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首页> 外文期刊>Molecular biology of the cell >Slipping or gripping? Fluorescent speckle microscopy in fish keratocytes reveals two different mechanisms for generating a retrograde flow of actin
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Slipping or gripping? Fluorescent speckle microscopy in fish keratocytes reveals two different mechanisms for generating a retrograde flow of actin

机译:滑倒或抓地力?鱼角化细胞中的荧光斑点显微镜显示出两种不同的机制来产生肌动蛋白逆行流动

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Fish keratocytes can generate rearward directed traction forces within front portions of the lamellipodium, suggesting that a retrograde flow of actin may also occur here but this was not detected by previous photoactivation experiments. To investigate the relationship between retrograde flow and traction force generation, we have transfected keratocytes with GFP-actin and used fluorescent speckle microscopy, to observe speckle flow. We detected a retrograde flow of actin within the leading lamellipodium that is inversely proportional to both protrusion rate and cell speed. To observe the effect of reducing contractility, we treated transfected cells with ML7, a potent inhibitor of myosin II. Surprisingly, ML7 treatment led to an increase in retrograde flow rate, together with a decrease in protrusion and cell speed, but only in rapidly moving cells. In slower moving cells, retrograde flow decreased, whereas protrusion rate and cell speed increased. Theme resultes suggest that there are two mechanisms for producing retrograde flow. One involves slippage between the cytoskeleton and adhesions, that decreases traction force production. The other involves slippage between adhesions and the substratum, which increases traction force production. We conclude that a biphasic relationship exists between retrograde actin flow and adhesiveness in moving keratocytes.
机译:鱼的角膜细胞可在片状脂质体的前部产生向后的牵引力,这表明此处也可能发生肌动蛋白的逆行流动,但以前的光活化实验未检测到。为了研究逆行血流与牵引力产生之间的关系,我们用GFP-肌动蛋白转染了角膜细胞,并使用荧光斑点显微镜观察斑点血流。我们检测到领先的lalamlipodium中肌动蛋白的逆行流动与突出率和细胞速度成反比。为了观察降低收缩力的效果,我们用ML7(一种肌球蛋白II的有效抑制剂)处理了转染的细胞。出乎意料的是,ML7处理导致逆行流速增加,同时突起和细胞速度下降,但仅在快速移动的细胞中发生。在运动较慢的细胞中,逆行血流减少,而突出率和细胞速度增加。主题结果表明,存在两种产生逆流的机制。一种涉及细胞骨架与粘连之间的打滑,从而降低了牵引力的产生。另一个涉及粘着层和基底之间的滑动,这增加了牵引力的产生。我们得出的结论是,逆行肌动蛋白流量与运动性角膜细胞的粘附性之间存在两相关系。

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