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首页> 外文期刊>American Journal of Physiology >Imaging signal transduction during phagocytosis: phospholipids, surface charge, and electrostatic interactions.
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Imaging signal transduction during phagocytosis: phospholipids, surface charge, and electrostatic interactions.

机译:吞噬作用期间的成像信号转导:磷脂,表面电荷和静电相互作用。

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摘要

Together with the development of genetically encoded fluorescent probes, digital imaging has provided great impetus to the study of cell signaling by providing enhanced sensitivity and much-improved spatial and temporal resolution. We have used phagocytosis as a paradigm of signal transduction, taking advantage of the generous size of phagosomes and of their comparatively leisurely rate of formation. Aided by the design of specific probes, we demonstrated a highly localized and elegantly choreographed sequence of changes in the level of several phosphoinositides and were able to also monitor the fate of phosphatidylserine. The net changes in the content of these anionic phospholipids are accompanied by marked alterations in the surface charge of the membrane of nascent phagosomes. These, in turn, cause the relocation of proteins that associate with the membrane by electrostatic interactions. Our studies suggest that anionic lipids control protein targeting not only through stereospecific recognition by specialized domains but also by electrostatic association mediated by polycationic motifs. The "electrostatic switch" can be turned on or off by altering the charge of the protein ligand (e.g., by phosphorylation) or, alternatively, by modifying the lipid composition of the target membrane.
机译:随着遗传编码的荧光探针的发展,数字成像通过提供增强的灵敏度和更高的空间和时间分辨率来研究细胞信号传导的重要推动。我们使用吞噬作用作为信号转导的范例,利用吞噬粒度的大部分和它们相对悠闲的形成速率。通过特定探针的设计辅助,我们证明了几种磷酸阳性水平的高度本地化和典雅的思想变化,并且能够监测磷脂酰丝氨酸的命运。这些阴离子磷脂含量的净变化伴随着新生吞噬体的膜的表面电荷的标记改变。反过来,这些导致通过静电相互作用与膜相关的蛋白质的重新定位。我们的研究表明,阴离子脂质对照蛋白不仅通过专业结构域通过立体特异性识别,而且还通过由聚丙烯基序介导的静电关联。通过改变蛋白质配体的电荷(例如,通过磷酸化)或通过改变靶膜的脂质组合物来改变蛋白质配体(例如,通过磷酸化),可以打开或关闭“静电开关”。

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