Kristina Ottens, Jalyn Schneider, Anne B Satterthwaite
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Abstract
Mice deficient in Lyn, a tyrosine kinase that limits B cell activation, develop a lupus-like autoimmune disease characterized by the accumulation of splenic plasma cells and the production of autoantibodies. Lyn-/- mice have reduced numbers of marginal zone (MZ) B cells, a B cell subset that is enriched in autoreactivity and prone to plasma cell differentiation. We hypothesized that this is due to unchecked terminal differentiation of this potentially pathogenic B cell subpopulation. However, impairing MZ B cell development in Lyn-/- mice did not reduce plasma cell accumulation or autoantibodies, and preventing plasma cell differentiation did not restore MZ B cell numbers. Instead, Lyn-/- mice accumulated B-1a cells when plasma cell differentiation was impaired. Similar to MZ B cells, B-1a cells tend to be polyreactive or weakly autoreactive and are primed for terminal differentiation. Our results implicate B-1a cells, but not MZ B cells, as contributors to the autoreactive plasma cell pool in Lyn-/- mice.
Lyn是一种限制B细胞活化的酪氨酸激酶,缺乏Lyn的小鼠会患上一种狼疮样自身免疫性疾病,其特征是脾浆细胞聚集和自身抗体的产生。Lyn-/-小鼠的边缘区(MZ)B细胞数量减少,这种B细胞亚群富含自体活性,容易向浆细胞分化。我们推测这是由于这一潜在致病性 B 细胞亚群的末端分化未得到控制所致。然而,损害Lyn-/-小鼠的MZ B细胞发育并不能减少浆细胞积累或自身抗体,阻止浆细胞分化也不能恢复MZ B细胞的数量。相反,当浆细胞分化受损时,Lyn-/-小鼠会积累B-1a细胞。与 MZ B 细胞类似,B-1a 细胞也倾向于多反应性或弱自反应性,并为终末分化做好了准备。我们的研究结果表明,B-1a 细胞而非 MZ B 细胞是 Lyn-/- 小鼠自反应性浆细胞池的贡献者。
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