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二肽基肽酶IV活性和/或结构同源物在癌症中的表达模式

Expression pattern of dipeptidyl peptidase IV activity and/or structure homologues in cancer.

作者信息

Kotacková L, Baláziová E, Sedo A

机构信息

Charles University in Prague, First Faculty of Medicine, Institute of Biochemistry and Experimental Oncology, Joint Laboratory of Cancer Cell Biology, and Institute of Physiology, Academy of Sciences of the Czech Republic, Prague, Czech Republic.

出版信息

Folia Biol (Praha). 2009;55(3):77-84.

Abstract

Proline at the second position of the N-terminus of biologically active peptides involved in cell growth regulation is an evolutionarily conserved motif protecting them against cleavage by non-specific proteases. Just a small number of proline-specific hydrolases including dipeptidyl peptidase IV (DPP-IV) and related molecules is capable of cleaving such post-prolyl bond. DPP-IV, originally described on the basis of its enzymatic activity, is a ubiquitous, multifunctional homodimeric plasma membrane glycoprotein of type II. Subsequently, several other molecules related to DPP-IV by their enzymatic activity and/or sequence were discovered and classified as "dipeptidyl peptidase IV activity and/or structure homologues" (DASH). Along with canonical DPP-IV this group comprises DPP-IVbeta, DPP-II, DPP6, DPP8, DPP9, DPP10 and fibroblast activation protein alpha (FAP-alpha). Recent observations of deregulated expression of several DASH molecules in multiple human cancers led to the assumptions of their pathogenetic relevance in cancerogenesis. Here we review recent information about selected DASH molecules in human malignancies.

摘要

参与细胞生长调节的生物活性肽N端第二个位置的脯氨酸是一种进化上保守的基序,可保护它们不被非特异性蛋白酶切割。只有少数脯氨酸特异性水解酶,包括二肽基肽酶IV(DPP-IV)及相关分子,能够切割这种脯氨酸后肽键。DPP-IV最初是根据其酶活性描述的,是一种普遍存在的、多功能的II型同二聚体细胞膜糖蛋白。随后,发现了其他几种通过酶活性和/或序列与DPP-IV相关的分子,并将其归类为“二肽基肽酶IV活性和/或结构同源物”(DASH)。除了典型的DPP-IV,该组还包括DPP-IVβ、DPP-II、DPP6、DPP8、DPP9、DPP10和成纤维细胞活化蛋白α(FAP-α)。最近在多种人类癌症中观察到几种DASH分子的表达失调,这导致人们推测它们在癌症发生中的致病相关性。在此,我们综述了有关人类恶性肿瘤中选定DASH分子的最新信息。

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