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Met/HGF受体在人类骨肉瘤中过度表达,并通过旁分泌或自分泌途径被激活。

The Met/HGF receptor is over-expressed in human osteosarcomas and is activated by either a paracrine or an autocrine circuit.

作者信息

Ferracini R, Di Renzo M F, Scotlandi K, Baldini N, Olivero M, Lollini P, Cremona O, Campanacci M, Comoglio P M

机构信息

Saluzzo General Hospital, Italy.

出版信息

Oncogene. 1995 Feb 16;10(4):739-49.

PMID:7862451
Abstract

The c-MET oncogene encodes the receptor for the Hepatocyte Growth Factor/Scatter Factor (HGF), a cytokine that stimulates the invasive growth of normal and neoplastic cells. The Met/HGF receptor is expressed by epithelial cells and its ligand by cells of mesenchymal origin. Receptor-ligand interaction occurs via a paracrine circuit. We studied the expression of the Met/HGF receptor and of its ligand in mesenchymal human tumours by examining 39 clinical samples of bone tumours. The Met/HGF receptor was not detectable in the majority of bone tumours, as expected from their mesenchymal origin. Notably, the receptor was overexpressed in 60% of the osteosarcomas examined. In 12 osteosarcoma cell lines the Met/HGF receptor was overexpressed, phosphorylated by HGF stimulation and fully functional. HGF was detected in two out of seven clinical specimens of osteosarcoma. The ligand and the receptor are co-expressed in two clonal osteosarcoma cell lines. In these lines the Met/HGF receptor was constitutively phosphorylated; phosphorylation was suppressed by suramin treatment, a known blocker of autocrine loops. These data suggest that activation of the Met/HGF receptor by a paracrine or an autocrine mechanism might play a role in the particularly aggressive behaviour of osteosarcomas.

摘要

c-MET原癌基因编码肝细胞生长因子/分散因子(HGF)的受体,HGF是一种刺激正常细胞和肿瘤细胞侵袭性生长的细胞因子。Met/HGF受体由上皮细胞表达,其配体由间充质来源的细胞表达。受体-配体相互作用通过旁分泌回路发生。我们通过检测39例骨肿瘤临床样本,研究了Met/HGF受体及其配体在人间充质肿瘤中的表达。正如从其间充质起源所预期的那样,在大多数骨肿瘤中未检测到Met/HGF受体。值得注意的是,在所检测的骨肉瘤中,60%的肿瘤该受体过度表达。在12种骨肉瘤细胞系中,Met/HGF受体过度表达,经HGF刺激后发生磷酸化且功能完全正常。在7例骨肉瘤临床标本中有2例检测到HGF。在两种骨肉瘤克隆细胞系中配体和受体共同表达。在这些细胞系中,Met/HGF受体持续磷酸化;苏拉明处理可抑制磷酸化,苏拉明是一种已知的自分泌回路阻断剂。这些数据表明,旁分泌或自分泌机制激活Met/HGF受体可能在骨肉瘤特别具有侵袭性的行为中起作用。

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