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衰老新生儿红细胞中的细胞脱水与免疫球蛋白结合

Cellular dehydration and immunoglobulin binding in senescent neonatal erythrocytes.

作者信息

Lane P A, Galili U, Iarocci T A, Shew R L, Mentzer W C

机构信息

Department of Pediatrics, University of California, San Francisco 94143.

出版信息

Pediatr Res. 1988 Mar;23(3):288-92. doi: 10.1203/00006450-198803000-00012.

Abstract

The life span of neonatal erythrocytes (60-80 days) is shorter than that of adult erythrocytes (120 days). We studied neonatal red blood cells separated on stractan density gradients to further characterize the aging process and to explore the possibility that senescence antigens play a role in the destruction of neonatal erythrocytes. Quantitation of membrane proteins 4.1a and 4.1b served as a marker for cell age and confirmed an enrichment for senescent red cells in the most dense layers of the gradients. Despite the shorter life span of neonatal erythrocytes, cord blood contained a larger percentage of very dense, K+-depleted red cells than did adult blood. ATP levels in dense neonatal and adult cells were decreased to 50-80% of normal values for unseparated red cells. Levels of reduced glutathione did not fall with increasing cell density. Sodium dodecyl sulfate polyacrylamide gel electrophoresis of red cell membrane proteins showed increased membrane-associated globin in senescent neonatal cells, but such gels run without reducing agents did not show oxidative protein cross-linking. Membrane bound immunoglobulins were detected on senescent neonatal and adult red cells by the rosetting antiglobulin test. We conclude that senescence antigens are revealed during the aging process of neonatal erythrocytes, thereby labeling them for antibody-mediated destruction in the reticuloendothelial system.

摘要

新生儿红细胞的寿命(60 - 80天)比成人红细胞的寿命(120天)短。我们研究了通过葡聚糖密度梯度分离的新生儿红细胞,以进一步描述衰老过程,并探讨衰老抗原在新生儿红细胞破坏中发挥作用的可能性。膜蛋白4.1a和4.1b的定量作为细胞年龄的标志物,证实了梯度最致密层中衰老红细胞的富集。尽管新生儿红细胞寿命较短,但脐血中非常致密、低钾的红细胞百分比高于成人血液。致密的新生儿和成人细胞中的ATP水平降至未分离红细胞正常水平的50 - 80%。还原型谷胱甘肽水平不会随着细胞密度增加而下降。红细胞膜蛋白的十二烷基硫酸钠聚丙烯酰胺凝胶电泳显示,衰老新生儿细胞中与膜相关的珠蛋白增加,但在无还原剂情况下进行的此类凝胶电泳未显示氧化蛋白交联。通过玫瑰花结抗球蛋白试验在衰老的新生儿和成人红细胞上检测到膜结合免疫球蛋白。我们得出结论,衰老抗原在新生儿红细胞衰老过程中被揭示出来,从而将它们标记为在网状内皮系统中被抗体介导破坏的对象。

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