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HIV gp120对人类和无脊椎动物免疫细胞中DAMA和白细胞介素-1α诱导的趋化反应的改变。

HIV gp120 alteration of DAMA and IL-1 alpha induced chemotaxic responses in human and invertebrate immunocytes.

作者信息

Stefano G B, Smith E M, Cadet P, Hughes T K

机构信息

Old Westbury Neuroscience Institute, State University of New York 11568.

出版信息

J Neuroimmunol. 1993 Mar;43(1-2):177-84. doi: 10.1016/0165-5728(93)90089-h.

Abstract

The effects of a synthetic peptide fragment of human immunodeficiency virus gp120 (HIV gp120) on opioid (D-ala2-D-met5 enkephalinamide; DAMA) and interleukin-1 (IL-1) induced chemotactic responses in human granulocytes and monocytes and invertebrate (Mytilus edulis) immunocytes were studied. Both DAMA and IL-1 increased the velocity of cell migration from both species and the response is chemotactic (e.g. directed). Non-treated control cells move randomly or not at all. The addition of gp120 to DAMA or IL-1 treated human granulocytes or monocytes results in a slower movement which is chemokinetic (loss of directionality or random) in nature. A similar phenomenon occurs in the invertebrate immunocytes. If gp120 alone is added, it inhibits the movement of spontaneously active human granulocytes and Mytilus edulis immunocytes. In contrast, it stimulates chemokinesis of spontaneously active human monocytes. These responses occur immediately after addition of the peptide. Based on experiments with the selective calcium channel antagonist nimodipine, it appears that the gp120 causes its effects by irreversible binding to a calcium channel. Our results suggest a universal inhibitory mechanism is occurring since the invertebrate immunocytes must recognize HIV gp120 peptide to result in this effect, possibly through a CD4 or other type of surface determinant.

摘要

研究了人类免疫缺陷病毒gp120(HIV gp120)的合成肽片段对阿片样物质(D-丙氨酸2-D-蛋氨酸5脑啡肽酰胺;DAMA)和白细胞介素-1(IL-1)诱导的人类粒细胞、单核细胞以及无脊椎动物(紫贻贝)免疫细胞趋化反应的影响。DAMA和IL-1均提高了这两种细胞的迁移速度,且该反应具有趋化性(即有方向性)。未经处理的对照细胞随机移动或根本不移动。向经DAMA或IL-1处理的人类粒细胞或单核细胞中添加gp120会导致移动速度减慢,这种移动在本质上是化学动力学的(方向性丧失或随机)。在无脊椎动物免疫细胞中也会出现类似现象。如果单独添加gp120,它会抑制自发活跃的人类粒细胞和紫贻贝免疫细胞的移动。相反,它会刺激自发活跃的人类单核细胞的化学运动。添加该肽后这些反应立即发生。基于使用选择性钙通道拮抗剂尼莫地平的实验,似乎gp120通过与钙通道不可逆结合来产生其效应。我们的结果表明存在一种普遍的抑制机制,因为无脊椎动物免疫细胞必须识别HIV gp120肽才能产生这种效应,可能是通过CD4或其他类型的表面决定簇。

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