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小鼠体内红细胞生成过程中细胞骨架mRNA表达和蛋白质合成的变化模式。

Changing patterns in cytoskeletal mRNA expression and protein synthesis during murine erythropoiesis in vivo.

作者信息

Peters L L, White R A, Birkenmeier C S, Bloom M L, Lux S E, Barker J E

机构信息

Jackson Laboratory, Bar Harbor, ME 04609.

出版信息

Proc Natl Acad Sci U S A. 1992 Jul 1;89(13):5749-53. doi: 10.1073/pnas.89.13.5749.

Abstract

The major cytoskeletal proteins alpha-spectrin, beta-spectrin, and ankyrin are synthesized and assembled into a supportive membrane skeleton during erythroid differentiation. Information on the temporal appearance of mRNA and protein species is essential for understanding both the cytoskeletal assembly process and the function of various isoforms. We have isolated highly enriched populations of fetal erythroid cells at various stages of maturation. mRNAs for erythroid ankyrin, alpha-spectrin, and beta-spectrin were expressed at all stages but there were differences in transcript types and levels. The ratio of 9-kilobase (kb) to 7.5-kb erythroid ankyrin transcripts decreased markedly during differentiation, but there was no change in the ratio of the 10.1-kb and 9.3-kb erythroid beta-spectrin transcripts. The relative amounts of ankyrin, alpha-spectrin, and beta-spectrin mRNA increased during yolk sac cell differentiation, whereas only alpha-spectrin mRNA increased during differentiation of the fetal liver cells. The amounts of beta-spectrin mRNA exceeded the amounts of alpha-spectrin mRNA in the early precursors from both yolk sac and fetal liver; protein synthetic levels showed the same pattern. The 16-day fetal peripheral reticulocytes, on the other hand, had the adult mRNA and protein synthetic ratios with alpha/beta greater than 1. The data indicate that at least two mechanisms exist to meet changing erythroid membrane cytoskeletal requirements during development in utero: (i) stage-specific processing of the mRNA for the major cytoskeletal linker protein ankyrin and (ii) developmentally regulated alpha/beta-spectrin protein synthetic rates.

摘要

主要的细胞骨架蛋白α-血影蛋白、β-血影蛋白和锚蛋白在红细胞分化过程中合成并组装成支持性的膜骨架。关于mRNA和蛋白质种类的出现时间的信息对于理解细胞骨架组装过程和各种同工型的功能至关重要。我们分离了处于不同成熟阶段的高度富集的胎儿红细胞群体。红细胞锚蛋白、α-血影蛋白和β-血影蛋白的mRNA在所有阶段均有表达,但转录本类型和水平存在差异。在分化过程中,9千碱基(kb)与7.5 kb的红细胞锚蛋白转录本的比例显著下降,但10.1 kb和9.3 kb的红细胞β-血影蛋白转录本的比例没有变化。在卵黄囊细胞分化过程中,锚蛋白、α-血影蛋白和β-血影蛋白mRNA的相对量增加,而在胎儿肝细胞分化过程中只有α-血影蛋白mRNA增加。在来自卵黄囊和胎儿肝脏的早期前体细胞中,β-血影蛋白mRNA的量超过了α-血影蛋白mRNA的量;蛋白质合成水平呈现相同的模式。另一方面,16天胎儿外周网织红细胞具有成人的mRNA和蛋白质合成比例,α/β大于1。数据表明,在子宫内发育过程中,至少存在两种机制来满足不断变化的红细胞膜细胞骨架需求:(i)主要细胞骨架连接蛋白锚蛋白的mRNA的阶段特异性加工,以及(ii)发育调控的α/β-血影蛋白蛋白质合成速率。

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