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错配修复缺陷的结直肠肿瘤中的APC突变

APC mutations in colorectal tumors with mismatch repair deficiency.

作者信息

Huang J, Papadopoulos N, McKinley A J, Farrington S M, Curtis L J, Wyllie A H, Zheng S, Willson J K, Markowitz S D, Morin P, Kinzler K W, Vogelstein B, Dunlop M G

机构信息

University of Edinburgh, Department of Surgery, Royal Infirmary, United Kingdom.

出版信息

Proc Natl Acad Sci U S A. 1996 Aug 20;93(17):9049-54. doi: 10.1073/pnas.93.17.9049.

Abstract

We have investigated the influence of genetic instability [replication error (RER) phenotype] on APC (adenomatous polyposis coli), a gene thought to initiate colorectal tumorigenesis. The prevalence of APC mutations was similar in RER and non-RER tumors, indicating that both tumor types share this step in neoplastic transformation. However, in a total of 101 sequenced mutations, we noted a substantial excess of APC frameshift mutations in the RER cases (70% in RER tumors versus 47% in non-RER tumors, P < 0.04). These frameshifts were characteristic of mutations arising in cells deficient in DNA mismatch repair, with a predilection for mononucleotide repeats in the RER tumors (P < 0.0002), particularly (A)n tracts (P < 0.00007). These findings suggest that the genetic instability that is reflected by the RER phenotype precedes, and is responsible for, APC mutation in RER large bowel tumors and have important implications for understanding the very earliest stages of neoplasia in patients with tumors deficient in mismatch repair.

摘要

我们研究了遗传不稳定性[复制错误(RER)表型]对APC(腺瘤性息肉病 coli)的影响,APC是一种被认为启动结直肠癌发生的基因。RER肿瘤和非RER肿瘤中APC突变的发生率相似,表明这两种肿瘤类型在肿瘤转化过程中都有这一步骤。然而,在总共101个测序突变中,我们注意到RER病例中APC移码突变明显过多(RER肿瘤中为70%,非RER肿瘤中为47%,P < 0.04)。这些移码突变是DNA错配修复缺陷细胞中产生的突变的特征,在RER肿瘤中倾向于单核苷酸重复(P < 0.0002),尤其是(A)n序列(P < 0.00007)。这些发现表明,RER表型所反映的遗传不稳定性在RER大肠肿瘤中先于APC突变并导致其发生,对于理解错配修复缺陷肿瘤患者肿瘤形成的最早阶段具有重要意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4942/38593/d7e6c6d47a8e/pnas01521-0263-a.jpg

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