Understanding sensitivity to BH3 mimetics: ABT-737 as a case study to foresee the complexities of personalized medicine.

Q2 Biochemistry, Genetics and Molecular Biology Journal of Molecular Signaling Pub Date : 2012-08-16 DOI:10.1186/1750-2187-7-12
Vasileios A Stamelos, Charles W Redman, Alan Richardson
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引用次数: 21

Abstract

BH3 mimetics such as ABT-737 and navitoclax bind to the BCL-2 family of proteins and induce apoptosis through the intrinsic apoptosis pathway. There is considerable variability in the sensitivity of different cells to these drugs. Understanding the molecular basis of this variability will help to determine which patients will benefit from these drugs. Furthermore, this understanding aids in the design of rational strategies to increase the sensitivity of cells which are otherwise resistant to BH3 mimetics. We discuss how the expression of BCL-2 family proteins regulates the sensitivity to ABT-737. One of these, MCL-1, has been widely described as contributing to resistance to ABT-737 which might suggest a poor response in patients with cancers that express levels of MCL-1. In some cases, resistance to ABT-737 conferred by MCL-1 is overcome by the expression of pro-apoptotic proteins that bind to apoptosis inhibitors such as MCL-1. However, the distribution of the pro-apoptotic proteins amongst the various apoptosis inhibitors also influences sensitivity to ABT-737. Furthermore, the expression of both pro- and anti-apoptotic proteins can change dynamically in response to exposure to ABT-737. Thus, there is significant complexity associated with predicting response to ABT-737. This provides a paradigm for the multiplicity of intricate factors that determine drug sensitivity which must be considered for the full implementation of personalized medicine.

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了解BH3模拟物的敏感性:以ABT-737为例研究,以预见个性化医疗的复杂性。
BH3模拟物如ABT-737和navitoclax结合BCL-2蛋白家族并通过内在凋亡途径诱导细胞凋亡。不同细胞对这些药物的敏感性有相当大的差异。了解这种变异的分子基础将有助于确定哪些患者将受益于这些药物。此外,这种理解有助于设计合理的策略,以增加对BH3模拟物具有抗性的细胞的敏感性。我们讨论了BCL-2家族蛋白的表达如何调节ABT-737的敏感性。其中一种MCL-1已被广泛描述为有助于对ABT-737产生耐药性,这可能表明MCL-1表达水平的癌症患者的反应较差。在某些情况下,MCL-1赋予ABT-737的耐药性被与凋亡抑制剂如MCL-1结合的促凋亡蛋白的表达所克服。然而,促凋亡蛋白在各种细胞凋亡抑制剂中的分布也影响对ABT-737的敏感性。此外,ABT-737暴露后,促凋亡蛋白和抗凋亡蛋白的表达都会发生动态变化。因此,预测对ABT-737的响应具有显著的复杂性。这为决定药物敏感性的复杂因素的多样性提供了一个范例,这些因素必须考虑到个体化医疗的全面实施。
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Journal of Molecular Signaling
Journal of Molecular Signaling Biochemistry, Genetics and Molecular Biology-Biochemistry
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期刊介绍: Journal of Molecular Signaling is an open access, peer-reviewed online journal that encompasses all aspects of molecular signaling. Molecular signaling is an exponentially growing field that encompasses different molecular aspects of cell signaling underlying normal and pathological conditions. Specifically, the research area of the journal is on the normal or aberrant molecular mechanisms involving receptors, G-proteins, kinases, phosphatases, and transcription factors in regulating cell proliferation, differentiation, apoptosis, and oncogenesis in mammalian cells. This area also covers the genetic and epigenetic changes that modulate the signaling properties of cells and the resultant physiological conditions.
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