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CD3亲和力减弱对T细胞结合双特异性抗体的影响:真的那么简单吗?

The impact of CD3 affinity-attenuation on T cell engaging bispecific antibodies: is it really that simple?

作者信息

Abdelmotaleb Omar, Schneider Anneliese, Gassner Christian, Märsch Stephan, Klein Christian

机构信息

Roche Pharma Research and Early Development, pRED, Roche Innovation Center Zurich, Schlieren, Switzerland.

Molecular and Systems Toxicology, Department of Pharmaceutical Sciences, University of Basel, Basel, Switzerland.

出版信息

Expert Opin Drug Discov. 2025 Aug;20(8):943-949. doi: 10.1080/17460441.2025.2522088. Epub 2025 Jun 23.

Abstract

INTRODUCTION

The first generation of approved T cell engagers (TCEs) showing promising efficacy in hematological and solid tumors relies on high binding affinity to CD3. Treatment of tumors with TCEs has been clinically associated with toxicities related to cytokine release syndrome (CRS). In addition to clinical strategies to mitigate CRS, antibody engineering efforts have been undertaken to generate TCEs with optimized therapeutic index. Strategies pursued in this context include affinity attenuation of CD3 binding arm, to achieve potent tumor cell killing with minimal cytokine secretion.

AREAS COVERED

A literature search was conducted to identify peer-reviewed articles related to CD3 affinity and T cell engagers. Here, we provide an overview of the current state and recent developments in CD3 affinity-attenuation, both preclinically and clinically, with a focus on the challenges of developing TCEs with attenuated affinity to CD3 as well as identifying possible areas of improvement.

EXPERT OPINION

CD3 affinity reduction can effectively lower cytokine levels preclinically; however, it is crucial to consider all factors influencing the mode of action of TCEs. Prioritizing the use of the most translatable preclinical models is essential to identify the right candidates for further development.

摘要

引言

第一代经批准的T细胞衔接器(TCEs)在血液系统肿瘤和实体瘤中显示出有前景的疗效,其依赖于对CD3的高结合亲和力。用TCEs治疗肿瘤在临床上与细胞因子释放综合征(CRS)相关的毒性有关。除了减轻CRS的临床策略外,还进行了抗体工程研究以产生具有优化治疗指数的TCEs。在此背景下采用的策略包括减弱CD3结合臂的亲和力,以在最小化细胞因子分泌的情况下实现有效的肿瘤细胞杀伤。

涵盖领域

进行了文献检索以识别与CD3亲和力和T细胞衔接器相关的同行评审文章。在此,我们概述了临床前和临床中CD3亲和力减弱的当前状态和最新进展,重点关注开发对CD3亲和力减弱的TCEs的挑战以及确定可能的改进领域。

专家意见

降低CD3亲和力可在临床前有效降低细胞因子水平;然而,考虑影响TCEs作用方式的所有因素至关重要。优先使用最具可转化性的临床前模型对于确定进一步开发的合适候选者至关重要。

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