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Treatment of Tuberculosis: New Case Module 7A – March 2010.

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Presentation on theme: "Treatment of Tuberculosis: New Case Module 7A – March 2010."— Presentation transcript:

1 Treatment of Tuberculosis: New Case Module 7A – March 2010

2 Project Partners Funded by the Health Resources and Services Administration (HRSA)

3 Module Overview  Drugs and treatment standards  Standard new case regimens and dosages  Treatment of EPTB and in special situations Smear-negative PTB Pregnancy Liver disorders Renal disease International Standards 7, 8 & 10

4 Learning Objectives At the end of this presentation, participants will be able to:  Describe the drug regimens used to treat new TB cases (pulmonary and extrapulmonary)  Identify treatment and management approaches in special situations (e.g., smear-negative PTB, pregnancy, presence of co-morbidities)  Describe the essential monitoring based on site of disease, bacteriological status, and in special populations

5 First Line Anti-Tuberculosis Drugs  Isoniazid (INH, H)  Rifampicin (RIF, R)  Pyrazinamide (PZA, Z)  Ethambutol (EMB, E)  Streptomycin (SM, S)

6 Standards for Treatment

7 Standard 7: Public Health Effects of Treatment Practitioners assume an important public health responsibility in ensuring both appropriate treatment regimens and assessment of treatment adherence for their patients.

8 Effect of Treatment on Public Health Why is TB Treatment a Public Health Measure?  Providing the patient with an effective treatment that kills the organisms will rapidly reduce and ultimately eliminate the bacillary population in respiratory secretions, thus reducing the potential for transmission  Effective multiple-drug treatment, using fixed-dose combination tablets, greatly reduces the risk of resistant organisms emerging  Effective treatment decreases the duration and severity of illness and reduces the risk of death

9 Effect of Treatment on Public Health (2) 100 120 140 160 180 200 220 1980198519901995 2000 Pulmonary TB cases/100,000 DOTS 1990 PTB falling at 6%/yr case finding Effects of Treatment on the Incidence of Tuberculosis in Peru

10 Standard 8: Treatment New Cases 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 2 months of isoniazid, rifampicin, pyrazinamide and ethambutol  The continuation phase should consist of isoniazid and rifampicin given for four months

11 Antituberculosis Drug Activity Drug Early bactericidal activity Preventing drug resistance Sterilizing activity Isoniazid +++++++++ Rifampicin +++++++++ Pyrazinamide +++++ Ethambutol ++ - ++++++ Highest ++++ High +++ Intermediate ++ Low +

12 Microbiological Goals - Anti-TB Drugs  Kill tubercle bacilli rapidly (early bactericidal effect)  Prevent the emergence of drug resistance  Eliminate persistent bacilli to prevent relapse (sterilizing effect) Microbiological Goals of Antituberculosis Chemotherapy

13 Adequate TB treatment requires:  An appropriate combination of anti-TB medications to prevent resistance  Correctly prescribed dosage  Taken regularly by the patient  Treatment for a sufficient period of time to prevent relapse  All doses directly observed (DOT)  Never add a single drug to a failing regimen

14 Mixed population (susceptible and resistant) INH resistant bacilli Emergence of INH resistant strain because of ineffective treatment (INH monotherapy ) Effective multi-drug therapy Treatment Effect on Bacillary Population Weeks Log cfu 0 2 4 6 8 10 12 14 16 18 20 22 24

15 Unintended Monotherapy and Resistance Months of Rx0579 INH RIF EMB Smear++++ Culture++++ Susceptibility INHR*RRR RIFS*RRR EMBS*SSR * Results not known to clinician

16 Standard Regimens by Patient Group  New Patient – factors influencing regimen: Presumed to have drug susceptible TB Patient also HIV co-infected Setting known to have high prevalence of INH resistance in new patients  Previously Treated Patient – regimen is based on: Availability of drug sensitivity testing Likelihood of multi-drug resistance (MDR)

17 Benefits of Standard Regimens  Reduces errors in prescriptions  Facilitates estimates of drug need, purchasing, distribution and monitoring  Facilitates staff training  Reduces cost  Facilitates regular drug supply  Makes outcome evaluation convenient and comparable

18 Treatment Recommendations New Patient Groups TB treatment regimens Initial phase (2 mos.) Continuation phase Presumed or known drug susceptible Optimal HRZE a Optimal HR, 4 mos. Acceptable HRZE a or HRZE a, b, 3x/wk Acceptable HR 3x/wk, 4 mos. H = Isoniazid; R = Rifampicin; Z = Pyrazinamide; E = Ethambutol Twice weekly dosing for full course of treatment should not occur unless done in context of formal research

19 Treatment Recommendations (2) New Patient Groups TB treatment regimens Initial phase (2 mos.) Continuation phase Presumed or known drug- susceptible and living with HIV or in a high HIV prevalence setting Optimal HRZE a Optimal HR, 4 mos. Acceptable HRZE a Acceptable HR c 7 mos.

20 DST = drug susceptibility testing Treatment Recommendations (3) New Patient Groups TB treatment regimens Initial phase (2 mos.) Continuation phase Setting with high levels of INH resistance where DST at start of treatment is not universal Acceptable HRZE a daily Acceptable HRE, 4 mos. Settings where >3% of new patients have MDR Obtain DST at the start if therapy

21 Standard 8: Drug Formulations and Doses  The doses of anti-tuberculosis drugs used should conform to international recommendations  Fixed-dose combinations (FDC) of two (INH and RIF), three (INH, RIF, and PZA), and four (INH, RIF, PZA, and EMB) drugs are highly recommended

22 Adult Daily Dose of FDC Tabs Body Weight KG Initial Phase [RHZE] Continuation Phase [RH] 30-3722 38-5433 55-7444 ≥7555

23 12-15 Pills Per Day to Only 4-5 FDCs Image source: Pierre VirotImage source: Jad Davenport

24 Dose Recommendations Doses of First-line Anti-TB Drugs in Adults Drugs Recommended dose in mg/kg body weight Daily ( mg/kg range)3 x weekly Isoniazid (INH, H) 5 (4-6), max 300mg/day 10 (8-12) max 900/dose Rifampicin (RIF, R) 10 (8-12), max 600mg/day 10 (8-12) max 600/dose Pyrazinamide (PZA, Z) 25 (20-30), max 2000mg/day 35 (30-40) max 3000/dose Ethambutol (EMB, E) 15 (15-20), max 1600mg/day 30 (25-35) max 2400/dose Streptomycin d (SM, S) 15 (12-18), max 1000mg/day 15 (12-18)

25 Treatment Outcomes for Pulmonary TB 98% 64% 32% 20% 18% 50% 10% Dead Sputum negative Sputum positive No Chemotherapy Poor Chemotherapy Good Chemotherapy 0.8% 1.2% Grzybowski S et al, Bull Int Union Tuberc 1978; (53)2: 70-5

26 ISTC Standard 10  Response to therapy in patients with pulmonary tuberculosis should be monitored by follow-up sputum microscopy (two specimens) at the time of completion of the initial phase of treatment (two months)  If the sputum smear is positive at completion of the initial phase, sputum smears should be examined again at 3 months and, if positive, culture and drug susceptibility testing should be performed

27 ISTC Standard 10 (2) In patients with extrapulmonary tuberculosis and in children, the response to treatment is best assessed clinically.

28 Required Monitoring  New sputum smear-positive patients should have sputum smear exams monthly  Other clinical markers of treatment response to monitor: Weight at initiation of treatment, then monthly until weight is stable Review of TB symptoms present at time of diagnosis and documentation when symptoms resolve  With the RIF-based regimen throughout, WHO no longer recommends extending initial phase if smear-positive at 2 months

29 Treatment of Extrapulmonary TB (EPTB) and Special Situations

30 Treatment: Extrapulmonary TB  In general, EPTB is treated the same as PTB except: Streptomycin replaces EMB when treating CNS TB Corticosteroids may be useful in some forms of EPTB Some experts recommend extending the duration of therapy in patients with: – CNS tuberculosis – Bone/joint tuberculosis  WHO no longer recommends option to omit EMB during initial phase in HIV-negative EPTB patients

31 Treatment Duration and Use of Steroids Treatment: Extrapulmonary TB (2) SiteLength of Rx (mos.)Corticosteroids Lymph node6No Bone/Joint6-9No Pleural6No Pericarditis6Yes CNS9-12Yes Disseminated6No Genitourinary6No Abd/Peritoneal6No ATS/CDC/IDSA 2003

32 New Sputum Smear-Negative PTB  If also HIV-positive and/or severely ill: Obtain CXR and sputum TB culture Start antibiotic treatment for pneumonia (non- FQN) and if CXR findings suggest that TB is likely (positive or negative TB smear) then register as a new TB case and initiate TB treatment  If HIV-negative and/or mild/moderate illness: Obtain CXR and sputum TB culture If CXR findings suggest that TB is likely or TB culture is positive then register as a new case and initiate TB treatment

33 Treatment During Pregnancy  Increased risk of spontaneous abortion  Increase in perinatal mortality  Small for gestational age births  Increased maternal morbidity  Congenital TB  Increased risk of perinatal and early postnatal transmission Risk to mother and fetus is far greater from untreated TB than from the drugs used to treat TB:

34 Treatment During Pregnancy (2)  Isoniazid (INH), rifampicin (RIF) and ethambutol (EMB) are known to be safe for administration during pregnancy  Supplement with pyridoxine 25mg/day  Streptomycin should be avoided  Monitor for signs of hepatotoxicity during pregnancy and immediate post-partum

35 Breastfeeding  Most of the TB medications are secreted into breast milk but not in significant concentrations (usually <1-12% of levels measured in the serum)  Levels are not likely to lead to toxicity in the infant  Levels will not be sufficient to protect the infant – infant should receive IPT  Supplement Mom with B6 while breastfeeding

36 TB Treatment and Liver Disease  Use standard short-course regimen for patients without clinical evidence of chronic liver disease but history of: Hepatitis virus carriage Past history of acute hepatitis Current excessive alcohol consumption  Hepatotoxic reactions are more common in these patients and should therefore be anticipated

37 TB Treatment and Liver Disease  Use a liver sparing regimen for patients with established chronic liver disease: Two hepatotoxic drugs – 9HR+E (until or unless INH susceptibility documented) – 2HRSE/6HR – 6-9RZE One hepatotoxic drug – 2HES/10HE No hepatotoxic drugs – 18-24SE+Fluoroquinolone

38 Hepatitis  Hepatitis (asymptomatic elevation AST/ALT occurs in 20% patients on 4 drugs) Drug induced hepatitis =  AST or ALT ≥3 times upper limits of normal in the presence of symptoms OR  >5 times if asymptomatic INH, PZA and RIF can all cause hepatotoxicity – Hepatitis from INH is age related, from PZA is dose related, and RIF is unpredictable and less common

39 TB Treatment and Hepatitis  If  >3x normal with symptoms or > 5x normal without symptoms: stop all anti-TB medications and evaluate patient refer patient to doctor for clinical evaluation try to rule out other causes of acute liver disease if severely ill, may start 3 non-hepatotoxic drugs after AST < 2 times upper limit of normal — re-challenge drugs one-by-one starting with drugs that are not hepatotoxic

40 The Renal Impaired TB Patient  Patients with end stage renal disease (ESRD) have increased risk for progression to active TB disease Risk is 10 – 25 times greater for persons with ESRD than in the general population

41 The Renal Impaired TB Patient (2)  If CrCl <30ml/min., including hemodialysis patients, administer anti-TB treatment thrice weekly after dialysis at the following doses: Isoniazid and rifampicin 10mg/kg PZA 25-mg/kg EMB 15-mg/kg  Include supplemental pyridoxine 25-50mg with the thrice weekly regimen to prevent peripheral neuropathy

42 Summary  Appropriate treatment and assessment of adherence to treatment is an important public health issue  The use of internationally accepted first-line treatment regimens is associated with a high cure rate and a low risk of acquired drug resistance  Pulmonary and EPTB are generally treated with the same regimens (Exception: extended duration in meningeal/CNS and bone/joint disease)  Monitoring for both response to treatment and for potential adverse events is essential

43 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. Standard 8: All patients who have not been previously treated should receive an internationally accepted treatment regimen:  Initial phase: 2 months INH, RIF, PZA, and EMB  Continuation phase: 4 months INH and RIF * Abbreviated versions

44 Summary: ISTC Standards Covered* Standard 8: (continued)  The doses of anti-tuberculosis drugs used should conform to international recommendations. Fixed-dose combinations are highly recommended. Standard 10: Response to therapy in patients with pulmonary TB should be monitored by follow-up sputum microscopy (2 specimens), if positive, sputum smears should be examined again at 3 months. If positive, culture and DST should be performed. * Abbreviated versions


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