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A Balancing Act: p53 Activity from Tumor Suppression to Pathology and Therapeutic Implications
Annual Review of Pathology: Mechanisms of Disease ( IF 36.2 ) Pub Date : 2022-01-24 , DOI: 10.1146/annurev-pathol-042320-025840
Mengxiong Wang 1 , Laura D Attardi 1, 2
Affiliation  

TP53, encoding the p53 transcription factor, is the most frequently mutated tumor suppressor gene across all human cancer types. While p53 has long been appreciated to induce antiproliferative cell cycle arrest, apoptosis, and senescence programs in response to diverse stress signals, various studies in recent years have revealed additional important functions for p53 that likely also contribute to tumor suppression, including roles in regulating tumor metabolism, ferroptosis, signaling in the tumor microenvironment, and stem cell self-renewal/differentiation. Not only does p53 loss or mutation cause cancer, but hyperactive p53 also drives various pathologies, including developmental phenotypes, premature aging, neurodegeneration, and side effects of cancer therapies. These findings underscore the importance of balanced p53 activity and influence our thinking of how to best develop cancer therapies based on modulating the p53 pathway.

中文翻译:


平衡法:从肿瘤抑制到病理学和治疗意义的 p53 活性

TP53编码 p53 转录因子,是所有人类癌症类型中最常发生突变的肿瘤抑制基因。虽然 p53 长期以来一直被认为可诱导抗增殖细胞周期停滞、细胞凋亡和衰老程序以响应不同的应激信号,但近年来的各种研究揭示了 p53 的其他重要功能,这些功能可能也有助于肿瘤抑制,包括在调节肿瘤中的作用代谢、铁死亡、肿瘤微环境中的信号传导和干细胞自我更新/分化。不仅p53缺失或突变会导致癌症,但过度活跃的 p53 也会导致各种病理变化,包括发育表型、过早衰老、神经退行性变和癌症治疗的副作用。这些发现强调了平衡 p53 活性的重要性,并影响了我们对如何最好地开发基于调节 p53 途径的癌症疗法的思考。

更新日期:2022-01-25
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