Differential effects of anti-CD20 therapy on CD4 and CD8 T cells and implication of CD20-expressing CD8 T cells in MS disease activity

CD8型 CD20 免疫学 CD38 CD19 免疫系统 细胞毒性T细胞 生物 医学 流式细胞术 癌症研究 抗原 川地34 细胞生物学 干细胞 遗传学 体外
作者
Koji Sumii,Rui Li,Ayman Rezk,Ina Mexhitaj,Kristina R. Patterson,Mihir Kakara,Leah Zuroff,Jeffrey L. Bennett,H.‐Christian von Büdingen,Robert Carruthers,Keith R. Edwards,Robert J. Fallis,Paul S. Giacomini,Benjamin Greenberg,David A. Hafler,Carolina Ionete,Ulrike Kaunzner,Christopher Lock,Erin E. Longbrake,Gabriel Pardo,Fredrik Piehl,Martin Weber,Tjalf Ziemssen,Dina Jacobs,Jeffrey M. Gelfand,Anne H. Cross,Briana Cameron,B Musch,Ryan C. Winger,Xiaoming Jia,Christopher Harp,Ann Herman,Amit Bar‐Or
出处
期刊:Proceedings of the National Academy of Sciences of the United States of America [Proceedings of the National Academy of Sciences]
卷期号:120 (3) 被引量:8
标识
DOI:10.1073/pnas.2207291120
摘要

A small proportion of multiple sclerosis (MS) patients develop new disease activity soon after starting anti-CD20 therapy. This activity does not recur with further dosing, possibly reflecting deeper depletion of CD20-expressing cells with repeat infusions. We assessed cellular immune profiles and their association with transient disease activity following anti-CD20 initiation as a window into relapsing disease biology. Peripheral blood mononuclear cells from independent discovery and validation cohorts of MS patients initiating ocrelizumab were assessed for phenotypic and functional profiles using multiparametric flow cytometry. Pretreatment CD20-expressing T cells, especially CD20 dim CD8 + T cells with a highly inflammatory and central nervous system (CNS)-homing phenotype, were significantly inversely correlated with pretreatment MRI gadolinium-lesion counts, and also predictive of early disease activity observed after anti-CD20 initiation. Direct removal of pretreatment proinflammatory CD20 dim CD8 + T cells had a greater contribution to treatment-associated changes in the CD8 + T cell pool than was the case for CD4 + T cells. Early disease activity following anti-CD20 initiation was not associated with reconstituting CD20 dim CD8 + T cells, which were less proinflammatory compared with pretreatment. Similarly, this disease activity did not correlate with early reconstituting B cells, which were predominantly transitional CD19 + CD24 high CD38 high with a more anti-inflammatory profile. We provide insights into the mode-of-action of anti-CD20 and highlight a potential role for CD20 dim CD8 + T cells in MS relapse biology; their strong inverse correlation with both pretreatment and early posttreatment disease activity suggests that CD20-expressing CD8 + T cells leaving the circulation (possibly to the CNS) play a particularly early role in the immune cascades involved in relapse development.
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