Department of Human Genetics, Yokohama City University Graduate School of Medicine, Yokohama, Kanagawa 236-0004, Japan.
BITS Company, Limited, Tokyo 101-0062, Japan.
Genome Res. 2023 Mar;33(3):435-447. doi: 10.1101/gr.277335.122. Epub 2023 Mar 27.
Tandem repeats (TRs) are one of the largest sources of polymorphism, and their length is associated with gene regulation. Although previous studies reported several tandem repeats regulating gene splicing in (spl-TRs), no large-scale study has been conducted. In this study, we established a genome-wide catalog of 9537 spl-TRs with a total of 58,290 significant TR-splicing associations across 49 tissues (false discovery rate 5%) by using Genotype-Tissue expression (GTex) Project data. Regression models explaining splicing variation by using spl-TRs and other flanking variants suggest that at least some of the spl-TRs directly modulate splicing. In our catalog, two spl-TRs are known loci for repeat expansion diseases, spinocerebellar ataxia 6 (SCA6) and 12 (SCA12). Splicing alterations by these spl-TRs were compatible with those observed in SCA6 and SCA12. Thus, our comprehensive spl-TR catalog may help elucidate the pathomechanism of genetic diseases.
串联重复(TRs)是最大的多态性来源之一,其长度与基因调控有关。尽管之前的研究报道了几个串联重复调节基因剪接(spl-TRs),但尚未进行大规模研究。在这项研究中,我们通过使用基因型-组织表达(GTex)项目数据,建立了一个包含 9537 个 spl-TRs 的全基因组目录,这些 TRs 总共与 49 种组织中的 58290 个显著的 TR-剪接关联相关(错误发现率为 5%)。通过使用 spl-TRs 和其他侧翼变体来解释剪接变异的回归模型表明,至少有一些 spl-TRs 可以直接调节剪接。在我们的目录中,有两个 spl-TRs 是已知的重复扩展疾病的基因座,即脊髓小脑共济失调 6 型(SCA6)和 12 型(SCA12)。这些 spl-TRs 引起的剪接改变与在 SCA6 和 SCA12 中观察到的改变一致。因此,我们全面的 spl-TR 目录可能有助于阐明遗传疾病的发病机制。
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