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XDR-TB and management options Ninth Technical Advisory Group and National TB Programme Managers Meeting TB Control in the Western Pacific Region, Manila,

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Presentation on theme: "XDR-TB and management options Ninth Technical Advisory Group and National TB Programme Managers Meeting TB Control in the Western Pacific Region, Manila,"— Presentation transcript:

1 XDR-TB and management options Ninth Technical Advisory Group and National TB Programme Managers Meeting TB Control in the Western Pacific Region, Manila, Philippines, 9-12 December 2014 CHIANG Chen-Yuan MD, MPH, DrPhilos

2 Global estimates of MDR-TB 3.5% (95% CI: 2.2–4.7%) among new cases 20.5% (95%CI: 13.6–27.5%)of previously treated cases 480 000 (range: 350 000‒610 000) new MDR-TB cases worldwide 300 000 (range: 230 000–380 000) MDR-TB cases among patients with pulmonary TB notified in 2013. 9.0% (95% CI: 6.5–11.5%) of MDR-TB cases have XDR-TB Global Tuberculosis Report 2014

3 Fluoroquinolone-resistant MDR-TB Without previous treatment of MDR-TB – use of fluoroquinolone in the treatment of lower respiratory tract infection – use of fluoroquinolone in the treatment of non- MDR tuberculosis, such as HREZ + fluoroqunolone (+ injectable) for retreatment TB cases With previous treatment of MDR-TB

4 Transition from drug-resistant TB to XDR-TB INH-resistant TB INH- and Quinolone-resistant TB XDR-TB Use of quinolone in the treatment of community acquired pneumonia Failure to successfully treat MDR-TB using second line drugs MDR-TB MDR-TB plus Quinolone resistance Failure to successfully treat TB using first line drugs Chiang C-Y, et al. Expert Rev Resp Med 2008;2:47-54

5 Resistance to anti-tuberculosis drugs by multidrug-resistant tuberculosis (MDR-TB) patient group 5 Falzon D, et al Eur Respir J 2013; 42: 156–168

6 Treatment outcomes for patients diagnosed with MDR- TB by WHO region, 2007–2011 cohorts 6 WHO. Global Tuberculosis Report 2014

7 Short Standardized Treatment of Multidrug- resistant Tuberculosis Intensive phase: GEZC KHP 4 months, extended till sputum conversion Continuation phase: GEZC 5 months Kanamycin (K) Prothionamide (P) Isoniazid (H)* Gatifloxacin (G)* Clofazimine, C Ethambutol, E Pyrazinamide, P 7 *high dose Van Deun A, et al. Am J Respir Crit Care Med 2010;182:684–692

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9 GenoType® MTBDRplus test procedure 1)DNA Extraction From NALC/NaOH Processed sputum 2) Amplification by PCR 3) Hybridization Reverse hybridization of amplified nucleic acids to specific DNA probes bound on strips 4) Evaluation

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11 Genetic Mutations Associated with M. tuberculosis Resistance to Amikacin, Kanamycin and Capreomycin: A Systematic Review gene mutations believed to confer resistance to the injectable drugs: the rrs and tlyA genes, and the eis promoter. Georghiou SB, et al. PLoS ONE 7(3): e33275. doi:10.1371/journal.pone.0033275

12 Performance Assessment of the GenoType MTBDRsl Test for Detection of Second-Line and Ethambutol Drug Resistance among MDR-TB Patients high levels of specificity: 95.8 to 100%. the sensitivities of resistance detection using the GenoType MTBDRsl test were – Fluoroquinolone 85.1% – kanamycin 43.2%, – amikacin 84.2%, – capreomycin 71.4% – Ethambutol 56.2% with the inclusion of an extra gene, eis, in sequencing, the sensitivity reached 70.3% for detection of KM resistance. Huang W-L. et al. 2011

13 Forest plots of MTBDRsl sensitivity and specificity when performed indirectly or directly for fluoroquinolone resistance detection and using phenotypic culture-based DST as a reference standard

14 The diagnostic accuracy of the GenoType® MTBDRsl assay As a test for fluoroquinolone resistance measured against culture-based DST Pooled sensitivity (95% CI ) Pooled specificity (95% CI ) Direct test85.1% (71.9% to 92.7%) 98.2% (96.8% to 99.0%) Indirect test83.1% (78.7% to 86.7%) 97.7% (94.3% to 99.1%) Cochrane Database of Systematic Reviews 2014, Issue 10. Art. No.: CD010705. DOI: 10.1002/14651858.CD010705.pub2.

15 Forest plots of MTBDRsl sensitivity and specificity when performed indirectly for the detection of resistance to amikacin (Ak), kanamycin (Kn) and capreomycin (Cm) using culture as a reference standard.

16 The diagnostic accuracy of the GenoType® MTBDRsl assay As a test for second-line injectable drugs (amikacin,kanamycin and capreomycin) resistance measured against culture-based DST when performed indirectly Pooled sensitivity (95% CI ) Pooled specificity (95% CI ) SLIDs76.9% (61.1% to 87.6%)99.5% (97.1% to 99.9%) amikacin87.9% (82.1% to 92.0%)99.5% (97.5% to 99.9%) kanamycin66.9% (44.1% to 83.8%)98.6% (96.1% to 99.5%) capreomycin79.5% (58.3% to 91.4%)95.8% (93.4% to 97.3%) Cochrane Database of Systematic Reviews 2014, Issue 10. Art. No.: CD010705. DOI: 10.1002/14651858.CD010705.pub2.

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18 Clofazimine 18 Study designed and supervised by: Jacques Grosset, MD And conducted by: Sandeep Tyagi, BS, Si-yang Li, BS, Deepak Almeida, PhD, Paul Converse, PhD

19 Long-term outcomes of patients with extensively drug-resistant tuberculosis in South Africa: a cohort study predictors of net culture conversion – no history of multidrug-resistant tuberculosis (p=0·0007) – use of clofazimine (p=0·0069). predictors of survival – net culture conversion (p<0·0001) – treatment with clofazimine (p=0·021). – Antiretroviral therapy in patients with HIV (p=0·003). Pietersen E, et al. Lancet 2014; 383: 1230–39

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21 Linezolid for Treatment of Chronic XDR-TB 21 N Engl J Med 2012;367:1508-18

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23 Clinical use of the meropenem- clavulanate combination for XDR-TB 23 Int J Tuberc Lung Dis 2012;16:558–560

24 Mechanisms of action of new compounds in clinical development for tuberculosis Ma Z, et al. Lancet 2010; 375: 2100–09

25 Diacon AH, et al. N Engl J Med 2014;371:723-32 phase 2b trial, Bedaquiline

26 Multidrug-Resistant Tuberculosis and Culture Conversion with Bedaquiline In this phase 2b trial, Bedaquiline – reduced the median time to culture conversion from 125 days to 83 days (hazard ratio 2.44 (95% CI 1.57-3.80) – Increased the rate of culture conversion at 24 weeks (79% vs. 58%, P = 0.008) and at 120 weeks (62% vs. 44%, P = 0.04). The overall incidence of adverse events was similar in the two groups. There were 10 deaths in the bedaquiline group and 2 in the placebo group, with no causal pattern evident. Diacon AH, et al. N Engl J Med 2014;371:723-32

27 Diacon AH, et al. N Engl J Med 2014;371:723-32

28 Mean changes from baseline in QTcF* over time among patients treated with bedaquiline plus background regimen † (BR) versus placebo plus BR, Study C208 (Stage 2) MMWR / October 25, 2013 / Vol. 62 / No. 9

29 WHO Companion Handbook 2014 1.the QT interval needs to be adjusted (corrected) for the heart rate 2.the Fredericia method (QTcF): dividing the QT interval by the cubed root of the interval in seconds between the peak of two successive R waves (RR)

30 Flowchart of intent-to-treat patients in delamanid (DLM) Trial 204, Trial 208 and Study 116 Eur Respir J 2013; 41: 1393–1400

31 Long-term (24 month) treatment outcomes after treatment with delamanid in combination with an optimised background treatment regimen: MDR- and XDR-TB patients Eur Respir J 2013; 41: 1393–1400

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33 Cascade of regimens RifampicinQuinoloneTreatment approach SusceptibleFirst line anti-TB treatment ResistantSusceptibleSecond line anti-TB treatment (9-month regimen) Resistant New drugs and potential group 5 drugs

34 In Summary Globally, 9.0% (95% CI: 6.5–11.5%) of MDR-TB cases have XDR-TB. Rapid diagnosis of resistance to rifampicin, fluoroquinolone and second line injectables will be helpful in the choice of regimens. Do not add a new drug to a failing MDR-TB regimen. Evidence is emerging that proper use of clofazimine, linezolid, meropenem, and new drugs improves the outcome of XDR-TB. However, experience is insufficient in terms of the type of drugs, the number of drugs and the duration required for the treatment of XDR-TB. Would countries be interested in using a standardized protocol for the treatment of quinolone-resistant TB and XDR-TB?

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