Drug-resistant tuberculosis treatment
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GDG considerations. The GDG acknowledged that, during the analysis, the intervention and
comparator groups were made as comparable as possible. However, the GDG considered possible unmeasured confounding due to a lack of systematic collection of information on comorbidities and radiological findings through the EDRWeb system, as well as methodological challenges, such as a potential selection bias. However, apart from the selection criteria listed, the risk of major selection bias was considered low, given that this intervention represented a complete and comprehensive switch in the countrywide programmatic approach. The GDG further discussed modifications to the shorter all-oral bedaquiline-containing regimen, which was adjusted in 2018 by removing ethionamide 30 and including linezolid for countrywide enrolment (50). 31 However, in the patient records for 2017 provided for this guideline development process, only 0.5% of patients received linezolid, and no treatment outcomes were available for these patients. Given the incomplete data and inability to analyse these data separately owing to the small numbers, the GDG decided to exclude all patients who received linezolid. A further sensitivity analysis within subgroups defined by the use of specific combinations of drugs was attempted, to explore whether the addition of medicines such as linezolid to bedaquiline-containing regimens would improve treatment outcomes. No data on this combination were available in the data source used for the primary analysis; therefore, longer regimens containing both bedaquiline and linezolid were compared to longer regimens in which other companion drugs plus bedaquiline only were used. Results of this analysis suggested that regimens containing both bedaquiline and linezolid were associated with significantly lower rates of death (aOR: 1.6; 95% CI: 1.1–2.3) as well as a significantly better composite outcome of success versus all unfavourable outcomes (aOR: 1.5; 95% CI: 1.1–2.0). 29 Recommendations released by WHO in December 2018 emphasized that fully oral longer regimens should be prioritized and become the preferred option for most patients, and that injectable agents were no longer among the priority medicines to consider when designing longer MDR-TB regimens (11). 30 The decision to modify this regimen followed results from a National TB Drug Resistance Survey conducted in South Africa in 2012–2014, and published in 2018. The survey found that 44.7% of M. tuberculosis isolates were resistant to ethionamide (95% CI: 25.9–63.6%) (49). 31 Linezolid was to be included routinely within the regimen up front, to protect bedaquiline in the early stages of treatment, particularly in MDR/RR-TB cases where resistance to fluoroquinolones was yet to be detected. WHO consolidated guidelines on tuberculosis: drug-resistant tuberculosis treatment 15 Owing to the evidence being insufficient and indirect, the GDG was unable to use these data and consider the value of further modification of the all-oral shorter regimen at this stage. During the evidence assessment process, members of the GDG further assessed the overall certainty in the quality of evidence, the balance between benefits and harms of the shorter all-oral bedaquiline- containing regimen in addition to treatment outcomes, values and preferences, as well as considerations on equity, acceptability and feasibility (51, 52). One of the areas that required further discussion was related to potential for confounding and generalizability. Even though confounding was reduced through double-adjustment in propensity score matching, 32 members of the GDG remained concerned about the risk of unmeasured or residual confounding and potential selection bias by indication. In addition, the GDG acknowledged that although well-collected and unbiased programmatic data hold promise and may better reflect real-world practices, these data typically lead to a low-quality grading of evidence and have important shortcomings compared with more robust randomized controlled trial (RCT) generated data. It is also important to consider the extent to which these findings could be applied in other settings; factors that may limit the generalizability of the study findings to other settings include high prevalence of HIV, use of ART, specific M. tuberculosis strains and drug-resistance patterns, and the quality of health care services, including adherence strategies in South Africa. Overall, the GDG agreed that the certainty in the evidence on the efficacy of all-oral shorter regimens was “very low” due to concerns about unmeasured or residual confounding and potential risk of bias. The GDG considered all outcomes of interest, without any prioritization; the outcome for success versus Download 1.73 Mb. Do'stlaringiz bilan baham: 
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