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一个基因位点调控来自多个转录单元的组织特异性mRNA的表达。

A genetic locus regulates the expression of tissue-specific mRNAs from multiple transcription units.

作者信息

Levy D E, Lerner R A, Wilson M C

出版信息

Proc Natl Acad Sci U S A. 1982 Oct;79(19):5823-7. doi: 10.1073/pnas.79.19.5823.

Abstract

129 GIX- mice, unlike animals of the congeneic partner strain GIX+, do not express significant amounts of the retroviral antigens gp70 and p30. Evidence is presented indicating that the GIX phenotype is specified by a distinct regulatory gene acting on multiple transcription units to control the levels of accumulation of specific mRNA species. The steady-state levels of retroviral-homologous mRNA from the tissues of GIX+ and GIX- mice were examined by blot hybridization using as probes DNA fragments from cloned murine leukemia viruses. RNA potentially encoding viral antigens was reduced or absent in GIX- mice, even though no differences in integrated viral genomes were detected between these congeneic strains by DNA blotting. Tissue-specific patterns of accumulation of these RNA species were detected in brain, epididymis, liver, spleen, and thymus, and several distinct RNA species were found to be coordinately regulated with the GIX phenotype. Measurements of RNA synthesis suggest a major role for transcriptional control in the regulation of some retroviral messages.

摘要

129只GIX-小鼠与同基因对照品系GIX+小鼠不同,不表达大量逆转录病毒抗原gp70和p30。有证据表明,GIX表型由一个独特的调控基因决定,该基因作用于多个转录单元,以控制特定mRNA种类的积累水平。使用克隆的鼠白血病病毒的DNA片段作为探针,通过印迹杂交检测了GIX+和GIX-小鼠组织中逆转录病毒同源mRNA的稳态水平。尽管通过DNA印迹在这些同基因品系之间未检测到整合病毒基因组的差异,但GIX-小鼠中潜在编码病毒抗原的RNA减少或缺失。在脑、附睾、肝脏、脾脏和胸腺中检测到了这些RNA种类的组织特异性积累模式,并且发现几种不同的RNA种类与GIX表型协同调控。RNA合成的测量表明转录控制在某些逆转录病毒信息的调控中起主要作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bedd/347002/007fca304f2a/pnas00458-0074-a.jpg

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