摘要
G-protein-coupled receptors receive many different signals to activate different functions such as cell growth, proliferation, and migration. KiSS1 is a metastasis suppressor gene that has been shown to inhibit metastasis of human melanomas and breast carcinomas. The human KiSS1 gene encodes a COOH-terminally amidated active peptide, and this peptide is the ligand of a novel G-protein-coupled receptor. However, the mechanism of the antimetastatic actions of KiSS1 and its G-protein-coupled receptor has not been elucidated. In this study, we identified the mouse homologues of the KiSS1 peptide and its G-protein-coupled receptor and characterized the signaling pathways mediated by the activation of the KiSS1 receptor. Although human and mouse KiSS1 proteins share relatively low overall homology (52%), the active peptides (10-amino-acid residues) are highly conserved between mouse and human KiSS1 proteins, varying by only one conserved amino acid [Tyr (Y) to Phe (F)]. Activation of the receptor by KiSS1 peptide leads to the activation of G-protein-activated phospholipase C (PLC-β), which suggests direct coupling of the KiSS1 peptide to the Gaαq-mediate PLC-Ca2+ signaling pathway. Furthermore, activation of the KiSS1 receptor inhibits cell proliferation and cell migration, key characteristics of tumor metastasis.
| 源语言 | 英语 |
|---|---|
| 页(从-至) | 5399-5404 |
| 页数 | 6 |
| 期刊 | Cancer Research |
| 卷 | 62 |
| 期 | 19 |
| 出版状态 | 已出版 - 1 10月 2002 |
| 已对外发布 | 是 |
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可持续发展目标 3 良好健康与福祉
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