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人类结直肠癌中SMAD-2基因的体细胞改变。

Somatic alterations of the SMAD-2 gene in human colorectal cancers.

作者信息

Takagi Y, Koumura H, Futamura M, Aoki S, Ymaguchi K, Kida H, Tanemura H, Shimokawa K, Saji S

机构信息

Department of Surgery II, Gifu University School of Medicine, Japan.

出版信息

Br J Cancer. 1998 Nov;78(9):1152-5. doi: 10.1038/bjc.1998.645.

Abstract

The SMAD-2 gene, which is located at 18q21, has been identified as a candidate tumour-suppressor gene from work on colorectal cancers. The aim of the present study was to determine the clinical alterations and the significance of its mutations in a series of colorectal cancers previously examined for SMAD-4/DPC-4 gene. Mutation analyses of the SMAD-2 gene were carried out on cDNA samples from 36 primary colorectal cancer specimens using a combination of the polymerase chain reaction (PCR), single-strand conformation polymorphism (SSCP) and DNA sequencing. Only one missense mutation (2.8%), producing an amino acid substitution in the highly conserved region, and two homozygous deletions (5.5%) of the total coding region of the SMAD-2 gene were detected in the 36 cancers. The SMAD-2 gene may play a role as a candidate tumour-suppressor gene in a small fraction of colorectal cancers. However, allelic loss at 18q21 is very often seen in this type of tumour. Even in combination with changes in SMAD-4, the observed frequency was not sufficient to account for all 18q21 deletions in colorectal cancers. Thus, another tumour-suppressor gene, such as DCC, discovered as the first tumour-suppressor candidate in the region may also exist in this chromosome region.

摘要

位于18q21的SMAD - 2基因已被确定为在结直肠癌研究中作为候选肿瘤抑制基因。本研究的目的是确定在一系列先前检测过SMAD - 4/DPC - 4基因的结直肠癌中其突变的临床改变及意义。使用聚合酶链反应(PCR)、单链构象多态性(SSCP)和DNA测序相结合的方法,对36例原发性结直肠癌标本的cDNA样本进行了SMAD - 2基因的突变分析。在这36例癌症中,仅检测到1个错义突变(2.8%),在高度保守区域产生了氨基酸替换,以及2个SMAD - 2基因总编码区域的纯合缺失(5.5%)。SMAD - 2基因可能在一小部分结直肠癌中作为候选肿瘤抑制基因发挥作用。然而,在这类肿瘤中经常可见18q21处的等位基因缺失。即使与SMAD - 4的变化相结合,观察到的频率也不足以解释结直肠癌中所有的18q21缺失。因此,在该区域作为首个肿瘤抑制候选基因被发现的另一个肿瘤抑制基因,如DCC,可能也存在于该染色体区域。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1d9e/2063002/c410193eba66/brjcancer00013-0036-a.jpg

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