Neidhart M, Pataki F, Schönbächler J, Brühlmann P
Department of Rheumatology, University Hospital, Zürich, Switzerland.
Rheumatol Int. 1996;16(2):77-87. doi: 10.1007/BF01816439.
The aim of this study was to quantify and characterize the CD4+ and CD8+, CD45RA+, CD45RO- T-lymphocytes that paradoxically expressed the CD29 bright+ phenotype in health and in rheumatoid arthritis. We further evaluated their clinical implications. Blood samples were obtained from 100 patients with rheumatoid arthritis and 40 age- and sex-matched controls. Cell surface antigens and interleukin-2 (IL-2) binding were detected on CD4+ and CD8+ peripheral blood T-lymphocytes (T-PBL) by three-colour flow cytometry. One-third of the patients were clinically evaluated at the time of blood sampling. In healthy donors, we found 16 +/- 14% of CD29 bright+ cells among CD4+, CD45RA+, RO- T-PBL. These "false naive" CD4+ T-PBL were Leu-8+, and a majority expressed the CD25/p55 receptor (IL-2R alpha chain), while a minority showed the CD11a bright+, CD69+ and/or CD122/p75+ (IL-2R beta chain) phenotype, and few cells were CD31 bright+ and HLA-DR+. In rheumatoid arthritis, their proportion among CD4+, CD45RA+, RO- cells increased to 25 +/- 15% (P < 0.001, compared with controls). In patients, the reductions in CD31 and CD38 expression (P < 0.05 for both), as well as the enhanced CD25 expression (P < 0.001) on CD4+, CD45RA+, RO- T-PBL reflected a more differentiated phenotype. The occurrences of CD25 and CD122 were increased on false naive CD4+ T-PBL (0.01 < P < 0.001); however, the binding of IL-2 remained very low (in contrast to the binding of IL-2 on CD45RO+ T-PBL). Furthermore, a major subset of CD8+, CD45RA+, RO- T-PBL (45 +/- 17% in controls) expressed the CD29 bright+ phenotype. These "false naive" CD8+ T-PBL included a great many of CD11b+, CD28- cells, while a minority showed the HLA-DR+, CD69+ and/or CD122+ phenotypes. Patients with low levels of IgM rheumatoid factors (IgM-RF; but with active disease) had an elevated proportion of CD45RA+, RO- cells among the CD8+ T-PBL, in part due to an increased proportion of false naive cells (P < 0.05). In patients, the false naive CD8+ T-PBL showed down-regulated CD11b and an increased expression of IL-2 receptor chains (CD25 and CD122; 0.05 < P < 0.01), but without a significant increase in IL-2 binding. More CD69 on false naive CD8+ T-PBL was found in patients with high levels of IgM-RF (P < 0.005 compared to patients with low IgM-RF). Finally, both false naive CD4+ and CD8+ T-PBL correlated with the clinical process and outcome variables (0.05 < P < 0.01). The levels of activated false naive (CD4+ T-PBL (CD25+ and/or CD122+) or CD8+ T-PBL (CD69+ and/or CD122+) were associated with clinical parameters of disease activity (0.05 < P < 0.01). Thus, in rheumatoid arthritis, false naive T-PBL showed important qualitative differences. The levels of activated false naive T-PBL could be particularly interesting for monitoring disease evolution.
本研究的目的是对健康人群和类风湿关节炎患者中反常表达CD29高表达+表型的CD4+和CD8+、CD45RA+、CD45RO- T淋巴细胞进行定量和特征分析。我们进一步评估了它们的临床意义。从100例类风湿关节炎患者和40例年龄及性别匹配的对照者中采集血样。通过三色流式细胞术检测CD4+和CD8+外周血T淋巴细胞(T-PBL)上的细胞表面抗原和白细胞介素-2(IL-2)结合情况。三分之一的患者在采血时进行了临床评估。在健康供者中,我们在CD4+、CD45RA+、RO- T-PBL中发现16±14%的CD29高表达+细胞。这些“假幼稚”CD4+ T-PBL为Leu-8+,大多数表达CD25/p55受体(IL-2Rα链),而少数表现为CD11a高表达+、CD69+和/或CD122/p75+(IL-2Rβ链)表型,很少细胞为CD31高表达+和HLA-DR+。在类风湿关节炎患者中,它们在CD4+、CD45RA+、RO-细胞中的比例增加到25±15%(与对照组相比,P<0.001)。在患者中,CD4+、CD45RA+ RO- T-PBL上CD31和CD38表达的降低(两者均P<0.05)以及CD25表达的增强(P<0.001)反映了一种更分化的表型。“假幼稚”CD4+ T-PBL上CD25和CD122的出现增加(0.01<P<0.001);然而,IL-2的结合仍然非常低(与CD45RO+ T-PBL上IL-2的结合情况相反)。此外,CD8+、CD45RA+、RO- T-PBL的一个主要亚群(对照组中为45±17%)表达CD29高表达+表型。这些“假幼稚”CD8+ T-PBL包括许多CD11b+、CD28-细胞,而少数表现为HLA-DR+、CD69+和/或CD122+表型。IgM类风湿因子(IgM-RF)水平低(但疾病活动)的患者,CD8+ T-PBL中CD4!RA+、RO-细胞的比例升高,部分原因是假幼稚细胞的比例增加(P<0.05)。在患者中,“假幼稚”CD8+ T-PBL显示CD11b下调,IL-2受体链(CD25和CD122)表达增加(0.05<P<0.01),但IL-2结合无显著增加。在IgM-RF水平高的患者中,“假幼稚”CD8+ T-PBL上发现更多的CD69(与IgM-RF水平低的患者相比,P<0.005)。最后,“假幼稚”CD4+和CD8+ T-PBL均与临床过程和结局变量相关(0.05<P<0.01)。活化的“假幼稚”(CD4+ T-PBL(CD25+和/或CD122+)或CD8+ T-PBL(CD69+和/或CD122+)水平与疾病活动的临床参数相关(0.05<P<0.01)。因此,在类风湿关节炎中,“假幼稚”T-PBL表现出重要的质的差异。活化的“假幼稚”T-PBL水平对于监测疾病进展可能特别有意义。
