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α-肌球蛋白重链cDNA结构及在成年、胎儿和早产狒狒心肌中的基因表达。

Alpha-myosin heavy chain cDNA structure and gene expression in adult, fetal, and premature baboon myocardium.

作者信息

Hixson J E, Henkel R D, Britten M L, Vernier D T, deLemos R A, VandeBerg J L, Walsh R A

机构信息

Department of Genetics, Southwest Foundation for Biomedical Research, San Antonio, TX 78284.

出版信息

J Mol Cell Cardiol. 1989 Oct;21(10):1073-86. doi: 10.1016/0022-2828(89)90805-5.

Abstract

To examine cardiac myosin gene structure and expression in a non-human primate model for human heart development and disease, we have constructed a cDNA library from baboon atrium and used baboon beta-myosin heavy chain (beta-MHC)* cDNA probes to isolate atrial MHC clones. The nucleotide sequence of one such clone, lambda BMHC alpha 3, contains sequences that encode part of the light meromyosin region (LMM) and the 3' untranslated region of the baboon alpha-MHC. To study cardiac MHC gene transcription, we constructed probes from the baboon alpha-MHC cDNA for S1 nuclease analyses of RNA from atria and ventricles. To examine translational regulation of cardiac MHC gene expression, we used monoclonal antibodies (MAb) against specific alpha- and beta-MHC epitopes for Western blot analyses. In atria and ventricles from adult baboons, we detected predominantly alpha- and beta-MHC gene transcripts, respectively. In ventricles from fetal baboons at two stages of development (140 and 160 days gestation), we also detected predominantly beta-MHC gene transcripts and isoforms. To investigate changes induced by parturition, we obtained ventricles from baboons that were prematurely delivered at 140 days gestation and supported for 10 days in an extrauterine environment. In contrast to adult and fetal patterns, we observed an increase in alpha-MHC transcripts and isoforms in ventricles of premature baboons. Because alpha-MHC gene expression is increased in premature baboons (total age of 150 days) compared to their older 160 day fetal counterparts, the induction of ventricular alpha-MHC synthesis must have resulted from factor(s) associated with parturition or prolonged mechanical ventilation rather than at predetermined stages of gestational development.

摘要

为了在人类心脏发育和疾病的非人类灵长类动物模型中研究心肌肌球蛋白基因结构和表达,我们构建了一个来自狒狒心房的cDNA文库,并使用狒狒β - 肌球蛋白重链(β - MHC)* cDNA探针分离心房MHC克隆。其中一个这样的克隆,λBMHCα3的核苷酸序列,包含编码轻酶解肌球蛋白区域(LMM)部分序列以及狒狒α - MHC的3'非翻译区。为了研究心脏MHC基因转录,我们从狒狒α - MHC cDNA构建探针,用于对心房和心室RNA进行S1核酸酶分析。为了检查心脏MHC基因表达的翻译调控,我们使用针对特定α - 和β - MHC表位的单克隆抗体(MAb)进行蛋白质印迹分析。在成年狒狒的心房和心室中,我们分别主要检测到α - 和β - MHC基因转录本。在发育两个阶段(妊娠140天和160天)的胎儿狒狒心室中,我们也主要检测到β - MHC基因转录本和异构体。为了研究分娩引起的变化,我们从妊娠140天早产并在子宫外环境中维持10天的狒狒获取心室。与成年和胎儿模式相反,我们观察到早产狒狒心室中α - MHC转录本和异构体增加。由于与160天胎龄的较大胎儿相比,早产狒狒(总年龄150天)的α - MHC基因表达增加,心室α - MHC合成的诱导必定是由与分娩或长时间机械通气相关的因素引起的,而不是妊娠发育的预定阶段。

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