Generation of specific antibodies during an immune response to infection or vaccination depends on the ability to rapidly and accurately select clones of antibody-secreting B lymphocytes for expansion. Antigen-specific B cell clones undergo the cell fate decision to differentiate into antibody-secreting plasma cells, memory B cells, or germinal center B cells. The E26-transformation-specific (ETS) transcription factors Spi-B and Spi-C are important regulators of B cell development and function. Spi-B is expressed throughout B cell development and is downregulated upon plasma cell differentiation. Spi-C is highly related to Spi-B and has similar DNA-binding specificity. Heterozygosity for Spic rescues B cell development and B cell proliferation defects observed in Spi-B knockout mice. In this study, we show that heterozygosity for Spic rescued defective IgG1 secondary antibody responses in Spib(-/-) mice. Plasma cell differentiation was accelerated in Spib(-/-) B cells. Gene expression, ChIP-seq, and reporter gene analysis showed that Spi-B and Spi-C differentially regulated Bach2, encoding a key regulator of plasma cell and memory B cell differentiation. These results suggest that Spi-B and Spi-C oppose the function of one another to regulate B cell differentiation and function.
Opposing Roles for the Related ETS-Family Transcription Factors Spi-B and Spi-C in Regulating B Cell Differentiation and Function.
ETS家族相关转录因子Spi-B和Spi-C在调节B细胞分化和功能中发挥相反的作用
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作者:Laramée Anne-Sophie, Raczkowski Hannah, Shao Peng, Batista Carolina, Shukla Devanshi, Xu Li, Haeryfar S M Mansour, Tesfagiorgis Yodit, Kerfoot Steven, DeKoter Rodney
| 期刊: | Frontiers in Immunology | 影响因子: | 5.900 |
| 时间: | 2020 | 起止号: | 2020 May 8; 11:841 |
| doi: | 10.3389/fimmu.2020.00841 | 研究方向: | 细胞生物学 |
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