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bcl-2 Transgene Expression Inhibits Apoptosis in the Germinal Center and Reveals Differences in the Selection of Memory B Cells and Bone Marrow Antibody-Forming Cells

机译:bcl-2转基因表达抑制生殖中心的凋亡,并揭示记忆B细胞和骨髓抗体形成细胞选择的差异

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摘要

Immunization with T cell–dependent antigens generates long-lived memory B cells and antibody-forming cells (AFCs). Both populations originate in germinal centers and, predominantly, produce antibodies with high affinity for antigen. The means by which germinal center B cells are recruited into these populations remains unclear. We have examined affinity maturation of antigen-specific B cells in mice expressing the cell death inhibitor bcl-2 as a transgene. Such mice had reduced apoptosis in germinal centers and an excessive number of memory B cells with a low frequency of V gene somatic mutation, including those mutations encoding amino acid exchanges known to enhance affinity. Despite the frequency of AFCs being increased in bcl-2–transgenic mice, the fraction secreting high-affinity antibody in the bone marrow at day 42 remained unchanged compared with controls. The inability of BCL-2 to alter selection of bone marrow AFCs is consistent with these cells being selected within the germinal center on the basis of their affinity being above some threshold rather than their survival being due to a selective competition for an antigen-based signal. Continuous competition for antigen does, however, explain formation of the memory compartment.
机译:用T细胞依赖性抗原免疫可产生长寿命的记忆B细胞和抗体形成细胞(AFC)。两种种群都起源于生发中心,并且主要产生对抗原具有高亲和力的抗体。尚不清楚将生发中心B细胞募集到这些种群中的方法。我们已经检查了小鼠中表达细胞死亡抑制剂bcl-2为转基因的抗原特异性B细胞的亲和力成熟。这类小鼠的生发中心细胞凋亡减少,且记忆B细胞数量过多,V基因体细胞突变的频率较低,包括那些编码已知可增强亲和力的氨基酸交换的突变。尽管在bcl-2转基因小鼠中AFC的频率增加,但与对照组相比,在第42天时,在骨髓中分泌高亲和力抗体的部分仍未改变。 BCL-2不能改变骨髓AFC的选择与这些细胞在生发中心内被选择是一致的,这是基于它们的亲和力高于某个阈值,而不是其存活是由于对基于抗原的信号的选择性竞争。然而,对抗原的持续竞争确实解释了记忆区室的形成。

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