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糖皮质激素对牛中性粒细胞上L-选择素和CD18的调节作用:皮质醇和地塞米松的影响

Regulation of L-selectin and CD18 on bovine neutrophils by glucocorticoids: effects of cortisol and dexamethasone.

作者信息

Burton J L, Kehrli M E, Kapil S, Horst R L

机构信息

Metabolic Diseases and Immunology Research Unit, National Animal Disease Center-Agricultural Research Service-United States Department of Agriculture, Ames, Iowa 50010-0070.

出版信息

J Leukoc Biol. 1995 Feb;57(2):317-25. doi: 10.1002/jlb.57.2.317.

Abstract

The responsiveness of bovine neutrophil L-selectin and CD18 to in vivo glucocorticoid administration was characterized by flow cytometric analysis. Blood was sampled intensively from dairy cows treated for 3 days with placebo, cortisol, or dexamethasone. Immunostaining was performed on whole blood (100 microliters) that was left unstimulated or was stimulated with platelet-activating factor (PAF; 1 microgram/ml blood) prior to incubation with fluorescein isothiocyanate-conjugated monoclonal antibodies against L-selectin and CD18. Results were expressed as the percentage of positive-staining cells and as mean fluorescence intensity (MFI) of those cells. Total leukocyte count and leukocyte differentials were also performed on all blood samples. Dexamethasone caused nearly complete down-regulation of L-selectin (P < .01) on the surface of gated cells and reduced to half the MFI of CD18 (P < .01). Compared with values for the placebo group, dexamethasone began to cause L-selectin down-regulation within 8 h after the first injection and these effects persisted until 48 h after the third injection. This was correlated in time with an acute reduction in the proportion of cells that stained positive for L-selectin (from 98% before dexamethasone injections to a low of 17% by 40 h after the first injection). Dexamethasone also caused leukocytosis and neutrophilia during this time interval. In contrast, CD18 down-regulation was delayed until 16 h after the second dexamethasone injection and persisted for roughly 8 days. However, at no time during the experiment did dexamethasone influence the proportion of gated cells staining positive for CD18 (always 100%). Effects of cortisol were generally similar in pattern to those of dexamethasone but were more subtle and more readily detected when PAF was added to blood prior to immunostaining. These results strongly suggest that one mechanism of the anti-inflammatory action of glucocorticoids is to induce dramatic down-regulation of L-selectin and CD18 adhesion molecules on blood neutrophils.

摘要

通过流式细胞术分析,对牛中性粒细胞L-选择素和CD18对体内给予糖皮质激素的反应性进行了表征。从用安慰剂、皮质醇或地塞米松处理3天的奶牛中密集采集血液。在用异硫氰酸荧光素偶联的抗L-选择素和CD18单克隆抗体孵育之前,对未刺激或用血小板活化因子(PAF;1微克/毫升血液)刺激的全血(100微升)进行免疫染色。结果以阳性染色细胞的百分比和这些细胞的平均荧光强度(MFI)表示。还对所有血样进行了白细胞总数和白细胞分类计数。地塞米松导致门控细胞表面的L-选择素几乎完全下调(P < 0.01),并使CD18的MFI降低至一半(P < 0.01)。与安慰剂组的值相比,地塞米松在首次注射后8小时内开始导致L-选择素下调,这些作用持续到第三次注射后48小时。这在时间上与L-选择素染色阳性细胞比例的急剧下降相关(从地塞米松注射前的98%降至首次注射后40小时的低至17%)。在此时间间隔内,地塞米松还导致白细胞增多和中性粒细胞增多。相比之下,CD18下调延迟至第二次地塞米松注射后16小时,并持续约8天。然而,在实验期间的任何时候,地塞米松都没有影响门控细胞中CD18染色阳性的比例(始终为100%)。皮质醇的作用模式通常与地塞米松相似,但在免疫染色前向血液中添加PAF时更微妙且更容易检测到。这些结果强烈表明,糖皮质激素抗炎作用的一种机制是诱导血液中性粒细胞上的L-选择素和CD18粘附分子显著下调。

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