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在伴刀豆球蛋白A帽形成的不同阶段对其进行分离,并研究它们与肌动蛋白和肌球蛋白的关联。

Isolation of concanavalin A caps during various stages of formation and their association with actin and myosin.

作者信息

Condeelis J

出版信息

J Cell Biol. 1979 Mar;80(3):751-8. doi: 10.1083/jcb.80.3.751.

Abstract

Regions of plasma membrane of dictyostelium discoideum amoebae that contain concanavalin A (Con A)-receptor complexes are more resistant to disruption by Triton X-100. This resistance makes possible the isolation of Con A-associated membrane fragments in sufficient quantity and homogeneity to permit the direct biochemical and ultrastructural study of receptor-cytoskeletal interactions across the cell membrane. After specific binding of Con A to the cell surface, a large amount of the cell's actin and myosin copurifies with the plasma membrane fragments. Myosin is more loosely bound to the isolated membranes that actin and is efficiently removed by treating membranes with ATP and low ionic strength. If cells are not lysed immediately after lectin binding, all of the Con A that is bound to the cell surface is swept into a cap in a process requiring metabolic energy. When cells are lysed at different stages of cap formation, the amount of actin and myosin that copurifies with the isolated membranes remains the same. Thick and thin filaments that are attached to the protoplasmic surface of the isolated membranes underlie lectin-receptor complexes during all stages of cap formation. Once the cap is complete, the amount of actin and myosin that tightly bound to the plasma membrane is concentrated into the cap along with the Con A-receptor complexes. These results suggest that the ATP-dependent sliding of membrane-associated actin and myosin filaments is responsible for the accumulation of Con A-receptor complexes into a cap on the cell surface.

摘要

盘基网柄菌变形虫的质膜区域含有伴刀豆球蛋白A(Con A)受体复合物,对Triton X - 100的破坏更具抗性。这种抗性使得能够分离出足够数量且均一的与Con A相关的膜片段,从而可以直接对跨细胞膜的受体 - 细胞骨架相互作用进行生化和超微结构研究。Con A与细胞表面特异性结合后,大量细胞的肌动蛋白和肌球蛋白与质膜片段一起被纯化出来。肌球蛋白与分离出的膜的结合比肌动蛋白更松散,通过用ATP和低离子强度处理膜可以有效地将其去除。如果在凝集素结合后不立即裂解细胞,所有结合到细胞表面的Con A会在一个需要代谢能量的过程中被扫入帽状结构中。当在帽状结构形成的不同阶段裂解细胞时,与分离出的膜一起被纯化出来的肌动蛋白和肌球蛋白的量保持不变。在帽状结构形成的所有阶段,附着在分离出的膜的原生质表面的粗细肌丝构成凝集素 - 受体复合物的基础。一旦帽状结构完成,紧密结合到质膜上的肌动蛋白和肌球蛋白的量会与Con A - 受体复合物一起集中到帽状结构中。这些结果表明,膜相关的肌动蛋白和肌球蛋白丝的ATP依赖性滑动负责Con A - 受体复合物在细胞表面聚集成帽状结构。

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