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嗜中性粒细胞的爬行样运动、对固体基质的黏附及化学趋化作用。

Crawling-like movements, adhesion to solid substrata and chemokinesis of neutrophil granulocytes.

作者信息

Keller H U, Zimmermann A, Cottier H

出版信息

J Cell Sci. 1983 Nov;64:89-106. doi: 10.1242/jcs.64.1.89.

Abstract

We analysed the chemokinetic actions of fMet-Leu-Phe (FMLP) and human serum albumin (HSA) on preparations of human neutrophils. Our work focused on the extent to which these agents, individually or in combination, affected locomotion by inducing changes in motile activity and/or the degree of cellular adhesion to the substratum. Because polymorphonuclear leucocyte (PMN) preparations derived from different individuals were found to exhibit broad variations in their basal motility and level of adhesiveness to glass substrata, it became of major interest to clarify mechanisms responsible for the reported variations in neutrophil responses to FMLP. We performed detailed studies on three separate PMN preparations, which differed in terms of their basal motility and adhesiveness. The unequivocal findings that emerged from this study were as follows: (1) HSA did not stimulate or modify motility of cells in suspension. Its orthokinetic effect was exclusively due to its capacity to decrease adhesion to the substratum. It prevented immobilization of motile cells that made contact with the substratum. (2) The orthokinetic effect of FMLP was primarily due to its effects on motility, but there were also secondary effects on spreading and adhesion. The peak chemokinetic activity of FMLP occurred at 10(-8)M, when measured by the two-filter count method and this was correlated with the percentage of polarized neutrophils in suspension. (3) The response to HSA and/or FMLP depended on the basal activity of the cells. If the cells were non-motile and spherical, HSA had no chemokinetic effect. Such an effect was only observed with cells that were initially motile. In contrast, the stimulatory effect of FMLP on motility and locomotion was marked in cases where basal motile activity of the neutrophils was low. If the basal motile activity was high, motility and locomotion could not be stimulated further. Therefore, the chemokinetic effects of HSA and FMLP can be predicted when one knows the basal motile activity of the neutrophils. The variable effect of FMLP on adhesion may also contribute to the regulation of locomotion. These findings help to explain earlier conflicting reports on the chemokinetic effect of FMLP. (4) FMLP can elicit simultaneous changes in motility and adhesiveness, which may have synergistic or antagonistic effects on locomotion. (5) The average speed of the whole neutrophil population is essentially regulated by changes in the proportion of locomoting cells and not, or to a lesser extent, by changes in the speed of the locomoting subset.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

我们分析了甲酰甲硫氨酸-亮氨酸-苯丙氨酸(FMLP)和人血清白蛋白(HSA)对人中性粒细胞制剂的化学动力学作用。我们的工作重点在于这些试剂单独或联合使用时,通过诱导运动活性变化和/或细胞与基质的黏附程度变化来影响运动的程度。由于发现来自不同个体的多形核白细胞(PMN)制剂在其基础运动性和对玻璃基质的黏附水平上表现出广泛差异,因此阐明导致报道的中性粒细胞对FMLP反应差异的机制变得尤为重要。我们对三种基础运动性和黏附性不同的PMN制剂进行了详细研究。这项研究得出的明确结果如下:(1)HSA不会刺激或改变悬浮细胞的运动性。其同向运动效应完全归因于其降低与基质黏附的能力。它能防止与基质接触的运动细胞固定化。(2)FMLP的同向运动效应主要归因于其对运动性的影响,但对铺展和黏附也有次要影响。用双滤器计数法测量时,FMLP的化学动力学活性峰值出现在10^(-8)M,这与悬浮中极化中性粒细胞的百分比相关。(3)对HSA和/或FMLP的反应取决于细胞的基础活性。如果细胞不运动且呈球形,HSA没有化学动力学效应。只有对最初运动的细胞才观察到这种效应。相反,当中性粒细胞的基础运动活性较低时,FMLP对运动性和移动的刺激作用明显。如果基础运动活性较高,则运动性和移动不能进一步被刺激。因此,当知道中性粒细胞的基础运动活性时,就可以预测HSA和FMLP的化学动力学效应。FMLP对黏附的可变效应也可能有助于调节移动。这些发现有助于解释早期关于FMLP化学动力学效应的相互矛盾的报道。(4)FMLP可同时引起运动性和黏附性的变化,这可能对移动产生协同或拮抗作用。(5)整个中性粒细胞群体的平均速度基本上由移动细胞比例的变化调节,而不是由移动亚群速度的变化调节,或者在较小程度上受其调节。(摘要截选至250字)

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