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非裔美国狼疮患者的 B 细胞表现出激活表型。

B cells from African American lupus patients exhibit an activated phenotype.

机构信息

Discovery Translational Sciences, Bristol-Myers Squibb Company, Princeton, New Jersey, USA.

Immunoscience Translational Bioinformatics, Bristol-Myers Squibb Company, Pennington, New Jersey, USA.

出版信息

JCI Insight. 2016 Jun 16;1(9):e87310. doi: 10.1172/jci.insight.87310.

Abstract

Systemic lupus erythematosus (SLE) is a complex systemic autoimmune disease driven by both innate and adaptive immune cells. African Americans tend to present with more severe disease at an earlier age compared with patients of European ancestry. In order to better understand the immunological differences between African American and European American patients, we analyzed the frequencies of B cell subsets and the expression of B cell activation markers from a total of 68 SLE patients and 69 normal healthy volunteers. We found that B cells expressing the activation markers CD86, CD80, PD1, and CD40L, as well as CD19CD27IgD double-negative B cells, were enriched in African American patients vs. patients of European ancestry. In addition to increased expression of CD40L, surface levels of CD40 on B cells were lower, suggesting the engagement of the CD40 pathway. In vitro experiments confirmed that CD40L expressed by B cells could lead to CD40 activation and internalization on adjacent B cells. To conclude, these results indicate that, compared with European American patients, African American SLE patients present with a particularly active B cell component, possibly via the activation of the CD40/CD40L pathway. These data may help guide the development of novel therapies.

摘要

系统性红斑狼疮 (SLE) 是一种由先天和适应性免疫细胞驱动的复杂系统性自身免疫性疾病。与欧洲血统的患者相比,非裔美国人往往在更早的年龄出现更严重的疾病。为了更好地了解非裔美国人和欧洲裔美国人患者之间的免疫差异,我们分析了总共 68 名 SLE 患者和 69 名正常健康志愿者的 B 细胞亚群频率和 B 细胞活化标志物的表达。我们发现,表达活化标志物 CD86、CD80、PD1 和 CD40L 的 B 细胞以及 CD19CD27IgD 双阴性 B 细胞在非裔美国患者中比在欧洲裔患者中更为丰富。除了 CD40L 的表达增加外,B 细胞表面 CD40 的水平也较低,提示 CD40 途径的参与。体外实验证实,B 细胞表达的 CD40L 可导致相邻 B 细胞上的 CD40 活化和内化。总之,这些结果表明,与欧洲裔患者相比,非裔美国 SLE 患者表现出特别活跃的 B 细胞成分,可能通过 CD40/CD40L 途径的激活。这些数据可能有助于指导新疗法的开发。

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