摘要
Membranous Met 因为其在癌症转移中的作用被典型的识别,而核会见与更具侵入性的,积极的和增殖的癌症相关。全长Met或N-末端跨膜结构的裂解Met可以以细胞生长和pH依赖性的方式进入细胞核,同时也以两配体依赖性(全长Met)和独立的方式(切割Met)进入。nMET可能在肿瘤复发中发挥了更大的作用相比它的膜而言。例如,在前列腺癌中已经发现,雄激素受体(AR)可抑制膜表达Met,基于前列腺癌治疗的抗雄激素促进了核表达(nMET),我们最近在前列腺癌复发中发现了一种新的nMET/SOX9/ β-Catenin/AR 通路,这可能有助于MET/nMET的AR激活反馈回路的形成。新的证据表明,nMET的可能性是复发癌的预后指标。本文综述了关于nMET和复发癌独特作用最新的研究结果。
关键词: Met;核易位;癌基因;复发。
Current Cancer Drug Targets
Title:nMET, A New Target in Recurrent Cancer
Volume: 16 Issue: 7
Author(s): Yingqiu Xie, Sholpan Istayeva, Zhanlin Chen, Tursonjan Tokay, Zhaxybay Zhumadilov, Denglong Wu, Gonzalo Hortelano, Jinfu Zhang
Affiliation:
关键词: Met;核易位;癌基因;复发。
摘要: Membranous Met is classically identified with its role in cancer metastases, while nuclear Met is associated with a more invasive, aggressive and proliferative form of cancer. Full-length Met or N-terminal transmembrane domain cleaved Met can translocate into nucleus in a cell growth and pH dependent but both ligand-dependent (full length Met) and -independent (cleaved Met) manner. nMET may play greater essential roles in cancer recurrence than membranous Met. For example, in prostate cancer, it has been found that androgen receptor (AR) may inhibit the expression of membranous Met so anti-androgen based prostate cancer therapy may promote the expression of nuclear Met (nMET). We recently found a novel nMET/SOX9/ β-Catenin/AR pathway in relapsed prostate cancer which may contribute to the formation of the feedback loop of AR reactivation via MET/nMET. Emerging evidence suggests the possibility of nMET as a prognostic marker in relapsed cancer. This review summarizes recent findings about nMET and its unique role in recurrent cancer.
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Yingqiu Xie, Sholpan Istayeva, Zhanlin Chen, Tursonjan Tokay, Zhaxybay Zhumadilov, Denglong Wu, Gonzalo Hortelano, Jinfu Zhang , nMET, A New Target in Recurrent Cancer, Current Cancer Drug Targets 2016; 16 (7) . https://dx.doi.org/10.2174/1568009616666160105105250
DOI https://dx.doi.org/10.2174/1568009616666160105105250 |
Print ISSN 1568-0096 |
Publisher Name Bentham Science Publisher |
Online ISSN 1873-5576 |
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