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红细胞的膜变形性及形状改变能力。

Membrane deformability and the capacity for shape change in the erythrocyte.

作者信息

Chasis J A, Schrier S L

机构信息

Department of Medicine, University of California, San Francisco 94143-0128.

出版信息

Blood. 1989 Nov 15;74(7):2562-8.

PMID:2804378
Abstract

Erythrocytes must have the capacity to undergo marked membrane deformation and shape changes in order to circulate through capillaries and respond to a range of shear stresses. To study the interrelationships between membrane deformability and the capacity for shape transformation, we created rigid membranes using several agents and then examined the ability of these erythrocytes with rigid membranes to undergo amphipath-induced shape change. We have previously shown that wheat germ agglutinin (WGA) and a monoclonal antibody to glycophorin A (R-10) cause membrane rigidity as measured by ektacytometry. Experiments were therefore designed to produced comparably rigid membranes using WGA, R-10, and diamide, and then to test the ability of lysophosphatidylcholine to produce echinocytes, and primaquine to produce stomatocytes. We found that diamide treatment substantially blocked both types of shape change. In contrast, R-10 binding did not impair either primaquine- or lysophosphatidylcholine-induce shape change. Further, WGA blocked echinocyte transformation, as previously reported, but not stomatocytosis. Using reduced and unreduced gel electrophoresis and Triton extraction, we compared the biochemical changes associated with WGA-, diamide-, and R-10-induced rigidity, and found them to be different. We conclude that not all rigid cells are incapable of shape change, and therefore that decreased membrane deformability is not predictive of impaired capacity for shape change.

摘要

红细胞必须具备显著的膜变形能力和形状改变能力,才能在毛细血管中循环并应对一系列剪切应力。为了研究膜变形性与形状转变能力之间的相互关系,我们使用多种试剂制备了刚性膜,然后检测这些带有刚性膜的红细胞发生两亲性诱导形状改变的能力。我们之前已经表明,通过激光衍射法测定,麦胚凝集素(WGA)和抗血型糖蛋白A单克隆抗体(R-10)可导致膜刚性。因此,设计实验使用WGA、R-10和二酰胺制备具有相当刚性的膜,然后检测溶血磷脂酰胆碱诱导棘红细胞生成以及伯氨喹诱导口形红细胞生成的能力。我们发现,二酰胺处理可显著阻断这两种类型的形状改变。相比之下,R-10结合并不损害伯氨喹或溶血磷脂酰胆碱诱导的形状改变。此外,正如之前报道的,WGA可阻断棘红细胞转变,但不影响口形红细胞生成。我们使用还原和非还原凝胶电泳以及Triton抽提,比较了与WGA、二酰胺和R-10诱导的刚性相关的生化变化,发现它们各不相同。我们得出结论,并非所有刚性细胞都无法发生形状改变,因此膜变形性降低并不能预测形状改变能力受损。

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