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Immune biomarkers for predicting response to adoptive cell transfer as cancer treatment

机译:免疫生物标记物用于预测对过继细胞转移作为癌症治疗的反应

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摘要

Adoptive cell transfer (ACT) is a form of personalised immunotherapy which has shown promising results in metastasised cancer. For this treatment, autologous T lymphocytes are selected and stimulated in vitro before re-administration in large numbers. However, only a fraction of patients benefit from ACT, and it is not yet known what biomarkers can predict treatment outcome. In this review, we describe what tumour characteristics are associated with response to ACT. Based on the current knowledge, the best candidate biomarker for a good anti-tumour response seems to be a large number of neoantigens with a homogeneous distribution across the tumour in combination with sufficient MHC-I expression level. Additionally, it is necessary to be able to isolate a diverse population of T cells reactive to these neoantigens from tumour tissue or peripheral blood. Additional promising candidate biomarkers shared with other cancer immunotherapies are a large number of tumour-infiltrating cytotoxic and memory T cells, normal levels of glycolysis, and a pro-inflammatory cytokine profile within the tumour. Intense research in this field will hopefully result in identification of more biomarkers for cancers with low mutational load.
机译:过继细胞转移(ACT)是一种个性化免疫疗法,已在转移癌中显示出令人鼓舞的结果。对于这种治疗,在大量重新施用之前,选择并刺激体外自体T淋巴细胞。但是,只有一小部分患者会从ACT中受益,而且尚不清楚哪种生物标记物可以预测治疗结果。在这篇综述中,我们描述了哪些肿瘤特征与对ACT的反应有关。基于目前的知识,对于良好的抗肿瘤应答而言,最佳候选生物标记似乎是大量新抗原,在肿瘤中分布均匀,并具有足够的MHC-1表达水平。另外,有必要能够从肿瘤组织或外周血中分离出对这些新抗原具有反应性的多种T细胞。与其他癌症免疫疗法共有的其他有希望的候选生物标志物是大量浸润肿瘤的细胞毒性和记忆T细胞,正常水平的糖酵解以及肿瘤内的促炎性细胞因子谱。该领域的深入研究有望导致鉴定更多具有低突变负荷的癌症的生物标志物。

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