生物
B细胞
生发中心
抗原
记忆B细胞
免疫系统
人口
免疫学
多样性(政治)
选择(遗传算法)
否定选择
抗体
幼稚B细胞
B细胞受体
遗传学
独特型
体液免疫
免疫
克隆选择
获得性免疫系统
细胞生物学
体细胞突变
受体
计算生物学
细胞
亲和力成熟
T细胞受体
表型
B-1电池
进化生物学
多克隆B细胞反应
抗体反应
作者
Isaak Quast,David M. Tarlinton
标识
DOI:10.1146/annurev-immunol-082323-031320
摘要
Affinity for antigen is a fundamental parameter of humoral immunity. It determines the B cell clones that participate in the response, it is a readout of clonal selection as the response progresses, and the magnitude of its improvement in T cell-dependent responses is a major criterion of success. But another important attribute of immunity at initiation, propagation, and cessation is the diversity of antigen binding by B cells and antibodies. As such, the diversity of antigen receptors is important at the outset of the response in providing a broad population from which B cell fates can be selected. Equally, within the germinal center, specific mechanisms operate to diversify the B cell population for affinity-based selection, which itself promotes clonal restriction to achieve its goals. However, the importance of sustaining diversity of antigen recognition at all stages of the response, not only in the composition of the B cell memory compartments, is often lost by the focus on affinity as the key measure of immunity. In this article, we consider recent developments in understanding B cell selection into, persistence within, and exit from T cell-dependent immune responses and how these processes are calibrated to ensure diversity of antigen recognition persists into memory in spite of the clonal narrowing that is the usual outcome of affinity-driven selection.
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