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葡萄糖向经磷脂酶A2或C处理的人红细胞内的转运。

Glucose transport into human erythrocytes treated with phospholipase A2 or C.

作者信息

Fujii H, Miwa I, Okuda J, Tamura A, Fujii T

出版信息

Biochim Biophys Acta. 1986 Aug 6;883(1):77-82. doi: 10.1016/0304-4165(86)90137-6.

Abstract

Phospholipase A2 induced crenation of human erythrocytes and decreased glucose transport activity (influx rate) by 40% when 51% of phosphatidylcholine (PC) in the membrane was hydrolyzed. On the other hand, phospholipase C induced invagination of the cells and negligibly affected the glucose transport in the case of 21% hydrolysis of the PC. By altering the pH of the medium for suspending cells treated with phospholipase A2 from 7.4 to 6.0, cell shape was changed from clear crenation to slight invagination, but glucose transport activity was not affected. Cells that were treated with phospholipase A2 and then washed with albumin to remove free fatty acids produced in the cell membrane showed an almost normal cell shape and slightly higher glucose transport activity than did untreated cells. The ratios of beta-D-glucose transport rate to alpha-D-glucose transport rate in untreated cells, cells treated with phospholipase A2 and cells treated with phospholipase C were 1.13, 1.04, and 1.20, respectively. These results demonstrate that the drastic morphological change (invagination or crenation) induced by the treatment with phospholipases bears no clear relationship to the activity of glucose transport and suggest that the increase in the volume of the outer half of the lipid bilayer might reduce the rate of glucose transport across the human erythrocyte membrane and change the anomeric preference of glucose transport.

摘要

磷脂酶A2可诱导人红细胞皱缩,当膜中51%的磷脂酰胆碱(PC)被水解时,葡萄糖转运活性(流入速率)降低40%。另一方面,在PC水解21%的情况下,磷脂酶C可诱导细胞内陷,对葡萄糖转运的影响可忽略不计。将用磷脂酶A2处理的细胞悬浮液的培养基pH从7.4改变为6.0,细胞形状从明显皱缩变为轻微内陷,但葡萄糖转运活性不受影响。用磷脂酶A2处理后再用白蛋白洗涤以去除细胞膜中产生的游离脂肪酸的细胞,其细胞形状几乎正常,葡萄糖转运活性略高于未处理的细胞。未处理细胞、用磷脂酶A2处理的细胞和用磷脂酶C处理的细胞中,β-D-葡萄糖转运速率与α-D-葡萄糖转运速率的比值分别为1.13、1.04和1.20。这些结果表明,磷脂酶处理诱导的剧烈形态变化(内陷或皱缩)与葡萄糖转运活性没有明显关系,并表明脂质双层外半部分体积的增加可能会降低葡萄糖跨人红细胞膜的转运速率,并改变葡萄糖转运的异头物偏好。

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