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甲酰肽刺激并使ATPγS增强人中性粒细胞中[3H]胞苷5'-二磷酸甘油酯的积累。

Formyl peptide stimulates and ATP gamma S potentiates [3H]cytidine 5'-diphosphate diglyceride accumulation in human neutrophils.

作者信息

Stubbs E B, Walker B A, Owens C A, Ward P A, Agranoff B W

机构信息

Department of Biological Chemistry, University of Michigan, Ann Arbor 48104-1687.

出版信息

J Immunol. 1992 Apr 1;148(7):2242-7.

PMID:1545129
Abstract

Although it is evident that the chemotactic peptide FMLP activates O2-formation in neutrophils via the phosphoinositidase-mediated second messenger system, it is less clear how endogenous priming agents such as ATP and platelet activating factor potentiate FMLP action. In our study, we have examined the possible effects of the stable ATP analog adenosine 5'-O-[3-thiotriphosphate] (ATP gamma S) on cellular levels of inositol 1,4,5-trisphosphate, [Ca2+]i and diglyceride (DG), in resting and in FMLP-stimulated neutrophils. Although all three measures were increased in the presence of FMLP, only the increase in DG was enhanced by pretreatment (priming) with ATP gamma S. We also measured the accumulation of the phosphoinositide cycle intermediate cytidine 5'-diphosphate (CDP)-DG to assess possible effects of priming on phosphoinositide resynthesis. The addition of FMLP to [3H]cytidine-prelabeled neutrophils elicited an increase in the accumulation of [3H]CDP-DG that was maximally enhanced in cells that were pretreated with cytochalasin B. The stimulated accumulation of [3H]CDP-DG was completely reversed by the addition of myo-inositol. Treatment of [3H]cytidine-prelabeled neutrophils with ATP gamma S (10-100 microM) resulted in a dose-dependent synergistic increase in FMLP-stimulated [3H]CDP-DG accumulation, whereas ATP gamma S alone had no effect. The observed increases in DG and in [3H]CDP-DG, in contrast to inositol 1,4,5-trisphosphate and [Ca2+]i responses, correlates well with the ATP gamma S-priming of FMLP-induced O2-formation. A similar potentiation of FMLP-induced stimulation of CDP-DG formation was also observed with platelet-activating factor. It is proposed that the priming of FMLP responses in neutrophils proceeds via a mechanism that selectively enhances DG production through a mechanism that is independent of FMLP-induced breakdown of phosphatidylinositol bisphosphate.

摘要

虽然很明显趋化肽FMLP通过磷酸肌醇酶介导的第二信使系统激活中性粒细胞中O2的形成,但内源性启动剂如ATP和血小板活化因子如何增强FMLP的作用尚不清楚。在我们的研究中,我们检测了稳定的ATP类似物腺苷5'-O-3-硫代三磷酸对静息和FMLP刺激的中性粒细胞中肌醇1,4,5-三磷酸、[Ca2+]i和二酰甘油(DG)细胞水平的可能影响。虽然在FMLP存在下所有这三种指标都增加了,但只有DG的增加通过用ATPγS预处理(启动)而增强。我们还测量了磷酸肌醇循环中间体胞苷5'-二磷酸(CDP)-DG的积累,以评估启动对磷酸肌醇再合成的可能影响。向用[3H]胞苷预标记的中性粒细胞中添加FMLP会引起[3H]CDP-DG积累的增加,在用细胞松弛素B预处理的细胞中这种增加最大。添加肌醇可完全逆转刺激的[3H]CDP-DG积累。用ATPγS(10-100μM)处理[3H]胞苷预标记的中性粒细胞导致FMLP刺激的[3H]CDP-DG积累呈剂量依赖性协同增加,而单独的ATPγS没有作用。与肌醇1,4,5-三磷酸和[Ca2+]i反应相反,观察到的DG和[3H]CDP-DG的增加与FMLP诱导的O2形成的ATPγS启动密切相关。用血小板活化因子也观察到FMLP诱导的CDP-DG形成刺激的类似增强。有人提出,中性粒细胞中FMLP反应的启动是通过一种机制进行的,该机制通过一种独立于FMLP诱导的磷脂酰肌醇二磷酸分解的机制选择性地增强DG的产生

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