原发性干燥综合征的特征是 IgD+ 未转换记忆 B 细胞具有独特的表型和转录特征。
Primary Sjögren's syndrome is characterized by distinct phenotypic and transcriptional profiles of IgD+ unswitched memory B cells.
机构信息
University of Rochester Medical Center, Rochester, New York.
出版信息
Arthritis Rheumatol. 2014 Sep;66(9):2558-69. doi: 10.1002/art.38734.
OBJECTIVE
The significance of distinct B cell abnormalities in primary Sjögren's syndrome (SS) remains to be established. We undertook this study to analyze the phenotype and messenger RNA (mRNA) transcript profiles of B cell subsets in patients with primary SS and to compare them with those in sicca syndrome patients and healthy controls.
METHODS
CD19+ B cells from 26 patients with primary SS, 27 sicca syndrome patients, and 22 healthy controls were analyzed by flow cytometry. Gene expression profiles of purified B cell subsets (from 3-5 subjects per group per test) were analyzed using Affymetrix gene arrays.
RESULTS
Patients with primary SS had lower frequencies of CD27+IgD- switched memory B cells and CD27+IgD+ unswitched memory B cells compared with healthy controls. Unswitched memory B cell frequencies were also lower in sicca syndrome patients and correlated inversely with serologic hyperactivity in both disease states. Further, unswitched memory B cells in primary SS had lower expression of CD1c and CD21. Gene expression analysis of CD27+ memory B cells separated patients with primary SS from healthy controls and identified a subgroup of sicca syndrome patients with a primary SS-like transcript profile. Moreover, unswitched memory B cell gene expression analysis identified 187 genes differentially expressed between patients with primary SS and healthy controls.
CONCLUSION
A decrease in unswitched memory B cells with serologic hyperactivity is characteristic of both established primary SS and a subgroup of sicca syndrome, which suggests the value of these B cells both as biomarkers of future disease progression and for understanding disease pathogenesis. Overall, the mRNA transcript analysis of unswitched memory B cells suggests that their activation in primary SS takes place through innate immune pathways in the context of attenuated antigen-mediated adaptive signaling. Thus, our findings provide important insight into the mechanisms and potential consequences of decreased unswitched memory B cells in primary SS.
目的
原发性干燥综合征(SS)中不同 B 细胞异常的意义尚待确定。我们进行这项研究,旨在分析原发性 SS 患者 B 细胞亚群的表型和信使 RNA(mRNA)转录谱,并将其与干燥综合征患者和健康对照者进行比较。
方法
采用流式细胞术分析 26 例原发性 SS 患者、27 例干燥综合征患者和 22 例健康对照者的 CD19+B 细胞。使用 Affymetrix 基因芯片分析纯化 B 细胞亚群(每组 3-5 例)的基因表达谱。
结果
与健康对照组相比,原发性 SS 患者的 CD27+IgD-记忆 B 细胞和 CD27+IgD+未成熟记忆 B 细胞频率较低。干燥综合征患者的未成熟记忆 B 细胞频率也较低,且在两种疾病状态下均与血清学高活性呈负相关。此外,原发性 SS 中的未成熟记忆 B 细胞 CD1c 和 CD21 的表达水平较低。分离原发性 SS 患者与健康对照者的 CD27+记忆 B 细胞的基因表达分析,鉴定出一组具有原发性 SS 样转录谱的干燥综合征患者。此外,未成熟记忆 B 细胞基因表达分析鉴定出原发性 SS 患者与健康对照者之间差异表达的 187 个基因。
结论
具有血清学高活性的未成熟记忆 B 细胞减少是已确诊的原发性 SS 和干燥综合征亚组的特征,这提示这些 B 细胞不仅可作为未来疾病进展的生物标志物,而且有助于理解疾病发病机制。总的来说,未成熟记忆 B 细胞的 mRNA 转录分析表明,原发性 SS 中它们的激活是在抗原呈递适应性信号减弱的情况下通过固有免疫途径发生的。因此,我们的研究结果为原发性 SS 中未成熟记忆 B 细胞减少的机制和潜在后果提供了重要的见解。
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