[一个凝血因子VII和X联合缺乏的近亲家系的表型和基因型分析]
[Phenotype and genotype analysis for a consanguineous pedigree with combined coagulation factor VII and X deficiency].
作者信息
Jin Yanhui, Wang Mingshan, Wang Yingyu, Yang Xiaoli, Yang Lihong, Xie Yaosheng, Xie Haixiao, Zhu Liqing, Yu Fangyou
机构信息
Laboratory Medicine Center, the First Affiliated Hospital of Wenzhou Medical University, Wenzhou, Zhejiang 325015, P.R.China.
出版信息
Zhonghua Yi Xue Yi Chuan Xue Za Zhi. 2014 Feb;31(1):16-20. doi: 10.3760/cma.j.issn.1003-9406.2014.01.004.
OBJECTIVE
To identify potential mutations and explore the molecular mechanism underlying combined inherited coagulation factors VII(FVII) and X(FX) deficiency for a family featuring consanguineous marriage between maternal cousins.
METHODS
Prothrombin time (PT), activated partial thromboplastin time (APTT), fibrinogen, FVII activity (FVII:C), FX activity (FX:C), FVII antigen (FVII:Ag), FX antigen (FX:Ag) and other coagulant parameters of the proband and 5 family members were measured. Potential mutations in exons, exon-intron boundaries and 5', 3' untranslated sequences of F7 and F10 genes were screened by polymerase chain reaction and direct sequencing. Suspected mutations were confirmed by sequencing the opposite strand.
RESULTS
PT and APTT of the proband were obviously prolonged to become 76.4 s and 60.2 s, respectively. FVII:C, FVII:Ag,FX:C and FX:Ag of the proband were obviously reduced to become 4%, 6%, 6% and 33%, respectively. Both PT and APTT of her grandmother, father, mother and daughter were slightly prolonged, which have measured 16.4 s, 15.8 s,16.9 s, 16.5 s, and 44.0 s, 42.1 s, 41.1 s, 43.5 s, respectively. And their FVII:C (34%, 39%, 31%, 40%, respectively), FX:C (50%, 58%, 47%, 42%, respectively) and FX:Ag (51%, 54%, 58%, 47%, respectively) were slightly reduced, while FVII:Ag was in the normal range. The coagulant parameters of her younger brother were within normal range. Two homozygous mutations, g.11267C to T in exon 8 of F7 gene, which resulted in an Arg277Cys substitution, and g.28139G to T in exon 8 of F10 gene which led to a Val384Phe substitution, were identified in the proband. The proband's grandmother, parents and daughter were heterozygous for both Arg277Cys and Val384Phe mutationss. Wild-type alleles of both F7 and F10 genes were also found in the younger brother.
CONCLUSION
A homozygous Arg277Cys mutation and a Val384Phe mutation have been respectively identified in the F7 and F10 genes, which can explain the low levels of FVII and FX in this family. The former has been inherited from the consanguineous parents.
目的
对于一个母系表亲近亲结婚的家族,鉴定潜在突变并探究联合遗传性凝血因子VII(FVII)和X(FX)缺乏症的分子机制。
方法
检测了先证者及5名家庭成员的凝血酶原时间(PT)、活化部分凝血活酶时间(APTT)、纤维蛋白原、FVII活性(FVII:C)、FX活性(FX:C)、FVII抗原(FVII:Ag)、FX抗原(FX:Ag)及其他凝血参数。通过聚合酶链反应和直接测序筛选F7和F10基因外显子、外显子-内含子边界及5'、3'非翻译序列中的潜在突变。通过对互补链测序确认疑似突变。
结果
先证者的PT和APTT明显延长,分别变为76.4秒和60.2秒。先证者的FVII:C、FVII:Ag、FX:C和FX:Ag明显降低,分别变为4%、6%、6%和33%。她的祖母、父亲、母亲和女儿的PT和APTT均略有延长,分别测得16.4秒、15.8秒、16.9秒、16.5秒和44.0秒、42.1秒、41.1秒、43.5秒。他们的FVII:C(分别为34%、39%、31%、40%)、FX:C(分别为50%、58%、47%、42%)和FX:Ag(分别为51%、54%、58%、47%)略有降低,而FVII:Ag在正常范围内。她弟弟的凝血参数在正常范围内。在先证者中鉴定出两个纯合突变,F7基因第8外显子的g.11267C突变为T,导致Arg277Cys替换,F10基因第8外显子的g.28139G突变为T,导致Val384Phe替换。先证者的祖母、父母和女儿对于Arg277Cys和Val384Phe突变均为杂合子。在弟弟中也发现了F7和F10基因的野生型等位基因。
结论
在F7和F10基因中分别鉴定出一个纯合的Arg277Cys突变和一个Val384Phe突变,这可以解释该家族中FVII和FX水平较低的原因。前者是从近亲父母遗传而来。
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