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新生大鼠心室细胞α-肾上腺素能刺激过程中心房利钠因子和心肌肌球蛋白轻链-2基因的共同调控。鉴定胚胎期和组成型收缩蛋白基因中介导诱导性表达的顺式序列。

Co-regulation of the atrial natriuretic factor and cardiac myosin light chain-2 genes during alpha-adrenergic stimulation of neonatal rat ventricular cells. Identification of cis sequences within an embryonic and a constitutive contractile protein gene which mediate inducible expression.

作者信息

Knowlton K U, Baracchini E, Ross R S, Harris A N, Henderson S A, Evans S M, Glembotski C C, Chien K R

机构信息

Department of Medicine, University of California, San Diego, La Jolla 92093.

出版信息

J Biol Chem. 1991 Apr 25;266(12):7759-68.

PMID:1850419
Abstract

To study the mechanisms which mediate the transcriptional activation of cardiac genes during alpha adrenergic stimulation, the present study examined the regulated expression of three cardiac genes, a ventricular embryonic gene (atrial natriuretic factor, ANF), a constitutively expressed contractile protein gene (cardiac MLC-2), and a cardiac sodium channel gene. alpha 1-Adrenergic stimulation activates the expression and release of ANF from neonatal ventricular cells. As assessed by RNase protection analyses, treatment with alpha-adrenergic agonists increases the steady-state levels of ANF mRNA by greater than 15-fold. However, a rat cardiac sodium channel gene mRNA is not induced, indicating that alpha-adrenergic stimulation does not lead to an increase in the expression of all cardiac genes. Studies employing a series of rat ANF luciferase and rat MLC-2 luciferase fusion genes identify 315- and 92-base pair cis regulatory sequences within an embryonic gene (ANF) and a constitutively expressed contractile protein gene (MLC-2), respectively, which mediate alpha-adrenergic-inducible gene expression. Transfection of various ANF luciferase reporters into neonatal rat ventricular cells demonstrated that upstream sequences which mediate tissue-specific expression (-3003 to -638) can be segregated from those responsible for inducibility. The lack of inducibility of a cardiac Na+ channel gene, and the segregation of ANF gene sequences which mediate cardiac specific from those which mediate inducible expression, provides further insight into the relationship between muscle-specific and inducible expression during cardiac myocyte hypertrophy. Based on these results, a testable model is proposed for the induction of embryonic cardiac genes and constitutively expressed contractile protein genes and the noninducibility of a subset of cardiac genes during alpha-adrenergic stimulation of neonatal rat ventricular cells.

摘要

为了研究在α肾上腺素能刺激过程中介导心脏基因转录激活的机制,本研究检测了三个心脏基因的表达调控,一个心室胚胎基因(心房利钠因子,ANF)、一个组成性表达的收缩蛋白基因(心脏肌球蛋白轻链-2,cardiac MLC-2)和一个心脏钠通道基因。α1肾上腺素能刺激可激活新生心室细胞中ANF的表达和释放。通过核糖核酸酶保护分析评估,用α肾上腺素能激动剂处理可使ANF mRNA的稳态水平增加超过15倍。然而,大鼠心脏钠通道基因mRNA未被诱导,这表明α肾上腺素能刺激不会导致所有心脏基因的表达增加。采用一系列大鼠ANF荧光素酶和大鼠MLC-2荧光素酶融合基因的研究分别在一个胚胎基因(ANF)和一个组成性表达的收缩蛋白基因(MLC-2)中鉴定出315和92个碱基对的顺式调控序列,这些序列介导α肾上腺素能诱导的基因表达。将各种ANF荧光素酶报告基因转染到新生大鼠心室细胞中表明,介导组织特异性表达的上游序列(-3003至-638)可与负责诱导性的序列分开。心脏Na+通道基因缺乏诱导性,以及介导心脏特异性的ANF基因序列与介导诱导性表达的序列分开,这为心肌细胞肥大期间肌肉特异性表达和诱导性表达之间的关系提供了进一步的见解。基于这些结果,提出了一个可测试的模型,用于解释新生大鼠心室细胞在α肾上腺素能刺激期间胚胎心脏基因和组成性表达的收缩蛋白基因的诱导以及一部分心脏基因的非诱导性。

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