CD137mAb对T细胞的共刺激能力取决于复杂的CRD结构,而不取决于阻断配体-受体结合。

IF 4.5 3区 医学 Q2 IMMUNOLOGY
Xin Jin, Ling Yi, Xiaojue Wang, Zhuohong Yan, Panjian Wei, Bin Yang, Hongtao Zhang
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引用次数: 0

摘要

CD137主要是CD8+T细胞的共刺激受体。两种具有代表性的CD137抗体,utomilumab和urelumab,在临床试验中显示出不同的共刺激能力。平衡CD137信号激活的T细胞的抗肿瘤作用和全身毒性是一个需要临床考虑的挑战。在本研究中,制备了一组特异性抗人CD137单克隆抗体(mAb),并分析了它们的亲和力、同种型、CD137-CRD(富含半胱氨酸的结构域)结合区、对小鼠和恒河猴CD137的交叉反应性、对配体-受体结合的抑制和共刺激活性。结果表明,抗人CD137mAb与恒河猴CD137具有较高的交叉反应性。单克隆抗体根据其CD137细胞外结构域的不同结合区分为三个簇。它们绑定到CRDI+CRDII、CRDIII或CRDIV+STP。CRDIII结合mAb具有最强的阻断活性。高共刺激性CD137mAb显示出更强的促进CD8+T细胞增殖的能力。然而,单克隆抗体对T细胞的共刺激能力与其阻断CD137L-CD137结合的能力并不密切相关,并且可能受到更精细的CRD构象结构的控制。这项研究为开发下一代CD137mAb以满足临床需求提供了额外的信息。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Costimulatory capacity of CD137 mAbs on T cells depends on elaborate CRD structures but not on blocking ligand‒receptor binding

Costimulatory capacity of CD137 mAbs on T cells depends on elaborate CRD structures but not on blocking ligand‒receptor binding

CD137 is mainly a costimulatory receptor of CD8+ T cells. Two representative CD137 antibodies, utomilumab, and urelumab, show different costimulatory capacities in clinical trials. Balancing the antitumor effect and systemic toxicity of T cells activated by CD137 signaling is a challenge that requires clinical consideration. In this study, a panel of specific anti-human CD137 monoclonal antibodies (mAbs) were prepared and their affinities, isotypes, CD137-CRD (cysteine-rich domain) binding regions, cross-reactivity to mouse and rhesus CD137, inhibition of ligand‒receptor binding and costimulatory activities were analyzed. The results showed that anti-human CD137 mAbs had high cross-reactivity with rhesus CD137. MAbs fell into three clusters according to their different binding regions of the CD137 extracellular domain. They bound to CRDI+CRDII, CRDIII or CRDIV+STP. CRDIII-binding mAbs had the strongest blocking activity. Highly costimulatory CD137 mAbs showed stronger abilities to promote CD8+ T-cell proliferation. However, the costimulatory capacity of mAbs on T cells was not closely related to their ability to block CD137L-CD137 binding and may be controlled by more elaborate CRD conformational structures. This study provides additional information for the development of next-generation CD137 mAbs to meet clinical needs.

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来源期刊
CiteScore
8.30
自引率
3.70%
发文量
224
审稿时长
2 months
期刊介绍: The European Journal of Immunology (EJI) is an official journal of EFIS. Established in 1971, EJI continues to serve the needs of the global immunology community covering basic, translational and clinical research, ranging from adaptive and innate immunity through to vaccines and immunotherapy, cancer, autoimmunity, allergy and more. Mechanistic insights and thought-provoking immunological findings are of interest, as are studies using the latest omics technologies. We offer fast track review for competitive situations, including recently scooped papers, format free submission, transparent and fair peer review and more as detailed in our policies.
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