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采用电穿孔加载和闪光光解技术研究细胞内和细胞间的钙离子信号传导。

Electroporation loading and flash photolysis to investigate intra- and intercellular Ca2+ signaling.

作者信息

Decrock Elke, De Bock Marijke, Wang Nan, Bol Mélissa, Gadicherla Ashish K, Leybaert Luc

机构信息

Department of Basic Medical Sciences, Physiology Group, Ghent University, 9000 Ghent, Belgium.

出版信息

Cold Spring Harb Protoc. 2015 Mar 2;2015(3):239-49. doi: 10.1101/pdb.top066068.

DOI:10.1101/pdb.top066068
PMID:25734071
Abstract

Many cellular functions are driven by variations in the intracellular Ca(2+) concentration ([Ca(2+)]i), which may appear as a single-event transient [Ca(2+)]i elevation, repetitive [Ca(2+)]i increases known as Ca(2+) oscillations, or [Ca(2+)]i increases propagating in the cytoplasm as Ca(2+) waves. Additionally, [Ca(2+)]i changes can be communicated between cells as intercellular Ca(2+) waves (ICWs). ICWs are mediated by two possible mechanisms acting in parallel: one involving gap junctions that form channels directly linking the cytoplasm of adjacent cells and one involving a paracrine messenger, in most cases ATP, that is released into the extracellular space, leading to [Ca(2+)]i changes in neighboring cells. The intracellular messenger inositol 1,4,5-trisphosphate (IP3) that triggers Ca(2+) release from Ca(2+) stores is crucial in these two ICW propagation scenarios, and is also a potent trigger to initiate ICWs. Loading inactive, "caged" IP3 into cells followed by photolytic "uncaging" with UV light, thereby liberating IP3, is a well-established method to trigger [Ca(2+)]i changes in single cells that is also effective in initiating ICWs. We here describe a method to load cells with caged IP3 by local electroporation of monolayer cell cultures and to apply flash photolysis to increase intracellular IP3 and induce [Ca(2+)]i changes, or initiate ICWs. Moreover, the electroporation method allows loading of membrane-impermeable agents that interfere with IP3 and Ca(2+) signaling.

摘要

许多细胞功能是由细胞内钙离子浓度([Ca(2+)]i)的变化驱动的,这种变化可能表现为单次事件的瞬时[Ca(2+)]i升高、称为钙离子振荡的重复性[Ca(2+)]i增加,或者[Ca(2+)]i在细胞质中作为钙离子波传播。此外,[Ca(2+)]i的变化可以作为细胞间钙离子波(ICW)在细胞之间传递。ICW由两种可能并行起作用的机制介导:一种涉及形成直接连接相邻细胞细胞质通道的间隙连接,另一种涉及旁分泌信使,在大多数情况下是ATP,它释放到细胞外空间,导致相邻细胞中的[Ca(2+)]i变化。触发钙离子从钙库中释放的细胞内信使肌醇1,4,5-三磷酸(IP3)在这两种ICW传播情况下至关重要,也是启动ICW的有效触发因素。将无活性的“笼化”IP3加载到细胞中,然后用紫外光进行光解“脱笼”,从而释放IP3,这是一种在单个细胞中触发[Ca(2+)]i变化的成熟方法,在启动ICW方面也很有效。我们在此描述一种通过单层细胞培养物的局部电穿孔将笼化IP3加载到细胞中,并应用闪光光解来增加细胞内IP3并诱导[Ca(2+)]i变化或启动ICW的方法。此外,电穿孔方法允许加载干扰IP3和钙离子信号传导的膜不可渗透剂。

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