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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Spatiotemporal organization, regulation, and functions of tractions during neutrophil chemotaxis
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Spatiotemporal organization, regulation, and functions of tractions during neutrophil chemotaxis

机译:中性粒细胞趋化过程中时空的组织,调节和功能

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Despite recent advances in our understanding of biochemical regulation of neutrophil chemotaxis, little is known about how mechanical factors control neutrophils' persistent polarity and rapid motility. Here, using a human neutrophil-like cell line and human primary neutrophils, we describe a dynamic spatiotemporal pattern of tractions during chemotaxis. Tractions are located at both the leading and the trailing edge of neutrophils, where they oscillate with a defined periodicity. Interestingly, traction oscillations at the leading and the trailing edge are out of phase with the tractions at the front leading those at the back, suggesting a temporal mechanism that coordinates leading edge and trailing edge activities. The magnitude and periodicity of tractions depend on the activity of nonmuscle myosin IIA. Specifically, traction development at the leading edge requires myosin light chain kinase-mediated myosin II contractility and is necessary for α5β1-integrin activation and leading edge adhesion. Localized myosin II activation induced by spatially activated small GTPase Rho, and its downstream kinase p160-ROCK, as previously reported, leads to contraction of actin-myosin II complexes at the trailing edge, causing it to de-adhere. Our data identify a key biomechanical mechanism for persistent cell polarity and motility.
机译:尽管在了解中性粒细胞趋化性的生化调节方面有了新进展,但对于机械因素如何控制中性粒细胞的持久极性和快速运动性知之甚少。在这里,使用人类嗜中性粒细胞样细胞系和人类主要嗜中性粒细胞,我们描述了趋化过程中动态的时空牵引模式。牵引线位于嗜中性粒细胞的前缘和后缘,在此处它们以规定的周期振荡。有趣的是,前缘和后缘的牵引振动与前缘的牵引振动领先于后缘的牵引振动,这表明相位机制协调了前缘和后缘的活动。牵引力的大小和周期性取决于非肌肉肌球蛋白IIA的活性。具体而言,在前缘的牵引力发展需要肌球蛋白轻链激酶介导的肌球蛋白II收缩力,并且对于α5β1-整联蛋白激活和前缘粘附是必需的。如先前报道,由空间激活的小GTPase Rho诱导的局部肌球蛋白II激活及其下游激酶p160-ROCK导致肌动蛋白-肌球蛋白II复合物在后缘收缩,从而使其脱离。我们的数据确定了持久的细胞极性和运动性的关键生物力学机制。

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