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格雷夫斯病患者单核细胞极化和树突状细胞聚集的缺陷。一种与逆转录病毒p15E相关的非特异性免疫调节因子的假定作用。

Defects in monocyte polarization and dendritic cell clustering in patients with Graves' disease. A putative role for a non-specific immunoregulatory factor related to retroviral p15E.

作者信息

Tas M, de Haan-Meulman M, Kabel P J, Drexhage H A

机构信息

Department of Immunology, Erasmus University/Dijkzigt Hospital, Rotterdam, The Netherlands.

出版信息

Clin Endocrinol (Oxf). 1991 Jun;34(6):441-8. doi: 10.1111/j.1365-2265.1991.tb00323.x.

Abstract

A depressed chemotactic responsiveness of monocytes and a depressed cluster capability of dendritic cells have been found in diseases such as chronic purulent infections of the respiratory tract and in various types of malignancies. These impairments in monocyte and dendritic cell function could be ascribed to the action of a low molecular weight factor (LMWF; less than 25 kDa) circulating in the serum of the patients. The factor, which seems to be a non-specific immunoregulatory factor, shares a structural homology with p15E, the capsular protein of murine and feline leukaemogenic retroviruses. In order to study the chemotactic responsiveness of monocytes and the cluster capability of dendritic cells of Graves' patients, monocytes were isolated from the peripheral blood and dendritic cells were prepared from these peripheral blood monocytes by exposure to metrizamide. Monocytes were studied for their chemotactic responsiveness measuring their capability to polarize (morphological changes determined by light microscopy) after stimulation with the chemoattractant fMLP. Dendritic cells were studied for their capability to form clusters with allogeneic lymphocytes. A defective fMLP-induced monocyte polarization was found (16 vs 37% in healthy controls), whereas the dendritic cells showed a defective clustering (60 clusters vs 151 clusters in healthy controls). The effect of fractions of less than 25 kDa prepared from the serum of Graves' patients on healthy donor monocytes and dendritic cells was studied to test the presence of p15E-like factors. The serum fractions had a significant inhibitory effect on monocyte polarization and dendritic cell clustering.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

在诸如呼吸道慢性化脓性感染等疾病以及各类恶性肿瘤中,已发现单核细胞的趋化反应性降低和树突状细胞的聚集能力降低。单核细胞和树突状细胞功能的这些损害可归因于患者血清中循环的一种低分子量因子(LMWF;小于25 kDa)的作用。该因子似乎是一种非特异性免疫调节因子,与鼠类和猫类致白血病逆转录病毒的包膜蛋白p15E具有结构同源性。为了研究格雷夫斯病患者单核细胞的趋化反应性和树突状细胞的聚集能力,从外周血中分离出单核细胞,并通过暴露于甲泛葡胺从这些外周血单核细胞中制备树突状细胞。研究单核细胞在趋化因子fMLP刺激后极化的能力(通过光学显微镜确定形态变化)以评估其趋化反应性。研究树突状细胞与同种异体淋巴细胞形成聚集的能力。发现fMLP诱导的单核细胞极化存在缺陷(健康对照中为37%,而患者中为16%),而树突状细胞显示出聚集缺陷(健康对照中为151个聚集物,而患者中为60个聚集物)。研究了从格雷夫斯病患者血清中制备的小于25 kDa的组分对健康供体单核细胞和树突状细胞的影响,以测试是否存在p15E样因子。血清组分对单核细胞极化和树突状细胞聚集有显著抑制作用。(摘要截短于250字)

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