首页> 美国卫生研究院文献>The Journal of Biophysical and Biochemical Cytology >Ponticulin is the major high affinity link between the plasma membrane and the cortical actin network in Dictyostelium
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Ponticulin is the major high affinity link between the plasma membrane and the cortical actin network in Dictyostelium

机译:桥蛋白是双壁皮膜质膜和皮质肌动蛋白网络之间的主要高亲和力连接

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摘要

Interactions between the plasma membrane and underlying actin-based cortex have been implicated in membrane organization and stability, the control of cell shape, and various motile processes. To ascertain the function of high affinity actin-membrane associations, we have disrupted by homologous recombination the gene encoding ponticulin, the major high affinity actin-membrane link in Dictyostelium discoideum amoebae. Cells lacking detectable amounts of ponticulin message and protein also are deficient in high affinity actin-membrane binding by several criteria. First, only 10-13% as much endogenous actin cosediments through sucrose and crude plasma membranes from ponticulin- minus cells, as compared with membranes from the parental strain. Second, purified plasma membranes exhibit little or no binding or nucleation of exogenous actin in vitro. Finally, only 10-30% as much endogenous actin partitions with plasma membranes from ponticulin-minus cells after these cells are mechanically unroofed with polylysine- coated coverslips. The loss of the cell's major actin-binding membrane protein appears to be surprisingly benign under laboratory conditions. Ponticulin-minus cells grow normally in axenic culture and pinocytose FITC-dextran at the same rate as do parental cells. The rate of phagocytosis of particles by ponticulin-minus cells in growth media also is unaffected. By contrast, after initiation of development, cells lacking ponticulin aggregate faster than the parental cells. Subsequent morphogenesis proceeds asynchronously, but viable spores can form. These results indicate that ponticulin is not required for cellular translocation, but apparently plays a role in cell patterning during development.
机译:质膜和基于肌动蛋白的皮层之间的相互作用已经涉及到膜的组织和稳定性,细胞形状的控制以及各种运动过程。为了确定高亲和力肌动蛋白-膜关联的功能,我们已经通过同源重组破坏了编码桥连蛋白的基因,该蛋白是盘基网柄菌中主要的高亲和力肌动蛋白-膜连接。缺乏可检测量的桥蛋白信息和蛋白质的细胞也缺乏高亲和性肌动蛋白-膜结合的几个标准。首先,与来自亲本菌株的膜相比,通过桥糖和负性膜细胞的蔗糖和粗质膜的内源性肌动蛋白沉积只有10-13%。其次,纯化的质膜在体外几乎没有或没有外源肌动蛋白的结合或成核。最后,在用聚赖氨酸包被的盖玻片对这些细胞进行机械顶盖处理后,只有这些细胞的内源性肌动蛋白与来自桥蛋白负细胞的质膜之间的分配比例为10-30%。在实验室条件下,细胞主要肌动蛋白结合膜蛋白的丢失似乎是良性的。桥菌素减号细胞在轴突培养物中正常生长,并以与亲代细胞相同的速率生长于胞饮酶FITC-葡聚糖中。生长介质中桥联蛋白-负细胞对颗粒的吞噬作用的速率也不受影响。相反,在发育开始后,缺乏桥蛋白的细胞比亲代细胞聚集更快。随后的形态发生异步进行,但可以形成有活力的孢子。这些结果表明,桥联蛋白不是细胞转运所必需的,但显然在发育过程中在细胞模式中起作用。

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