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缺乏转录因子EBF的小鼠中B细胞分化失败。

Failure of B-cell differentiation in mice lacking the transcription factor EBF.

作者信息

Lin H, Grosschedl R

机构信息

Howard Hughes Medical Institute, Department of Microbiology and Immunology, University of California, San Francisco 94143, USA.

出版信息

Nature. 1995 Jul 20;376(6537):263-7. doi: 10.1038/376263a0.

Abstract

Early B-cell factor (EBF) is a cell type-specific transcription factor that is expressed at all antigen-independent stages of B-lymphocyte differentiation and participates in the regulation of the mb-1 gene. Here we show, by targeted gene disruption in mice, that EBF is necessary for the generation of immunoglobulin-expressing B cells. EBF-deficient mice lack B cells that have rearranged their immunoglobulin D and JH gene segments, but contain B220+CD43+ progenitor cells that express germline mu and IL-7 receptor transcripts. Various non-lymphoid tissues that express EBF are apparently normal in homozygous mutant mice, including olfactory neurons in which EBF was identified as Olf-1 (refs 5, 6). Together, these data suggest that EBF plays a specific and important role in the transcriptional control of B-cell differentiation at a stage before Ig (immunoglobulin) gene rearrangement but after commitment of cells to the B-lymphoid lineage.

摘要

早期B细胞因子(EBF)是一种细胞类型特异性转录因子,在B淋巴细胞分化的所有抗原非依赖阶段均有表达,并参与mb-1基因的调控。在此我们通过对小鼠进行靶向基因敲除表明,EBF对于表达免疫球蛋白的B细胞的产生是必需的。EBF缺陷型小鼠缺乏已重排其免疫球蛋白D和JH基因片段的B细胞,但含有表达种系μ链和IL-7受体转录本的B220+CD43+祖细胞。在纯合突变小鼠中,各种表达EBF的非淋巴组织显然正常,包括其中EBF被鉴定为Olf-1的嗅觉神经元(参考文献5、6)。这些数据共同表明,EBF在Ig(免疫球蛋白)基因重排之前但在细胞定向至B淋巴细胞系之后的阶段,在B细胞分化的转录控制中发挥着特定且重要的作用。

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