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B-cell subpopulations in humans and their differential susceptibility to depletion with anti-CD20 monoclonal antibodies

机译:人类B细胞亚群及其对抗CD20单克隆抗体耗竭的差异敏感性

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In humans, different B-cell subpopulations can be distinguished in peripheral blood and other tissues on the basis of differential expression of various surface markers. These different subsets correspond to different stages of maturation, activation and differentiation. B-cell depletion therapy based on rituximab, an anti-CD20 mAb, is widely used in the treatment of various malignant and autoimmune diseases. Rituximab induces a very significant depletion of B-cell subpopulations in the peripheral blood usually for a period of 6 to 9 months after one cycle of therapy. Cells detected circulating during depletion are mainly CD20 negative plasmablasts. Data on depletion of CD20-expressing B cells in solid tissues are limited but show that depletion is significant but not complete, with bone marrow and spleen being more easily depleted than lymph nodes. Factors influencing depletion are thought to include not only the total drug dose administered and distribution into various tissues, but also B-cell intrinsic and microenvironment factors influencing recruitment of effector mechanisms and antigen and effector modulation. Available studies show that the degree of depletion varies between individuals, even if treated with the same dose, but that it tends to be consistent in the same individual. This suggests that individual factors are important in determining the final extent of depletion.
机译:在人类中,根据各种表面标志物的差异表达,可以在外周血和其他组织中区分出不同的B细胞亚群。这些不同的子集对应于成熟,激活和分化的不同阶段。基于利妥昔单抗(一种抗CD20 mAb)的B细胞耗竭疗法被广泛用于治疗各种恶性和自身免疫性疾病。利妥昔单抗在治疗的一个周期后通常在6到9个月的时间内诱导外周血中B细胞亚群的大量消耗。在耗竭过程中检测到循环的细胞主要是CD20阴性浆母细胞。关于实体组织中表达CD20的B细胞耗竭的数据是有限的,但显示耗竭是明显的,但并不完全,骨髓和脾脏比淋巴结更容易耗竭。认为影响耗竭的因素不仅包括所施用的总药物剂量和分布到各种组织中,还包括影响效应子机制募集以及抗原和效应子调节的B细胞内在和微环境因素。现有的研究表明,即使使用相同剂量的药物治疗,个体之间的耗竭程度也会有所不同,但是在同一个体中耗竭程度往往是一致的。这表明个体因素对于确定最终的耗竭程度很重要。

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