| Literature DB >> 28198996 |
Paul Batty1, Steve K Austin2,3, Kate Khair4, Carolyn M Millar5, Ben Palmer6, Savita Rangarajan3, Jan-Phillip Stümpel1, Murugaiyan Thanigaikumar7, Thynn T Yee8, Daniel P Hart1.
Abstract
Inhibitor formation in non-severe haemophilia A is a life-long risk and associated with morbidity and mortality. There is a paucity of data to understand real-world inhibitor screening practice. We evaluated the treatment burden, haemostatic strategies, F8 genotyping and inhibitor screening practices in non-severe haemophilia A in seven London haemophilia centres. In the 2-year study period, 44% (377/853) patients received at least one haemostatic treatment. Seventy-nine percent of those treated (296/377) received factor VIII (FVIII) concentrate. F8 genotype was known in 88% (331/377) of individuals. Eighteen per cent (58/331) had 'high-risk' F8 genotypes. In patients with 'standard-risk' F8 genotypes treated on-demand with FVIII concentrate, 51·3% episodes (243/474) were screened within 1 year. However, poor screening compliance was observed after 'high-risk' treatment episodes. In patients with 'standard-risk' F8 genotypes, 12·3% (28/227) of treatment episodes were screened in the subsequent 6 weeks after surgery or a bleed requiring ≥5 exposure days. Similarly, in the context of 'high-risk' F8 genotypes after any FVIII exposure, only 13·6% (12/88) of episodes were screened within 6 weeks. Further study is required to assess optimal practice of inhibitor screening in non-severe haemophilia A to inform subsequent clinical decisions and provide more robust prevalence data to further understand the underlying immunological mechanism.Entities:
Keywords: audit; haemophilia; inhibitor; non-severe; screening
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Year: 2017 PMID: 28198996 DOI: 10.1111/bjh.14543
Source DB: PubMed Journal: Br J Haematol ISSN: 0007-1048 Impact factor: 6.998