首页> 外文期刊>Annals of the Rheumatic Diseases: A Journal of Clinical Rheumatology and Connective Tissue Research >B-cell-activating factor receptor expression on naive and memory B cells: relationship with relapse in patients with rheumatoid arthritis following B-cell depletion therapy.
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B-cell-activating factor receptor expression on naive and memory B cells: relationship with relapse in patients with rheumatoid arthritis following B-cell depletion therapy.

机译:幼稚和记忆B细胞上的B细胞活化因子受体表达:类风湿关节炎患者B细胞耗竭治疗后与复发的关系。

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OBJECTIVES: To examine the expression of B-cell-activating factor receptor (BAFF-R) on naive CD27- and memory CD27+ B cells in normal individuals and patients with rheumatoid arthritis (RA) undergoing B-cell depletion therapy with rituximab. Patients and METHODS: BAFF-R expression on B-cell subsets was determined in normal controls (NC; n = 11), active patients with RA pre-rituximab (pre-RX; n = 15), relapsing patients either concordant for B-cell repopulation (C-R, n = 13) or discordant, with relapse more than 3 months after repopulation (D-R, n = 11) and patients in remission over 3 months postrepopulation (discordant non-relapsing (D-NR), n = 5). Serum BAFF was measured by ELISA and analysed using Mann-Whitney. RESULTS: There was no significant difference between NC, pre-RX and D-NR patients in %BAFF-R-positive B cells or mean fluorescence intensity (MFI) in naive and memory B cells. Relapsing patients had significantly lower MFI and %BAFF-R-positive cells in both naive and memory compartments from NC and pre-RX (C-R and D-R; p < 0.01). BAFF levels in pre-RX patients were within the normal range and did not correlate with BAFF-R expression in any patient group. D-NR patients had relatively lower proportions of pre and postswitch CD27+ B cells than pre-RX patients (D-NR vs pre-RX; p < 0.05 for both) and also lower numbers of postswitch B cells than D-R patients (D-NR vs D-R, p < 0.05). CONCLUSION: BAFF-R expression was significantly reduced on both naive and memory B cells in patients at relapse, regardless of the relationship with B-cell repopulation or serum BAFF levels. Re-establishment of active disease was also associated with an increase in class-switch recombination. Factors responsible for lower levels of BAFF-R may relate to altered thresholds for autoreactive B-cell generation at relapse in patients with RA.
机译:目的:研究在正常个体和接受利妥昔单抗B细胞治疗的类风湿关节炎(RA)患者中,B细胞活化因子受体(BAFF-R)在幼稚CD27-和记忆CD27 + B细胞上的表达。患者与方法:在正常对照组(NC; n = 11),活动期RA前利妥昔单抗(RX前; n = 15),复发或与B-concord相符的患者中确定了BFF亚群上的BAFF-R表达细胞增生(CR,n = 13)或不一致,在增生后3个月内复发(DR,n = 11),且在增生后3个月内缓解的患者(不一致的非复发性(D-NR),n = 5) 。通过ELISA测量血清BAFF,并使用Mann-Whitney进行分析。结果:%BAFF-R阳性B细胞的NC,RX前和D-NR患者之间无显着差异,而幼稚和记忆B细胞的平均荧光强度(MFI)无明显差异。复发患者在NC和RX之前的幼稚和记忆区室中MFI和%BAFF-R阳性细胞均显着降低(C-R和D-R; p <0.01)。 RX前患者的BAFF水平在正常范围内,与任何患者组中的BAFF-R表达均不相关。 D-NR患者转换前和转换后CD27 + B细胞的比例相对于RX前患者相对较低(D-NR与RX-pre;两者均p <0.05),并且转换后B细胞的数量也低于DR患者(D-NR相对于DR,p <0.05)。结论:复发患者的幼稚和记忆B细胞中BAFF-R的表达均显着降低,无论与B细胞再填充或血清BAFF水平的关系如何。活动性疾病的重建也与类别转换重组的增加有关。导致BAFF-R水平降低的因素可能与RA患者复发时自身反应性B细胞生成的阈值改变有关。

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