The First Affiliated Hospital of Soochow University, Jiangsu Institute of Hematology, Key Laboratory of Thrombosis and Hemostasis of Ministry of Health, Suzhou, China.
Haemophilia. 2011 Jan;17(1):65-9. doi: 10.1111/j.1365-2516.2010.02369.x. Epub 2010 Aug 16.
We studied two families in which the probands had severe bleeding tendency and showed low plasma levels of coagulation factor V (FV) antigen and activity. Sequence analysis of the FV gene on proband 1 demonstrated a novel G16088C homozygous missense mutation in exon 3 resulting in an Asp 68 to His substitution and on proband 2, a C69969T homozygous missense mutation in exon 23 leading to Gly2079Val. The parents of both families were each heterozygous for the corresponding FV gene defect. During their second pregnancy, the two families requested prenatal diagnosis. Chorionic villi were analysed at 12 weeks of gestation and cord blood samples were tested at 22 weeks. Microsatellite analysis performed in family 1 showed that the foetus sample was not contaminated by maternal tissue. The foetus 1 was found to be heterozygous for the familiar G16088C mutation with lower FV activity in the cord blood; the foetus 2 was a normal one. The diagnosis was confirmed after the birth. This is the first report of prenatal diagnosis for FV deficiency.
我们研究了两个家系,先证者有严重出血倾向,表现为凝血因子 V(FV)抗原和活性水平降低。先证者 1 的 FV 基因序列分析显示第 3 外显子存在 novel G16088C 纯合错义突变,导致 Asp 68 突变为 His,先证者 2 的第 23 外显子存在 C69969T 纯合错义突变,导致 Gly2079Val。两个家系的父母均为相应的 FV 基因缺陷的杂合子。在他们的第二次妊娠期间,两个家系要求进行产前诊断。在妊娠 12 周时分析绒毛膜,在妊娠 22 周时检测脐带血样本。家系 1 中的微卫星分析表明胎儿样本未被母体组织污染。胎儿 1 为杂合子,存在熟悉的 G16088C 突变,脐带血中 FV 活性较低;胎儿 2 为正常。出生后证实了这一诊断。这是首例 FV 缺乏症的产前诊断报告。
