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Exploiting the pro-apoptotic function of NOXA as a therapeutic modality in cancer

机译:利用NOXA作为癌症治疗方式的亲凋亡函数

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Introduction: Direct targeting of Bcl-2 members for therapeutic purposes in cancer has become a clinical reality with the FDA approval of ABT-199/Venetoclax. Other highly specific BH3-mimetics are in pre-clinical development. Understanding the functional interactions among the Bcl-2 family is of prime importance to fully exploit their potential. NOXA is considered a rather weak BH3-only member but it has unexplored potential in various settings, which are of relevance in cancer. NOXA is best known as a selective inhibitor of MCL1, itself overexpressed in many cancers, and this protein pair forms an important rheostat in many forms of cell stress.
机译:介绍:直接靶向BCL-2成员在癌症中的治疗目的已成为ABT-199 / VENETOCLAX的FDA批准的临床现实。 其他高度特异性的BH3模仿在临床前发展。 了解BCL-2家族之间的功能互动是完全剥削其潜力的主要重要性。 Noxa被认为是一个相当弱的BH3的成员,但它在各种环境中具有未探明的潜力,这在癌症中具有相关性。 Noxa是最符合MCL1的选择性抑制剂,本身在许多癌症中过表达,并且该蛋白质对以多种形式的细胞应激形成重要的变阻性。

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