Division of Angiology and Hemostasis, University Hospitals of Geneva and Faculty of Medicine.
Division of Gynaecology, University Hospitals of Geneva.
Blood Coagul Fibrinolysis. 2023 Jun 1;34(4):250-253. doi: 10.1097/MBC.0000000000001217. Epub 2023 Apr 4.
Heavy menstrual bleeding is one of the most common causes of consultation in haematology. We present the clinical case of a 20-year-old woman referred by her gynaecologist due to heavy menstrual bleeding since menarche, complicated by iron deficiency anaemia. Haemostasis work-up was initially suggestive of a von Willebrand disease type 1. Genetic analyses by whole exome sequencing lead to a fortuitous discovery of haemophilia by identifying a heterozygous missense mutation in F8 , exon 8 c.1127T>G:p.Val376Gly, previously reported in a patient with mild haemophilia A. The bleeding phenotype worsened by concomitant low von Willebrand factor (VWF) due to VWF variants influencing VWF levels. Our case highlights how whole exome sequencing can help to correct an erroneous diagnosis and identify polymorphisms that eventually contribute to the overall haemostatic balance.
月经过多是血液科最常见的就诊原因之一。我们报告了一例 20 岁女性病例,该患者因初潮以来月经过多,伴有缺铁性贫血,由妇科医生转介。止血检查最初提示为 1 型血管性血友病。全外显子组测序的基因分析偶然发现 F8 基因外显子 8 c.1127T>G:p.Val376Gly 存在杂合错义突变,该突变之前在一名轻度血友病 A 患者中报道过,导致因子 8 (F8)异常,从而确诊为血友病。同时由于血管性血友病因子(VWF)变异影响 VWF 水平,导致 VWF 降低,加重了出血表型。本病例强调了全外显子组测序如何有助于纠正错误诊断,并识别最终有助于整体止血平衡的多态性。
