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Combining Immune Checkpoint Inhibitors and Kinase-Inhibiting Supramolecular Therapeutics for Enhanced Anticancer Efficacy

机译:结合免疫检查点抑制剂和抑制激酶的超分子疗法来增强抗癌功​​效

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摘要

A major limitation of immune checkpoint inhibitors is that only a small subset of patients achieve durable clinical responses. This necessitates the development of combinatorial regimens with immunotherapy. However, some combinations, such as MEK- or PI3K-inhibitors with a PD1-PDL1 checkpoint inhibitor, are pharmacologically challenging to implement. We rationalized that such combinations can be enabled using nanoscale supramolecular targeted therapeutics, which spatially home into tumors and exert temporally sustained inhibition of the target. Here we describe two case studies where nanoscale MEK- and PI3K-targeting supramolecular therapeutics were engineered using a quantum mechanical all-atomistic simulation-based approach. The combinations of nanoscale MEK- and PI3K-targeting supramolecular therapeutics with checkpoint PDL1 and PD1 inhibitors exert enhanced antitumor outcome in melanoma and breast cancers in vivo, respectively. Additionally, the temporal sequence of administration impacts the outcome. The combination of supramolecular therapeutics and immunotherapy could emerge as a paradigm shift in the treatment of cancer.
机译:免疫检查点抑制剂的主要局限性在于,只有一小部分患者获得了持久的临床反应。这就需要开发免疫疗法的组合方案。但是,某些组合(例如MEK或PI3K抑制剂与PD1-PDL1检查点抑制剂)在药理上难以实施。我们合理地认为,可以使用纳米级超分子靶向治疗剂实现这种组合,该治疗剂在空间上归巢于肿瘤并在时间上持续抑制目标。在这里,我们描述了两个案例研究,其中使用基于量子力学全原子模拟的方法设计了靶向纳米MEK和PI3K的超分子疗法。纳米级靶向MEK和PI3K的超分子疗法与检查点PDL1和PD1抑制剂的组合分别在体内的黑色素瘤和乳腺癌中发挥增强的抗肿瘤作用。另外,给药的时间顺序会影响结果。超分子疗法和免疫疗法的结合可能会以癌症治疗的范式转变出现。

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