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首页> 外文期刊>PLoS Biology >Creatine Kinase–Mediated ATP Supply Fuels Actin-Based Events in Phagocytosis
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Creatine Kinase–Mediated ATP Supply Fuels Actin-Based Events in Phagocytosis

机译:肌酸激酶介导的ATP供应促进吞噬作用中基于肌动蛋白的事件。

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摘要

Phagocytosis requires locally coordinated cytoskeletal rearrangements driven by actin polymerization and myosin motor activity. How this actomyosin dynamics is dependent upon systems that provide access to ATP at phagosome microdomains has not been determined. We analyzed the role of brain-type creatine kinase (CK-B), an enzyme involved in high-energy phosphoryl transfer. We demonstrate that endogenous CK-B in macrophages is mobilized from the cytosolic pool and coaccumulates with F-actin at nascent phagosomes. Live cell imaging with XFP-tagged CK-B and β-actin revealed the transient and specific nature of this partitioning process. Overexpression of a catalytic dead CK-B or CK-specific cyclocreatine inhibition caused a significant reduction of actin accumulation in the phagocytic cup area, and reduced complement receptor–mediated, but not Fc-γR–mediated, ingestion capacity of macrophages. Finally, we found that inhibition of CK-B affected phagocytosis already at the stage of particle adhesion, most likely via effects on actin polymerization behavior. We propose that CK-B activity in macrophages contributes to complement-induced F-actin assembly events in early phagocytosis by providing local ATP supply.
机译:吞噬作用需要由肌动蛋白聚合和肌球蛋白运动活性驱动的局部协调的细胞骨架重排。尚未确定这种放线菌素动力学如何取决于在吞噬体微结构域提供对ATP的访问的系统。我们分析了脑型肌酸激酶(CK-B),一种参与高能磷酸基转移的酶的作用。我们证明巨噬细胞中的内源性CK-B是从胞质池中动员起来的,并与F-肌动蛋白在新生吞噬体中共同蓄积。 XFP标记的CK-B和β-肌动蛋白的活细胞成像揭示了这种分配过程的短暂性和特异性。催化性死CK-B或CK特异性环肌酸的过表达抑制作用导致吞噬杯区域肌动蛋白的蓄积显着减少,并减少了补体受体介导的但不是Fc-γR介导的巨噬细胞的摄取能力。最后,我们发现抑制CK-B已在颗粒粘附阶段影响吞噬作用,最可能是通过对肌动蛋白聚合行为的影响。我们提出,巨噬细胞中的CK-B活性通过提供局部ATP的供应而有助于在早期吞噬作用中补体诱导的F-肌动蛋白组装事件。

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