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白细胞介素-8的受体介导内吞作用:荧光显微镜证据及该过程在人中性粒细胞配体诱导生物反应中的意义

Receptor-mediated endocytosis of IL-8: a fluorescent microscopic evidence and implication of the process in ligand-induced biological response in human neutrophils.

作者信息

Ray E, Samanta A K

机构信息

Division of Immunobiology, Indian Institute of Chemical Biology, Calcutta-700 032, India.

出版信息

Cytokine. 1997 Aug;9(8):587-96. doi: 10.1006/cyto.1997.0206.

DOI:10.1006/cyto.1997.0206
PMID:9245487
Abstract

Interleukin 8 (IL-8), a neurophil-activating and chemotactic cytokine, is known to play a key role in the pathogenesis of a large number of neutrophil-driven inflammatory diseases. Although the cytokine is rapidly internalized at 37 degrees C with its receptors, there was no direct evidence for the ligand-induced endocytosis of the receptor or that of the interaction of receptor ligand complex at 37 degrees C. As a result, our understanding about the regulation of Il-8 induced biological response is very limited. In the present study, using FITC-IL-8 conjugate as a probe, we have demonstrated the time- and temperature-dependent endocytosis of IL-8 under fluorescent microscope. We have also shown that the bright fluorescent light on the surface of neutrophils gradually disappears and it becomes almost dark after 120 min of incubation. Monodansyl cadaverine (MDC, 900 microM), however, was found to retain the fluorescent light of FITC coupled with Il-8 on the cells. MDC and ouabain (2.5 mM) can inhibit the ligand induced endocytosis by 76% and 96%, respectively, compared to control. With respect to control, IL-8 induced biological responses e.g. IL-8 directed migration, intracellular Ca2+ release and superoxide release are significantly reduced by 77%, 94% and 76%, respectively, in presence of MDC. The study presents a direct visual evidence of the time and temperature-dependent receptor-mediated endocytosis of IL-8 which is inhibited by MDC and ouabain. This information is useful for understanding the ligand receptor interaction at 37 degrees C and may be useful for developing anti-inflammatory agents against IL-8.

摘要

白细胞介素8(IL-8)是一种激活中性粒细胞并具有趋化作用的细胞因子,已知在许多由中性粒细胞驱动的炎症性疾病的发病机制中起关键作用。尽管该细胞因子在37℃时会与其受体迅速内化,但尚无直接证据表明受体存在配体诱导的内吞作用,也没有证据表明在37℃时受体-配体复合物会发生相互作用。因此,我们对IL-8诱导的生物学反应的调节了解非常有限。在本研究中,我们使用FITC-IL-8偶联物作为探针,在荧光显微镜下证明了IL-8的时间和温度依赖性内吞作用。我们还表明,中性粒细胞表面的明亮荧光在孵育120分钟后逐渐消失,几乎变为黑暗。然而,发现单丹磺酰尸胺(MDC,900 microM)能使与IL-8偶联的FITC在细胞上保留荧光。与对照相比,MDC和哇巴因(2.5 mM)分别可抑制配体诱导的内吞作用76%和96%。与对照相比,在存在MDC的情况下,IL-8诱导的生物学反应,如IL-8介导的迁移、细胞内Ca2+释放和超氧化物释放,分别显著降低了77%、94%和76%。该研究提供了IL-8时间和温度依赖性受体介导内吞作用的直接视觉证据,这种内吞作用受到MDC和哇巴因的抑制。这些信息有助于理解37℃时的配体-受体相互作用,可能对开发抗IL-8的抗炎药物有用。

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