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红细胞变形的分子图谱:隐藏的弹性和原位连通性。

Molecular maps of red cell deformation: hidden elasticity and in situ connectivity.

作者信息

Discher D E, Mohandas N, Evans E A

机构信息

Joint Graduate Group in Bioengineering, University of California, Berkeley, San Francisco 94720.

出版信息

Science. 1994 Nov 11;266(5187):1032-5. doi: 10.1126/science.7973655.

Abstract

Fluorescence-imaged micropipette aspiration was used to map redistribution of the proteins and lipids in highly extended human red blood cell membranes. Whereas the fluid bilayer distributed uniformly (+/- 10 percent), the underlying, solidlike cytoskeleton of spectrin, actin, and protein 4.1 exhibited a steep gradient in density along the aspirated projection, which was reversible on release from deformation. Quantitation of the cytoskeletal protein density gradients showed that skeletal elasticity is well represented by a grafted polymer network with a ratio of surface dilation modulus to shear modulus of approximately 2:1. Fractionally mobile integral proteins, such as band 3, and highly mobile receptors, such as CD59 as well as glycophorin C in protein 4.1-deficient cells, appeared to be squeezed out of areas dense in the underlying network and enriched in areas of network dilation. This complementary segregation demonstrates patterning of cell surface components by cytoskeletal dilation.

摘要

利用荧光成像微吸管抽吸技术来绘制高度伸展的人类红细胞膜中蛋白质和脂质的重新分布情况。虽然流体双层均匀分布(±10%),但由血影蛋白、肌动蛋白和蛋白质4.1构成的底层类固体细胞骨架在抽吸突起上沿密度呈现陡峭梯度,在从变形状态释放后这种梯度是可逆的。细胞骨架蛋白密度梯度的定量分析表明,骨架弹性可以很好地由表面膨胀模量与剪切模量之比约为2:1的接枝聚合物网络来表示。部分可移动的整合蛋白,如带3蛋白,以及高移动性受体,如CD59以及4.1蛋白缺陷细胞中的血型糖蛋白C,似乎被挤出了底层网络密集的区域,并富集在网络扩张的区域。这种互补性分离表明细胞表面成分通过细胞骨架扩张形成了图案化。

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