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RUNX3 在多种实体瘤的致癌作用中具有多功能性。

RUNX3 is multifunctional in carcinogenesis of multiple solid tumors.

机构信息

Cancer Biology Program, Cancer Science Institute of Singapore, National University of Singapore, Singapore.

出版信息

Oncogene. 2010 May 6;29(18):2605-15. doi: 10.1038/onc.2010.88. Epub 2010 Mar 29.

Abstract

The study of RUNX3 in tumor pathogenesis is a rapidly expanding area of cancer research. Functional inactivation of RUNX3-through mutation, epigenetic silencing, or cytoplasmic mislocalization-is frequently observed in solid tumors of diverse origins. This alone indicates that RUNX3 inactivation is a major risk factor in tumorigenesis and that it occurs early during progression to malignancy. Conversely, RUNX3 has also been described to have an oncogenic function in a subset of tumors. Although the mechanism of how RUNX3 switches from tumor suppressive to oncogenic activity is unclear, this is of clinical relevance with implications for cancer detection and prognosis. Recent developments have significantly contributed to our understanding of the pleiotropic tumor suppressive properties of RUNX3 that regulate major signaling pathways. This review summarizes the important findings that link RUNX3 to tumor suppression.

摘要

RUNX3 在肿瘤发病机制中的研究是癌症研究中一个迅速扩展的领域。在不同来源的实体肿瘤中,RUNX3 的功能失活(通过突变、表观遗传沉默或细胞质定位错误)经常被观察到。仅这一点就表明,RUNX3 失活是肿瘤发生的一个主要危险因素,而且它发生在向恶性进展的早期。相反,RUNX3 也被描述为在一部分肿瘤中具有致癌功能。尽管 RUNX3 如何从肿瘤抑制活性转变为致癌活性的机制尚不清楚,但这与癌症检测和预后具有临床相关性。最近的研究进展极大地促进了我们对 RUNX3 调节主要信号通路的多效性肿瘤抑制特性的理解。这篇综述总结了将 RUNX3 与肿瘤抑制联系起来的重要发现。

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