HIV) A transmissible retrovirus that causes AIDS in humans. infection in patients with tuberculosis in Nairobi, Kenya. Am Rev Respir Dis. 1992;146:849-54. (7.) Elliott AM, Halwiindi B, Hayes RJ. The impact of human immunodeficiency virus on mortality of patients treated for tuberculosis in a cohort study in Zambia. Trans R Soc Trop Med Hyg. 1995;89: 78-82. (8.) Freudenberg N, Fahs M, Galea S galea /ga·lea/ (ga´le-ah) [L.] a helmet-shaped structure. galea aponeuro´tica the aponeurosis connecting the two bellies of the occipitofrontalis muscle. , Greenberg A. The impact of New York New York, state, United States New York, Middle Atlantic state of the United States. It is bordered by Vermont, Massachusetts, Connecticut, and the Atlantic Ocean (E), New Jersey and Pennsylvania (S), Lakes Erie and Ontario and the Canadian province of City's 1975 fiscal crisis on tuberculosis, HIV, and homicide syndemic. Am J Public Health. 2006;96:424-34. (9.) 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Decline in the AIDS and death rates in the EuroSIDA study: an observational study In statistics, the goal of an observational study is to draw inferences about the possible effect of a treatment on subjects, where the assignment of subjects into a treated group versus a control group is outside the control of the investigator. . Lancet. 2003;362:22-9. (12.) Palella FJ Jr, Delaney KM, Moorman AC, Loveless MO, Fuhrer füh·rer also fueh·rer n. A leader, especially one exercising the powers of a tyrant. [German, from Middle High German vüerer, from vüeren, to lead, from Old High German J, Satten GA, et al., and the HIV outpatient study investigators. Declining morbidity and mortality Morbidity and Mortality can refer to:
(13.) World Health Organization. TB/HIV: a clinical manual, second edition. 2004. Geneva: The Organization; 2004. [cited 30 Apr 2007]. Available from http://whqlibdoc.who.int/publications/2004/9241546344.pdf (14.) Dheda K, Lampe FC, Johnson MA, Lipman MC. Outcome of HIV-associated tuberculosis in the era of highly active anti-retroviral therapy. J 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. Dis. 2004; 190:1670-6. (15.) Dean GL, Edwards SG, Ives NJ, Mathews G, Fox EF, Navaratne L, et al. Treatment of tuberculosis in HIV-infected persons in the era of highly active antiretroviral therapy Noun 1. highly active antiretroviral therapy - a combination of protease inhibitors taken with reverse transcriptase inhibitors; used in treating AIDS and HIV drug cocktail, HAART . AIDS. 2002;16:75-83. (16.) Burman W, Benator D, Vernon A, Khan A, Jones B, Silva C, et al. Acquired rifamycin rifamycin /rif·a·my·cin/ (rif?ah-mi´sin) any of a family of antibiotics biosynthesized by a strain of Streptomyces mediterranei, resistance with twice-weekly treatment of HIV-related tuberculosis. Am J Respir Crit Care Med. 2006;173:350-6. (17.) Breen RA, Miller RF, Gorsuch T, Smith CJ, Ainsworth J, Ballinger J, et al. Virological virological pertaining to viruses. response to highly active anti-retroviral therapy is unaffected by anti-tuberculosis therapy. J Infect Dis. 2006;193:1437-40. (18.) Manosuthi W, Chottanapand S, Thongyen S, Chaovavanich A, Sungkanuparph S. Survival rate and risk factors of mortality among HIV/tuberculosis-coinfected patients with and without antiretroviral therapy. J Acquir Immune Defic Syndr. 2006;43:42-6. (19.) World Health Organization. Treatment of tuberculosis: guidelines for national programmes. Geneva, Switzerland: The Organization; 2003. [cited 30 Apr 2007].Available from http://whqlibdoc.who.int/hq/2003/WHO_CDS_TB_2003.313_eng.pdf (20.) Yu LM, Easterbrook PJ, Marshall Y. Relationship between CD4 count and CD4% in HIV-infected people. Int J Epidemiol. 1997;26: 1367-73. (21.) Jones BE, Young SMM (System Management Mode) An energy conservation mode built into Intel SL Enhanced 486 and Pentium CPUs. During inactive periods, SMM initiates a sleep mode that turns off peripherals or the entire system. , Antoniskis D, Davidson PT, Kramer F, Barnes PE Relationship of the manifestations of tuberculosis to CD4 cell CD4 cell CD4+ lymphocyte A circulating T cell with a 'helper' phenotype; in AIDS Pts, the levels of CD4+ cells is a crude indicator of immune status and susceptibility to certain AIDS-related conditions; these Pts may suffer KS as CD4+ cells fall below 0. counts in patients with human immunodeficiency virus infection. Am Rev Respir Dis. 1993;148:1292-7. (22.) Kaplan JE, Hanson D, Dworkin MS, Frederick T, Bertolli J, Lindegren ML, et al. Epidemiology of human immunodeficiency virus associated opportunistic infections in the United States in the era of highly active anti-retroviral therapy. Clin Infect Dis. 2000;30: S5-14. (23.) Martin DJ, Sim (1) (Society for Information Management, Chicago, IL, www.simnet.org) Founded in 1968 as the Society for MIS, it is a membership organization made up of corporate and division heads of IT organizations. JG, Sole G J, Rymer L, Shalekoff S, van Niekerk AB, et al. CD4+ lymphocyte count in African patients co-infected with HIV and tuberculosis. J Acquir Immune Defic Syndr Hum Retrovirol. 1995;8:386-91. (24.) Teck R, Ascurra O, Gomani P, Manzi M, Pasulani O, Kusamale J, et al. WHO clinical staging of HIV infection and disease, tuberculosis and eligibility for anti-retroviral treatment: relationship to CD4 lymphocyte counts. Int J Tuberc Lung Dis. 2005;9:258-62. (25.) Morris L, Martin DJ, Bredell H, Nyoka SN, Sacks L, Pendle S Pendle is a local government district and borough of Lancashire, England, on the North Yorkshire and West Yorkshire borders. It adjoins the Lancashire boroughs of Burnley and Ribble Valley. , et al. 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--1 RNA RNA: see nucleic acid. RNA in full ribonucleic acid One of the two main types of nucleic acid (the other being DNA), which functions in cellular protein synthesis in all living cells and replaces DNA as the carrier of genetic levels and CD4 lymphocyte counts, during treatment for active tuberculosis, in South African patients. J Infect Dis. 2003; 187:1967-71. (26.) Abouya L, Coulibaly IM, Wiktor SZ, Coulibaly D, N'kragbo M, N'gbo A, et al. The Cote d'Ivoire national HIV counseling and testing program for tuberculosis patients: implementation and analysis of epidemiologic data. AIDS. 1998;12:505-12. (27.) Wiktor SZ, Sassan-Morokro M, Grant AD, Abouya L, Karon JM, Maurice C, et al. Efficacy of trimethoprim-sulphamethoxazole prophylaxis to decrease morbidity and mortality in HIV-l-infected patients with tuberculosis in Abidjan, Cote d'Ivoire: a 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" controlled trial 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. . Lancet. 1999;353:1469-75. (28.) Tansuphasawadikul S, Amomkul PN, Tanchanpong C, Limpakarnjanarat K, Kaewkungwal J, Likanonsakul S, et al. Clinical presentation of hospitalized adult patients with HIV infection and AIDS in Bangkok, Thailand. J Acquir Immune Defic Syndr. 1999;21: 326-32. Address for correspondence: Jay Vanna, CDC/HIV, Box 68, American Embassy, APO apo- 1 A prefix indicating a protein component in a conjugated molecule–eg, apoferritin, apolipoprotein, see there 2 Apolipoprotein, see there , P 96546; email: jvarma@cdc.gov All material published in Emerging Infectious Diseases An emerging infectious disease (EID) is an infectious disease whose incidence has increased in the past 20 years and threatens to increase in the near future. EIDs include diseases caused by a newly identified microorganism or newly identified strain of a known microorganism (e.g. is in the public domain and may be used and reprinted without special permission; proper citation, however, is required. (1) Data from this manuscript have been presented in part at the 36th UNION World Conference on Lung Health, Paris, October 2005, and the 15th Annual International AIDS Conference Education, networking and the promotion of best practice are essential to enhancing the response to HIV/AIDS. IAS conferences provide opportunities to share experience, and increase the knowledge and expertise of professionals working in HIV/AIDS. , Bangkok, July 2004. Somsak Akksilp, * Opart Karnkawinpong, * Wanpen Wattanaamornkiat, * Daranee Viriyakitja, ([dagger]) Patama Monkongdee, ([double dagger double dagger n. A reference mark (  ) used in printing and writing. Also called diesis.Noun 1. ]) Walya Sitti, * Dhanida Rienthong, ([dagger]) Taweesap Siraprapasiri, ([dagger]) ([double dagger]) Charles D. Wells, ([section]) Jordan W. Tappero, ([section]) [double dagger]), and Jay K. Varma ([section]) ([double dagger]) * Ministry of Public Health, Ubon-ratchathani, Thailand; ([dagger]) Ministry of Public Health, Nonthaburi, Thailand; and ([double dagger]) Thailand Ministry of Public Health--Centers for Disease Control and Prevention Collaboration, Nonthaburi, Thailand; and ([section]) Centers for Disease Control and Prevention, Atlanta, Georgia, USA Dr Akksilp is a physician and public health official with the Thailand Ministry of Public Health. His interests include expanding access to diagnosis and treatment of TB, MDR-TB MDR-TB Multi-Drug Resistant Tuberculosis , and TB/HIV.
Table 1. Characteristics of HIV-infected patients with
(TB), Ubon-ratchathani, February 2003 through January 24
Patients
(N = 329),
Characteristic no. (%)
Female 112 (34)
Median age, y (range) 32 (0.8-68)
Type, location of TB
Sputum smear-positive, pulmonary 120 (36)
Sputum smear-negative, pulmonary 107 (33)
Extrapulmonary 102 (31)
Category of TB
New 307 (93)
Treatment alter interruption, failure, 11 (4)
default, or relapse
Other 11 (3)
HIV status known before TB diagnosis 225 (68)
CD4 count (cells/[mm.sup.3])
<50 95 (29)
50-99 39 (12)
100-199 36 (11)
[greater than or equal to] 200 25 (8)
Unknown 134 (41)
Received co-trimoxazole during TB 225 (68)
treatment
Received antiretroviral therapy (ART)
Before TB diagnosis 30 (9)
During TB treatment 45 (14)
Not prescribed ART 254 (77)
Among patients receiving ART, regimen
prescribed (n = 75)
Stavudine/Lamivudine/Nevirapine 38 (51)
Stavudine/Lamivudine/Efavirenz 35 (47)
Other 2 (2)
Treatment outcome
Cured 61 (19)
Completed 126 (38)
Failure 4 (1)
Default 31
Transfer 4 (1)
Change of diagnosis 4 (1)
Died 99 (30)
Table 2. Results of culture and susceptibility testing performed on
HIV-infected patients with pulmonary TB, stratified by sputum
smear-positive versus -negative results, Ubon-ratchathani, February
2003 through January 2004 *
Smear-positive Smear-negative
(n = 120), (n = 107),
Characteristic no. (%) no. (%)
Sputum culture performed 93/120 (78) 52/107 (49)
Culture positive for 2/93 (2) 0/52 (0)
nontuberculous mycobacteria
Contaminated 5/93 (5) 6/52 (12)
Culture negative 21/93 (23) 43/52 (83)
Culture positive for 65/93 (70) 3/52 (6)
Mycobacterium tuberculosis
Multidrug-resistant TB 4/65 (6) 0/3 (0)
Previously treated 1/4 (25) NA
* TB, tuberculosis; NA, not available.
Table 3. Univariate analysis of risk factors for death among
HIV-infected TB patients with outcomes of cured, completed, failed, or
died, stratified by all patients versus pulmonary, smear-positive
patients, Ubon-ratchathani, February 2003 through January 2004 *
All TB patients (N = 286)
Died, no./
Characteristic total (%) RR (95% CI)
Sex
Male 69/193 (36) 1.2 (0.8-1.6)
Female 30/97 (31) Ref
Age
<18 y 4/19 (21) 0.6 (0.2-1.4)
18-34 y 60/168 (36) Ref
[greater than or equal 35/103 (34) 1.0 (0.7-1.3)
to] 35 y
Type, location of TB
Sputum smear-positive, 40/107 (37) Ref
pulmonary
Sputum smear-negative, 38/96 (40) 1.1 (0.8-1.5)
pulmonary
Extrapulmonary 21/87 (24) 0.7 (0.4-1.0)
CD4 count (cells/[mm.sup.3])
[greater than or equal 1/22 (5) Ref
to] 200
100-199 5/33 (15) 3.3 (0.4-26.6)
50-99 9/35 (26) 5.7 (0.8-41.6)
<50 22/92 (24) 5.3 (0.8-37.0)
Unknown 62/108 (57) 12.6 (1.9-86.3)
Co-trimoxazole during
TB treatment
Received 57/208 (27) 0.5 (0.4-0.7)
Did not receive 42/82 (51) Ref
Antiretroviral therapy
before or during TB
treatment
Received 5/71 (7) 0.2 (0.1-0.4)
Did not receive 94/219 (43) Ref
Sputum culture ([dagger])
Culture positive 18/60 (30) Ref
Not culture positive 81/230 (35) 1.2 (0.8-1.8)
([double dagger])
Culture negative 21/60 (35) 1.2 (0.7-2.0)
([double dagger])
Smear-positive TB patients (n = 104)
Died, no./
Characteristic total (%) RR (95% CI)
Sex
Male 33/72 (46) 2.3 (1.1-4.7)
Female 7/35 (20) Ref
Age
<18 y 0/1 (0) 0 (0-0)
18-34 y 26/60 (43) Ref
[greater than or equal 14/46 (30) 0.7 (0.4-1.2)
to] 35 y
Type, location of TB
Sputum smear-positive, NA NA
pulmonary
Sputum smear-negative, NA NA
pulmonary
Extrapulmonary NA NA
CD4 count (cells/[mm.sup.3])
[greater than or equal 0/8 (0) Ref
to] 200
100-199 2/12 (17) Undefined
50-99 1/10 (10) Undefined
<50 9/34 (27) Undefined
Unknown 28/43 (65) Undefined
Co-trimoxazole during
TB treatment
Received 21/71 (30) 0.6 (0.4-0.9)
Did not receive 19/36 (53) Ref
Antiretroviral therapy
before or during TB
treatment
Received 1/23 (4) 0.1 (0.0-0.7)
Did not receive 39/84 (46) Ref
Sputum culture A9
Culture positive 18/59 (31) Ref
Not culture positive 22/48 (46) 1.5 (0.9-2.5)
([double dagger])
Culture negative 9/20 (45) 1.5 (0.8-2.7)
([double dagger])
* TB, tuberculosis; RR, relative risk; CI, confidence interval; Ref,
referent; NA, not applicable.
([dagger]) "Culture positive' includes all patients with a sputum
culture positive for Mycobacterium tuberculosis (MTB). "Not culture
positive" includes any patients without a culture positive for MTB,
regardless of whether they had a specimen sent for culture or not.
"Culture negative" includes only patients with a sputum culture
negative for MTB.
([dagger]) Compared with culture positive.
Table 4. Multivariate analysis of risk factors for death among
HIV-infected TB patients with outcomes of cured, completed, failed, or
died and adjusted for site of treating facility, * Ubon-ratchathani,
February 2003 through January 2004 ([dagger])
Adjusted OR
Characteristic (95% CI)
Antiretroviral therapy before or 0.2 (0.1-0.5)
during TB treatment
Co-trimoxazole during TB treatment 1.1 (0.6-2.3)
CD4 count (cells/mm3)
[greater than or equal to] 200 Referent
100-199 5.5 (0.6-52.6)
50-99 9.3 (1.0-82.9)
<50 9.7 (1.2-78.4)
Unknown 29.9 (3.8-238.0)
Type, location of TB
Sputum smear-positive, pulmonary Referent
Sputum smear-negative, pulmonary 1.3 (0.7-2.6)
Extrapulmonary 0.5 (0.2-1.0)
* Data not shown
([dagger]) TB, tuberculosis; OR, odds ratio; CI confindence interval.
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