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Development of Noxa-like BH3 mimetics for apoptosis-based therapeutic strategy in chronic lymphocytic leukemia

机译:基于Noxa的BH3模拟物的开发,用于基于细胞凋亡的慢性淋巴细胞白血病治疗策略

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Despite real advances made in chemoimmunotherapy, chronic lymphocytic leukemia (CLL) is still an incurable disease. New therapeutic strategies based on the restoration of the cell death program seemed relevant. Some members of the Bcl-2 family are critical players in the defective apoptotic program in CLL cells and/or targets of apoptosis inducers in vitro. The concept of BH3 mimetics has led to the characterization of small molecules mimicking proapoptotic BH3-only members of the Bcl-2 family by their ability to bind and antagonize the prosurvival members. Some putative or actual BH3 mimetics are already being tested in clinical trials with somewhat promising results. However, none of them has a high enough interaction affinity with Mcl-1, a crucial antiapoptotic factor in CLL. It has been suggested that resistance to BH3 mimetics can be overcome by using inhibitors of Mcl-1 expression. An alternative and more direct strategy is to design mimetics of the Noxa BH3 domain, which is a specific antagonistic Mcl-1 ligand. The development of such Noxa-like BH3 mimetics, capable of directly interacting with Mcl-1 and efficiently neutralizing its antiapoptotic activity, is extremely important to evaluate their impact on the clinical outcome of patients with CLL.
机译:尽管化学免疫疗法取得了真正的进步,但慢性淋巴细胞性白血病(CLL)仍然是无法治愈的疾病。基于细胞死亡程序恢复的新治疗策略似乎很重要。 Bcl-2家族的某些成员是CLL细胞和/或体外凋亡诱导剂靶标中凋亡程序缺陷的关键参与者。 BH3模拟物的概念已通过模仿Bcl-2家族的促凋亡BH3仅成员来结合和拮抗存活成员的能力来表征小分子。一些推定或实际的BH3模拟物已经在临床试验中进行了测试,结果有些许希望。然而,它们都没有与CCL中至关重要的抗凋亡因子Mcl-1具有足够高的相互作用亲和力。已经提出,通过使用Mcl-1表达的抑制剂可以克服对BH3模拟物的抗性。另一种更直接的策略是设计Noxa BH3域的模拟物,该模拟物是一种特异性的拮抗性Mcl-1配体。能够直接与Mcl-1相互作用并有效中和其抗凋亡活性的此类Noxa样BH3模拟物的开发对于评估其对CLL患者临床结果的影响极为重要。

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