生发中心
抗原
抗体
免疫学
生物
断点群集区域
等离子体电池
B细胞
B细胞受体
自身免疫
细胞生物学
受体
遗传学
作者
Christopher C. Goodnow,Carola G. Vinuesa,Katrina L. Randall,Fabienne Mackay,Robert Brink
摘要
This paper synthesizes recent progress toward understanding the integrated control systems and fail-safes that guide the quality and quantity of antibody produced by B cells. We focus on four key decisions: (1) the choice between proliferation or death in perifollicular B cells in the first 3 days after antigen encounter; (2) differentiation of proliferating perifollicular B cells into extrafollicular plasma cells or germinal center B cells; (3) positive selection of B cell antigen receptor (BCR) affinity for foreign antigen versus negative selection of BCR affinity for self antigen in germinal center B cells; and (4) survival versus death of antibody-secreting plasma cells. Understanding the engineering of these control systems represents a challenging future step for treating disorders of antibody production in autoimmunity, allergy and immunodeficiency.
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