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肝细胞生长因子(HGF)刺激原癌基因c-MET编码的受体的酪氨酸激酶活性。

Hepatocyte growth factor (HGF) stimulates the tyrosine kinase activity of the receptor encoded by the proto-oncogene c-MET.

作者信息

Naldini L, Vigna E, Narsimhan R P, Gaudino G, Zarnegar R, Michalopoulos G K, Comoglio P M

机构信息

Department of Biomedical Sciences & Oncology, University of Torino, School of Medicine, Italy.

出版信息

Oncogene. 1991 Apr;6(4):501-4.

PMID:1827664
Abstract

The human proto-oncogene c-MET encodes a heterodimeric 190 kDa transmembrane protein (p190c-met) with structural features of a tyrosine kinase receptor. The ligand for this putative receptor has not yet been identified. By Northern blot hybridization we found that, among a restricted number of human tissues, c-MET is highly expressed in the liver. This prompted us to test the hypothesis of a functional interaction between the c-MET receptor and Hepatocyte Growth Factor (HGF), a heparin-binding polypeptide consisting of heavy and light chains of 65 and 35 kDa. Nanomolar concentrations of highly purified HGF added to GTL-16 cells, which overexpress the c-MET receptor, enhanced the phosphorylation on tyrosine of the p190c-met kinase. Addition of other known growth factors or serum was ineffective. The kinase activity of the c-MET receptor was also stimulated by HGF in an in vitro assay, after detergent solubilization and partial purification of p190c-met. Moreover, elution of immunoprecipitates obtained with anti-MET antibodies from GTL-16 cell lysates yielded an HGF-responsive kinase activity. These results suggest that HGF, or a growth factor structurally related to HGF, is a candidate ligand for the receptor encoded by c-MET.

摘要

人类原癌基因c-MET编码一种190 kDa的异二聚体跨膜蛋白(p190c-met),具有酪氨酸激酶受体的结构特征。该假定受体的配体尚未确定。通过Northern印迹杂交,我们发现在有限数量的人体组织中,c-MET在肝脏中高度表达。这促使我们检验c-MET受体与肝细胞生长因子(HGF)之间功能相互作用的假设,HGF是一种由65 kDa和35 kDa的重链和轻链组成的肝素结合多肽。将纳摩尔浓度的高度纯化的HGF添加到过表达c-MET受体的GTL-16细胞中,可增强p190c-met激酶酪氨酸位点的磷酸化。添加其他已知生长因子或血清则无效。在对p190c-met进行去污剂溶解和部分纯化后,HGF在体外试验中也刺激了c-MET受体的激酶活性。此外,从GTL-16细胞裂解物中用抗MET抗体获得的免疫沉淀物洗脱后产生了HGF反应性激酶活性。这些结果表明,HGF或与HGF结构相关的生长因子是c-MET编码受体的候选配体。

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