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肝素结合生长相关分子的分泌及生物学活性。重组蛋白和组织来源蛋白促进神经突生长及有丝分裂的作用。

Secretion and biological activities of heparin-binding growth-associated molecule. Neurite outgrowth-promoting and mitogenic actions of the recombinant and tissue-derived protein.

作者信息

Raulo E, Julkunen I, Merenmies J, Pihlaskari R, Rauvala H

机构信息

Institute of Biotechnology, University of Helsinki, Finland.

出版信息

J Biol Chem. 1992 Jun 5;267(16):11408-16.

PMID:1597470
Abstract

The cDNA for the developmentally regulated, neurite outgrowth-promoting protein HB-GAM (heparin-binding growth-associated molecule) was recently cloned and shown to encode a novel lysine-rich sequence that is homologous with retinoic acid-induced sequences suggested to function in cell differentiation (Merenmies, J., and Rauvala, H. (1990) J. Biol. Chem. 265, 16721-16724). The same sequence was found for the mitogenic and neurite outgrowth-promoting protein pleiotrophin (Li, Y.-S., Milner, P. G., Chauhan, A. K., Watson, M. A., Hoffman, R. M., Kodner, C. M., Milbrandt, J., and Deuel, T. F. (1990) Science 250, 1690-1694). In this study, we have constructed a recombinant baculovirus using the cDNA that encodes the putative preprotein of HB-GAM. The putative secretion signal of HB-GAM is cleaved off in the baculovirus expression system, and the recombinant protein is rapidly secreted to the culture medium. Recombinant HB-GAM purified from the culture medium retains the biochemical characteristics and the neurite outgrowth-promoting activity found for the tissue-derived protein. Studies on the neurite outgrowth-promoting activity suggest that HB-GAM functions as an extracellular matrix-associated protein that enhances axonal growth in perinatal cerebral neurons of the rat. Since the same predicted amino acid sequence has been ascribed to a mitogenic protein, mitogenic activities of the recombinant HB-GAM and of tissue-derived HB-GAM fractions were also studied. Recombinant HB-GAM did not display any significant mitogenic activity, suggesting that tissue-derived HB-GAM preparations may contain other heparin-binding mitogenic factors. We identified in brain-derived HB-GAM fractions a 17-kDa protein (p17) that is detached from heparin by a slightly higher salt concentration as compared to HB-GAM. We suggest that p17 is structurally distinct from HB-GAM and responsible for the mitogenic actions of tissue-derived HB-GAM fractions.

摘要

发育调控的、促进神经突生长的蛋白HB-GAM(肝素结合生长相关分子)的cDNA最近被克隆出来,结果显示其编码一种富含赖氨酸的新序列,该序列与推测在细胞分化中起作用的视黄酸诱导序列同源(梅伦米耶斯,J.,和劳瓦拉,H.(1990年)《生物化学杂志》265,16721 - 16724)。促有丝分裂和促进神经突生长的蛋白多效生长因子也发现了相同序列(李,Y.-S.,米尔纳,P.G.,乔汉,A.K.,沃森,M.A.,霍夫曼,R.M.,科德纳,C.M.,米尔布兰特,J.,和迪尤尔,T.F.(1990年)《科学》250,1690 - 1694)。在本研究中,我们利用编码HB-GAM假定前体蛋白的cDNA构建了一种重组杆状病毒。HB-GAM的假定分泌信号在杆状病毒表达系统中被切除,重组蛋白迅速分泌到培养基中。从培养基中纯化的重组HB-GAM保留了组织来源蛋白的生化特性和促进神经突生长的活性。对促进神经突生长活性的研究表明,HB-GAM作为一种细胞外基质相关蛋白发挥作用,可增强大鼠围产期脑神经元的轴突生长。由于相同的预测氨基酸序列已被归因于一种促有丝分裂蛋白,因此还研究了重组HB-GAM和组织来源的HB-GAM组分的促有丝分裂活性。重组HB-GAM未显示出任何显著的促有丝分裂活性,这表明组织来源的HB-GAM制剂可能含有其他肝素结合促有丝分裂因子。我们在脑来源的HB-GAM组分中鉴定出一种17 kDa的蛋白(p17),与HB-GAM相比,它在稍高的盐浓度下从肝素上解离。我们认为p17在结构上与HB-GAM不同,并且是组织来源的HB-GAM组分促有丝分裂作用的原因。

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