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包含单个盒式外显子的人类基因中的内含子CpG含量与可变剪接

Intronic CpG content and alternative splicing in human genes containing a single cassette exon.

作者信息

Malousi Andigoni, Maglaveras Nicos, Kouidou Sofia

机构信息

Laboratory of Medical Informatics, Aristotle University of Thessaloniki, Thessaloniki, Greece.

出版信息

Epigenetics. 2008 Mar-Apr;3(2):69-73. doi: 10.4161/epi.3.2.6066. Epub 2008 Apr 8.

Abstract

Clinical data provide evidence for the association of missplicing with methyl-binding protein mutations and inhibition of methylation. In this study, we analyzed a 373 human gene database containing a single alternatively spliced exon (cassette) and 1,039 constitutive introns, and showed that CpG frequencies are higher in alternative compared to constitutive introns, particularly in donors preceding cassette exons (p < 0.0001). Donors with more than three CpGs within 50 nt from splice junctions are mostly upstream alternative (21.83% vs. 3.21% for constitutive and 4.68% for downstream introns). Significant differences are also observed beyond the 7(th) nucleotide of the donors. Upstream CpG-rich motifs are not related to Alus, while the latter are frequent in downstream donors. The association of epigenetic modification sites and alternative splicing, indicated above, is not reflected in the computationally obtained splicing potentials.

摘要

临床数据为剪接异常与甲基结合蛋白突变及甲基化抑制之间的关联提供了证据。在本研究中,我们分析了一个包含单个可变剪接外显子(盒式外显子)和1039个组成型内含子的373个人类基因数据库,并表明与组成型内含子相比,可变内含子中的CpG频率更高,尤其是在盒式外显子之前的供体区域(p < 0.0001)。在距剪接接头50 nt范围内有超过三个CpG的供体大多位于上游可变区域(组成型内含子为3.21%,下游内含子为4.68%,而上游可变区域为21.83%)。在供体的第7个核苷酸之后也观察到了显著差异。富含CpG的上游基序与Alu元件无关,而Alu元件在下游供体中很常见。上述表观遗传修饰位点与可变剪接之间的关联在通过计算获得的剪接潜能中并未体现出来。

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