Multidrug-resistant tuberculosis management in resource-limited settings.Evidence of successful management of multidrug-resistant 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, (MDRTB) is mainly generated from referral hospitals in high-income countries. We evaluate the management of MDRTB in 5 resource-limited countries: Estonia, Latvia, Peru, the Philippines, and the Russian Federation Russian Federation: see Russia. . All projects were approved by the Green Light Committee for access to quality-assured second-line drugs second-line drug Any therapeutic agent that is not the drug of choice, or the 1st normally used to treat a particular condition; in rheumatoid arthritis, 2nd provided at reduced price for MDRTB management. Of 1,047 MDRTB patients evaluated, 119 (11%) were new, and 928 (89%) had received treatment previously. More than 50% of previously treated patients had received both first- and second-line drugs, and 65% of all patients had infections that were resistant to both first- and second-line drugs. Treatment was successful in 70% of all patients, but success rate was higher among new (77%) than among previously treated patients (69%). In resource-limited settings, treatment of MDRTB provided through, or in collaboration with, national TB programs can yield results similar to those from wealthier settings. ********** Multidrug-resistant tuberculosis (MDRTB), defined as TB resistant to at least 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. and 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. , represents an obstacle to TB control, especially in areas where MDRTB prevalence is high (1). New World Health Organization (WHO) estimates suggest that 424,203 MDRTB cases occurred in 2004 (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%. 376,019-620,061), or 4.3% of all new and previously treated TB cases. More than half of the estimated MDRTB cases were in China and India, while the highest estimated prevalences were in countries of the former Soviet Union and certain provinces of China (2). DOTS is the internationally recommended strategy for TB control and is based on a 6-month treatment 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. with first-line drugs (isoniazid, rifampin, pyrazinamide pyrazinamide /pyr·a·zin·amide/ (pir?ah-zin´ah-mid) an antibacterial derived from nicotinic acid, used as a tuberculostatic. pyrazinamide , and 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 ) for new patients and an 8-month treatment regimen with isoniazid, rifampin, pyrazinamide, ethambutol, and streptomycin streptomycin (strĕp'tōmī`sĭn), antibiotic produced by soil bacteria of the genus Streptomyces and active against both gram-positive and gram-negative bacteria (see Gram's stain), including species resistant to other for re-treatment patients (3). While DOTS prevents the emergence of drug resistance in drug-susceptible cases, in patients with MDRTB, this treatment yields inadequate cure rates (4-7). A retrospective LAW, RETROSPECTIVE. A retrospective law is one that is to take effect, in point of time, before it was passed. 2. Whenever a law of this kind impairs the obligation of contracts, it is void. 3 Dall. 391. 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 of treatment of MDRTB with this regimen in 6 countries showed treatment success rates of 52% (range 11%-60%) in new cases and 29% (range 18%-36%) in previously treated cases (5). In addition, the frequency of TB recurrence recurrence /re·cur·rence/ (-ker´ens) the return of symptoms after a remission.recur´rent re·cur·rence n. 1. among MDRTB patients previously considered to be cured after this treatment has been reported at 28% (6). Treating MDRTB with second-line drugs may cure >65% of patients and stop ongoing transmission (8-10). However, most of the evidence of successful MDRTB management is generated from high-income countries where treatment is provided in referral hospitals (10). In 1999, WHO and partner agencies launched DOTS-Plus to manage MDRTB in resource-limited settings, a term that was recently abolished since it was used for the piloting of the management of MDRTB within the context of DOTS programs. Effective MDRTB control builds on the 5 tenets of the DOTS strategy (3) and expands each of these areas to address the complexities associated with treating MDRTB (11). As part of this strategy, a novel partnership known as the Green Light Committee (GLC) was created to foster access to, and rational use of, second-line drugs (11-13). The second-line drugs included in the WHO Model List of Essential Medicines are amikacin amikacin /am·i·ka·cin/ (am?i-ka´sin) a semisynthetic aminoglycoside antibiotic derived from kanamycin, used as the sulfate salt in the treatment of a wide range of infections due to aerobic gram-negative bacilli. , capreomycin capreomycin /cap·reo·my·cin/ (kap?re-o-mi´sin) a polypeptide antibiotic produced by Streptomyces capreolus, which is active against human strains of Mycobacterium tuberculosis ; used as the disulfate salt. , ciprofloxacin ciprofloxacin /cip·ro·flox·a·cin/ (sip?ro-flok´sah-sin) a synthetic antibacterial effective against many gram-positive and gram-negative bacteria; used as the hydrochloride salt. cip·ro·flox·a·cin n. , cycloserine cycloserine /cy·clo·ser·ine/ (-se´ren) an antibiotic produced by Streptomyces orchidaceus or obtained synthetically; used as a tuberculostatic and in treatment of urinary tract infections. , ethionamide ethionamide /ethi·on·am·ide/ (e-thi?on-am´id) an antibacterial, effective against Mycobacterium tuberculosis; used in the treatment of pulmonary tuberculosis. , kanamycin kanamycin /kan·a·my·cin/ (kan?ah-mi´sin) an aminoglycoside antibiotic derived from Streptomyces kanamyceticus, effective against aerobic gram-negative bacilli and some gram-positive bacteria, including mycobacteria; used as the , levofloxacin levofloxacin /le·vo·flox·a·cin/ (-flok´sah-sin) a broad-spectrum antibacterial agent for systemic and ophthalmic use. le·vo·flox·a·cin n. , ofloxacin ofloxacin /oflox·a·cin/ (o-flok´sah-sin) an antibacterial agent effective against a wide variety of gram-negative and gram-positive aerobic organisms. o·flox·a·cin n. , p-aminosalicylic acid p- aminosalicylic acid /p- ami·no·sal·i·cyl·ic ac·id/ (PAS) (PASA) an analogue of aminobenzoic acid (PABA) with antibacterial properties; used to inhibit growth and multiplication of the tubercle bacillus.. , and prothionamide (11). GLC reviews applications from projects that wish to integrate MDRTB management into a DOTS-based TB control program. If the applicant proposes a strategy consistent with international recommendations and agrees to the monitoring procedures of GLC, then access to reduced-price, quality-assured second-line drugs is granted. Some of the requirements for GLC endorsement include a well-functioning DOTS program, long-term political commitment, rational case-finding strategies, diagnosis of MDRTB through quality-assured culture and drug susceptibility testing susceptibility test Antimicrobial susceptibility test, see there (DST (1) (DeSTination) Contrast with SRC, which is an abbreviation of "source." (2) (Digital Signal Trust Company, Salt Lake City, UT, www.digsigtrust.com) An organization that sets up and manages PKI systems for companies and industry groups. ), treatment strategies that use second-line drugs under proper management conditions, uninterrupted supply of quality-assured second-line drugs, and a recording and reporting system designed for MDRTB control programs that enables monitoring and evaluation of program performance and treatment outcome (11,13,14). These conditions represent the MDRTB control framework. Projects must be tailored to site-specific epidemiologic ep·i·de·mi·ol·o·gy n. The branch of medicine that deals with the study of the causes, distribution, and control of disease in populations. [Medieval Latin epid and programmatic pro·gram·mat·ic adj. 1. Of, relating to, or having a program. 2. Following an overall plan or schedule: a step-by-step, programmatic approach to problem solving. 3. conditions within this framework. As a result, MDRTB control programs may differ substantially between settings (11). Some aspects in which MDRTB control programs may vary include whether all TB patients are tested with culture and DST or only patients with an increased risk for MDRTB, use of standardized standardized pertaining to data that have been submitted to standardization procedures. standardized morbidity rate see morbidity rate. standardized mortality rate see mortality rate. or individualized in·di·vid·u·al·ize tr.v. in·di·vid·u·al·ized, in·di·vid·u·al·iz·ing, in·di·vid·u·al·iz·es 1. To give individuality to. 2. To consider or treat individually; particularize. 3. second-line treatment regimen, and hospitalization hospitalization /hos·pi·tal·iza·tion/ (hos?pi-t'l-i-za´shun) 1. the placing of a patient in a hospital for treatment. 2. the term of confinement in a hospital. of MDRTB patients or provision of treatment on an ambulatory Movable; revocable; subject to change; capable of alteration. An ambulatory court was the former name of the Court of King's Bench in England. It would convene wherever the king who presided over it could be found, moving its location as the king moved. basis. This analysis of the first 5 GLC-endorsed MDRTB control programs provides, for the first time, results on management of MDRTB under DOTS-based program conditions in multiple resource-limited countries by using standardized treatment outcome definitions. Methods This is a study of MDRTB patients enrolled in Estonia, Latvia, Lima (Peru), Manila Manila (mənĭl`ə), city (1990 pop. 1,601,234), capital of the Philippines, SW Luzon, on Manila Bay. Manila is the center of the country's largest metropolitan area, its chief port, and the focus of all governmental, commercial, industrial, (the Philippines), and Tomsk Oblast Tomsk Oblast (Russian: То́мская о́бласть, Tomskaya oblast) is a federal subject of Russia (an oblast). (Russian Federation). The data were collected prospectively. The enrollment period started in 1999 for Lima and Manila, 2000 for Latvia and Tomsk, and 2001 for Estonia and ended December 31, 2001. All patients evaluated were managed under GLC-approved protocols and had the opportunity to receive [greater than or equal to] 24 months of treatment. In addition, follow-up data on successfully treated patients were collected at the beginning of 2006, two years after the last patient's treatment ended (December 31, 2003). A new MDRTB patient was defined as a patient who had never received TB treatment or who had received TB treatment for <1 month. An MDRTB patient previously treated with only first-line drugs was defined as an MDRTB patient who had been treated for >1 month with only first-line anti-TB drugs. An MDRTB patient previously treated with second-line drugs was defined as an MDRTB patient who had been treated for >1 month with [greater than or equal to] 1 second-line anti-TB drug (with or without first-line drugs). Six standard and mutually exclusive Adj. 1. mutually exclusive - unable to be both true at the same time contradictory incompatible - not compatible; "incompatible personalities"; "incompatible colors" categories were used to define treatment outcome: cure, treatment completed, death, default, failure, and transfer out (14) (Table 1). The treatment success percentage was obtained by adding the percentage of cured patients to the percentage of patients who completed treatment. Outcome data were recorded by the individual projects in centralized cen·tral·ize v. cen·tral·ized, cen·tral·iz·ing, cen·tral·iz·es v.tr. 1. To draw into or toward a center; consolidate. 2. electronic registers. International standards for core data collection in MDRTB control programs were developed in 2000 (11). Projects developed their own standardized forms and electronic databases that included all of the core data elements. Aggregated program and patient data were collected from each project with a data collection form developed by GLC. The accuracy of laboratory methods was verified ver·i·fy tr.v. ver·i·fied, ver·i·fy·ing, ver·i·fies 1. To prove the truth of by presentation of evidence or testimony; substantiate. 2. though regular quality assurance exercises performed by a network of WHO/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; supranational Supranational An international organization, or union, whereby member states transcend national boundaries or interests to share in the decision-making and vote on issues pertaining to the wider grouping. TB reference laboratories, as previously described (1). For each project, data submitted to WHO were checked for completeness and consistency; all errors or discrepancies were corrected in consultation with the project's investigators. Statistical tests were performed with the Fisher exact test for 2x2 comparisons and the [chi square chi square (kī), n a nonparametric statistic used with discrete data in the form of frequency count (nominal data) or percentages or proportions that can be reduced to frequencies. ] test for the other tables. For all statistical tests, we regarded a p value <0.05 as significant. Data were analyzed an·a·lyze tr.v. an·a·lyzed, an·a·lyz·ing, an·a·lyz·es 1. To examine methodically by separating into parts and studying their interrelations. 2. Chemistry To make a chemical analysis of. 3. in Stata Stata (Statistics/Data Analysis) is a statistical program created in 1985 by Statacorp that is used by many businesses and academic institutions around the world. Most of its users work in research, especially in the fields of economics, sociology, political science, and version 8 (StataCorp LP, College Station, TX, USA). Results The 5 programs are described in Table 2. All projects are conducted in well-established DOTS programs. Four projects are integrated into the national TB program (NTP (Network Time Protocol) A TCP/IP protocol used to synchronize the real time clock in computers, network devices and other electronic equipment that is time sensitive. It is also used to maintain the correct time in NTP-based wall and desk clocks. ): Estonia, Latvia, Lima, and Tomsk. The project in Manila is conducted by a nongovernmental organization nongovernmental organization (NGO) Organization that is not part of any government. A key distinction is between not-for-profit groups and for-profit corporations; the vast majority of NGOs are not-for-profit. at a private tertiary tertiary (tûr`shēârē), in the Roman Catholic Church, member of a third order. The third orders are chiefly supplements of the friars—Franciscans (the most numerous), Dominicans, and Carmelites. hospital, in close collaboration with NTP. All projects provide free care to MDRTB patients. The programs in Estonia, Latvia, and Tomsk are the only available treatment options for MDRTB, while in Lima and Manila, treatment in the private sector is also available. In all projects, financing is obtained through both national healthcare budgets and external sources. All projects work in collaboration with technical agencies and, in Lima and Tomsk, nongovernmental organizations Transnational organizations of private citizens that maintain a consultative status with the Economic and Social Council of the United Nations. Nongovernmental organizations may be professional associations, foundations, multinational businesses, or simply groups with a common interest in . Directly observed treatment Directly Observed Treatment (DOT) or Directly Observed Therapy is watching the patient take his/her medication to ensure medications are taken in the right combination and for the correct duration. (DOT) is standard care in all projects. Treatment is observed by a range of persons, including healthcare workers (primarily nurses) and community volunteers. DOT worker incentives are provided in Estonia, Lima, and Tomsk, primarily consisting of money (Estonia) and food and money (Lima and Tomsk). Patient incentives, food and free transportation, are provided in all projects except for those in Manila. In Lima, patients also receive housing and social, educational, and financial support, as needed as needed prn. See prn order. . Lima and Manila offer patient support groups. Sputum culture 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 and DST to first- and second-line drugs are performed at each project site except for Lima and Tomsk, which rely on an international laboratory for DST to second-line drugs. All projects test for susceptibility susceptibility the state of being susceptible. Refers usually to infectious disease but may be to physical factors such as wetting or to psychological factors such as harassment. to several first- and second-line drugs. In 3 projects, those in Estonia, Latvia, and Tomsk, MDRTB patients are hospitalized in a separate ward or building until they are noninfectious. In Peru and Manila, only severely ill patients and patients with side effects Side effects Effects of a proposed project on other parts of the firm. are hospitalized. The 5 projects use different case-finding strategies and treatment options (use of empiric treatment regimens while awaiting DST results or not) (Table 2). In Estonia, Latvia, and Tomsk, all (new and previously treated) patients received DST at the start of treatment. However, in this study MDRTB patients from Tomsk were all previously treated patients on a waiting list for treatment. In Lima, DST is only performed on isolates from patients in whom treatment failed or suspicion of MDRTB is high. Most patients in Lima were referred to the GLC-approved MDRTB control program only after failure of a standardized regimen, which contained second-line drugs and was used by the Peruvian NTP. In Manila, patients had a range of treatment histories; most came after failure of treatment provided by private physicians outside the DOTS program. Because of the long turnaround times (1) In batch processing, the time it takes to receive finished reports after submission of documents or files for processing. In an online environment, turnaround time is the same as response time. for DST results from the international laboratory, patients in Lima and Tomsk often received empiric treatment after culture conversion. For each program, the drugs against which the strains were tested are given in Table 2; however, not all strains were tested against all the drugs listed for each program. All projects used DST results and previous treatment history to design the individualized regimen. Across the 5 projects, regimens contained [greater than or equal to] 4 drugs, and most patients received >4 drugs initially. All regimens included an injectable in·ject·a·ble adj. Capable of being injected. Used of a drug. n. A drug or medicine that can be injected. agent (amikacin, capreomycin, kanamycin, or streptomycin) and a fluoroquinolone fluoroquinolone /flu·o·ro·quin·o·lone/ (-kwin´o-lon) any of a subgroup of fluorine-substituted quinolones, having a broader spectrum of activity than nalidixic acid. fluor·o·quin·o·lone n. (ciprofloxacin, levofloxacin, or ofloxacin). Nearly all drugs were administered for the duration of treatment except for the injectable agent, which was given for a specified interval after the patient's specimens were culture negative. Treatment duration was 18-24 months, and the exact length was usually determined individually for each patient. The frequency of drugs used in the regimens is shown in Table 3. The median duration of patient follow-up after a patient's having been declared cured or treatment completed was 24 months (range 12 months [Lima and Tomsk] to 36 months [Estonia]). Drugs were administered under direct observation. In Lima, Tomsk, and Manila, drugs were administered 6 days per week; in Estonia and Latvia, drugs were given 7 days during the hospital phase and then 5 or 6 days a week after discharge. Monitoring of treatment regimens was based on the results of monthly 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 and culture. Chest radiographs were also performed every 3 months in Estonia, Latvia, and Tomsk and every 6 months in Lima and Manila. All projects except that in Manila had access to adjunctive ad·junct n. 1. Something attached to another in a dependent or subordinate position. See Synonyms at appendage. 2. A person associated with another in a subordinate or auxiliary capacity. 3. surgery for major interventions such as lung resection resection /re·sec·tion/ (-sek´shun) excision. root resection apicoectomy. transurethral resection of the prostate (TURP), transurethral prostatic resection . Each project provided patients with ancillary Subordinate; aiding. A legal proceeding that is not the primary dispute but which aids the judgment rendered in or the outcome of the main action. A descriptive term that denotes a legal claim, the existence of which is dependent upon or reasonably linked to a main claim. drugs to manage adverse events. MDRTB program cohort cohort /co·hort/ (ko´hort) 1. in epidemiology, a group of individuals sharing a common characteristic and observed over time in the group. 2. characteristics are shown in Table 4. Among 1,047 MDRTB patients, 119 (11%) were new, and 928 (89%) were previously treated. Among the 919 previously treated patients from whom details could be obtained, 438 (48%) had received only first-line drugs and 481 (52%) first and second-line drugs. Few patients' isolates were resistant to only rifampin and isoniazid (2.6%); most (65%) were resistant to first- and second-line drugs. 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. coinfection was identified in 0% (Estonia and Tomsk) and 4.5% (Latvia) of patients. (In Lima and Tomsk, all MDRTB patients were tested for HIV; in Estonia and Latvia, 67% and 90% of MDRTB patients were tested; and in Manila 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. was not performed.) Frequency of hospitalization varied from 5.0% (Manila) to 100% (Latvia), and duration of hospitalization ranged from 29 days (Manila) to 267 days (Tomsk). The treatment outcomes of new, previously treated, and all MDRTB patients are shown in Table 5 and Figure 1. Treatment was successful in 70% of 1,047 patients (range 59%-83%). Failure occurred in 3.3% to 11% of patients, default in 6.3% to 16%, and death in 3.7% to 19%. In Estonia and Latvia, MDRTB patients not previously treated for TB had a higher treatment success rate (80% vs. 61%, odds ratio [OR] 2.54, 95% confidence interval [CI] 1.47-4.37, p<0.005) and a lower failure rate (4.4% vs. 15%, OR 0.26, 95% CI 0.10-0.67, p<0.005) than previously treated patients. Adverse events led to treatment cessation cessation Vox populi The stopping of a thing. See Smoking cessation. in 3.2% of patients (range 0% [Tomsk] to 8.6% [Manila]). By the end of 2005, a total of 14 of 670 patients (2.1%) who were followed-up after cure or treatment completion had relapsed (range 1.1% [Lima] to 10.0% [Estonia]) (Table 6). [FIGURE 1 OMITTED] Discussion Today, management of MDRTB is included as a recommended part of the new Stop TB Strategy (15). WHO's guidelines guidelines, n.pl a set of standards, criteria, or specifications to be used or followed in the performance of certain tasks. have also been revised to encourage countries to collect drug resistance surveillance data from patients in different retreatment categories and to build capacity to diagnose diagnose /di·ag·nose/ (di´ag-nos) to identify or recognize a disease. di·ag·nose v. 1. To distinguish or identify a disease by diagnosis. 2. and treat MDRTB within the context of DOTS (16). However, few NTPs in resource-limited settings have integrated effective treatment strategies for resistant cases (17). The major perceived barrier to MDRTB treatment is the high cost of quality-assured second-line drugs. Additional barriers include extensive laboratory and monitoring requirements, adverse events associated with second-line drugs, low availability of quality-assured second-line drugs, difficulties in ensuring adequate patient support (including DOT) during the long treatment course, and the risk for resistance to second-line drugs (18,19). Consequently, many NTPs focus on achieving high cure rates in their DOTS programs and neither diagnose nor treat MDRTB (17). This study represents the first multicountry evaluation of MDRTB patients treated in resource-limited settings under the GLC mechanism and endorsed by the respective NTP of each country. Although program design and patient management varied, the results show that treating MDRTB in resource-limited settings is feasible and effective. Treatment with second-line drugs is more successful than a 6- to 8-month regimen of first-line drugs for such patients and, in spite of in opposition to all efforts of; in defiance or contempt of; notwithstanding. See also: Spite a patient population characterized char·ac·ter·ize tr.v. character·ized, character·iz·ing, character·iz·es 1. To describe the qualities or peculiarities of: characterized the warden as ruthless. 2. by high proportions of severe chronic cases with extensive resistance patterns, treatment outcomes of these projects match the outcomes of treatment with second-line drugs in wealthier settings (10). However, in each project, extensive training on managerial, laboratory, clinical, and social aspects of MDRTB control took place before GLC approval and initiation of treatment. Socioeconomic so·ci·o·ec·o·nom·ic adj. Of or involving both social and economic factors. socioeconomic Adjective of or involving economic and social factors Adj. 1. support was provided to the patients in 4 of the 5 sites, and in all sites a patient-centered approach was used for treatment delivery, with DOT ensured during the full course of treatment. These efforts may partly explain why the relapse rates were low (2.1%) and suggest such best practices are essential for a successful outcome. In addition, all projects were supported by technical agencies, and some benefited from extensive NGO NGO abbr. nongovernmental organization Noun 1. NGO - an organization that is not part of the local or state or federal government nongovernmental organization support. Significant differences were seen in favorable fa·vor·a·ble adj. 1. Advantageous; helpful: favorable winds. 2. Encouraging; propitious: a favorable diagnosis. 3. (cure and completed) and unfavorable (default, failure, died, and transferred out) outcomes between projects (p = 0.002), and although patient populations cannot be compared between projects as a result of different TB epidemiologic features in different countries, some general observations can be made with respect to the differences in treatment outcomes. Default rates were higher in Estonia, Latvia, and Manila than in Lima and Tomsk. TB specialists in Estonia and Latvia attributed the high default rates to a high proportion of patients with severe alcohol abuse disorders for whom adherence to treatment adherence to treatment Compliance Therapeutics The following of a recommended course of treatment by taking all prescribed medications for the length of time necessary is difficult. A recent study in Latvia could not confirm that alcohol misuse was clearly linked to default, but the number of nonadherent patients was small and the statistical power correspondingly weak (9). Although the project in Tomsk also experienced problems with alcoholism alcoholism, disease characterized by impaired control over the consumption of alcoholic beverages. Alcoholism is a serious problem worldwide; in the United States the wide availability of alcoholic beverages makes alcohol the most accessible drug, and alcoholism is , default rates were low because a large proportion of patients were imprisoned im·pris·on tr.v. im·pris·oned, im·pris·on·ing, im·pris·ons To put in or as if in prison; confine. [Middle English emprisonen, from Old French emprisoner : en- (41%) during the treatment period. The high default rate in Manila appeared to be related to the facts that at the beginning of Manila's project, treatment was delivered in a single site that was not easily accessible to all patients and that drugs to manage adverse reactions adverse reactions, n.pl unfavorable reactions resulting from administration of a local anesthetic; responsible factors include the drug used, concentration, and route of administration. had to be purchased by the patients. In addition, during the reporting period, the program in Manila did not provide any patient or DOT worker incentives. The low default rates in Lima and Tomsk could be attributed to a large variety of treatment delivery options and incentive and enabler programs for patients. The high frequency of death in Lima likely reflects the fact that in a high proportion of patients, a standard MDRTB treatment regimen with second-line drugs was unsuccessful (20). The proportion of patients previously treated with second-line drugs was much higher in Lima (75%) than in other projects (14%-45%) (Figure 2). However, the proportions of patients with infections resistant to first- and second-line drugs were similar in Latvia, Lima, Manila, and Tomsk (p = 0.47). In Estonia, resistance patterns to first- and second-line drugs differed substantially when compared with patterns in the other 4 projects (p<0.0001), and in Estonia all patients had infections resistant to first- and second-line drugs (Table 4). [FIGURE 2 OMITTED] During the study period, only Estonia and Latvia routinely attempted to identify MDRTB patients at the start of their first treatment for TB, and the results show that early identification and referral may reduce death and treatment failure and thus improve treatment success. This finding is consistent with those of Turett et al. (21). The delay in the diagnosis of MDRTB results in treatment of patients with chronic disease, progressive parenchymal pa·ren·chy·ma n. 1. Anatomy The tissue characteristic of an organ, as distinguished from associated connective or supporting tissues. 2. destruction, higher bacillary bacillary /bac·il·la·ry/ (bas´i-lar?e) pertaining to bacilli or to rodlike structures. bac·il·lar·y or ba·cil·lar adj. 1. Shaped like a rod. 2. loads, and continuing transmission (22). The study confirms that adverse events are manageable in the treatment of MDRTB in resource-limited settings. Few patients stopped treatment because of adverse events, which is similar to a previous report. Each project, however, applied intensive approaches to manage adverse events, including altering dosages when appropriate, administering ancillary drugs to treat adverse events, and discontinuing drugs. In addition, all projects conducted special training on adverse events to second-line drugs and used standard protocols for their registration (23). Studies of the cost and cost-effectiveness of MDRTB management have been completed in Estonia (unpub. data), Manila (24), and Tomsk (25). From the health system perspective, the average cost per patient treated was approximately US $3,400 in the Philippines and US $9,000-$10,000 in Estonia and Tomsk. The higher costs in Estonia and Tomsk reflect considerable hospitalization during treatment (30%-50% of overall costs compared to 3% in the Philippines). The second-line drug costs ranged from US $1,600 in the Philippines to US $3,700 in Tomsk; second-line drugs were the highest cost items in the Philippines and Tomsk and the second highest in Estonia. Our study has several limitations. First, risk factors for poor treatment outcomes could not be examined because data were in an aggregate form, not as individual patient data. The second limitation is that the results are not representative of all GLC-approved projects currently functioning. As mentioned, GLC projects are tailored to the local health infrastructure, human and financial resources, and the epidemiologic situation. As a result, costs and outcomes differ between projects. Several projects have been approved by GLC that use standardized treatment regimens based on representative drug resistance surveillance data in relevant patient categories. In settings without a history of second-line drug use, MDRTB control is likely to yield better treatment outcome results. In these settings, susceptibility to the most effective second-line drugs may be preserved, permitting perhaps shorter regimens with fewer, less toxic drugs. As all GLC-approved MDRTB control projects record the same core data, information on success within each of the different approaches will be available within the next 3 years. Conclusion After successful piloting of MDRTB management within TB control programs, WHO and partners have reached the phase of expanding MDRTB control as a component of a comprehensive TB control program, which is described in the WHO guidelines for the treatment of TB (3), the new Stop TB Strategy (15), and in the new WHO guidelines for the programmatic management of drug-resistant tuberculosis (26). As countries are purchasing and using second-line drugs, the likelihood of misuse and creation of strains of TB resistant to all known anti-TB drugs increases. The GLC mechanism offers a way to provide access to care while ensuring rational and effective use of drugs. Beginning in 2002, the Global Fund to Fight AIDS, Tuberculosis and Malaria malaria, infectious parasitic disease that can be either acute or chronic and is frequently recurrent. Malaria is common in Africa, Central and South America, the Mediterranean countries, Asia, and many of the Pacific islands. (GFATM GFATM Global Fund to Fight AIDS, Tuberculosis and Malaria ) mandated that requests for second-line drugs for managing MDRTB should go through GLC to prevent their misuse. The GLC model has been proposed to improve access to malaria (27) and HIV/AIDS HIV/AIDS Human Immunodeficiency Virus/Acquired Immune Deficiency Syndrome treatment (28,29). As of May 2006, a total of 41 MDRTB control projects in 37 countries were endorsed by GLC, and >21,000 MDRTB patients were approved for treatment. The number of GLC-approved MDRTB control programs is increasing rapidly, both as a result of more funding for TB control from the GFATM and mainstreaming of MDRTB management into general TB control efforts. However, with the estimated incidence of 424,203 MDRTB cases, most cases remain undiagnosed and untreated. Expanding projects and accelerating evidence gathering are necessary to further develop international policies. The future success of MDRTB management in resource-limited settings will depend on the ability of the donor The party conferring a power. One who makes a gift. One who creates a trust. donor n. a person or entity making a gift or donation. DONOR. He who makes a gift. (q.v.) community and technical agencies, as well as TB-endemic countries themselves, to expand and strengthen MDRTB control programs. Acknowledgments Other members of the study were Annika Krunner in Estonia; Vija Riekstina and Evija Zarovska in Latvia; Pedro Huamani and Epifanio Sanchez in Peru; Nellie See Sooty albatross V. Mangubat, Ruth B. Orillaza, and Imelda D. Quelapio in the Philippines; and Evgeny (3. Andreev, Aivar K. Strelis, and Tamara P. Tonkel in Tomsk. We are also grateful to former GLC members Malgosia Grzemska, Myriam Henkens, Jim Y. Kim, and Francis Varaine and to Chris Dye and Brian Williams This article is about the American journalist. For other uses, see Brian Williams (disambiguation). Brian Douglas Williams (born May 5, 1959) is an anchor and managing editor of NBC Nightly News, the flagship evening news program of the NBC television network. for critical review of the document. The work was supported in part by grants given to WHO from the US Agency for International Development and the Bill and Melinda Gates Foundation Bill and Melinda Gates Foundation, philanthropic institution founded in 1994 by Microsoft chairman Bill Gates and his wife, Melinda, to improve the lives of the poor throughout the world, primarily through grants for projects relating to global health care, . References (1.) World Health Organization/International Union Against Tuberculosis and Lung Disease. Anti-tuberculosis drug resistance in the world, third global report. 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; 2003. 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Gupta R, Kim JY, Espinal MA, Caudron JM, Pecoul B, Farmer PE, et al. Responding to market failures in tuberculosis control. Science. 2001;293:1049-51. (13.) Gupta R, Cegielski JP, Espinal MA, Henkens M, Kim JY, Lambregtsvan Weezenbeek CS, et al. Increasing transparency (1) The quality of being able to see through a material. The terms transparency and translucency are often used synonymously; however, transparent would technically mean "seeing through clear glass," while translucent would mean "seeing through frosted glass." See alpha blending. in partnerships for health--introducing the Green Light Committee. Trop Med Int Health. 2002;7:970-6. (14.) Laserson KF, Thorpe LE, Leimane V, Weyer K, Mitnick C, Riekstina V, et al. Speaking the same language: treatment outcome definitions for multidrug-resistant tuberculosis. Int J Tuberc Lung Dis. 2005;9:640-5. (15.) Raviglione MC, Uplekar MW. WHO's new Stop TB Strategy. Lancet. 2006;367:952-5. (16.) World Health Organization. Guidelines for surveillance of drug resistance in tuberculosis. Geneva: The Organization; 2003. Publication WHO/CDS/TB/2003.320. Available from http://www.who.int/docstore/gtb/publications/drugresistance/tb_2003_320/ surveillance_guidelinespdf.pdf (17.) World Health Organization. Global tuberculosis control: surveillance, planning, financing. WHO report 2005. Geneva: The Organization; 2005. Publication WHO/HTM/2005.349. Available from http://www.who.int/tb/publications/global_report/2005/en/index.html (18.) Enarson DA, Rieder HL, Arnadottir T, Trebucq A. Management of tuberculosis: a guide for low income countries. Paris: International Union Against Tuberculosis and Lung Disease; 2000. Available from http://www.iuatld.org/pdf/en/guides_publications/management of tb.pdf (19.) World Health Organization. Guidelines for the management of drug-resistant tuberculosis. Geneva: The Organization; 1996. Publication WHO/TB/96.210. Available from http://www.who.int/docstore/gtb/publications/gmdrt/index.htm (20.) Suarez PG, Floyd K, Portocarrero J, Alarcon E, Rapiti E, Ramos G, et al. Feasibility and cost-effectiveness of standardised second-line drug treatment for chronic tuberculosis patients: a national cohort study in Peru. Lancet. 2002;359:1980-9. (21.) Turett GS, Telzak EE, Torian LV, Blum S Blum , Léon 1872-1950. French socialist politician who served as premier (1936-1937, 1938, and 1946-1947). He was imprisoned (1940-1945) by the Vichy government during World War II. , Alland D, Weisfuse I, et al. Improved outcomes for patients with multidrug-resistant tuberculosis. Clin infect Dis. 1995;21:1238-44. (22.) Park MM, Davis AL, Schluger NW, Cohen cohen or kohen (Hebrew: “priest”) Jewish priest descended from Zadok (a descendant of Aaron), priest at the First Temple of Jerusalem. The biblical priesthood was hereditary and male. H, Rom WN. Outcome of MDR-TB patients, 1983-1993. Prolonged pro·long tr.v. pro·longed, pro·long·ing, pro·longs 1. To lengthen in duration; protract. 2. To lengthen in extent. survival with appropriate therapy. Am J Respir Crit Care Med. 1996;153:317-24. (23.) Nathanson E, Gupta R, Huamani P, Leimane V, Pasechnikov AD, Tupasi TE, et al. Adverse events in the treatment of multidrug-resistant tuberculosis: results from the DOTS-Plus initiative. Int J Tuberc Lung Dis. 2004;8:1382-4. (24.) Tupasi TE, Gupta R, Quelapio ID, Orillaza RB, Mira NR, Mangubat NV, et al. Feasibility and cost-effectiveness of treating patients with multidrug-resistant tuberculosis using the DOTS-Plus strategy: a cohort study in the Philippines. PLoS Medicine PLoS Medicine is a scientific journal covering the full spectrum of the medical sciences it began operation on October 19, 2004. It was the second journal of the Public Library of Science (PLoS) a non-profit organization which releases scientific content under open access . 2006. In press. (25.) World Health Organization. The feasibility and efficiency of controlling MDR-TB using the DOTS-Plus strategy in the Russian Federation. Geneva: The Organization; 2005. Publication WHO/HTM/TB/2005.357C. Available from http://whqlibdoc. who.int/hq/2005/WHO_HTM_TB_2005.357_3_eng.pdf (26.) World Health Organization. Guidelines for the programmatic management of drug-resistant tuberculosis. Geneva: The Organization; 2006. Publication WHO/HTM/2006.361. Available from http://whqlibdoc.who.int/publications/2006/9241546956_eng.pdf (27.) Attaran A, Barnes KI, Curtis C, d'Alessandro U, Fanello CI, Galinski MR, et al. WHO, the Global Fund, and medical malpractice Improper, unskilled, or negligent treatment of a patient by a physician, dentist, nurse, pharmacist, or other health care professional. in malaria treatment. Lancet. 2004;363:237-40. (28.) Gupta R, Irwin A, Raviglione MC, Kim JY. Scaling up treatment for HIV/AIDS: lessons learned from multidrug-resistant tuberculosis. Lancet. 2004;363:320-4. (29.) Farmer P, Leandre F, Mukherjee JS, Claude M, Nevil P, Smith-Fawzi MC, et al. Community based approaches to HIV treatment in resource poor settings. Lancet. 2001;358:404-9. Eva Nathanson, * Catharina Lambregts-van Weezenbeek, ([dagger]) Michael L. Rich, ([double dagger double dagger n. A reference mark (  ) used in printing and writing. Also called diesis.Noun 1. ]) Rajesh Gupta, * Jaime Bayona, ([double dagger])([section]) Kai kai Noun NZ informal food [Maori] kai noun N.Z. (informal) food, grub (slang) provisions, fare, board, commons, eats (slang Blondal, ([dagger]) Jose A. Caminero, ([paragraph]) J. Peter Cegielski, # Manfred Danilovits, ** Marcos A. Espinal, * Vahur Hollo, ([dagger])([dagger]) Ernesto Jaramillo, * Vaira Leimane, ([double dagger])([double dagger]) Carole D. Mitnick, ([subsection subsection Noun any of the smaller parts into which a section may be divided Noun 1. subsection - a section of a section; a part of a part; i.e. ]) Joia S Joia is a Swedish record label founded by Luciano Ingrosso, uncle to Sebastian Ingrosso. Joia is one of Sweden's largest house music labels. Joia has a sublabel called Nero. . Mukherjee, ([subsection]) Paul Nunn, * Alexander Pasechnikov, ([double dagger]) ([paragraphs]) Thelma Tupasi, (##) Charles Wells, (#) and Marie C. Raviglione * * World Health Organization, Geneva, Switzerland; ([dagger]) KNCV KNCV Koninklijke Nederlandse Chemische Vereniging (Royal Dutch Chemical Association) KNCV Koninklijke Nederlandse Centrale Vereniging tot bestrijding der Tuberculose (Dutch Tuberculosis Foundation) Tuberculosis Foundation, The Hague, the Hague, The (hāg), Du. 's Gravenhage or Den Haag, Fr. La Haye, city (1994 pop. 445,279), administrative and governmental seat of the Kingdom of the Netherlands, capital of South Holland prov., W Netherlands, on the North Sea. Netherlands; ([double dagger]) Partners In Health, Boston, Massachusetts “Boston” redirects here. For other uses, see Boston (disambiguation). Boston is the capital and most populous city of Massachusetts.[3] The largest city in New England, Boston is considered the unofficial economic and cultural center of the entire New , USA; ([section]) Socios En Salud, Lima, Peru; ([paragraph]) International Union Against Tuberculosis and Lung Disease, Paris, France; # 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. , Atlanta, Georgia, USA; ** Tartu University Clinics, Tartu, Estonia; ([dagger]) ([dagger]) National TB Programme, Tallinn, Estonia; ([double dagger]) ([double dagger]) State Centre of Tuberculosis and Lung Diseases of Latvia, Riga, Latvia; ([subsection]) Harvard Medical School Harvard Medical School (HMS) is one of the graduate schools of Harvard University. It is a prestigious American medical school located in the Longwood Medical Area of the Mission Hill neighborhood of Boston, Massachusetts. , Boston, Massachusetts, USA; ([paragraphs]) MDR-TB Project in Tomsk Oblast, Tomsk, Russian Federation; and ## Makati Medical Center, Makati, the Philippines Ms Nathanson has spent the last 8 years working at WHO to control TB and MDRTB, primarily in the countries of the former Soviet Union but also worldwide. Her main research interests are programmatic management of TB and MDRTB. Address for correspondence: Eva Nathanson, Stop TB Department, World Health Organization, 20 Ave Appia CH-1211, Geneva, Switzerland; email: nathansone@who.int
Table 1. Treatment outcome definitions for multidrug-resistant
tuberculosis (MDRTB) patients (14)
Category Definition
Cure Completed treatment according to country protocol
and been consistently culture-negative ([greater
than or equal to] 5 results) for final 12 mo of
treatment. If only 1 positive culture is reported
during that time with no concomitant clinical
evidence of deterioration, patient may still be
considered cured, provided that positive culture
is followed by >3 consecutive negative cultures
taken [greater than or equal to] 30 d apart.
Treatment Completed treatment according to country protocol
completed but does not meet definition for cure or treatment
failure because of lack of bacteriologic results
(i.e., [less than or equal to] 5 cultures were
performed in the final 12 mo of therapy).
Death Died for any reason during the course of MDRTB
treatment.
Treatment Treatment was interrupted for [greater than or
default equal to] 2 consecutive months for any reason.
Treatment [greater than or equal to] 2 of 5 cultures recorded
failure in the final 12 mo are positive or if any of the final
3 cultures is positive. Treatment will also be considered
to have failed if a clinical decision has been made to
terminate treatment early due to poor response or adverse
events.
Transfer Transferred to another reporting and recording unit
out and the treatment outcome is unknown.
Table 2. Description of MDRTB control programs *
Factor Estonia Latvia
Start of enrollment 1 Aug 2001 1 Jan 2001
Project size Country Country
Project population 1,364,101 2,350,000
Prisons included? Yes Yes
% MDRTB, new cases 11.9 9.8
(2002)
% MDRTB, previously 29.3 26.7
treated cases (2002)
Voluntary HIV Yes Yes
counseling/testing?
Empiric regimen? No Yes
([double dagger])
Surgery used? Yes Yes
DOT (days per wk) 7 hosp, 6 amb 7 hosp, 5-6 amb
Incentives to patients? Yes Yes
Incentives to providers? Yes No
Culture monitoring Monthly Monthly
X-ray monitoring Every 3 mo Every 3 mo
Drugs for which DST is H, R, E, S, Z, Amk, H, R, E, S, Z, Cm,
performed ([section]) Cm, Eth, Km, Ofx, Cs, Eth, Km, Ofx,
Pth Pas, T
Factor Lima Manila
Start of enrollment 1 Feb 1999 15 Apr 1999
Project size Region District
Project population 7,748,258 9,930,000
Prisons included? Yes (1 prison) No
% MDRTB, new cases NA ([dagger]) NA ([dagger])
(2002)
% MDRTB, previously NA ([dagger]) NA ([dagger])
treated cases (2002)
Voluntary HIV Yes No
counseling/testing?
Empiric regimen? Yes No
([double dagger])
Surgery used? Yes No
DOT (days per wk) 6 6
Incentives to patients? Yes No
Incentives to providers? Yes No
Culture monitoring Monthly Monthly
X-ray monitoring Every 6 mo Every 6 mo
Drugs for which DST is H, R, E, S, Z, Amk, H, R, E, S, Z,
performed ([section]) Cfx, Cm, Cs, Eth, Amc, ([section])
Km Amk, Km, Cfx, Clr,
([section]) Lfx, Ofx
Factor Tomsk
Start of enrollment 12 Sep 2000
Project size Region
Project population 1,032,400
Prisons included? Yes
% MDRTB, new cases 13.7
(2002)
% MDRTB, previously 43.6
treated cases (2002)
Voluntary HIV Yes
counseling/testing?
Empiric regimen? Yes
([double dagger])
Surgery used? Yes
DOT (days per wk) 6
Incentives to patients? Yes
Incentives to providers? Yes
Culture monitoring Monthly
X-ray monitoring Every 3 mo
Drugs for which DST is H, R, E, S, Z, Cm,
performed ([section]) Cs, Km, Ofx, Pas,
Pth
* MDRTB, multidrug-resistant tuberculosis; NA, not applicable;
DOT, directly observed treatment; hosp, hospital; amb, ambulatory;
DST, drug susceptibility testing; H, isoniazid; R, rifampin; E,
ethambutol; S, streptomycin; Z, pyrazinamide; Amk, amikacin; Cm,
capreomycin; Eth, ethionamide; Km, kanamycin; Ofx, ofloxacin; Pth,
prothionamide; Cs, cycloserine; Pas, p-aminosalicylic acid; T,
thiacetazone; Cfx, ciprofloxacin; Amc, amoxicillin-clavulanic acid;
Clr, clarithromycin; Lfx, levofloxacin.
([dagger]) Lima and Manila do not perform routine drug resistance
surveillance.
([double dagger]) Use of treatment regimens based on the history
of drugs used by the patient while awaiting DST results.
([section]) Amc and Clr and are not included on the World Health
Organization Model List of Essential Drugs and are therefore not
purchased through the Green Light Committee. However, each project
used additional drugs at its discretion.
Table 3. Frequency of drugs used in multidrug-resistant tuberculosis
control program treatment regimens
Drug Estonia, n (%) Latvia, n (%)
Ethambutol 44 (95.7) 117 (47.8)
Pyrazinamide 1 (2.2) 99 (40.4)
Streptomycin 1 (2.2) 9 (3.7)
Capreomycin 11 (23.9) 115 (46.9)
Cycloserine 45 (97.8) 189 (77.1)
Ciprofloxacin 0 0
Clofazimine 0 0
Kanamycin 7 (15.2) 129 (52.7)
Levofloxacin 1 (2.2) 0
Ofloxacin 35 (76.1) 242 (98.8)
p-Aminosalicylic acid 26 (56.6) 71 (29.0)
Prothionamide or ethionamide 38 (82.6) 154 (62.9)
Augmentin 4 (8.7) 7 (2.9)
Clarithromycin 4 98.7) 1 (0.4)
Sparfloxacin 0 0
Thiacetazone 0 164 (66.9)
Drug Lima n (%) Manila, n (%)
Ethambutol 102 (20.1) 43 (41.0)
Pyrazinamide 146 (28.7) 88 (83.8)
Streptomycin 104 (20.5) 51 (48.6)
Capreomycin 199 (39.2) 23 (21.9)
Cycloserine 316 (62.2) 100 (95.2)
Ciprofloxacin 257 (50.6) 18 (17.1)
Clofazimine 13 (2.6) 0
Kanamycin 167 (32.9) 91 (86.7)
Levofloxacin 0 30 (28.6)
Ofloxacin 44 (8.7) 87 (82.9)
p-Aminosalicylic acid 323 (63.3) 98 (93.3)
Prothionamide or ethionamide 244 (48.0) 104 (99.0)
Augmentin 325 (64.0) 0
Clarithromycin 67 (13.2) 46 (43.8)
Sparfloxacin 0 14 (13.3)
Thiacetazone 0 0
Drug Tomsk, n (%) Total, n (%)
Ethambutol 28 (19.6) 334 (31.9)
Pyrazinamide 84 (58.7) 418 (39.9)
Streptomycin 0 165 (15.8)
Capreomycin 94 (65.7) 442 (42.2)
Cycloserine 142 (99.3) 792 (75.6)
Ciprofloxacin 0 275 (26.3)
Clofazimine 0 13 (1.2)
Kanamycin 47 (32.9) 441 (42.1)
Levofloxacin 0 31 (3.0)
Ofloxacin 142 (99.3) 550 (52.5)
p-Aminosalicylic acid 118 (82.5) 636 (60.7)
Prothionamide or ethionamide 94 (65.7) 634 (60.6)
Augmentin 2 (1.4) 338 (32.3)
Clarithromycin 3 (2.1) 121 (11.6)
Sparfloxacin 0 14 (1.3)
Thiacetazone 0 164 (15.7)
Table 4. Multidrug-resistant tuberculosis control program cohort
characteristics *
Characteristic Estonia n (%) Latvia, n (%)
Total no. cases 46 (100.0) 245 (100.0)
New cases 22 (47.8) 91 (37.1)
Previously treated cases 24 (52.2) 154 (62.9)
Cases previously treated 19 (79.2) 132 (85.7)
with first- line drugs
Cases previously treated 5 (20.8) 22 (14.3)
with first- and second-line
drugs
Resistance to only H and R 0 7 (2.9)
Resistance to only H, R, and 0 78 (31.8)
other first-line drugs
Resistance to first- and 46 (100.0) 160 (65.3)
second-line drugs
Treatment cessation because 3 (6.5) 5 (2.0)
of adverse events
HIV coinfection 0 11 (4.5)
Surgery performed 1 (2.2) 18 (7.30
No. patients hospitalized 41 (89.1) 245 (100.0)
Average no. drugs in 5.4 5.5
treatment regimen
Characteristic Lima, n (%) Manila, n (%)
Total no. cases 508 (100.0) 105 (100.0)
New cases 1 (0.20 5 (4.8)
Previously treated cases 507 (99.8) 100 (95.2)
Cases previously treated 125 (25.0) 53 (54.6)
with first- line drugs ([dagger]) ([dagger])
Cases previously treated 376 (75.0) 44 (45.4)
with first- and second-line ([dagger]) ([dagger])
drugs
Resistance to only H and R 11 (2.2) 9 (8.60
Resistance to only H, R, and 182 (35.8) 26 (24.8)
other first-line drugs
Resistance to first- and 315 (62.0) 70 (66.7)
second-line drugs
Treatment cessation because NA 9 (8.6)
of adverse events
HIV coinfection 5 (1.0) NA
Surgery performed 78 (15.4) 0
No. patients hospitalized NA 5 (5.0)
Average no. drugs in NA 6.28
treatment regimen
Characteristic Tomsk, n (%) Total, n (%)
Total no. cases 143 (100.0) 1,047 (100.0)
New cases 0 119 (11.4)
Previously treated cases 143 (100.0) 928 (88.6)
Cases previously treated 109 (76.2) 438 (47.7)
with first- line drugs
Cases previously treated 34 (23.8) 481 (52.3)
with first- and second-line
drugs
Resistance to only H and R 0 27 (2.6)
Resistance to only H, R, and 55 (38.5) 341 (32.6)
other first-line drugs
Resistance to first- and 88 (61.5) 679 (64.9)
second-line drugs
Treatment cessation because 0 17 (3.2)
of adverse events
HIV coinfection 0 16 (1.7)
Surgery performed 17 (11.9) 114 (10.9)
No. patients hospitalized 71 (49.7) 362 (67.2)
Average no. drugs in 5.3
treatment regimen
* H, isoniazid; R, rifampin; NA, not applicable.
([dagger]) Information is lacking from 6 patients (Lima) and
3 patients (Manila) on previous treatment with first-line drugs
only or with first- and second-line drugs.
Table 5. Treatment outcomes of new, previously treated, and all
multidrug-resistant tuberculosis patients
Patients Estonia, n (%) Latvia, n (%)
New patients
Cured 16 (72.7) 72 (79.1)
Completed 1 (4.5) 1 (1.1)
Default 3 (13.6) 13 (14.3)
Failed 1 (4.5) 4 (4.4)
Died 1 (4.5) 1 (1.1)
Transferred 0 0
Total 22 (100.0) 91 (100.0)
Treatment success 17 (77.3) 73 (80.2)
Previously treated patients
Cured 12 (50.0) 93 (60.4)
Completed 1 (4.2) 2 (1.3)
Default 4 (16.7) 27 (17.5)
Failed 3 (12.5) 24 (15.6)
Died 4 (16.7) 8 (5.2)
Transferred 0 0
Total 24 (100.0) 154 (100.0)
Treatment success 13 (54.2) 95 (61.7)
All patients
Cured 28 (60.9) 165 (67.3)
Completed 2 (4.3) 3 (1.2)
Default 7 (15.2) 40 (16.3)
Failed 4 (8.6) 28 (11.4)
Died 5 (10.9) 9 (3.7)
Transferred 0 0
Total 46 (100.0) 245 (100.0)
Treatment success 30 (65.2) 168 (68.6)
Patients Lima, n (%) Manila, n (%)
New patients
Cured 0 1 (20.0)
Completed 0 1 (20.0)
Default 0 2 (40.0)
Failed 0 0
Died 1 (100.0) 1 (20.0)
Transferred 0 0
Total 1 (100.0) 5 (100.0)
Treatment success 0 2 (40.0)
Previously treated patients
Cured 351 (69.2) 60 (60.0)
Completed 0 0
Default 40 (7.9) 12 (12.0)
Failed 17 (3.4) 12 (12.0)
Died 98 (19.3) 15 (15.0)
Transferred 1 (0.2) 1 (1.0)
Total 507 (100.0) 100 (100.0)
Treatment success 351 (69.2) 60 (60.0)
All patients
Cured 351 (69.1) 61 (58.2)
Completed 0 1 (1.0)
Default 40 (7.9) 14 (13.3)
Failed 17 (3.3) 12 (11.4)
Died 99 (19.5) 16 (15.2)
Transferred 1 (0.2) 1 (1.0)
Total 508 (100.0) 105 (100.0)
Treatment success 351 (69.1) 62 (59.0)
Patients Tomsk, n (%) Total, n (%)
New patients
Cured 0 89 (74.8)
Completed 0 3 (2.5)
Default 0 18 (15.1)
Failed 0 5 (4.2)
Died 0 4 (3.4)
Transferred 0 0
Total 0 119 (100.0)
Treatment success 0 92 (77.3)
Previously treated patients
Cured 118 (82.5) 634 (68.3)
Completed 0 3 (0.3)
Default 9 (6.3) 92 (9.9)
Failed 9 (6.3) 65 (7.0)
Died 7 (4.9) 132 (14.2)
Transferred 0 2 (0.2)
Total 143 (100.0) 928 (100.0)
Treatment success 118 (82.5) 637 (68.6)
All patients
Cured 118 (825) 723 (69.1)
Completed 0 6 (0.6)
Default 9 (6.3) 110 (10.5)
Failed 9 (6.3) 70 (6.7)
Died 7 (4.9) 136 (13.0)
Transferred 0 2 (0.2)
Total 143 (100.0) 1047 (100.0)
Treatment success 118 (82.5) 729 (69.6)
Table 6. Clinical and bacteriologic progress after cure or treatment
completion and number of relapses identified by the beginning of 2006
Characteristic Estonia Latvia
Duration of follow-up after cure 36 24
or treatment completion (mo)
Frequency of follow-up after cure Every 6 mo Every 6 mo
or treatment completion
No. cured or completed treatment 30 168
No. followed up * 30 168
No. cured or completed treatment 3 5
who relapsed by 2006
Relapse rate (95% confidence interval) 10.0% 3.0%
(2.11-26.53) (0.97-6.81)
Characteristic Lima Manila
Duration of follow-up after cure 12 24
or treatment completion (mo)
Frequency of follow-up after cure Every 3 mo Every 6 mo
or treatment completion
No. cured or completed treatment 351 62
No. followed up * 351 62
No. cured or completed treatment 4 1
who relapsed by 2006
Relapse rate (95% confidence interval) 1.1% 1.6%
(0.31-2.89) (0.04-8.66)
Characteristic Tomsk Total
Duration of follow-up after cure 12
or treatment completion (mo)
Frequency of follow-up after cure Every 6 mo
or treatment completion
No. cured or completed treatment 118 729
No. followed up * 59 670
No. cured or completed treatment 1 14
who relapsed by 2006
Relapse rate (95% confidence interval) 1.7% 2.1%
(0.04-9.09) (1.14-3.51)
* In Tomsk, 59 patients left the region after having been declared
cured. These patients were lost to follow-up.
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