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人类中性粒细胞的运动性和黏附性。趋化因子诱导的黏附位点的重新分布。

Motility and adhesiveness in human neutrophils. Redistribution of chemotactic factor-induced adhesion sites.

作者信息

Smith C W, Hollers J C

出版信息

J Clin Invest. 1980 Apr;65(4):804-12. doi: 10.1172/JCI109731.

Abstract

Human peripheral blood neutrophils obtained from healthy adults were examined in vitro. We assessed the effects of sequential stepwise increases in the concentration of the chemotactic dipeptide N-formyl-l-methionyl-l-phenylalanine (f-Met-Phe) on neutrophil attachment to serum-coated glass, detachment from serum-coated glass and the distribution on the cell surface of binding sites for albumin-coated latex beads. The initial exposure to f-Met-Phe resulted in increased adhesiveness and binding of latex beads in a random pattern over the cell surface. The second exposure to f-Met-Phe resulted in decreased adherence, detachment of neutrophils from serum-coated glass, and movement of binding sites for latex beads to the uropod. Enhanced adhesiveness and redistribution of binding sites were blocked by 0.1 mM N-alpha-p-tosyl-l-lysine chloromethyl ketone, a concentration that did not reduce the change in cellular shape caused by f-Met-Phe. Cytochalasin B (5 mug/ml) blocked the redistribution of binding sites as well as the change in shape. The third exposure to f-Met-Phe was given along with the latex beads. The stimulus was stopped after 2 min by fixing cells in suspension with glutaraldehyde. If the third exposure was at a concentration higher than the second, the beads were bound in the region of the lamellipodia in 70% of the cells. If lower, binding to the lamellipodia was found in a significantly smaller proportion of cells (13%). The results support the concept that neutrophils develop a polarized distribution of f-Met-Phe-induced adhesion sites in response to increasing concentrations of f-Met-Phe, and these sites flow from the region of the lamellipodia to the uropod.

摘要

对从健康成年人获取的人外周血中性粒细胞进行了体外研究。我们评估了趋化二肽N-甲酰-L-蛋氨酰-L-苯丙氨酸(f-Met-Phe)浓度的逐步递增对中性粒细胞黏附于血清包被玻璃、从血清包被玻璃上脱离以及白蛋白包被乳胶珠结合位点在细胞表面分布的影响。首次暴露于f-Met-Phe导致细胞黏附性增加以及乳胶珠在细胞表面随机结合。第二次暴露于f-Met-Phe导致黏附性降低、中性粒细胞从血清包被玻璃上脱离,以及乳胶珠结合位点向尾足移动。0.1 mM N-α-对甲苯磺酰-L-赖氨酸氯甲基酮可阻断黏附性增强和结合位点的重新分布,该浓度不会降低f-Met-Phe引起的细胞形态变化。细胞松弛素B(5 μg/ml)可阻断结合位点的重新分布以及形态变化。第三次暴露于f-Met-Phe与乳胶珠同时进行。2分钟后通过用戊二醛固定悬浮细胞来终止刺激。如果第三次暴露的浓度高于第二次,70%的细胞中珠子结合在片状伪足区域。如果浓度较低,在显著较少比例的细胞(13%)中发现珠子与片状伪足结合。这些结果支持了中性粒细胞在f-Met-Phe浓度增加时会形成f-Met-Phe诱导的黏附位点极化分布的概念,并且这些位点从片状伪足区域流向尾足。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cde4/434466/cdb065e652d5/jcinvest00688-0032-a.jpg

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