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Mirage or long-awaited oasis: reinvigorating T-cell responses in pancreatic cancer

机译:MiRAGE或已长期待的OASIS:在胰腺癌中重新发明T细胞应答

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摘要

Pancreatic ductal adenocarcinoma (PDAC) is plagued by a dismal 5-year survival rate, early onset of metastasis and limited efficacy of systemic therapies. This scenario highlights the need to fervently pursue novel therapeutic strategies to treat this disease. Recent research has uncovered complicated dynamics within the tumor microenvironment (TME) of PDAC. An abundant stroma provides a framework for interactions between cancer-associated fibroblasts, suppressive myeloid cells and regulatory lymphocytes, which together create an inhospitable environment for adaptive immune responses. This accounts for the poor infiltration and exhausted phenotypes of effector T cells within pancreatic tumors. Innovative studies in genetically engineered mouse models have established that with appropriate pharmacological modulation of suppressive elements in the TME, T cells can be prompted to regress pancreatic tumors. In light of this knowledge, innovative combinatorial strategies involving immunotherapy and targeted therapies working in concert are rapidly emerging. This review will highlight recent advances in the field related to immune suppression in PDAC, emerging preclinical data and rationale for ongoing immunotherapy clinical trials. In particular, we draw attention to foundational findings involving T-cell activity in PDAC and encourage development of novel therapeutics to improve T-cell responses in this challenging disease.
机译:胰腺导管腺癌(PDAC)被令人沮丧的5年生存率,转移早期发作和系统疗法有限的疗效。这种情况强调了对治疗这种疾病的热切性追求新的治疗策略的必要性。最近的研究在PDAC的肿瘤微环境(TME)内发现了复杂的动态。一种丰富的基质提供了癌症相关成纤维细胞,抑制骨髓细胞和调节淋巴细胞之间相互作用的框架,其共同为适应性免疫反应产生了一种惰性环境。这考虑了胰腺肿瘤内效应T细胞的渗透性和耗尽表型。基因工程鼠标模型的创新研究已经确定,在TME中具有适当的药理调节,可以提示T细胞来衰退胰腺肿瘤。鉴于这一知识,涉及免疫疗法和主办音乐会的有针对性疗法的创新组合策略正在迅速涌现。本综述将突出与PDAC免疫抑制有关的近期进展,新兴的临床前数据和用于持续的免疫疗法临床试验。特别是,我们注意涉及PDAC中T细胞活性的基础发现,并鼓励新的治疗剂的发展,以改善这种挑战性疾病中的T细胞反应。

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