免疫球蛋白D
B细胞受体
B细胞
生物
幼稚B细胞
人口
分子生物学
断点群集区域
CD19
IGHD
B-1电池
免疫球蛋白类转换
免疫系统
抗体
免疫学
细胞生物学
T细胞
流式细胞术
受体
遗传学
抗原提呈细胞
医学
生长激素
生物化学
环境卫生
激素
生长激素缺乏
作者
Johannes Dirks,Oliver Andrés,Luisa Paul,Georgi Manukjan,Harald Schulze,Henner Morbach
标识
DOI:10.3389/fimmu.2023.1096019
摘要
B cell maturation and immunoglobulin (Ig) repertoire selection are governed by expression of a functional B cell receptor (BCR). Naïve B cells co-express their BCR as IgM and IgD isotype. However, the role of the additionally expressed IgD on naïve B cells is not known. Here we assessed the impact of IgD on naïve B cell maturation and Ig repertoire selection in 8 individuals from 3 different families with heterozygous loss-of-function or loss-of expression mutations in IGHD . Although naïve B cells from these individuals expressed IgM on their surface, the IGHD variant in heterozygous state entailed a chimeric situation by allelic exclusion with almost half of the naïve B cell population lacking surface IgD expression. Flow cytometric analyses revealed a distinct phenotype of IgD-negative naïve B cells with decreased expression of CD19, CD20 and CD21 as well as lower BAFF-R and integrin-β7 expression. IgD-negative B cells were less responsive in vitro after engaging the IgM-BCR, TLR7/9 or CD40 pathway. Additionally, a selective disadvantage of IgD-negative B cells within the T2 transitional and mature naïve B cell compartment as well as reduced frequencies of IgM lo/- B cells within the mature naïve B cell compartment lacking IgD were evident. RNA-Ig-seq of bulk sorted B cell populations showed an altered selection of distinct V H segments in the IgD-negative mature naïve B cell population. We conclude that IgD expression on human naïve B cells is redundant for generation of naïve B cells in general, but further shapes the naive B cell compartment starting from T2 transitional B cells. Our observations suggest an unexpected role of IgD expression to be critical for selection of distinct Ig V H segments into the pre-immune Ig repertoire and for the survival of IgM lo/- naïve B cells known to be enriched in poly-/autoreactive B cell clones.
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