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慢性 HCV 感染中杀伤 B 细胞的增加可能导致自身免疫和病毒载量增加。

Increased killer B cells in chronic HCV infection may lead to autoimmunity and increased viral load.

机构信息

Division of Allergy and Clinical Immunology, Bnai Zion Medical Center, Haifa, Israel.

Unit of Hepatology, Carmel Medical Center, Haifa, Israel.

出版信息

Clin Exp Immunol. 2018 Aug;193(2):183-193. doi: 10.1111/cei.13139.

Abstract

Regulatory B (B ) cells are characterized by various membrane markers and the secretion of different inhibitory cytokines. A new subset of B cells was identified as CD5 Fas-ligand (FasL) . Their main reported role is to suppress anti-viral and anti-tumour immune responses, and, hence they have been dubbed 'killer' B cells. In this study, we aim to assess the role of these cells in chronic hepatitis C virus (HCV) infection, and determine if they contribute to the increased viral load and persistence of HCV and its related autoimmunity. (i) FasL expression on CD5 B cells is increased significantly in HCV-infected patients compared to healthy individuals [28·06 ± 6·71 mean fluorescence intensity (MFI) ± standard error of the mean (s.e.m.), median = 27·9 versus 10·87 ± 3·97 MFI ± s.e.m., median = 10·3, respectively, P <  0·0001]. (ii) Killer B cells from HCV patients increased autologous CD4 T cell apoptosis compared to the apoptosis in healthy individuals [39·17% ± 7·18% mean ± standard deviation (s.d.), median = 39·6 versus 25·92 ± 8·65%, mean ± s.d., median = 24·1%, P <  0·0001, respectively]. A similar increase was observed in CD8 T cell apoptosis (54·67 ± 15·49% mean ± s.d., median = 57·3 versus 21·07% ± 7·4%, mean ± s.d., median = 20%, P = 0·0006, respectively). (iii) By neutralizing FasL with monoclonal anti-FasL antibodies, we have shown that the induction of apoptosis by killer B cells is FasL-dependent. (iv) Increased expression of FasL on CD5 B cells is correlated positively with an increased viral load and the presence of anti-nuclear antibodies and rheumatoid factor in HCV. This is the first study in which killer B cells have been suggested to play a pathogenic role in HCV. They seem to be involved in HCV's ability to escape efficient immune responses.

摘要

调节性 B (B ) 细胞的特征是具有各种膜标记物和分泌不同的抑制性细胞因子。一种新的 B 细胞亚群被鉴定为 CD5 Fas 配体 (FasL) 。它们的主要报告作用是抑制抗病毒和抗肿瘤免疫反应,因此被称为“杀伤”B 细胞。在这项研究中,我们旨在评估这些细胞在慢性丙型肝炎病毒 (HCV) 感染中的作用,并确定它们是否导致 HCV 及其相关自身免疫的病毒载量增加和持续存在。(i)与健康个体相比,HCV 感染患者的 CD5 B 细胞上 FasL 的表达显著增加[28·06 ± 6·71 平均荧光强度 (MFI) ± 标准误 (SEM),中位数= 27·9 与 10·87 ± 3·97 MFI ± SEM,中位数= 10·3,分别,P < 0·0001]。(ii)与健康个体相比,来自 HCV 患者的杀伤 B 细胞增加了自身 CD4 T 细胞凋亡[39·17% ± 7·18% 平均值 ± 标准差 (s.d.),中位数= 39·6 与 25·92 ± 8·65%,平均值 ± s.d.,中位数= 24·1%,P < 0·0001,分别]。在 CD8 T 细胞凋亡中观察到类似的增加(54·67 ± 15·49% 平均值 ± s.d.,中位数= 57·3 与 21·07% ± 7·4%,平均值 ± s.d.,中位数= 20%,P = 0·0006,分别)。(iii)通过用单克隆抗 FasL 抗体中和 FasL,我们已经证明杀伤 B 细胞诱导的凋亡是 FasL 依赖性的。(iv)CD5 B 细胞上 FasL 的表达增加与 HCV 中病毒载量增加以及抗核抗体和类风湿因子的存在呈正相关。这是首次提出杀伤 B 细胞在 HCV 中发挥致病作用的研究。它们似乎参与了 HCV 逃避有效免疫反应的能力。

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