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检测丹麦结直肠癌患者中鉴定出的 MLH1、MSH2 和 MSH6 内含子突变的功能。

Functional examination of MLH1, MSH2, and MSH6 intronic mutations identified in Danish colorectal cancer patients.

机构信息

Center for Genomic Medicine, Rigshospitalet, University of Copenhagen, Blegdamsvej 9, DK-2100 Copenhagen, Denmark.

出版信息

BMC Med Genet. 2013 Oct 3;14:103. doi: 10.1186/1471-2350-14-103.

DOI:10.1186/1471-2350-14-103
PMID:24090359
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3850734/
Abstract

BACKGROUND

Germ-line mutations in the DNA mismatch repair genes MLH1, MSH2, and MSH6 predispose to the development of colorectal cancer (Lynch syndrome or hereditary nonpolyposis colorectal cancer). These mutations include disease-causing frame-shift, nonsense, and splicing mutations as well as large genomic rearrangements. However, a large number of mutations, including missense, silent, and intronic variants, are classified as variants of unknown clinical significance.

METHODS

Intronic MLH1, MSH2, or MSH6 variants were investigated using in silico prediction tools and mini-gene assay to asses the effect on splicing.

RESULTS

We describe in silico and in vitro characterization of nine intronic MLH1, MSH2, or MSH6 mutations identified in Danish colorectal cancer patients, of which four mutations are novel. The analysis revealed aberrant splicing of five mutations (MLH1 c.588 + 5G > A, MLH1 c.677 + 3A > T, MLH1 c.1732-2A > T, MSH2 c.1276 + 1G > T, and MSH2 c.1662-2A > C), while four mutations had no effect on splicing compared to wild type (MLH1 c.117-34A > T, MLH1 c.1039-8 T > A, MSH2 c.2459-18delT, and MSH6 c.3439-16C > T).

CONCLUSIONS

In conclusion, we classify five MLH1/MSH2 mutations as pathogenic, whereas four MLH1/MSH2/MSH6 mutations are classified as neutral. This study supports the notion that in silico prediction tools and mini-gene assays are important for the classification of intronic variants, and thereby crucial for the genetic counseling of patients and their family members.

摘要

背景

DNA 错配修复基因 MLH1、MSH2 和 MSH6 的种系突变可导致结直肠癌(林奇综合征或遗传性非息肉病性结直肠癌)的发生。这些突变包括致病的移码、无义和剪接突变以及大片段基因组重排。然而,大量的突变,包括错义、沉默和内含子变体,被归类为临床意义不明的变体。

方法

使用计算机预测工具和迷你基因检测来研究 MLH1、MSH2 或 MSH6 的内含子变体,以评估其对剪接的影响。

结果

我们描述了在丹麦结直肠癌患者中发现的 9 种 MLH1、MSH2 或 MSH6 内含子突变的计算机和体外特征,其中 4 种突变是新的。分析显示 5 种突变存在异常剪接(MLH1 c.588+5G>A、MLH1 c.677+3A>T、MLH1 c.1732-2A>T、MSH2 c.1276+1G>T 和 MSH2 c.1662-2A>C),而 4 种突变与野生型相比对剪接没有影响(MLH1 c.117-34A>T、MLH1 c.1039-8T>A、MSH2 c.2459-18delT 和 MSH6 c.3439-16C>T)。

结论

总之,我们将 5 个 MLH1/MSH2 突变归类为致病性突变,而 4 个 MLH1/MSH2/MSH6 突变归类为中性突变。这项研究支持了这样一种观点,即计算机预测工具和迷你基因检测对于内含子变体的分类非常重要,因此对于患者及其家庭成员的遗传咨询至关重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e3da/3850734/ce624d54a885/1471-2350-14-103-1.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e3da/3850734/ce624d54a885/1471-2350-14-103-1.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e3da/3850734/ce624d54a885/1471-2350-14-103-1.jpg

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