Profiling the impact of anti-human CD20 monoclonal antibodies on lymphocyte B cell subsets and their precursors in the bone marrow and in lymphoid tissues in an immunocompromised mouse engrafted with human cells

IF 9.1 2区 医学 Q1 PHARMACOLOGY & PHARMACY
Annalisa Moregola , Fabrizia Bonacina , Giovanni Battista Vingiani , Roberta Frapolli , Renato Turrini , Giuseppe Danilo Norata
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Abstract

Ofatumumab (OFA) and ocrelizumab (OCRE) are two anti-CD20 monoclonal antibodies approved for the treatment of relapsing forms of multiple sclerosis due to their ability to deplete B lymphocytes. The aim of this study was to investigate the impact of these anti-hCD20 antibodies on B lymphocyte subsets in the circulation and in primary and secondary lymphoid organs in an immune system humanized mouse model (immunocompromised Rag2−/−Il2rg−/−CD47−/−) engrafted with human CD34+ hematopoietic stem cells. Three months after humanization, mice, which present adaptive immune cells only of human origin, were treated with OFA (0.3 mg/Kg; day 1, 3 and 5), or OCRE (10 mg/kg; day 1) or saline. Seven days after the last injection a robust (>90 %) decrease of circulating human CD20+ B lymphocytes was observed in both OFA- and OCRE-treated mice. A partial replenishment of B lymphocytes was detectable in blood 36 days from the last injection in OFA-treated mice, while no B lymphocytes could be detected in OCRE-treated mice up to 65 days post injection. Bone marrow profiling showed that during hCD20+ B cell depletion and replenishment, OCRE-treated mice preserved only preB-I cells in the bone marrow, while the bone marrow of OFA-treated mice presented both preB-I as well as preB-II cells, with the latter subset being the one closest to differentiate into immature B cells. These data together with changes in B cell distribution in other tissues suggest that ofatumumab preserve BM niches, critical for B lymphocyte replenishment, limiting potential side effects of the treatment associated with the increased risk of infection.
分析抗人 CD20 单克隆抗体对骨髓中淋巴细胞 B 细胞亚群及其前体的影响,以及免疫功能低下小鼠淋巴组织中与人细胞接种的淋巴细胞 B 细胞亚群及其前体的影响。
Ofatumumab(OFA)和ocrelizumab(OCRE)是两种抗CD20单克隆抗体,因其能消耗B淋巴细胞而被批准用于治疗复发性多发性硬化症。本研究的目的是在免疫系统人源化小鼠模型(免疫受损的Rag2-/-Il2rg-/-CD47-/-)中,研究这些抗hCD20抗体对血液循环中的B淋巴细胞亚群以及原发性和继发性淋巴器官中的B淋巴细胞亚群的影响。人源化三个月后,小鼠接受 OFA(0.3 毫克/千克;第 1、3 和 5 天)或 OCRE(10 毫克/千克;第 1 天)或生理盐水治疗,这些小鼠体内只有源于人类的适应性免疫细胞。最后一次注射七天后,在接受 OFA 和 OCRE 治疗的小鼠中均观察到循环中的人类 CD20+ B 淋巴细胞大量减少(>90%)。经 OFA 处理的小鼠在最后一次注射后 36 天的血液中可检测到 B 淋巴细胞的部分补充,而经 OCRE 处理的小鼠在注射后 65 天仍检测不到 B 淋巴细胞。骨髓图谱显示,在 hCD20+ B 细胞耗竭和补充过程中,OCRE 处理的小鼠骨髓中只保留了前 B-I 细胞,而 OFA 处理的小鼠骨髓中既有前 B-I 细胞,也有前 B-II 细胞,后者是最接近分化为未成熟 B 细胞的亚群。这些数据以及 B 细胞在其他组织中分布的变化表明,ofatumumab 能保护 BM 龛位,这对 B 淋巴细胞的补充至关重要,从而限制了治疗可能产生的副作用,即增加感染风险。
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来源期刊
Pharmacological research
Pharmacological research 医学-药学
CiteScore
18.70
自引率
3.20%
发文量
491
审稿时长
8 days
期刊介绍: Pharmacological Research publishes cutting-edge articles in biomedical sciences to cover a broad range of topics that move the pharmacological field forward. Pharmacological research publishes articles on molecular, biochemical, translational, and clinical research (including clinical trials); it is proud of its rapid publication of accepted papers that comprises a dedicated, fast acceptance and publication track for high profile articles.
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