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临床靶点混杂性:来自Ras分子试验的经验教训。

Clinical target promiscuity: lessons from ras molecular trials.

作者信息

Rengan Ramesh, Cengel Keith A, Hahn Stephen M

机构信息

Department of Radiation Oncology, University of Pennsylvania, 2-Donner, HUP, 3400 Spruce Street, Philadelphia, PA 19104, USA.

出版信息

Cancer Metastasis Rev. 2008 Sep;27(3):403-14. doi: 10.1007/s10555-008-9133-z.

Abstract

Mutated ras has been identified in approximately 30% of human tumors, and dysregulation of ras function and signal transduction pathways is a critical step in tumorigenesis. Herein, we review the early data that supports the concept that the intrinsic radiosensitivity of tumor cells can be altered by oncogenic ras expression and that this impacts the PI3K-dependent signaling cascade. This ras-induced radioresistance can be reversed using prenyl transferase inhibitors (PTIs.). We discuss the effects of PTIs as a radiosensitizer in both in vivo and in vitro studies and show that PTIs can lead to increased radiosensitization in vivo through a variety of potential mechanisms that enhance radiation-induced cell kill. We critically evaluate the use of ras biomarkers in predicting the clinical response to PTIs that may explain the mixed results seen thus far in clinical trials using PTIs as a clinical radiosensitizer. We conclude that Ras-mediated radioresistance is the result of multiple intercommunicating pathways functioning against a complex genetic background and a solitary biomarker may not be adequate to predict for PTI-mediated radiosensitization. Nonetheless, our knowledge of the ras-signaling pathway has led to development and testing of specific therapies directed against PI3K-AKT signaling pathways as a future approach towards clinical radiosensitization.

摘要

在大约30%的人类肿瘤中已发现ras基因发生突变,ras功能和信号转导通路的失调是肿瘤发生的关键步骤。在此,我们回顾早期数据,这些数据支持以下观点:致癌性ras表达可改变肿瘤细胞的内在放射敏感性,且这会影响PI3K依赖的信号级联反应。使用异戊二烯转移酶抑制剂(PTIs)可逆转这种由ras诱导的放射抗性。我们讨论了PTIs作为放射增敏剂在体内和体外研究中的作用,并表明PTIs可通过多种潜在机制在体内导致放射增敏作用增强,这些机制可增强辐射诱导的细胞杀伤。我们严格评估了ras生物标志物在预测对PTIs临床反应中的应用,这可能解释了迄今为止在将PTIs用作临床放射增敏剂的临床试验中所见到的混合结果。我们得出结论,Ras介导的放射抗性是在复杂遗传背景下起作用的多个相互连通的通路的结果,单一生物标志物可能不足以预测PTI介导的放射增敏作用。尽管如此,我们对ras信号通路的了解已促使针对PI3K - AKT信号通路开发和测试特定疗法,作为未来临床放射增敏的一种方法。

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