Inhibitor development according to concentrate in severe hemophilia: reporting on 1392 Previously Untreated Patients from Europe and Canada

Kai R Fischer ,Natasha Pardy,Myriam Landry ,Victoria Price,Jerry Teitel,Paula James,Dawn Goodyear,Jean St‐Louis ,N Samji,Chai Pua,Sean Dolan,Alfonso Iorio,Michelle Sholzberg,Jean‐François Castilloux ,Radosław Kaczmarek ,David Stammers,Ketan Kulkarni,Linda Sun,Anthony Chan,Georges E Rivard ,John Wu ,Kelsey Brose,Stéphanie Cloutier,Georges‐Étienne Rivard ,Margaret R Warner ,Victor S Blanchette ,Sue Robinson,Mike Makris ,Jayson Stoffman,Natalia Rydz,Davide Matino,Man‐Chiu Poon ,Roona Sinha,Janie Charlebois,Bruce Ritchie,David Lillicrap,Macgregor Steele,Manuel Carção ,Alan Tinmouth,Kulwant Gill,Amanda Bettle ,Thierry Lambert ,Shannon Jackson,Mary‐Margaret Keating ,Nicole Laferriere,Riitta Lassila ,Nizar Abdel-Samad,Alex Gatt ,Flora Peyvandi ,Robert E Hollingsworth ,Paul Moorehead,Robert J Klaassen

doi:10.1016/j.rpth.2023.102265

Kai R Fischer , Natasha Pardy + Show 50 more

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https://doi.org/10.1016/j.rpth.2023.102265

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Journal: Research and Practice in Thrombosis and Haemostasis	Publication Date: Nov 1, 2023
Citations: 1	License type: cc-by-nc-nd

Abstract

BackgroundClotting factor concentrates have been the mainstay of severe hemophilia treatment over the last 50 years. Differences in risk of neutralizing antibody (inhibitor) formation according to concentrate used remain clinically relevant. ObjectivesTo assess inhibitor development according to type of clotting factor concentrate in previously untreated patients (PUPs) with severe hemophilia A and B. MethodsThe European Haemophilia Safety Surveillance (EUHASS) and Canadian Bleeding Disorders Registry (CBDR) have been monitoring adverse events overall and according to concentrate for 11 and 8 years, respectively. Inhibitors were reported quarterly, and PUPs completed 50 exposure days without inhibitor development annually. Cumulative inhibitor incidences and 95% confidence intervals (CIs) were compared without adjustment for other risk factors. ResultsFifty-six European and 23 Canadian centers reported inhibitor development in 312 of 1219 (26%; CI, 23%-28%) PUPs with severe hemophilia A and 14 of 173 (8%; CI, 5%-13%) PUPs with severe hemophilia B. Inhibitor development was lower on plasma-derived factor (F)VIII (pdFVIII, 20%; CI, 14%-26%) than on standard half-life recombinant FVIII (SHL-rFVIII, 27%; CI, 24%-30% and odds ratio, 0.67; CI, 0.45%-0.98%; P = .04). Extended half-life recombinant FVIII (EHL-rFVIII, 22%; CI, 12%-36%) showed an intermediate inhibitor rate, while inhibitor rates for Advate (26%; CI, 22%-31%) and Kogenate/Helixate (30%; CI, 24%-36%) overlapped. For other SHL-rFVIII concentrates, inhibitor rates varied from 3% to 43%. Inhibitor development was similar for pdFIX (11%; CI, 3%-25%), SHL-rFIX (8%; CI, 3%-15%), and EHL-rFIX (7%; CI, 1%-22%). ConclusionWhile confirming expected rates of inhibitors in PUPs, inhibitor development was lower in pdFVIII than in SHL-rFVIII. Preliminary data suggest variation in inhibitor development among different SHL-rFVIII and EHL-rFVIII concentrates.

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