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Human Tregs Made Antigen Specific by Gene Modification: The Power to Treat Autoimmunity and Antidrug Antibodies with Precision

机译:基因修饰使人类Treg成为抗原特异性:精确治疗自身免疫和抗药抗体的能力

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Human regulatory CD4~(+)T cells (Tregs) are potent immunosuppressive lymphocytes responsible for immune tolerance and homeostasis. Since the seminal reports identifying Tregs, vast research has been channeled into understanding their genesis, signature molecular markers, mechanisms of suppression, and role in disease. This research has opened the doors for Tregs as a potential therapeutic for diseases and disorders such as multiple sclerosis, type I diabetes, transplantation, and immune responses to protein therapeutics, like factor VIII. Seminal clinical trials have used polyclonal Tregs, but the frequency of antigen-specific Tregs among polyclonal populations is low, and polyclonal Tregs may risk non-specific immunosuppression. Antigen-specific Treg therapy, which uses genetically modified Tregs expressing receptors specific for target antigens, greatly mitigates this risk. Building on the principles of T-cell receptor cloning, chimeric antigen receptors (CARs), and a novel CAR derivative, called B-cell antibody receptors, our lab has developed different types of antigen-specific Tregs. This review discusses the current research and optimization of gene-modified antigen-specific human Tregs in our lab in several disease models. The preparations and considerations for clinical use of such Tregs also are discussed.
机译:人类调节性CD4〜(+)T细胞(Tregs)是有效的免疫抑制淋巴细胞,负责免疫耐受和体内稳态。自从鉴定Treg的开创性报告以来,已经进行了广泛的研究,以了解Treg的起源,标志性分子标记,抑制机制以及在疾病中的作用。这项研究为Tregs开启了大门,Tregs可以作为疾病和病症的潜在疗法,例如多发性硬化症,I型糖尿病,移植以及对蛋白质疗法(如VIII因子)的免疫应答。开创性的临床试验使用了多克隆Treg,但是多克隆人群中抗原特异性Treg的频率很低,多克隆Treg可能会带来非特异性免疫抑制的风险。抗原特异性Treg治疗使用表达目标抗原特异性受体的基因修饰的Treg,大大降低了这种风险。基于T细胞受体克隆,嵌合抗原受体(CARs)和称为B细胞抗体受体的新型CAR衍生物的原理,我们的实验室开发了不同类型的抗原特异性Treg。这篇综述讨论了我们在几种疾病模型中实验室中基因修饰的抗原特异性人Tregs的当前研究和优化。还讨论了此类Treg的制备方法和临床使用注意事项。

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