【mTOR过度活跃和RICTOR扩增的重要性,以及恶性肿瘤中相关的靶向治疗可能性】。

Magyar onkologia Pub Date : 2023-09-28 Epub Date: 2023-09-13
Fatime Szalai, Ildikó Krencz, Dorottya Moldvai, Gábor Petővári, Titanilla Dankó, Noémi Nagy, Gergő Papp, Judit Pápay, Anna Sebestyén, Dániel Sztankovics
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引用次数: 0

摘要

抗肿瘤治疗的失败和耐药性引发了癌症治疗的困难,通常是由信号网络活性的改变引起的,包括致癌突变引起的PI3K/Akt/mTOR过度活跃。在这篇综述中,我们总结了几十年前发现的mTOR(雷帕霉素的机制靶点)失调的相关性,现在已知这是许多肿瘤的特征。在此背景下,我们提出了mTOR激酶复合物(mTORC1和mTORC2)在结构、调节机制和抑制剂敏感性方面的活性、功能和可测试性的差异。我们强调,基因改变,包括RICTOR扩增和相关的mTOR过动,与靶向治疗的发展有关。建议研究mTOR抑制剂治疗的患者的mTOR谱活性,因为目前的第一代mTOR抑制剂(雷帕霉素和类似物)在mTORC2过度活跃的情况下可能无效。正在进行的新抑制剂和联合疗法的阶段试验在分子标记物选择的晚期患者中很有希望。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
[he importance of mTOR hyperactivity and RICTOR amplification, and the associated targeted therapy possibilities in malignant tumours].

Failures of anti-tumour therapies and drug resistance initiate difficulties in cancer treatments often caused by alterations in signalling network activity, including PI3K/Akt/mTOR hyperactivity due to oncogenic mutations. In this review, we summarise the relevance of mTOR (mechanistic target of rapamycin) dysregulation identified decades ago, which is now known to be characteristic of many tumours. In this context, we present differences in activity, function and testability of mTOR kinase complexes (mTORC1 and mTORC2) differing in structure, regulatory mechanisms and inhibitor sensitivity. We highlight that genetic alterations, including RICTOR amplification and associated mTOR hyperactivity, are relevant in targeted therapy development. It is recommended to investigate mTOR profile activity in patients for whom mTOR inhibitor therapies are considered since the current first-generation mTOR inhibitors (rapamycin and analogues) may be ineffective in case of mTORC2 hyperactivity. Ongoing phase trials of new inhibitors and combination therapies are promising in advanced stage patients selected by molecular markers.

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