丹麦人群中蛋白质S (PROS1)基因的遗传变异和蛋白质S缺乏。

Ole Halfdan Larsen, Alisa D Kjaergaard, Anne-Mette Hvas, Peter H Nissen
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引用次数: 1

摘要

蛋白S (PS)缺乏是静脉血栓栓塞(VTE)的危险因素,可能是由编码蛋白S (PROS1)的基因变异引起的。本研究旨在评价ps缺陷患者PROS1基因分子分析的临床价值。我们对PROS1基因的编码区进行了Sanger测序和多重连接依赖探针扩增,以排除大的结构重排。采用颗粒增强免疫法测定游离PS,采用凝血法测定PS活性。共纳入87名ps缺陷者及其家庭成员。在22个索引参与者中,我们确定了13个PROS1编码变体。五种变体是新颖的。在21个索引参与者中,没有发现编码序列变异或结构重排。携带PROS1变异的指标参与者的游离PS水平低于未携带变异的指标参与者(0.51[0.32-0.61]对0.62 [0.57-0.73]× 103iu /L;与p.(Glu390Lys)变异(0.27 [0.24-0.37]× 103iu /L)相比,正常PROS1基因组p. PROS1变异为43%,正常PROS1基因组为17% (p = 0.05)。总之,我们报道了13个PROS1编码变体,其中包括5个新变体。PS水平因PROS1变异而异,当编码PROS1变异存在时,VTE的频率更高。因此,PROS1基因的分子分析可能在PS缺乏症的诊断工作中增加临床价值。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Genetic Variants in the Protein S ( PROS1 ) Gene and Protein S Deficiency in a Danish Population.

Protein S (PS) deficiency is a risk factor for venous thromboembolism (VTE) and can be caused by variants of the gene encoding PS ( PROS1 ). This study aimed to evaluate the clinical value of molecular analysis of the PROS1 gene in PS-deficient participants. We performed Sanger sequencing of the coding region of the PROS1 gene and multiplex ligation-dependent probe amplification to exclude large structural rearrangements. Free PS was measured by a particle-enhanced immunoassay, while PS activity was assessed by a clotting method. A total of 87 PS-deficient participants and family members were included. In 22 index participants, we identified 13 PROS1 coding variants. Five variants were novel. In 21 index participants, no coding sequence variants or structural rearrangements were identified. The free PS level was lower in index participants carrying a PROS1 variant compared with index participants with no variant (0.51 [0.32-0.61] vs. 0.62 [0.57-0.73] × 10 3 IU/L; p  < 0.05). The p.(Thr78Met) variant was associated with only slightly decreased free PS levels (0.59 [0.53-0.66] × 10 3 IU/L) compared with the p.(Glu390Lys) variant (0.27 [0.24-0.37] × 10 3 IU/L, p  < 0.01). The frequency of VTE in participants with a coding PROS1 variant was 43 and 17% in the group with normal PROS1 gene ( p  = 0.05). In conclusion, we report 13 PROS1 coding variants including five novel variants. PS levels differ by PROS1 variant and the frequency of VTE was higher when a coding PROS1 variant was present. Hence, molecular analysis of the PROS1 gene may add clinical value in the diagnostic work-up of PS deficiency.

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