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蛋白质合成的遗传控制:血红蛋白模型。

The genetic control of protein synthesis: The haemoglobin model.

作者信息

Weatherall D J

出版信息

J Clin Pathol Suppl (R Coll Pathol). 1974;8:1-11.

Abstract

The major steps in haemoglobin synthesis in red cell precursors are now worked out and only details of specific mechanisms remain to be filled in. Thus the major steps in the production of a globin chain are the transcription of large-molecular-weight precursor mRNA (Hn RNA) from the appropriate gene, the cleavage of Hn RNA to produce definitive template mRNA which diffuses into the cell cytoplasm, the processes of chain initiation, translation, and termination, and finally the association of subunits to form a stable tetramer. From what little information there is it appears that this complex series of events is controlled at several levels but that the major control mechanisms are mediated in the processes of transcription rather than translation. There is increasing evidence that the chromatin proteins, particularly the acidic proteins, have specific functions in maintaining areas of DNA repressed and the activation of the haemoglobin loci results from complex interactions with external inducers, the nature of which is not yet known. Virtually nothing is known about the factors involved in the switch from the intrauterine to adult haemoglobins although this appears to be a coordinated event throughout the erythropoietic tissue of the fetus. The isolation and characterization of human mRNA has made possible both the study of the function of thalassaemic mRNA in heterologous systems and , more recently, its quantitation in abnormal red-cell precursors. Furthermore the ability to make cDNA using viral re verse transcriptase has made possible the estimation of the number of haemoglobin genes, both in normal human subjects and in those with different forms of thalassaemia and other genetic disorders of haemoglobin production.

摘要

目前已明确红细胞前体中血红蛋白合成的主要步骤,仅特定机制的细节仍有待补充。因此,珠蛋白链产生的主要步骤包括:从相应基因转录出大分子前体mRNA(核不均一RNA);切割核不均一RNA以产生确定的模板mRNA,该mRNA扩散至细胞质中;起始、翻译和终止过程;最后亚基结合形成稳定的四聚体。根据现有的少量信息,这一系列复杂事件似乎在多个层面受到控制,但主要控制机制是在转录过程而非翻译过程中发挥作用。越来越多的证据表明,染色质蛋白,尤其是酸性蛋白,在维持DNA受抑制区域方面具有特定功能,而血红蛋白基因座的激活源于与外部诱导物的复杂相互作用,其性质尚不清楚。尽管从胎儿的整个造血组织来看,从胎儿血红蛋白向成人血红蛋白的转换似乎是一个协调的过程,但对于其中涉及的因素几乎一无所知。人mRNA的分离和特性分析使得在异源系统中研究地中海贫血mRNA的功能成为可能,并且最近还能对异常红细胞前体中的mRNA进行定量分析。此外,利用病毒逆转录酶制备cDNA的能力,使得估计正常人类个体以及患有不同形式地中海贫血和其他血红蛋白生成遗传性疾病的个体中的血红蛋白基因数量成为可能。

相似文献

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Human haemoglobin genetics.人类血红蛋白遗传学。
Ciba Found Symp. 1979(66):147-86. doi: 10.1002/9780470720486.ch7.
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[Synthesis of hemoglobin].[血红蛋白的合成]
Hamatol Bluttransfus. 1972;10:295-308.
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Molecular genetics of human hemoglobin.人类血红蛋白的分子遗传学
Annu Rev Genet. 1976;10:157-78. doi: 10.1146/annurev.ge.10.120176.001105.

本文引用的文献

6
Initiation of globin synthesis.珠蛋白合成的起始
FEBS Lett. 1972 Aug 15;24(3):310-314. doi: 10.1016/0014-5793(72)80379-x.
8
Gene regulation for higher cells: a theory.高等细胞的基因调控:一种理论
Science. 1969 Jul 25;165(3891):349-57. doi: 10.1126/science.165.3891.349.
9
Haemoglobin synthesis in beta-thalassaemia.β地中海贫血中的血红蛋白合成
Nature. 1968 Nov 16;220(5168):664-8. doi: 10.1038/220664a0.

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