Immature B cell homing shapes human lymphoid tissue structure and function

未成熟B细胞的归巢塑造了人类淋巴组织的结构和功能。

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Abstract

Shortly after the emergence of newly formed human B cells from bone marrow as transitional cells, they diverge along two developmental pathways that can be distinguished by the level of IgM they express and migratory biases. Here, we propose that differential tissue homing of immature B cell subsets contributes to human lymphoid tissue structure and function.

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