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人类中性粒细胞分泌、趋化因子受体动员与功能增强能力的相关性

Correlation of human neutrophil secretion, chemoattractant receptor mobilization, and enhanced functional capacity.

作者信息

Fletcher M P, Seligmann B E, Gallin J I

出版信息

J Immunol. 1982 Feb;128(2):941-8.

PMID:6274963
Abstract

Studies were performed to elucidate further the phenomenon of secretagogue-mediated enhancement in the binding of the chemoattractant f-met-leu-[3H]phe to human neutrophils (PMN). Specific f-met-leu-[3H]phe binding to unstimulated PMN reached maximum levels after 10 to 15 min of incubation at 0 degrees C with a saturating concentration of peptide, and consisted of a readily displaceable and a nondisplaceable component. PMN, preexposed to A23187 (2.5 X 10(-8) M) or PMA (0.5 ng/ml) for 30 min at 37 degrees C to stimulate limited and preferential release of specific (secondary) granules (10 to 20% of total lysozyme, no beta-glucuronidase), demonstrated an approximate doubling in the displaceable component of f-met-leu-["3H]phe binding, accompanied by an increasing nondisplaceable component that could not be explained by bulk pinocytosis of extracellular fluid (assessed by [3H]sucrose uptake). The increase in f-met-leu-[3H]phe binding was not affected by inhibitors of protein synthesis, could not be attributed to the secreted products lysosyme or lactoferrin acting on the cell, and, on the basis of studies with PMN from patients with chronic granulomatous disease, could not be attributed to the effects of reactive oxygen species generated in low concentration during stimulation. Functional studies on PMN indicated that preexposure to secretagogues at concentrations demonstrated to increase receptor availability also enhanced subsequent f-met-leu-phe-mediated superoxide and hydrogen peroxide generation. The present data demonstrate that secretagogues may activate PMN to enhance their subsequent responses in f-met-leu-phe-mediated processes, and, combined with previous reports, support the concept that specific granules provide a source of preformed membrane and receptor material that is translocated to the cell surface during the secretion associated with directed locomotion.

摘要

开展了多项研究以进一步阐明促分泌剂介导的趋化因子f-甲硫-亮-苯丙氨酸(f-met-leu-[³H]phe)与人类中性粒细胞(PMN)结合增强的现象。在0℃下用饱和浓度的肽孵育10至15分钟后,未刺激的PMN对f-甲硫-亮-苯丙氨酸(f-met-leu-[³H]phe)的特异性结合达到最大水平,且由一个易于置换的成分和一个不可置换的成分组成。将PMN在37℃下预先暴露于A23187(2.5×10⁻⁸M)或佛波酯(PMA,0.5 ng/ml)30分钟,以刺激特异性(次级)颗粒有限且优先释放(占总溶菌酶的10%至20%,无β-葡萄糖醛酸酶),结果显示f-甲硫-亮-苯丙氨酸(f-met-leu-[³H]phe)结合的可置换成分大约增加了一倍,同时不可置换成分也在增加,而这无法用细胞外液的大量胞饮作用来解释(通过[³H]蔗糖摄取评估)。f-甲硫-亮-苯丙氨酸(f-met-leu-[³H]phe)结合的增加不受蛋白质合成抑制剂的影响,不能归因于分泌产物溶菌酶或乳铁蛋白对细胞的作用,并且根据对慢性肉芽肿病患者的PMN研究,也不能归因于刺激过程中低浓度产生的活性氧物质的影响。对PMN的功能研究表明,预先暴露于已证明可增加受体可用性的浓度的促分泌剂,也会增强随后f-甲硫-亮-苯丙氨酸介导的超氧化物和过氧化氢的产生。目前的数据表明,促分泌剂可能激活PMN,以增强其在f-甲硫-亮-苯丙氨酸介导的过程中的后续反应,并且与先前的报道相结合,支持了这样一种概念,即特异性颗粒提供了一种预先形成的膜和受体物质的来源,在与定向运动相关的分泌过程中转移到细胞表面。

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