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Mechanisms of resistance to immune checkpoint inhibitors

机译:抵抗免疫检查点抑制剂的机制

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Immune checkpoint inhibitors (ICI) targeting CTLA-4 and the PD-1/PD-L1 axis have shown unprecedented clinical activity in several types of cancer and are rapidly transforming the practice of medical oncology. Whereas cytotoxic chemotherapy and small molecule inhibitors (‘targeted therapies’) largely act on cancer cells directly, immune checkpoint inhibitors reinvigorate anti-tumour immune responses by disrupting co-inhibitory T-cell signalling. While resistance routinely develops in patients treated with conventional cancer therapies and targeted therapies, durable responses suggestive of long-lasting immunologic memory are commonly seen in large subsets of patients treated with ICI. However, initial response appears to be a binary event, with most non-responders to single-agent ICI therapy progressing at a rate consistent with the natural history of disease. In addition, late relapses are now emerging with longer follow-up of clinical trial populations, suggesting the emergence of acquired resistance. As robust biomarkers to predict clinical response and/or resistance remain elusive, the mechanisms underlying innate (primary) and acquired (secondary) resistance are largely inferred from pre-clinical studies and correlative clinical data. Improved understanding of molecular and immunologic mechanisms of ICI response (and resistance) may not only identify novel predictive and/or prognostic biomarkers, but also ultimately guide optimal combination/sequencing of ICI therapy in the clinic. Here we review the emerging clinical and pre-clinical data identifying novel mechanisms of innate and acquired resistance to immune checkpoint inhibition.
机译:针对CTLA-4和PD-1 / PD-L1轴的免疫检查点抑制剂(ICI)在几种类型的癌症中均表现出前所未有的临床活性,并正在迅速改变医学肿瘤学的实践。细胞毒性化学疗法和小分子抑制剂(“靶向疗法”)在很大程度上直接作用于癌细胞,而免疫检查点抑制剂可通过破坏共同抑制性T细胞信号传导来增强抗肿瘤免疫反应。虽然在接受常规癌症治疗和靶向治疗的患者中通常会产生耐药性,但在接受ICI治疗的大部分患者中通常会看到表明免疫记忆力持久的持久反应。然而,最初的反应似乎是一个二元事件,大多数对单药ICI疗法无反应的患者进展的速度与疾病的自然病程一致。另外,随着临床试验人群的随访时间延长,现在出现了晚期复发,提示出现了获得性耐药。由于预测临床反应和/或耐药的可靠生物标志物仍然难以捉摸,因此先天性(原发性)和后天性(继发性)抗性的潜在机制很大程度上可从临床前研究和相关的临床数据中得出。对ICI应答(和耐药)的分子和免疫机制的进一步了解不仅可以识别新颖的预测和/或预后生物标志物,而且最终可以指导临床中ICI治疗的最佳组合/排序。在这里,我们回顾了新兴的临床和临床前数据,这些数据确定了先天和后天抵抗免疫检查点抑制的新机制。

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