NFAT1在B细胞自身耐受中的作用。
Involvement of NFAT1 in B cell self-tolerance.
作者信息
Barrington Robert A, Borde Madhuri, Rao Anjana, Carroll Michael C
机构信息
CBR Institute for Biomedical Research, Harvard University, Boston, MA 02115, USA.
出版信息
J Immunol. 2006 Aug 1;177(3):1510-5. doi: 10.4049/jimmunol.177.3.1510.
B cells from anti-lysozyme Ig/soluble lysozyme double-transgenic mice are chronically exposed to self-Ag in the periphery, resulting in an anergic phenotype. Chronic exposure to self-Ag leads to nuclear translocation of NFAT1 and NFAT2, suggesting that they are involved in anergy. To directly test a role for NFAT1 in B cell anergy, NFAT1-deficient mice were crossed with anti-lysozyme Ig transgenic mice. As expected, B cell anergy was evident in the presence of self-Ag based on reduced serum anti-lysozyme levels, percentage and number of mature B cells, and reduced B cell responsiveness. By contrast, B cell anergy was relieved in NFAT1(-/-) mice expressing soluble self-Ag. Bone marrow development was equivalent in NFAT1-sufficient and -deficient mice, suggesting that loss of anergy in the latter is due to selection later in development. Taken together, these studies provide direct evidence that the transcription factor NFAT1 is involved in B cell anergy.
来自抗溶菌酶Ig/可溶性溶菌酶双转基因小鼠的B细胞在周围组织中持续暴露于自身抗原,导致无反应性表型。持续暴露于自身抗原会导致NFAT1和NFAT2的核转位,表明它们参与了无反应性。为了直接测试NFAT1在B细胞无反应性中的作用,将NFAT1缺陷小鼠与抗溶菌酶Ig转基因小鼠杂交。正如预期的那样,基于血清抗溶菌酶水平降低、成熟B细胞的百分比和数量减少以及B细胞反应性降低,在存在自身抗原的情况下B细胞无反应性明显。相比之下,在表达可溶性自身抗原的NFAT1(-/-)小鼠中,B细胞无反应性得到缓解。NFAT1充足和缺陷的小鼠骨髓发育相当,表明后者无反应性的丧失是由于发育后期的选择。综上所述,这些研究提供了直接证据,证明转录因子NFAT1参与了B细胞无反应性。
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