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Results and challenges of immune checkpoint inhibitors in colorectal cancer

机译:显着癌症免疫检查点抑制剂的结果与挑战

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Introduction: Colorectal cancer (CRC) is the third most commonly diagnosed cancer worldwide and clinical outcome has improved substantially during the last two decades with targeted therapies. The immune system has a major role in cancers, especially the CD8 + T cells specific to tumor antigens. However, tumors can escape immune response by different mechanisms including upregulation of inhibitory immune checkpoint receptors, such as well-known Programmed cell Death protein-1 (PD-1)/Programmed cell Death Ligand 1 (PD-L1) interaction, leading CD8 + T cells to a state of anergy. Immunotherapy, with the so-called immune checkpoint inhibitors (CPIs), has recently been approved in treatment of multiple cancers due to its prolonged disease control and acceptable toxicities. The recent groundbreaking success involving anti-PD-1 CPIs in metastatic CRC with deficient mismatch repair system (dMMR) is promising, with several trials ongoing. Major challenges are ahead in order to determine how, when and for which patients we should use these CPIs in CRC. Areas covered: This review highlights some promises and challenges concerning personalized immunotherapy in CRC. First results and ongoing breakthrough trials are presented. The crucial role of biomarkers in selecting patient is also discussed. Expert opinion: As of now, dMMR and POLE mutations (DNA polymerase ? with ultramutator phenotype are the most powerful predictive biomarkers of CPI efficacy. The most challenging issue is pMMR mCRC and determination of how to convert a nonimmunogenic neoplasm into an immunogenic neoplasm, a combination of CPIs with radiation or MEK inhibitor probably being the most relevant strategy. Next-generation sequencing (NGS) assays to quantify mutational load could be more reliable predictive biomarkers of CPIs efficacy than PD-L1 expression or immune scores.
机译:介绍:结肠直肠癌(CRC)是全球第三次常见诊断的癌症,在过去二十年中,临床结果在有针对性疗法的最后二十年中得到了改善。免疫系统在癌症中具有重要作用,特别是特异于肿瘤抗原的CD8 + T细胞。然而,肿瘤可以通过不同机制逃避免疫应答,包括抑制性免疫检查点受体的上调,例如众所周知的编程细胞死亡蛋白-1(PD-1)/编程的细胞死亡配体1(PD-L1)相互作用,领先CD8 + T细胞到一个声音状态。免疫疗法,随着所谓的免疫检查点抑制剂(CPI),最近被批准用于治疗多种癌症,由于其延长的疾病控制和可接受的毒性。最近涉及缺陷CRC中的抗PD-1 CPI的突破性成功具有不匹配的修复系统(DMMR)的转移CRC是有前途的,有几项试验正在进行中。为了确定我们应该在CRC中使用这些CPI的患者,何时和何时,何时和何时,何时何地提前前进。涵盖了地区:本综述介绍了关于CRC个性化免疫疗法的一些承诺和挑战。介绍了第一次结果和正在进行的突破性试验。还讨论了生物标志物在选择患者方面的关键作用。专家意见:截至目前,DMMR和杆突变(DNA聚合酶?具有Ultramutator表型是CPI疗效最强大的预测生物标志物。最具挑战性的问题是PMMR MCRC,以及如何将非深化肿瘤转化为免疫原性肿瘤的测定方法。a CPI与辐射或MEK抑制剂的组合可能是最相关的策略。用于量化突变载荷的下一代测序(NGS)测定可能比PD-L1表达或免疫分数更可靠的预测生物标志物。

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