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癌基因诱导的细胞衰老。

Oncogene-induced cellular senescence.

机构信息

Department of Pathology, VU University Medical Center Amsterdam, Netherlands.

出版信息

Adv Anat Pathol. 2010 Jan;17(1):42-8. doi: 10.1097/PAP.0b013e3181c66f4e.

Abstract

Oncogene-induced senescence (OIS) is a robust and sustained antiproliferative response brought about by oncogenic signaling resulting from an activating mutation of an oncogene, or the inactivation of a tumor-suppressor gene. The pathways mediating OIS are complex and incompletely elucidated but, the proliferative arrest involves activation of both the RB and p53 pathways. In addition, whereas there are indications that at least in some situations, negative feedback loops abolish the increased mitogenic signaling resulting from the oncogenic mutations, also an unexpected contribution of interleukin-mediated signaling has recently been found. OIS brings about cessation of growth of some benign tumors, including melanocytic nevi and several other lesions, including pituitary and thyroid adenomas. It protects against progression to cancer, and in this way complements oncogene-induced apoptosis. Perhaps, OIS has evolved as an alternative to apoptosis especially regarding long-lived cell types that are not replaceable in large numbers. Contrary to the earlier belief, OIS is not entirely irreversible, at least in some well documented in vitro systems. This means that its induction does not entirely eliminate the oncogenic threat resulting from the mutated cell. It also means that OIS, or related phenomena that may affect a proportion of the tumor cells of some cancers, may have an influence on responsiveness to cytotoxic cancer therapies, because OIS is associated with an antiapoptosis phenotype.

摘要

癌基因诱导的衰老(OIS)是一种强大而持久的抗增殖反应,由癌基因的激活突变或肿瘤抑制基因的失活引起的致癌信号导致。介导 OIS 的途径复杂且不完全阐明,但增殖抑制涉及 RB 和 p53 途径的激活。此外,尽管有迹象表明,至少在某些情况下,负反馈环消除了致癌突变导致的有丝分裂信号的增加,但最近也发现了白细胞介素介导的信号的意外贡献。OIS 导致一些良性肿瘤(包括黑色素痣和其他几种病变,包括垂体和甲状腺腺瘤)的生长停止。它可以防止癌症的进展,因此与癌基因诱导的细胞凋亡互补。也许,OIS 已经进化为一种替代细胞凋亡的方式,尤其是对于那些不能大量替换的长寿细胞类型。与早期的观点相反,OIS 至少在一些有充分文献记载的体外系统中并不是完全不可逆的。这意味着其诱导并不能完全消除突变细胞引起的致癌威胁。这也意味着 OIS 或可能影响某些癌症的一部分肿瘤细胞的相关现象,可能会对细胞毒性癌症治疗的反应性产生影响,因为 OIS 与抗细胞凋亡表型相关。

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