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首页> 外文期刊>Emerging Topics in Life Sciences >The future of immune checkpoint combinations with tumor-targeted small molecule drugs
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The future of immune checkpoint combinations with tumor-targeted small molecule drugs

机译:免疫检查点与肿瘤靶向小分子药物的未来

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Immune-checkpoint blockade (ICB) has transformed the landscape of cancer treatment. However, there is much to understand around refractory or acquired resistance in patients in order to utilize ICB therapy to its full potential. In this perspective article, we discuss the opportunities and challenges that are emerging as our understanding of immuno-oncology resistance matures. Firstly, there has been remarkable progress made to understand the exquisite overlap between oncogenic and immune signaling pathways. Several cancer-signaling pathways are constitutively active in oncogenic settings and also play physiological roles in immune cell function. A growing number of precision oncology tumor-targeted drugs show remarkable immunogenic properties that might be harnessed with rational combination strategies. Secondly, we now understand that the immune system confers a strong selective pressure on tumors. Whilst this pressure can lead to novel tumor evolution and immune escape, there is a growing recognition of tumor-intrinsic dependencies that arise in immune pressured environments. Such dependencies provide a roadmap for novel tumor-intrinsic drug targets to alleviate ICB resistance. We anticipate that rational combinations with existing oncology drugs and a next wave of tumor-intrinsic drugs that specifically target immunological resistance will represent the next frontier of therapeutic opportunity.
机译:免疫检查封锁(ICB)已改变了癌症治疗的景观。但是,在患者的难治性或获得的耐药性方面有很多了解,以便利用ICB治疗具有全部潜力。在这篇观点文章中,我们讨论了随着我们对免疫肿瘤抵抗的理解而出现的机遇和挑战。首先,已经取得了显着的进展,以了解致癌和免疫信号通路之间的精美重叠。几种癌症信号途径在致癌环境中具有组成性活性,并且在免疫细胞功能中起生理作用。越来越多的精度肿瘤靶向肿瘤的药物显示出显着的免疫原性特性,这些特性可能具有合理的组合策略。其次,我们现在了解到免疫系统对肿瘤赋予了强烈的选择压力。尽管这种压力可以导致新型的肿瘤进化和免疫逃逸,但在免疫压力环境中出现的肿瘤内部依赖性越来越认识。此类依赖性为新型肿瘤中性药物靶标提供了路线图,以减轻ICB耐药性。我们预计,与现有肿瘤药物的合理组合和专门针对免疫学耐药性的下一波肿瘤内部药物的合理组合将代表下一个治疗机会的领域。

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