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一种新型人类神经突生长促进蛋白基因家族的两个成员的克隆、特性分析及发育调控

Cloning, characterization and developmental regulation of two members of a novel human gene family of neurite outgrowth-promoting proteins.

作者信息

Kretschmer P J, Fairhurst J L, Decker M M, Chan C P, Gluzman Y, Böhlen P, Kovesdi I

机构信息

Molecular Biology Research Section, American Cyanamid Company, Lederle Laboratories, Pearl River, New York 10965.

出版信息

Growth Factors. 1991;5(2):99-114. doi: 10.3109/08977199109000275.

Abstract

This report describes the cloning, expression and characterization of two members of a novel human gene family of proteins, HBNF and MK, which exhibit neurite outgrowth-promoting activity. The HBNF cDNA gene codes for a 168-residue protein which is a precursor for a previously described brain-derived heparin-binding protein of 136 amino acids. The second human gene identified in this study, called MK, codes for a 143-residue protein (including a 22-amino acid signal sequence) which is 46% homologous with HBNF. Complementary DNA constructs coding for the mature HBNF and MK proteins were expressed in bacteria and purified by heparin affinity chromatography. These recombinant proteins exhibited neurite-outgrowth promoting activity, but lacked mitogenic activity. The HBNF gene is expressed in the brain of adult mice and rats, but only minimal expression of MK was observed in this tissue. Different patterns of developmental expression were observed in the embryonic mouse, with MK expression peaking in the brain between days E12 and E14 and diminishing to minimal levels in the adult, while expression of HBNF mRNA was observed to gradually increase during embryogenesis, reaching a maximal level at birth and maintaining this level into adulthood. Expression of these genes was also observed in the human embryonal carcinoma cell line, NT2/D1. Retinoic acid induced the expression of HBNF and MK 6- and 11-fold, respectively, in this cell line. Our studies indicate that HBNF and MK are members of a new family of highly conserved, developmentally regulated genes that may play a role in nervous tissue development and/or maintenance.

摘要

本报告描述了一种新型人类蛋白质基因家族的两个成员HBNF和MK的克隆、表达及特性,它们具有促进神经突生长的活性。HBNF cDNA基因编码一种含168个氨基酸残基的蛋白质,该蛋白质是先前描述的含136个氨基酸的脑源性肝素结合蛋白的前体。本研究中鉴定出的第二个人类基因MK,编码一种含143个氨基酸残基的蛋白质(包括一个22个氨基酸的信号序列),它与HBNF有46%的同源性。编码成熟HBNF和MK蛋白的互补DNA构建体在细菌中表达,并通过肝素亲和层析进行纯化。这些重组蛋白具有促进神经突生长的活性,但缺乏促有丝分裂活性。HBNF基因在成年小鼠和大鼠的脑中表达,但在该组织中仅观察到MK的微量表达。在胚胎小鼠中观察到不同的发育表达模式,MK的表达在胚胎第12天至第14天之间在脑中达到峰值,在成年期降至最低水平,而HBNF mRNA的表达在胚胎发育过程中逐渐增加,在出生时达到最高水平并维持至成年期。在人类胚胎癌细胞系NT2/D1中也观察到了这些基因的表达。视黄酸分别在该细胞系中诱导HBNF和MK的表达增加6倍和11倍。我们的研究表明,HBNF和MK是一个新的高度保守、发育调控基因家族的成员,它们可能在神经组织发育和/或维持中发挥作用。

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