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系统性红斑狼疮患者初始B细胞区室中活化的抗原接触细胞群体扩大。

Expanded population of activated antigen-engaged cells within the naive B cell compartment of patients with systemic lupus erythematosus.

作者信息

Chang Nan-Hua, McKenzie Tamara, Bonventi Gabriel, Landolt-Marticorena Carolina, Fortin Paul R, Gladman Dafna, Urowitz Murray, Wither Joan E

机构信息

Arthritis Centre of Excellence, Toronto Western Hospital Research Institute, and Department of Medicine, University of Toronto, Ontario, Canada.

出版信息

J Immunol. 2008 Jan 15;180(2):1276-84. doi: 10.4049/jimmunol.180.2.1276.

DOI:10.4049/jimmunol.180.2.1276
PMID:18178868
Abstract

Polyclonal B cell activation is a well-described feature of systemic lupus erythematosus (SLE), but the immune mechanisms leading to this activation are unclear. To gain insight into these processes, we extensively characterized the activated peripheral blood B cell populations in SLE. PBMC from lupus patients and healthy controls were stained with various combinations of conjugated Ab to identify distinct peripheral B cell subsets, and activation was assessed by measurement of forward scatter and CD80 or CD86 expression using flow cytometry. SLE patients had altered proportions of several B cell subsets, many of which demonstrated increased activation as assessed by forward scatter. This activation occurred at an early developmental stage, as B cells in the transitional (T2) stage were already significantly larger than those seen in controls. Increased proportions of CD80- or CD86-expressing cells were also seen in multiple B cell subsets, with the most striking differences observed in the naive CD27-CD23+ population. Within the CD23+ subset, increased costimulatory molecule expression was most pronounced in an IgD+IgMlow population, suggesting that activation follows Ag engagement. Although controls also had IgD+IgMlowCD23+ cells, they were reduced in number and not activated. Thus, there is an altered response to Ig receptor engagement with self-Ags in lupus.

摘要

多克隆B细胞激活是系统性红斑狼疮(SLE)的一个已被充分描述的特征,但导致这种激活的免疫机制尚不清楚。为深入了解这些过程,我们对SLE中活化的外周血B细胞群体进行了广泛的特征分析。用结合抗体的各种组合对狼疮患者和健康对照的外周血单个核细胞(PBMC)进行染色,以鉴定不同的外周B细胞亚群,并通过流式细胞术测量前向散射和CD80或CD86表达来评估激活情况。SLE患者的几个B细胞亚群比例发生改变,其中许多亚群通过前向散射评估显示激活增加。这种激活发生在早期发育阶段,因为过渡(T2)阶段的B细胞已经明显大于对照组中的B细胞。在多个B细胞亚群中也观察到表达CD80或CD86的细胞比例增加,在幼稚CD27-CD23+群体中观察到的差异最为显著。在CD23+亚群中,共刺激分子表达增加在IgD+IgMlow群体中最为明显,表明激活是在抗原结合后发生的。虽然对照组也有IgD+IgMlowCD23+细胞,但它们数量减少且未被激活。因此,狼疮患者对自身抗原的Ig受体结合反应发生了改变。

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