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首页> 外文期刊>Genetics: A Periodical Record of Investigations Bearing on Heredity and Variation >Two genetic elements regulate murine beta-glucuronidase synthesis following transcript accumulation.
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Two genetic elements regulate murine beta-glucuronidase synthesis following transcript accumulation.

机译:转录物积累后,有两个遗传因子调节鼠类β-葡萄糖醛酸苷酶的合成。

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Mutant alleles of two genetic regulatory elements, which underlie a three- to sixfold reduction in beta-glucuronidase (GUS) activity levels, distinguish mice of the H haplotype from those of the other two common GUS haplotypes, A and B. Both elements are tightly linked to the GUS structural gene over which they exert control. One (Gus-u) exerts a cis-active effect upon GUS activity levels in all tissues at all times while the other (Gus-t) regulates GUS activity in trans after the 12th postnatal day in certain tissues. While previous studies show that differences in the rate of GUS synthesis account for the combined effects of these two elements in liver of adult mice, we demonstrate the separate effects of each on GUS synthesis at times during early postnatal development when their individual expressions can be distinguished. Assessments of the relative levels of S1 nuclease protection of a radiolabeled GUS antisense RNA probe after hybridization with total liver RNA preparations from adult mice of A and H haplotypes reveal no differences. These results argue that Gus-u and Gus-t exert their control of GUS expression subsequent to the accumulation of processed GUS transcripts.
机译:β-葡萄糖醛酸苷酶(GUS)活性水平降低三到六倍的两个遗传调控元件的突变等位基因,将H单倍型小鼠与其他两个常见GUS单倍型A和B的小鼠区分开。这两个元素紧密相关与他们控制的GUS结构基因相关。一种(Gus-u)始终对所有组织中的GUS活性水平起顺式作用,而另一种(Gus-t)在产后第12天后某些组织中反式调节GUS活性。尽管先前的研究表明,GUS合成速率的差异是这两种元素在成年小鼠肝脏中共同作用的原因,但我们证明了在出生后早期可以区分它们各自表达时,它们对GUS合成的单独作用。与来自A型和H型单倍体成年小鼠的总肝RNA制剂杂交后,对放射性标记的GUS反义RNA探针的S1核酸酶保护的相对水平的评估没有发现差异。这些结果表明,Gus-u和Gus-t在处理过的GUS转录物积累之后发挥了对GUS表达的控制作用。

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