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人类癌胚抗原家族两类基因的相反功能。

Opposite functions for two classes of genes of the human carcinoembryonic antigen family.

作者信息

Stanners C P, DeMarte L, Rojas M, Gold P, Fuks A

机构信息

McGill Cancer Centre, McGill University, Montreal, Canada.

出版信息

Tumour Biol. 1995;16(1):23-31. doi: 10.1159/000217925.

Abstract

The human carcinoembryonic antigen (CEA) family can be divided into two subgroups according to the means of anchorage of member glycoproteins to the cell membrane: glycophosphatidyl inositol (GPI) linkage and transmembrane linkage. The GPI-linked members tend to be up-regulated in human tumours, whereas the transmembrane-linked members tend to be down-regulated. Thus the question as to whether the GPI members could be formally considered to function as oncogenes and the transmembrane members as tumour suppressors deserves consideration. Members of both subgroups function in vitro as intercellular adhesion molecules, but the characteristics of this adhesion, including temperature and divalent-cation dependence, differ markedly between the groups. Even the mechanism of intermolecular adhesion appears to differ fundamentally in that GPI-linked CEA-CEA binding involves a double reciprocal bonding between two domains, whereas transmembrane-linked biliary glycoprotein (BGP)-BGP binding requires only one domain. Finally, the ectopic expression of CEA in myoblasts can block myogenic differentiation leaving the cells with the ability to divide, while expression of BGP does not affect or may even accelerate myogenic differentiation. These differences in phenotypic effects in vitro thus mirror the differences observed in expression in tumours and support the view that the GPI and transmembrane groups have opposite effects on cells in relation to the malignant phenotype.

摘要

人类癌胚抗原(CEA)家族可根据成员糖蛋白与细胞膜的锚定方式分为两个亚组:糖基磷脂酰肌醇(GPI)连接和跨膜连接。GPI连接的成员在人类肿瘤中往往上调,而跨膜连接的成员往往下调。因此,GPI成员是否可被正式视为癌基因,而跨膜成员是否可被视为肿瘤抑制基因,这一问题值得探讨。两个亚组的成员在体外均作为细胞间粘附分子发挥作用,但两组之间这种粘附的特性,包括温度和二价阳离子依赖性,存在显著差异。甚至分子间粘附的机制似乎也有根本不同,因为GPI连接的CEA-CEA结合涉及两个结构域之间的双相互作用,而跨膜连接的胆汁糖蛋白(BGP)-BGP结合仅需要一个结构域。最后,CEA在成肌细胞中的异位表达可阻断肌源性分化,使细胞具有分裂能力,而BGP的表达不影响甚至可能加速肌源性分化。因此,体外表型效应的这些差异反映了肿瘤中观察到的表达差异,并支持这样一种观点,即GPI和跨膜组在恶性表型方面对细胞具有相反的作用。

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