医学
阿勒姆图祖马
奥图穆马
免疫学
中性粒细胞减少症
美罗华
菲格拉斯汀
多发性硬化
芬戈莫德
纳塔利祖玛
CD20
CD52型
奥克列珠单抗
免疫系统
抗原
内科学
化疗
淋巴瘤
抗体
作者
David Baker,Angray S. Kang,Gavin Giovannoni,Klaus Schmierer
标识
DOI:10.1016/j.msard.2023.105400
摘要
Neutropenia serves as a risk factor for severe infection and is a consequence of some immune-depleting immunotherapies. This occurs in people with multiple sclerosis following chemotherapy-conditioning in haematopoietic stem cell transplantation and potent B cell targeting agents. Whilst CD52 is expressed by neutrophils and may contribute to early-onset neutropenia following alemtuzumab treatment, deoxycytidine kinase and CD20 antigen required for activity of cladribine tablets, off-label rituximab, ocrelizumab, ofatumumab and ublituximab are not or only weakly expressed by neutrophils. Therefore, alternative explanations are needed for the rare occurrence of early and late-onset neutropenia following such treatments. This probably occurs due to alterations in the balance of granulopoiesis and neutrophil removal. Neutrophils are short-lived, and their removal may be influenced by drug-associated infections, the killing mechanisms of the therapies and amplified by immune dyscrasia due to influences on neutropoiesis following growth factor rerouting for B cell recovery and cytokine deficits following lymphocyte depletion. This highlights the small but evident neutropenia risks following sustained B cell depletion with some treatments.
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