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TC21基因中的一种新型插入突变激活了其在人平滑肌肉瘤细胞系中的转化活性。

A novel insertional mutation in the TC21 gene activates its transforming activity in a human leiomyosarcoma cell line.

作者信息

Huang Y, Saez R, Chao L, Santos E, Aaronson S A, Chan A M

机构信息

Derald H. Ruttenberg Cancer Center, Mount Sinai Medical Center, New York, NY 10029, USA.

出版信息

Oncogene. 1995 Oct 5;11(7):1255-60.

PMID:7478545
Abstract

TC21 is the fourth member of the ras gene family to exhibit oncogenic activation in human tumor cells. To assess the prevalence of activated TC21 oncogenes in human tumors, we have developed sensitive single-strand conformational polymorphism (SSCP) conditions and immunological reagents for the detection of both single base alterations and/or overt overexpression in a wide spectrum of human tumor cell lines and surgical samples. In an initial examination of 33 human tumor specimens, we observed a novel nine basepair three amino acids insertion at TC21 codon 24 in one human uterine leiomyosarcoma cell line, SK-UT-1. This mutant allele when transfected into NIH3T3 cells, displayed high transforming activity comparable to that of the Leu72 oncogenic mutant identified by expression cDNA cloning from a human ovarian carcinoma cell line. Comparing the level of GTP-binding by the mutant and normal TC21 products revealed that this novel lesion increases the GTP-bound form of the TC21 molecule. These findings imply that the mechanism by which mutations activate the oncogenic properties of this ras-related molecule is analogous to that of previously known ras family members.

摘要

TC21是ras基因家族中第四个在人类肿瘤细胞中表现出致癌激活作用的成员。为了评估激活的TC21癌基因在人类肿瘤中的普遍性,我们开发了灵敏的单链构象多态性(SSCP)条件和免疫试剂,用于检测广泛的人类肿瘤细胞系和手术样本中的单碱基改变和/或明显的过表达。在对33个人类肿瘤标本的初步检查中,我们在一个人子宫平滑肌肉瘤细胞系SK-UT-1中观察到TC21密码子24处有一个新的9个碱基对(三个氨基酸)的插入。当将这个突变等位基因转染到NIH3T3细胞中时,它表现出与通过从人卵巢癌细胞系中表达cDNA克隆鉴定出的Leu72致癌突变体相当的高转化活性。比较突变型和正常TC21产物的GTP结合水平发现,这个新的病变增加了TC21分子的GTP结合形式。这些发现表明,突变激活这个与ras相关分子致癌特性的机制与先前已知的ras家族成员类似。

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