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胆汁糖蛋白对结肠肿瘤细胞生长的抑制作用。

Inhibition of colonic tumor cell growth by biliary glycoprotein.

作者信息

Kunath T, Ordoñez-Garcia C, Turbide C, Beauchemin N

机构信息

McGill Cancer Centre, McGill University, Montréal, Québec, Canada.

出版信息

Oncogene. 1995 Dec 7;11(11):2375-82.

PMID:8570189
Abstract

Biliary glycoproteins (BGPs) are members of the carcinoembryonic antigen (CEA) family. These glycoproteins function in vitro as intercellular adhesion molecules and, in vitro as intercellular adhesion molecules and, in the mouse, serve as receptors for the mouse hepatitis viruses. In previous studies, BGP expression has been reported to be generally downregulated in colon and liver carcinomas of human, rat and mouse origins. We now demonstrate that introduction of murine Bgp1 cDNA isoforms into a mouse colonic carcinoma cell line, negative for endogenous Bgpl expression, significantly alters the growth properties of these cells. Cells bearing two Bgp1 isoforms were growth-retarded and exhibited a reduced ability to form colonies in an in vitro transformation assay, when compared to parental or control neor cells. Furthermore, tumor formation was inhibited by 80% when cells bearing a full-length Bgp1 isoform were injected into BALB/c syngeneic mice, while cells expressing a Bgp1 isoform lacking most of the intracytoplasmic domain produced tumors as readily as the parental cells. There results indicate that a biliary glycoprotein isoform is involved in negative regulation of colonic tumor cell growth, by a process which requires its intracytoplasmic domain. The precise mechanisms causing Bgp-dependent tumor growth inhibition remain, however, to be defined.

摘要

胆汁糖蛋白(BGPs)是癌胚抗原(CEA)家族的成员。这些糖蛋白在体外作为细胞间粘附分子发挥作用,在小鼠体内作为小鼠肝炎病毒的受体。在先前的研究中,据报道,在人、大鼠和小鼠来源的结肠癌和肝癌中,BGP表达通常下调。我们现在证明,将小鼠Bgp1 cDNA异构体导入内源性Bgpl表达呈阴性的小鼠结肠癌细胞系中,会显著改变这些细胞的生长特性。与亲本或对照neor细胞相比,携带两种Bgp1异构体的细胞生长受阻,并且在体外转化试验中形成集落的能力降低。此外,当将携带全长Bgp1异构体的细胞注射到BALB/c同基因小鼠中时,肿瘤形成受到80%的抑制,而表达缺乏大部分胞质内结构域的Bgp1异构体的细胞与亲本细胞一样容易产生肿瘤。这些结果表明,一种胆汁糖蛋白异构体通过一种需要其胞质内结构域的过程参与结肠肿瘤细胞生长的负调控。然而,导致Bgp依赖性肿瘤生长抑制的确切机制仍有待确定。

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