MacroGenics, Inc. 9640 Medical Center Drive, Rockville, MD 20850, USA.
Clin Immunol. 2013 Dec;149(3):268-78. doi: 10.1016/j.clim.2013.05.001. Epub 2013 May 11.
Two humanized, anti-CD3 mAbs with reduced FcR binding, teplizumab and otelixizumab, have been evaluated in over 1500 subjects, ages 7-45, with new and recently diagnosed T1D with a range of intravenous doses (3-48mg) and regimens (6-14 days, single or repeat courses). In general, studies that used adequate dosing demonstrated improvement in stimulated C-peptide responses and reduced need for exogenous insulin for two years and even longer after diagnosis. Drug treatment causes a transient reduction in circulating T cells, but the available data suggest that the mechanism of action may involve induction of regulatory mechanisms. The adverse effects of anti-CD3 treatment are infusion-related and transient. The studies have identified significant differences in efficacy among patient groups suggesting that a key aspect for development of this immune therapy is identification of the demographic, metabolic, and immunologic features that distinguish subjects who are most likely to show beneficial clinical responses.
两种人源化、低 FcγR 结合的抗 CD3 mAb(teplizumab 和 otelixizumab)已在 1500 多名年龄在 7-45 岁的新诊断和近期诊断的 T1D 患者中进行了评估,这些患者接受了不同剂量(3-48mg)和方案(6-14 天,单次或多次疗程)的静脉给药。一般来说,使用足够剂量的研究显示,在诊断后两年甚至更长时间内,刺激 C 肽反应得到改善,对外源性胰岛素的需求减少。药物治疗会导致循环 T 细胞短暂减少,但现有数据表明,其作用机制可能涉及诱导调节机制。抗 CD3 治疗的不良反应为输注相关且短暂的。这些研究确定了患者群体之间疗效的显著差异,这表明这种免疫治疗的一个关键方面是确定可区分最有可能产生有益临床反应的受试者的人口统计学、代谢和免疫学特征。
Zotero 插件