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一种新型肿瘤源性 SGOL1 变异导致异常有丝分裂和不稳定的染色单体粘连。

A novel tumor-derived SGOL1 variant causes abnormal mitosis and unstable chromatid cohesion.

机构信息

First Department of Pathology, Hamamatsu University School of Medicine, Japan.

出版信息

Oncogene. 2011 Nov 3;30(44):4453-63. doi: 10.1038/onc.2011.152. Epub 2011 May 2.

DOI:10.1038/onc.2011.152
PMID:21532624
Abstract

Mitosis is the most conspicuous cell cycle phase, because it is the phase in which the dynamic physical distributions of cellular components into the two daughter cells occur. The separation of sister chromatids is especially important during mitosis, because of the extreme accuracy required for distribution to the next generation of cells. Shugoshin-like 1 (SGOL1) is a key protein in protecting sister chromatids from precocious separation. We have reported finding that chromosome instability is more likely in SGOL1-downregulated colorectal cancers, but it is still unknown whether there is an association between cancer and SGOL1 transcript variation. Here, we identified a novel SGOL1 variant, SGOL1-P1, in human colon cancer. The SGOL1-P1 transcript contains an exon-skip of exon 3 that results in a stop codon occurring within exon 4. Overexpression of SGOL1-P1 in HCT116 cells resulted in an increased number of cells with aberrant chromosome alignment, precociously separated chromatids and delayed mitotic progression, occasionally followed by inaccurate distribution of the chromosomes. These phenotypes, observed when SGOL1-P1 was present, were also observed very frequently in SGOL1-knockdown cells. Furthermore, the overexpression of SGOL1-P1 inhibited the localization of endogenous SGOL1 and cohesin subunit RAD21/SCC1 to the centromere. These results suggest that SGOL1-P1 may function as a negative factor to native SGOL1, and that abundant expression of SGOL1-P1 may be responsible for chromosomal instability.

摘要

有丝分裂是最显著的细胞周期阶段,因为它是细胞成分动态物理分配到两个子细胞中的阶段。姐妹染色单体的分离在有丝分裂中尤为重要,因为需要极高的准确性才能将其分配到下一代细胞中。Shugoshin-like 1 (SGOL1) 是保护姐妹染色单体免受过早分离的关键蛋白。我们已经报告发现,SGOL1 下调的结直肠癌更有可能出现染色体不稳定,但仍不清楚癌症与 SGOL1 转录变体之间是否存在关联。在这里,我们在人结肠癌中鉴定了一种新型的 SGOL1 变体 SGOL1-P1。SGOL1-P1 转录本包含外显子 3 的外显子跳跃,导致 4 号外显子中出现终止密码子。在 HCT116 细胞中过表达 SGOL1-P1 会导致具有异常染色体排列、过早分离的染色单体和延迟有丝分裂进展的细胞数量增加,偶尔会导致染色体分配不准确。当存在 SGOL1-P1 时观察到这些表型,在 SGOL1 敲低细胞中也非常频繁地观察到这些表型。此外,SGOL1-P1 的过表达抑制了内源性 SGOL1 和着丝粒亚基 RAD21/SCC1 到着丝粒的定位。这些结果表明,SGOL1-P1 可能作为负性因子起作用于天然 SGOL1,并且 SGOL1-P1 的大量表达可能是导致染色体不稳定的原因。

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A novel tumor-derived SGOL1 variant causes abnormal mitosis and unstable chromatid cohesion.一种新型肿瘤源性 SGOL1 变异导致异常有丝分裂和不稳定的染色单体粘连。
Oncogene. 2011 Nov 3;30(44):4453-63. doi: 10.1038/onc.2011.152. Epub 2011 May 2.
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Frameshift mutations of chromosome cohesion-related genes SGOL1 and PDS5B in gastric and colorectal cancers with high microsatellite instability.染色体凝聚相关基因 SGOL1 和 PDS5B 的移码突变与高微卫星不稳定的胃癌和结直肠癌。
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PHB2 protects sister-chromatid cohesion in mitosis.PHB2在有丝分裂中保护姐妹染色单体黏连。
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DNA mismatch repair is not disrupted in stage 0 colorectal cancer resected using endoscopic submucosal dissection.采用内镜下黏膜下剥离术切除的0期结直肠癌中,DNA错配修复未被破坏。
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