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与红细胞加速衰老相关的膜蛋白带3的改变。

Alteration in membrane protein band 3 associated with accelerated erythrocyte aging.

作者信息

Kay M M, Flowers N, Goodman J, Bosman G

机构信息

Department of Medicine, Texas A&M University, Temple.

出版信息

Proc Natl Acad Sci U S A. 1989 Aug;86(15):5834-8. doi: 10.1073/pnas.86.15.5834.

Abstract

We report a human band 3 alteration that is associated with anemia as determined by a reticulocyte count of 20%. Erythrocyte defects included increased IgG binding, increased breakdown products of band 3, and altered anion- and glucose-transport activity in middle-aged cells. These changes were observed during normal erythrocyte aging in situ. Binding of ankyrin to band 3 was normal. Serum/cell crossover studies indicated that a neoantigen appears on the propositus' erythrocytes to which IgG from both propositus and control serum binds as measured with a protein A binding assay. IgG eluted from the propositus' erythrocytes appeared to have a specificity for senescent cell antigen as determined by a phagocytosis inhibition assay. Immunoelectron microscopy showed that antibodies to band 3, which do not normally bind to intact erythrocytes, bound to the propositus' erythrocytes. Antibody 980 binds to normal old cells but not young or middle-aged cells. It also binds to a distinct region of band 3 in immunoblots of membranes from the propositus' middle-aged cells. Cells from both of the propositus' parents exhibited increased IgG binding and altered anion and glucose transport. The results of these studies suggest that (i) band 3 is aging prematurely in erythrocytes from the propositus, (ii) senescent cell antigen appears on the propositus' middle-aged red cells, and (iii) band 3 alterations observed in the propositus may have a genetic component.

摘要

我们报告了一种人类带3改变,通过网织红细胞计数20%确定其与贫血相关。红细胞缺陷包括IgG结合增加、带3降解产物增加以及中年细胞中阴离子和葡萄糖转运活性改变。这些变化是在原位正常红细胞衰老过程中观察到的。锚蛋白与带3的结合正常。血清/细胞交叉研究表明,先证者红细胞上出现一种新抗原,用蛋白A结合试验检测发现,先证者和对照血清中的IgG均能与其结合。通过吞噬抑制试验确定,从先证者红细胞洗脱的IgG似乎对衰老细胞抗原有特异性。免疫电子显微镜显示,通常不与完整红细胞结合的抗带3抗体与先证者红细胞结合。抗体980与正常衰老细胞结合,但不与年轻或中年细胞结合。它也与先证者中年细胞膜免疫印迹中带3的一个独特区域结合。先证者父母双方的细胞均表现出IgG结合增加以及阴离子和葡萄糖转运改变。这些研究结果表明:(i)先证者红细胞中的带3过早衰老;(ii)衰老细胞抗原出现在先证者的中年红细胞上;(iii)先证者中观察到的带3改变可能有遗传成分。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f0bd/297725/24f2430b3c3c/pnas00282-0174-a.jpg

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