Aim: To indirectly compare the efficacy and safety of elafibranor and seladelpar, as second-line treatments for primary biliary cholangitis. Materials ELATIVE NCT04526665 ) and (b) seladelpar (n = 128) versus placebo (n = 65; RESPONSE NCT03301506 ). Patients from ELATIVE not meeting the RESPONSE upper limit of normal (ULN) criteria for alkaline phosphatase (ALP) and total bilirubin were excluded (n = 16); summary statistics for ELATIVE were recalculated using the new dataset. Random-effects models assessed the outcomes of cholestasis response (ALP <1.67 × ULN, ALP reduction ≥15% from baseline and total bilirubin ≤ULN), ALP normalization, change from baseline in ALP and pruritus, pruritus as a treatment-emergent adverse event and all-cause discontinuation. Results: Elafibranor-treated patients had greater odds of achieving cholestasis response than placebo- (median odds ratio 95% credible interval: 84.79 12.49, 2513.00) or seladelpar-treated patients (13.02 1.45, 420.20), with posterior probabilities ≥99% that odds were higher with elafibranor than seladelpar or placebo. Among patients with ALP ≥350 U/l, the median odds ratio 95% credible interval of cholestasis response for elafibranor-treated patients versus seladelpar-treated patients was 18.71 0.65, 10,610.00, with a 95.2% posterior probability that odds were higher with elafibranor than seladelpar. For all other outcomes, there was no strong evidence of a difference between treatments. Conclusion: Bayesian network meta-analyses found strong probabilistic evidence supporting the treatment benefit of elafibranor compared with seladelpar for the achievement of cholestasis response at 52 weeks, while the treatment effect on other outcomes was uncertain. Head-to-head studies are needed to validate results of these indirect comparisons.
Jones et al. (Fri,) studied this question.