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吞噬细胞膜中的钙敏感钾通道。

Ca2+-sensitive K+ channels in phagocytic cell membranes.

作者信息

Oliveira-Castro G M

出版信息

Cell Calcium. 1983 Dec;4(5-6):475-92. doi: 10.1016/0143-4160(83)90023-4.

Abstract

In phagocytic cells evidence for properties of Ca2+-sensitive K+-selective channels comes mostly from electrophysiological studies. Macrophages and macrophage-like cells are compared with fibroblasts (L-cells) where the Ca+-dependent K+ conductance is better understood. This model shares a mesenchymal origin and an accessory phagocytic capacity with the professional phagocytes. In macrophages several values of transmembrane potentials have been measured by different groups, using various techniques. Microelectrode measurements have demonstrated a voltage-dependent K+ conductance involved in transition from low to high membrane potentials. Current-voltage relationships in mouse peritoneal exudate cells have revealed a region of negative slope resistance. Slow calcium spikes were found in a subpopulation of cells from human dialysis fluid that appear to be distinct from typical macrophages. Action potentials have been recorded from human monocyte-derived macrophages. Their ionic mechanism has not yet been established. Spontaneous and electrically elicited slow membrane hyperpolarizations have been described in macrophages and macrophage-like cells. Similar activity is well known in L-cells and in both cases it is possible to identify a Ca2+-sensitive K+ conductance as the underlying mechanism. Phagocytosis is a cell function that has been related to membrane hyperpolarization and to slow hyperpolarizing activity. In some cases no changes of electrical activity have been observed during the phagocytic process. Chemotactic factors induce membrane hyperpolarizations in macrophages, but the relation between electrical change and cell motility has not been established. Exocytosis, a is another Ca2+ sensitive cell function that awaits correlation with electrochemical changes. The evidences accumulated to date are compatible with several models for gating and modulation of the voltage-independent K+ conductance by Ca2+. The use of higher resolution techniques, such as patch-clamp, with well defined subpopulations of phagocytic cells may produce the missing link in the transduction of membrane signals into the specifically targeted cell functions.

摘要

在吞噬细胞中,钙敏感钾选择性通道特性的证据大多来自电生理学研究。将巨噬细胞和类巨噬细胞与成纤维细胞(L细胞)进行比较,在成纤维细胞中,钙依赖性钾电导的情况得到了更好的理解。该模型与专业吞噬细胞具有间充质起源和辅助吞噬能力。在巨噬细胞中,不同研究小组使用各种技术测量了多个跨膜电位值。微电极测量表明,电压依赖性钾电导参与了从低膜电位到高膜电位的转变。小鼠腹腔渗出细胞的电流-电压关系揭示了一个负斜率电阻区域。在人透析液来源的细胞亚群中发现了缓慢的钙尖峰,这些细胞似乎与典型巨噬细胞不同。已记录到来自人单核细胞衍生巨噬细胞的动作电位。其离子机制尚未确定。在巨噬细胞和类巨噬细胞中描述了自发和电诱发的缓慢膜超极化。在L细胞中也有类似的活动,在这两种情况下,都有可能确定钙敏感钾电导是其潜在机制。吞噬作用是一种与膜超极化和缓慢超极化活动相关的细胞功能。在某些情况下,吞噬过程中未观察到电活动的变化。趋化因子可诱导巨噬细胞膜超极化,但电变化与细胞运动之间的关系尚未确立。胞吐作用是另一种对钙敏感的细胞功能,有待与电化学变化建立关联。迄今为止积累的证据与几种钙门控和调节电压非依赖性钾电导的模型相符。使用更高分辨率的技术,如膜片钳技术,对明确界定的吞噬细胞亚群进行研究,可能会在将膜信号转导为特定靶向细胞功能的过程中找到缺失的环节。

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