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人类信号素A(V)和IV位于3p21.3小细胞肺癌缺失区域,并表现出不同的表达模式。

Human semaphorins A(V) and IV reside in the 3p21.3 small cell lung cancer deletion region and demonstrate distinct expression patterns.

作者信息

Sekido Y, Bader S, Latif F, Chen J Y, Duh F M, Wei M H, Albanesi J P, Lee C C, Lerman M I, Minna J D

机构信息

Hamon Center for Therapeutic Oncology Research, University of Texas Southwestern Medical Center, Dallas 75235, USA.

出版信息

Proc Natl Acad Sci U S A. 1996 Apr 30;93(9):4120-5. doi: 10.1073/pnas.93.9.4120.

Abstract

Semaphorins and collapsins make up a family of conserved genes that encode nerve growth cone guidance signals. We have identified two additional members of the human semaphorin family [human semaphorin A(V) and human semaphorin IV] in chromosome region 3p21.3, where several small cell lung cancer (SCLC) cell lines exhibit homozygous deletions indicative of a tumor suppressor gene. Human semaphorin A(V) has 86% amino acid homology with murine semaphorin A, whereas semaphorin IV is most closely related to murine semaphorin E, with 50% homology. These semaphorin genes are approximately 70 kb apart flanking two GTP-binding protein genes, GNAI-2 and GNAT-1. In contrast, other human semaphorin gene sequences (human semaphorin III and homologues of murine semaphorins B and C) are not located on chromosome 3. Human semaphorin A(V) is translated in vitro into a 90-kDa protein, which accumulates at the endoplasmic reticulum. The human semaphorin A(V) (3.4-kb mRNA) and IV (3.9- and 2.9-kb mRNAs) genes are expressed abundantly but differentially in a variety of human neural and nonneural tissues. Human semaphorin A(V) was expressed in only 1 out of 23 SCLCs and 7 out of 16 non-SCLCs, whereas semaphorin IV was expressed in 19 out of 23 SCLCs and 13 out of 16 non-SCLCs. Mutational analysis in semaphorin A(V) revealed mutations (germ line in one case) in 3 of 40 lung cancers. Our data suggest the need to determine the function of human semaphorins A(V) and IV in nonneural tissues and their role in the pathogenesis of lung cancer.

摘要

信号素和坍塌素构成了一个保守基因家族,该家族编码神经生长锥导向信号。我们在染色体区域3p21.3中鉴定出人类信号素家族的另外两个成员[人类信号素A(V)和人类信号素IV],在该区域,几个小细胞肺癌(SCLC)细胞系表现出纯合缺失,提示存在一个肿瘤抑制基因。人类信号素A(V)与小鼠信号素A有86%的氨基酸同源性,而信号素IV与小鼠信号素E关系最为密切,同源性为50%。这些信号素基因相隔约70 kb,位于两个GTP结合蛋白基因GNAI-2和GNAT-1两侧。相比之下,其他人类信号素基因序列(人类信号素III以及小鼠信号素B和C的同源物)并不位于3号染色体上。人类信号素A(V)在体外被翻译为一种90 kDa的蛋白质,该蛋白质在内质网中积累。人类信号素A(V)(3.4 kb mRNA)和IV(3.9 kb和2.9 kb mRNA)基因在多种人类神经和非神经组织中大量表达,但表达存在差异。人类信号素A(V)仅在23个SCLC中的1个以及16个非SCLC中的7个中表达,而信号素IV在23个SCLC中的19个以及16个非SCLC中的13个中表达。信号素A(V)的突变分析显示,40例肺癌中有3例发生了突变(其中1例为种系突变)。我们的数据表明,有必要确定人类信号素A(V)和IV在非神经组织中的功能及其在肺癌发病机制中的作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4564/39497/cc620fcfbb6e/pnas01516-0417-a.jpg

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