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Initial Treatment of Tuberculosis Your name Institution/organization Meeting Date International Standards 7, 8, 10, 13, 17, 21 Initial Treatment of Tuberculosis Objectives: At the end of this presentation, participants will have an understanding of: Drug regimens used in the initial treatment of both pulmonary and extrapulmonary tuberculosis The basis for the public health benefits of treating tuberculosis The clinical and microbiological effects of treatment The rationale for patient monitoring and reporting The main adverse effects of antituberculosis drugs ISTC TB Training Modules 2009 Initial Treatment of Tuberculosis Overview: Effect of appropriate treatment on public health First-line treatment recommendations Treatment of extrapulmonary tuberculosis Monitoring of treatment Adverse reactions Recording and reporting International Standards 7, 8, 10, 13, 17, and 21 ISTC TB Training Modules 2009 Standards for Treatment ISTC TB Training Modules 2009 Initial Treatment of Tuberculosis Standards 7 & 8 ISTC TB Training Modules 2009 Standard 7: Public Health Responsibility Any practitioner treating a patient for tuberculosis is assuming an important public health responsibility to prevent ongoing transmission of the infection and the development of drug resistance. To fulfill this responsibility the practitioner must not only prescribe an appropriate regimen, but also utilize local public health services and other agencies, when necessary, to assess the adherence of the patient and to address poor adherence when it occurs. ISTC TB Training Modules 2009 Effect of Treatment on Public Health Why is TB Treatment a Public Health Measure? Effective treatment rapidly kills organisms, reducing the bacillary population in respiratory secretions, thus reducing the potential for transmission. Effective multiple-drug treatment greatly reduces the risk of resistant organisms emerging. Effective treatment decreases the duration and severity of illness and reduces the risk of death. ISTC TB Training Modules 2009 Effect of Treatment on Public Health Pulmonary TB cases/100,000 Effects of Treatment on the Incidence of Tuberculosis in Peru 220 DOTS 1990 200 case finding 180 160 140 120 100 PTB falling at 6%/yr 1980 ISTC TB Training Modules 2009 1985 1990 1995 2000 Standard 8: Initiation of Treatment (1 of 2) All patients (including those with HIV infection) who have not been treated previously should receive an internationally accepted first-line treatment regimen using drugs of known bioavailability. The initial phase should consist of two months of isoniazid (INH), rifampicin (RIF), pyrazinamide (PZA), and ethambutol (EMB). ISTC TB Training Modules 2009 Effect of Treatment on Bacillary Population Mixed population (susceptible and resistant) INH resistant bacilli Log cfu Emergence of INH resistant strain because of ineffective treatment (INH monotherapy) Effective multi-drug therapy 0 2 4 6 8 10 12 14 Weeks ISTC TB Training Modules 2009 16 18 20 22 24 Unintended Monotherapy and Resistance Months of Rx 0 5 7 9 Smear + + + + Culture + + + + INH R* R R R RIF S* R R R EMB S* S S R INH RIF EMB Susceptibility * Results not known to clinician ISTC TB Training Modules 2009 Treatment Goals Microbiological Goals of Antituberculosis Chemotherapy Kill tubercle bacilli rapidly (early bactericidal effect) Prevent the emergence of drug resistance Eliminate persistent bacilli to prevent relapse (sterilizing effect) ISTC TB Training Modules 2009 Activities of Antituberculosis Drugs Drug Early bactericidal activity Preventing drug resistance Sterilizing activity Isoniazid ++++ +++ ++ Rifampicin ++ +++ ++++ Pyrazinamide + + +++ Streptomycin ++ ++ ++ Ethambutol ++ - +++ ++ + Highest ++++ ISTC TB Training Modules 2009 High +++ Intermediate ++ Low + Standard 8: Continuation of Treatment (2 of 2) The continuation phase should consist of isoniazid and rifampicin given for four months The doses of antituberculosis drugs used should conform to international recommendations Fixed-dose combinations (FDCs) of two (INH and RIF), three (INH, RIF, and PZA), and four (INH, RIF, PZA, and EMB) drugs are highly recommended ISTC TB Training Modules 2009 Treatment Recommendations New Patients (not previously treated) Initial Phase Continuation Phase (2 months) (4 months) INH, RIF, PZA, EMB daily INH, RIF daily INH, RIF, PZA, EMB1 3x/wk. INH, RIF 3x/wk 1. Associated with higher rate of acquired drug resistance and must be given using directly-observed therapy. Where feasible, daily dosing is preferred. May consider daily initiation phase, then 3x week continuation phase. 3x weekly dosing not recommended if living with HIV or living in an HIV-prevalent setting. ISTC TB Training Modules 2009 Dose Recommendations Adults: mg/kg (range) Drug Daily 3x Week INH 5 (4-6), max 300/d 10 (8-12), max 900/d RIF 10 (8-12), max 600/d 10 (8-12) max 600/ d PZA 25 (20-30), max 2000/d 35 (30-40), max 3000/d EMB 15 (15-20), max 1600/d 30 (25-35), max 2400/d Streptomycin ISTC TB Training Modules 2009 15 (12-18) 15 (12-18) Standard 17: Treat Co-morbid Disease (1 of 2) All providers should conduct a thorough assessment for co-morbid conditions that could affect tuberculosis treatment response or outcome At the time the treatment plan is developed, the provider should identify additional services that would support an optimal outcome for each patient and incorporate these services into an individualized plan of care ISTC TB Training Modules 2009 Standard 17: Treat Co-morbid Disease (2 of 2) This plan should include assessment of and referrals for treatment of other illnesses with particular attention to those known to affect treatment outcome, for instance care for diabetes mellitus, drug and alcohol treatment programs, tobacco smoking cessation programs, and other psychosocial support services, or to such services as antenatal or well baby care ISTC TB Training Modules 2009 Treatment of Extrapulmonary TB ISTC TB Training Modules 2009 Treatment of Extrapulmonary TB In general, extrapulmonary tuberculosis is treated the same as pulmonary tuberculosis Some experts recommend extending the duration of therapy in patients with: • Meningeal tuberculosis • Bone/joint tuberculosis Corticosteroids may be useful adjunctive treatment in some forms of extrapulmonary tuberculosis ISTC TB Training Modules 2009 Treatment of Extrapulmonary TB Treatment Duration and Use of Steroids Site Lymph node Length of Rx (mos.) Corticosteroids 6 No 6-9 No Pleural 6 No Pericarditis 6 Yes 9-12 Yes Disseminated 6 No Genitourinary 6 No Abd/Peritoneal 6 No Bone/Joint CNS ISTC TB Training Modules 2009 Monitoring Treatment for TB and Public Health Reporting Standards 10, 13, & 21 ISTC TB Training Modules 2009 Standard 10: Monitoring Treatment (1 of 2) Response to therapy in patients with pulmonary tuberculosis should be monitored by follow-up sputum smear microscopy (2 specimens) at the time of completion of the initial phase of treatment (2 months). If the sputum smear is positive at completion of the initial phase, sputum smears should be examined again at 3 months and, if possible, culture and drug susceptibility testing should be performed. ISTC TB Training Modules 2009 1 of 2 Standard 10: Monitoring Treatment (2 of 2) In patients with extrapulmonary TB and in children, the response to treatment is best assessed clinically. ISTC TB Training Modules 2009 2 of 2 Monitoring: Timing of Sputum Specimens Initial Phase Continuation Phase Isoniazid Rifampicin Pyrazinamide Ethambutol Months 0 Diagnostic 1 2 3 End of intensive phase 4 5 Assessment for failure 6 Completion [*Obtain if smear-positive at month 2] ISTC TB Training Modules 2009 Treatment Outcomes for Pulmonary TB 1.2% 10% 50% Dead 64% Sputum negative 98% Sputum positive 32% 18% 20% 0.8% No Poor Good Chemotherapy Chemotherapy Chemotherapy Grzybowski S et al, Bull Int Union Tuberc 1978; (53)2: 70-5 ISTC TB Training Modules 2009 Monitoring: Adverse Reactions Adverse Reaction Drugs Rash PZA, INH, RIF, EMB Gastrointestinal intolerance PZA, RIF Liver toxicity PZA, INH, RIF Peripheral neuropathy INH, (EMB) Optic neuritis EMB Gout PZA • Drugs are listed in order of relative likelihood of causing adverse reaction. • INH/RIF and RIF/PZA appear to have synergistic effects in causing hepatitis ISTC TB Training Modules 2009 Adverse Reactions: Rash Classic drug-related rash Severe skin rash from thioacetazone ISTC TB Training Modules 2009 Drug-induced Hepatotoxicity Hepatotoxic reactions: Transaminase elevation age-dependent with INH Transaminase elevation dose-dependent with PZA Cholestasis (increase in bilirubin and alkaline phosphatase) with RIF Symptoms imply significant hepatotoxicity (Mild transaminase elevation may not be clinically significant) ISTC TB Training Modules 2009 Managing Hepatotoxicity Management Hold all medications and follow liver enzymes for significant hepatotoxicity Re-challenge depends on circumstances and severity of liver dysfunction In general, patients should be restarted with EMB (the least hepatotoxic drug) and RIF, usually followed in several days by INH if there is no worsening of liver function ISTC TB Training Modules 2009 Standard 13: Monitoring Record A written record of all medications given, bacteriologic response, and adverse reactions should be maintained for all patients ISTC TB Training Modules 2009 Standard 21: Reporting Cases All providers must report both new and retreatment tuberculosis cases and their treatment outcomes to local public health authorities, in conformance with applicable legal requirements and policies. ISTC Training TB Training Modules Modules 2008 2009 Initial Treatment of Tuberculosis Summary: Appropriate treatment and assessment of adherence to treatment is an important public health issue. The use of internationally accepted firstline treatment regimens is associated with a high cure rate and a low risk of acquired drug resistance. ISTC TB Training Modules 2009 Initial Treatment of Tuberculosis Summary (cont.): Pulmonary and extrapulmonary TB are generally treated with the same regimens. (Exception: extended duration in meningeal and bone/joint disease.) Treatment includes assessment and services for co-morbid conditions that may effect tuberculosis treatment outcomes Monitoring for both response to treatment and for potential adverse events is essential. ISTC TB Training Modules 2009 Summary: ISTC Standards Covered* Standard 7: Practitioners assume an important public health responsibility in ensuring both appropriate treatment regimens and assessment of treatment adherence for their patients. * Abbreviated versions ISTC TB Training Modules 2009 Summary: ISTC Standards Covered* Standard 8: All patients (including those with HIV infection) who have not been previously treated should receive an internationally accepted treatment regimen of known bioavailability: • Initial phase: 2 months INH, RIF, PZA, and EMB • Continuation phase: 4 months INH and RIF The doses of anti-TB drugs used should conform to international recommendations. Fixed-dose combinations are highly recommended. * Abbreviated versions ISTC TB Training Modules 2009 Summary: ISTC Standards Covered* Standard 10: Response to therapy in patients with pulmonary TB should be monitored by followup 2 sputum smears at the end of the initial phase, and if positive, repeated at the end of 3 months (if positive at 3 months, obtain culture and DST). In extrapulmonary TB and in children, the response to treatment is best assessed clinically. * Abbreviated versions ISTC TB Training Modules 2009 Summary: ISTC Standards Covered* Standard 13: A written record of all medications given, bacteriologic responses, and adverse reactions should be maintained for all patients. Standard 17: All providers should conduct a thorough assessment and provide services or referrals for co-morbid conditions with particular attention to those known to effect treatment outcome * Abbreviated versions ISTC TB Training Modules 2009 Summary: ISTC Standards Covered* Standard 21: All providers must report both new and retreatment TB cases and their treatment outcomes to local public health authorities * Abbreviated versions ISTC TB Training Modules 2009 Alternate Slides ISTC TB Training Modules 2009 Purpose of ISTC ISTC TB Training Modules 2009 ISTC: Key Points 21 Standards (revised/renumbered in 2009) Differ from existing guidelines: standards present what should be done, whereas, guidelines describe how the action is to be accomplished Evidence-based, living document Developed in tandem with Patients’ Charter for Tuberculosis Care Handbook for using the International Standards for Tuberculosis Care ISTC TB Training Modules 2009 ISTC: Key Points Audience: all health care practitioners, public and private Scope: diagnosis, treatment, and public health responsibilities; intended to complement local and national guidelines Rationale: sound tuberculosis control requires the effective engagement of all providers in providing high quality care and in collaborating with TB control programs ISTC TB Training Modules 2009 Questions ISTC TB Training Modules 2009 Initial Treatment of Tuberculosis 1. A 28 year-old woman taking standard four-drug treatment for TB for five weeks now complains of nausea, vomiting, and right upper-quadrant discomfort. When seen in clinic she is noted to have scleral icterus and right upper-quadrant tenderness. Her urine is dark colored. What is the appropriate action to take at this time? A. Stop all drugs B. Stop isoniazid C. Give pyridoxine (vitamin B6) D. Replace pyrazinamide with streptomycin ISTC TB Training Modules 2009 Initial Treatment of Tuberculosis 2. A 68 year-old woman with smear-positive TB needs to start treatment. She lives too far to be given directlyobserved treatment (DOT) by your office. Which treatment regimen is preferred for this patient? A. Isoniazid and ethambutol for twelve months B. Isoniazid/rifampicin/ethambutol for the first two months, followed by isoniazid/rifampicin for an additional four months C. Fixed-dose combination of isoniazid/rifampicin/pyrazinamide for nine months D. Fixed-dose combinations of isoniazid/rifampicin/ethambutol/pyrazinamide for the first two months, followed by isoniazid/rifampicin for an additional four months ISTC TB Training Modules 2009 Initial Treatment of Tuberculosis 3. In considering treatment for extrapulmonary disease, all of the following statements are correct except: A. Extrapulmonary disease is a sign of disseminated disease, and therefore always requires a longer duration of treatment B. Most presentations of extrapulmonary TB can be treated with the same standard six month regimens used for pulmonary TB C. Extending the duration of therapy is recommended by many experts for central nervous system (CNS) and bone/joint extrapulmonary TB D. Corticosteroids are sometimes recommended for pericardial and central nervous system (CNS) extrapulmonary TB ISTC TB Training Modules 2009