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炎症性关节炎中外周血和滑液单核细胞的激活。I. 单核细胞分化抗原和II类抗原的细胞荧光研究及其受γ-干扰素的调节

Peripheral blood and synovial fluid monocyte activation in inflammatory arthritis. I. A cytofluorographic study of monocyte differentiation antigens and class II antigens and their regulation by gamma-interferon.

作者信息

Firestein G S, Zvaifler N J

出版信息

Arthritis Rheum. 1987 Aug;30(8):857-63. doi: 10.1002/art.1780300803.

Abstract

Recent study of the expression of monocyte differentiation antigens (MAg) and HLA-DR on peripheral blood monocytes (PBM) has led to the recognition of resting and activated monocyte phenotypes. The former is identified by the expression of large amounts of MAg (i.e., Mo2 and 63D3) and small amounts of HLA-DR, while the latter is identified by the reverse. We studied the phenotypes of PBM and synovial fluid monocytes (SFM) of patients with chronic inflammatory arthritis and found that PBM were primarily resting and SFM were usually activated. In addition, we measured the degree of modulation of MAg and HLA-DR by gamma-interferon (gamma-IFN). Patient PBM reacted the same as PBM from normal individuals (i.e., MAg decreased and HLA-DR increased after exposure to gamma-IFN). However, in patient SFM, HLA-DR did not increase with exposure to gamma-IFN because expression was already maximal. Interestingly, MAg could still be down-regulated on gamma-IFN-treated SFM, even when expression began at a very low level (i.e., activated phenotype). This independent regulation of MAg and HLA-DR suggests that macrophage activating factors other than gamma-IFN may be responsible, in part, for the activated phenotypes observed.

摘要

近期对外周血单核细胞(PBM)上单核细胞分化抗原(MAg)和HLA - DR表达的研究,使人们认识到静息和活化单核细胞表型。前者通过大量MAg(即Mo2和63D3)的表达和少量HLA - DR来识别,而后者则相反。我们研究了慢性炎症性关节炎患者的PBM和滑液单核细胞(SFM)的表型,发现PBM主要是静息的,而SFM通常是活化的。此外,我们测定了γ干扰素(γ - IFN)对MAg和HLA - DR的调节程度。患者的PBM与正常个体的PBM反应相同(即暴露于γ - IFN后MAg减少,HLA - DR增加)。然而,在患者的SFM中,暴露于γ - IFN后HLA - DR并未增加,因为其表达已经处于最大值。有趣的是,即使MAg的表达开始时水平很低(即活化表型),γ - IFN处理后的SFM上的MAg仍可被下调。MAg和HLA - DR的这种独立调节表明,除γ - IFN外的其他巨噬细胞活化因子可能部分地导致了所观察到的活化表型。

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