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Spotlight on Tocilizumab in the Treatment of CAR-T-Cell-Induced Cytokine Release Syndrome: Clinical Evidence to Date

机译:在CoIledumab上的聚光灯在治疗Car-T细胞诱导的细胞因子释放综合征:迄今为止的临床证据

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摘要

Immune-based therapies such as chimeric antigen receptor (CAR)-T-cell therapy have revolutionized the landscape of cancer treatment in recent years. Although this class of therapy has demonstrated impressive clinical efficacy against cancers that were once thought to be incurable, its success is in part limited by unique toxicities which can be severe or even fatal. Cytokine release syndrome (CRS) is the most commonly observed toxicity and occurs as a result of non-antigen specific immune activation. Similar to macrophage activation syndrome (MAS)/hemophagocytic lymphohistiocytosis (HLH), CRS is associated with elevated levels of several cytokines including interleukin-6 (IL-6) that serve as a driver for host immune dysregulation. As a direct anti-cytokine drug, tocilizumab has been a cornerstone in the treatment of CAR-T-associated CRS through its ability to dampen CRS without compromising CAR-T-cell function. However, optimal timing of administration is yet unknown. Here, we review the use of tocilizumab in the management of CAR-T-associated CRS, emphasizing on the clinical efficacy across various CAR constructs and its role in current CRS management algorithms. We also discuss alternative therapies that may be considered for refractory CRS therapy and the use of tocilizumab in the current COVID-19 global pandemic.
机译:嵌合抗原受体(汽车)-T-细胞治疗等免疫基疗法彻底改变了近年来癌症治疗的景观。虽然这类治疗已经表现出令人印象深刻的临床疗效,但曾经认为是可行的癌症,但其成功部分是有限的,这些毒性有限,可能是严重甚至致命的。细胞因子释放综合征(CRS)是最常见的毒性,并且由于非抗原特异性免疫活化而发生。类似于巨噬细胞激活综合征(MAS)/血糖淋巴管激尿剂(HLH),CRS与包括白细胞介素-6(IL-6)的升高水平,其用作宿主免疫失调的驾驶员。作为一种直接的抗细胞因子药物,Tocilizumab通过其在不损害CAR-T细胞功能的情况下通过其抑制CRS的能力来治疗CAR-T相关CRS的基石。但是,给药的最佳时间尚未赘述。在这里,我们审查在CAR-T相关CRS管理中使用托尔密子,强调各种汽车结构的临床疗效及其在当前CRS管理算法中的作用。我们还讨论了可能考虑用于难治性CRS治疗和在目前Covid-19全球大流行病中使用幼稚的替代疗法。

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