Abstract Background The HLADQA1*05GA genetic variation is a clinically-useful screening tool for identifying tumor necrosis factor-α antagonists (TNFA)anti-drug antibody (ADA) risk as well as TNFA loss of response and discontinuation. Aims We hypothesize that an additional use for HLADQA1*05GA screening is guiding the selection of TNFA vs non-TNFA-based advanced inflammatory bowel disease (IBD) treatments. Methods A prospective cohort study was conducted in IBD patients being considered for advanced therapy. Participants were assessed in one of 2 cohorts: 1) those where advanced therapy selection was based on physician preference (controls); 2) those where HLADQA1*05GA screening was used to select the use of TNFA vs non-TNFA advanced therapy (screened cohort). Specifically, TNFA therapy was selected for wildtype genotypes and non-TNFA therapy was selected for variant genotypes. Participants were assessed for clinical remission at 1-year, treatment discontinuation, adverse drug events, ADA formation, and other important clinical outcomes. Post-hoc analyses examined the effect of screening on individual genotype groups. Results A total of 233 participants seen at a tertiary care centre in London, ON were included in the final analyses (screened cohort, n = 75; control cohort, n = 158). The distribution of genotypes in the screened cohort was 48 GG, 20 GA, 7 AA. TNFA therapy was the most used advanced therapy in both groups (screened, N = 48/75, 64.0%; controls, N = 84/158, 53.2%). Screened participants were more likely to achieve clinical remission at 1-year vs controls (N = 61/75, 81.3% vs 102/158, 64.6%, p = 0.0093), less likely to be co-prescribed combination therapy (N = 4/75, 5.3% vs 71/158, 44.9%, p 0.0001), report fewer adverse drug events (ADE) (N = 13/75, 17.3% vs N = 56/158, 35.4%, p = 0.0055) and had a lower frequency of ADA formation (N = 0/75, 0.0% vs N = 11/158, 7.0%, p = 0.018). Similar frequencies of drug discontinuation, hospitalizations, surgery, dose escalation and rescue glucocorticoid use (RGU) were seen in both groups. Post-hoc analyses highlighted that HLADQA1*05GA variant carriers identified by screening derived the most clinical benefit. Screened variant carriers had the most clinical remission (92.6%) with the fewest ADEs (3.7%), fewest drug dose escalations (11.1%) and requiring less RGU (7.4%) compared to unscreened variant carriers and individuals with a wildtype genotype, with or without screening. Conclusions HLADQA1*05GA-screening was associated with disease remission, fewer adverse events and a lower incidence of ADA formation when used to select TNFA vs non-TNFA therapy. Variant carriers derive the most benefit from screening. We confirm an additional role for HLADQA1*05 screening is guiding TNFA vs non-TNFA IBD drug selection. Funding Agencies CIHRAcademic Medical Organization of Southwestern Ontario, Lawson Internal research Fund
Bueno et al. (Sun,) studied this question.
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