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残余血红素在红细胞膜中的长期嵌入会使细胞变形。

Long-term intercalation of residual hemin in erythrocyte membranes distorts the cell.

作者信息

Solar I, Muller-Eberhard U, Shviro Y, Shaklai N

机构信息

Sackler Institute of Molecular Medicine, Sackler School of Medicine, Tel Aviv University, Israel.

出版信息

Biochim Biophys Acta. 1991 Feb 11;1062(1):51-8. doi: 10.1016/0005-2736(91)90334-5.

Abstract

The effect of long-term incubation of residual globin-free hemin on whole red blood cell and isolated cytoskeletal proteins was studied. Hemin at concentrations found in pathological red cells was inserted to fresh erythrocytes. Increased hemolysis developed in the hemin-containing cells after a few days at 37 degrees C and after about four weeks at 4 degrees C. Since lipid and hemoglobin peroxidation did not depend on the presence of hemin, time-dependent effects on the cytoskeleton proteins were studied. Observations were: (1) spectrin and protein 4.1 exhibited a time-dependent increasing tendency to undergo hemin-induced peroxidative crosslinking. (2) The ability of the serum proteins, albumin and hemopexin, to draw hemin from spectrin, actin and protein 4.1 decreased with time of incubation with hemin. These results were attributed to time-dependent hemin-induced denaturation of the cytoskeletal proteins. Albumin taken as a control for physiological hemin trap was unaffected by hemin. Small amounts of hemo-spectrin (2-5%) were analyzed in circulating normal cells, and this in vivo hemo-spectrin also failed to release hemin. It was concluded that slow accumulation of hemin, a phenomenon increased in pathological cells, is a toxic event causing erythrocyte destruction.

摘要

研究了无残留珠蛋白血红素长期孵育对全红细胞和分离的细胞骨架蛋白的影响。将病理红细胞中发现的浓度的血红素加入新鲜红细胞中。含血红素的细胞在37℃孵育几天后以及在4℃孵育约四周后溶血增加。由于脂质和血红蛋白过氧化不依赖于血红素的存在,因此研究了对细胞骨架蛋白的时间依赖性影响。观察结果如下:(1)血影蛋白和蛋白4.1表现出时间依赖性增加的倾向,即发生血红素诱导的过氧化交联。(2)血清蛋白白蛋白和血红素结合蛋白从血影蛋白、肌动蛋白和蛋白4.1中摄取血红素的能力随着与血红素孵育时间的延长而降低。这些结果归因于血红素诱导的细胞骨架蛋白的时间依赖性变性。作为生理性血红素捕获对照的白蛋白不受血红素影响。在循环正常细胞中分析了少量的血红素-血影蛋白(2%-5%),并且这种体内血红素-血影蛋白也未能释放血红素。得出的结论是,血红素的缓慢积累是一种在病理细胞中增加的现象,是导致红细胞破坏的毒性事件。

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