A Rare Variant in CACNA1D Segregates with 7 Bipolar I Disorder Cases in a Large Pedigree

Jessica Ross, Erika Gedvilaite, J. Badner, C. Erdman, L. Baird, N. Matsunami, M. Leppert, Jinchuan Xing, W. Byerley
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引用次数: 20

Abstract

Whole-genome sequencing was performed on 3 bipolar I disorder (BPI) cases from a multiplex pedigree of European ancestry with 7 BPI cases. Within CACNA1D, a gene implicated by genome-wide association studies, a G to C nucleotide transversion at 53,835,340 base pairs (bps) was found predicting the substitution of proline for alanine at amino acid position 1751 (A1751P). Using Sanger sequencing, the DNA variant was shown to co-segregate with the remaining 4 BPI cases within the pedigree. A high-resolution DNA denaturing curve method was then used to screen for the presence of the A1751P change in 4,150 BPI cases from the NIMH Genetics Initiative. The A1751P variant was found in 4 BPI cases. A second variant within exon 43, a C to T nucleotide transition, was found in 1 case at 53,835,355 bps, predicting the substitution of tryptophan for arginine at amino acid position 1771 (R1771W). In the NHLBI Exome Sequencing Project database, the heterozygous A1751P variant was present in 3 of 4,300 subjects of European ancestry, and the R1771W change was not present in any subject. Given the rarity of these variants, large-scale case/control rare variant sequencing studies will be required for definitive conclusions.
一种罕见的CACNA1D变异与7例双相I型障碍的大谱系分离
对3例双相I型障碍(BPI)病例进行了全基因组测序,这些病例来自欧洲血统的多重谱系,其中7例为BPI。在全基因组关联研究中发现的CACNA1D基因中,53,835,340个碱基对(bps)的G到C核苷酸翻转预测了氨基酸位置1751 (A1751P)上脯氨酸取代丙氨酸。使用Sanger测序,显示DNA变体与系谱中其余4例BPI病例共分离。然后使用高分辨率DNA变性曲线方法筛选来自NIMH遗传学倡议的4,150例BPI病例中A1751P变化的存在。在4例BPI病例中发现A1751P变异。外显子43内的第二个变异是C到T核苷酸的转变,在53,835,355 bps的1例中被发现,预测色氨酸取代了氨基酸位置1771 (R1771W)的精氨酸。在NHLBI外显子组测序项目数据库中,4300名欧洲血统的受试者中有3人存在杂合的A1751P变异,而R1771W的变化没有出现在任何受试者中。鉴于这些变异的罕见性,需要进行大规模病例/对照罕见变异测序研究以得出明确的结论。
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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