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Familial Multiple Coagulation Factor Deficiencies (FMCFDs) in a Large Cohort of Patients - a Single-center Experience in Genetic Diagnosis
Barbara Preisler
Behnaz Pezeshkpoor
Atanas Banchev
Ronald Fischer
Barbara Zieger
Ute Scholz
Heiko Rühl
Bettina Kemkes-Matthes
Ursula Schmitt
Antje Karen Redlich
Sule Unal
Hans-Jürgen Laws
Martin Olivieri
Johannes Oldenburg
Anna Pavlova
出版
Universität
, 2021
URL
http://books.google.com.hk/books?id=_SFszgEACAAJ&hl=&source=gbs_api
註釋
Abstract: Background: Familial multiple coagulation factor deficiencies (FMCFDs) are a group of inherited hemostatic disorders with the simultaneous reduction of plasma activity of at least two coagulation factors. As consequence, the type and severity of symptoms and the management of bleeding/thrombotic episodes vary among patients. The aim of this study was to identify the underlying genetic defect in patients with FMCFDs. Methods: Activity levels were collected from the largest cohort of laboratory-diagnosed FMCFD patients described so far. Genetic analysis was performed using next-generation sequencing. Results: In total, 52 FMCFDs resulted from coincidental co-inheritance of single-factor deficiencies. All coagulation factors (except factor XII (FXII)) were involved in different combinations. Factor VII (FVII) deficiency showed the highest prevalence. The second group summarized 21 patients with FMCFDs due to a single-gene defect resulting in combined FV/FVIII deficiency or vitamin K-dependent coagulation factor deficiency. In the third group, nine patients with a combined deficiency of FVII and FX caused by the partial deletion of chromosome 13 were identified. The majority of patients exhibited bleeding symptoms while thrombotic events were uncommon. Conclusions: FMCFDs are heritable abnormalities of hemostasis with a very low population frequency rendering them orphan diseases. A combination of comprehensive screening of residual activities and molecular genetic analysis could avoid under- and misdiagnosis
