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Memory and naïve B-cell subsets in patients with multiple sclerosis

机译:多发性硬化症患者的记忆和幼稚B细胞亚群

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摘要

Memory and naïve B cells are considered to play distinct roles in immune regulation. However, the roles of memory and naïve B-cell subsets in multiple sclerosis (MS) have not yet been elucidated. In this study, we examined whether memory and naïve B-cell subsets differ between patients with MS and healthy subjects and whether interferon beta (IFNβ)-1b can affect these subsets in patients with MS. We also studied these subsets in relapsing and remitting stages of MS. Subjects included 31 patients with relapsing-remitting MS in the remitting stage, of which 15 were treated with IFNβ-1b and 16 were not treated, and 22 healthy control subjects. For 11 of the 16 untreated patients, blood samples were also obtained in the relapsing stage. Expression of CD5, CD80, CD86, CCR5, CXCR3, CD11a, and CD49d in memory and naïve B cells in blood samples was examined by flow cytometry. The percentages of CD86+ cells and CCR5+ cells in the naïve B-cell subset were significantly higher in untreated patients than in control subjects or IFNβ-treated patients. In patients with MS, the percentages of CD86+ cells and CCR5+ cells in the naïve B-cell subset and the percentage of CD5+ cells in the memory B-cell subset were significantly greater in the remitting stage than in the relapsing stage. These results indicate that memory and naïve B-cell subsets, especially CD86+ naïve B cells, CCR5+ naïve B cells, and CD5+ memory B cells, might be useful in the study of the pathogenesis of and therapy for MS.
机译:记忆和幼稚B细胞被认为在免疫调节中起着不同的作用。然而,尚未阐明记忆和幼稚B细胞亚群在多发性硬化症(MS)中的作用。在这项研究中,我们检查了MS患者与健康受试者之间的记忆和单纯B细胞亚群是否存在差异,以及干扰素β(IFNβ)-1b是否会影响MS患者的这些亚群。我们还研究了MS复发和缓解阶段的这些子集。受试者包括31例处于缓解期的复发缓解型MS患者,其中15例接受IFNβ-1b治疗,16例未接受治疗,以及22例健康对照组。在16名未接受治疗的患者中,有11名在复发阶段也获得了血液样本。通过流式细胞术检查血液样品中记忆和幼稚B细胞中CD5,CD80,CD86,CCR5,CXCR3,CD11a和CD49d的表达。未经治疗的患者中,未经治疗的B细胞亚群中CD86 +细胞和CCR5 +细胞的百分比显着高于对照组或接受IFNβ治疗的患者。在MS患者中,幼稚B细胞亚群中CD86 +细胞和CCR5 +细胞的百分比以及记忆B细胞亚群中CD5 +细胞的百分比在复发阶段显着高于复发阶段。这些结果表明记忆和幼稚的B细胞亚群,尤其是CD86 +幼稚的B细胞,CCR5 +幼稚的B细胞和CD5 +记忆性B细胞,可能在研究MS的发病机理和治疗中有用。

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