| Literature DB >> 32166693 |
Tomas Simurda1, Jana Zolkova2, Zuzana Kolkova3, Dusan Loderer3, Miroslava Dobrotova2, Ingrid Skornova2, Monika Brunclíkova2, Marian Grendar3, Zora Lasabova4, Jan Stasko2, Peter Kubisz2.
Abstract
Congenital dysfibrinogenemia (CD) is a rare disorder of hemostasis. The majority of cases are caused by heterozygous missense mutations in one of the three fibrinogen genes. Patients with CD may experience bleeding and thrombosis, but many are asymptomatic. To better describe the clinical, laboratory, and genotypic picture of CD, we evaluated 31 patients from seven unrelated families using standard coagulation tests and genetic analysis. The clinical phenotype consisted of bleeding in 13/31 (42%) patients; other patients (18/31; 58%) were asymptomatic. Among patients with bleeding, symptoms were mostly in single anatomical sites, with variable intensity of bleeding. Compared to results from a previous large systematic survey, our results showed a similar mean bleeding score, but a higher incidence of bleeding episodes without thrombotic complications. In the present study, we identified three known pathogenic point mutations in the FGA (c.95G > A, c.104G > A) and FGB (c.586C > T) genes. The variants of CD identified in this cross-sectional study were either asymptomatic or had bleeding manifestations and showed similar laboratory features, irrespective of genotype. Results from genetic and clinical studies will continue to yield valuable information on the structure and function of the fibrinogen molecule.Entities:
Keywords: Aα-chain; Bleeding phenotype; Bβ-chain; Dysfibrinogenemia; Genetic analysis; Hotspot mutations
Year: 2020 PMID: 32166693 DOI: 10.1007/s12185-020-02842-9
Source DB: PubMed Journal: Int J Hematol ISSN: 0925-5710 Impact factor: 2.490