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首页> 外文期刊>Clinical and vaccine immunology: CVI >Disturbed homeostasis and multiple signaling defects in the peripheral blood B-cell compartment of patients with severe chronic sarcoidosis
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Disturbed homeostasis and multiple signaling defects in the peripheral blood B-cell compartment of patients with severe chronic sarcoidosis

机译:干扰体内平衡和多个信号在外周血b细胞缺陷严重的慢性患者的室结节病

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摘要

The presence of hypergammaglobulinemia, autoantibodies, and circulating immune complexes suggests that humoral immunity may contribute to the pathogenesis of sarcoidosis. However, little is known about the role played by B cells in the development of this disease. Here we investigated the subpopulation distribution, response to stimulation, and levels of the nuclear transcription factor NF-κB/p65 in peripheral blood B cells from patients with severe chronic sarcoidosis. Patients with severe chronic sarcoidosis had absolute B-cell lymphopenia and exhibited significantly decreased frequencies and total numbers of memory (CD19 + CD27 +) B cells. The reduced numbers of memory B cells in these patients reflected a decrease in the total numbers of class-switched (CD19 + CD27 + IgD -) and unswitched (CD19 + CD27 + IgD +) memory B cells and coincided with an increased frequency of circulating (CD19 +/- CD20 - CD27 ++) plasmablasts. Polyclonal stimulation of sarcoid B cells resulted in reduced expression of activation markers (i.e., CD25, CD69, and CD86), decreased proliferation, and impaired plasma cell differentiation. Baseline expression of p65 in B cells was reduced in 65% of the patients. These results suggest disturbed homeostasis, intrinsic signaling defects, and anergy within the peripheral B-cell compartments of patients with severe chronic sarcoidosis.
机译:hypergammaglobulinemia的存在,自身抗体和循环免疫复合物表明,体液免疫可能导致结节病的发病机理。是已知的B细胞所扮演的角色呢这种疾病的发展。分组人口分布、响应刺激,和水平的核转录因子NF -κB / p65在外围血从严重的慢性患者B细胞结节病。结节病绝对b细胞淋巴细胞减少显著减少频率和展出总数量的内存(CD19 + CD27 +)的B细胞。这些记忆B细胞数目减少病人减少总反映出来数量的class-switched (CD19 + CD27 + IgD -)和unswitched (CD19 + CD27 + IgD +)记忆B细胞,恰逢频率增加循环(CD19 + / - CD20 CD27 + +)plasmablasts。细胞导致减少的表达激活标记(例如,CD25、CD69和CD86),减少扩散,浆细胞受损分化。细胞减少,65%的患者。结果表明干扰体内平衡,内在信号缺陷,和无力外围患者b细胞的隔间严重的慢性结节病。

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