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抑郁症期间全身免疫激活的证据:流式细胞术结合单克隆抗体染色进行白细胞计数的结果。

Evidence for a systemic immune activation during depression: results of leukocyte enumeration by flow cytometry in conjunction with monoclonal antibody staining.

作者信息

Maes M, Lambrechts J, Bosmans E, Jacobs J, Suy E, Vandervorst C, de Jonckheere C, Minner B, Raus J

机构信息

Psychiatric Centre, Munsterbilzen, Belgium.

出版信息

Psychol Med. 1992 Feb;22(1):45-53. doi: 10.1017/s0033291700032712.

DOI:10.1017/s0033291700032712
PMID:1574566
Abstract

Several studies have reported a suppressed immune function (e.g. blast transformation) during depression. In an attempt to define the cellular basis of the reported immune disorders, the present study investigates the leukocyte cell subset profile of minor, simple major, and melancholic depressives, versus normal controls. We have counted the number of white blood cells (WBC) lymphocytes, monocytes, and granulocytes, while the number of lymphocyte (sub)populations has been identified by phenotype, using monoclonal antibody staining in conjunction with flow cytometry. The following cell surface antigens were determined: CD3+ (pan T), CD19+ (pan B), CD4+ (T helper/inducer), CD8+ (T suppressor/cytotoxic), CD4+CD45RA (T-memory cells), CD4+CD45RA+ (T-virgin cells), surface Ig, class II MHC HLA-DR, and CD25+ (IL-2 receptor). By means of pattern recognition methods, we established distinct immunological changes in minor and simple major depressed and in melancholic patients, setting them apart from the reference population. Depression, per se, is characterized by a higher number of WBC, monocytes, class II MHC HLA-DR, and memory T cells. Minor and simple major depressives exhibited an increased T helper/suppressor ratio. Increased numbers of IL-2 receptor bearing cells are a hallmark for major depression. Melancholics showed an increased number of pan T, pan B and T suppressor/cytotoxic cells. It was concluded that the established immune cell profile of depressed patients may point towards the existence of a systemic immune activation during that illness.

摘要

多项研究报告称,抑郁症患者存在免疫功能受抑制(如细胞增殖)的情况。为了确定所报道免疫紊乱的细胞基础,本研究调查了轻度、单纯重度和抑郁性抑郁症患者与正常对照组的白细胞亚群分布情况。我们对白细胞(WBC)、淋巴细胞、单核细胞和粒细胞进行了计数,同时通过单克隆抗体染色结合流式细胞术,根据表型确定淋巴细胞(亚)群的数量。测定了以下细胞表面抗原:CD3 +(全T细胞)、CD19 +(全B细胞)、CD4 +(辅助性/诱导性T细胞)、CD8 +(抑制性/细胞毒性T细胞)、CD4 + CD45RA(记忆性T细胞)、CD4 + CD45RA +(初始T细胞)、表面免疫球蛋白、II类主要组织相容性复合体HLA - DR以及CD25 +(白细胞介素 - 2受体)。通过模式识别方法,我们在轻度和单纯重度抑郁症患者以及抑郁性患者中发现了明显的免疫学变化,将他们与参照人群区分开来。抑郁症本身的特征是白细胞、单核细胞、II类主要组织相容性复合体HLA - DR和记忆性T细胞数量增加。轻度和单纯重度抑郁症患者的辅助性T细胞/抑制性T细胞比例升高。携带白细胞介素 - 2受体的细胞数量增加是重度抑郁症的一个标志。抑郁性患者的全T细胞、全B细胞以及抑制性/细胞毒性T细胞数量增加。研究得出结论,抑郁症患者已确定的免疫细胞分布情况可能表明该疾病期间存在全身性免疫激活。

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