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CAR-T with License to Kill Solid Tumors in Search of a Winning Strategy

机译:CAR-T拥有杀灭实体肿瘤以寻求制胜策略的许可证

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摘要

Artificial receptors designed for adoptive immune therapies need to absolve dual functions: antigen recognition and abilities to trigger the lytic machinery of reprogrammed effector T lymphocytes. In this way, CAR-T cells deliver their cytotoxic hit to cancer cells expressing targeted tumor antigens, bypassing the limitation of HLA-restricted antigen recognition. Expanding technologies have proposed a wide repertoire of soluble and cellular “immunological weapons” to kill tumor cells; they include monoclonal antibodies recognizing tumor associated antigens on tumor cells and immune cell checkpoint inhibition receptors expressed on tumor specific T cells. Moreover, a wide range of formidable chimeric antigen receptors diversely conceived to sustain quality, strength and duration of signals delivered by engineered T cells have been designed to specifically target tumor cells while minimize off-target toxicities. The latter immunological weapons have shown distinct efficacy and outstanding palmarès in curing leukemia, but limited and durable effects for solid tumors. General experience with checkpoint inhibitors and CAR-T cell immunotherapy has identified a series of variables, weaknesses and strengths, influencing the clinical outcome of the oncologic illness. These aspects will be shortly outlined with the intent of identifying the still “missing strategy” to combat epithelial cancers.
机译:设计用于过继免疫疗法的人工受体需要消除双重功能:抗原识别和触发重新编程的效应T淋巴细胞裂解机制的能力。通过这种方式,CAR-T细胞将其细胞毒性命中传递给表达靶向肿瘤抗原的癌细胞,从而绕开了HLA限制性抗原识别的局限。不断发展的技术提出了广泛的可溶性和细胞“免疫武器”,以杀死肿瘤细胞。它们包括在肿瘤细胞上识别肿瘤相关抗原的单克隆抗体和在肿瘤特异性T细胞上表达的免疫细胞检查点抑制受体。而且,已经广泛设计了各种各样的强大的嵌合抗原受体,以维持由工程化的T细胞传递的信号的质量,强度和持续时间,以特异性地靶向肿瘤细胞,同时使脱靶毒性最小化。后者的免疫武器在治疗白血病方面显示出独特的功效和出色的手掌,但对实体瘤的作用有限且持久。检查点抑制剂和CAR-T细胞免疫疗法的一般经验已经确定了一系列变量,弱点和优点,这些变量会影响肿瘤疾病的临床结果。这些方面将在短期内概述,以期确定仍是对抗上皮癌的“缺失策略”。

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