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糖尿病大鼠心脏中肌酸激酶-M和肌酸激酶-B mRNA的胰岛素反应性。

Insulin responsiveness of CK-M and CK-B mRNA in the diabetic rat heart.

作者信息

Popovich B K, Sayen M R, Dillmann W H

机构信息

Department of Medicine, University of California, San Diego 92103.

出版信息

Am J Physiol. 1991 Sep;261(3 Pt 1):E377-81. doi: 10.1152/ajpendo.1991.261.3.E377.

DOI:10.1152/ajpendo.1991.261.3.E377
PMID:1887884
Abstract

Decreased cardiac performance is a known complication of diabetes mellitus, but the detailed molecular mechanisms that are responsible for this contractile abnormality are only incompletely explored, and cardiac gene products of known function, which are markedly and actively insulin responsive, have not been described. Recently, we found that creatine kinase (CK) enzyme activity and CK-M subunit mRNA levels are decreased in the heart of rats with experimental diabetes mellitus. These abnormalities could be restored to normal with chronic insulin administration. The CK-M and CK-B genes are expressed in the heart, and we wanted to determine whether diabetes also induces a change in CK-B mRNA levels. Quantitation of CK-M and CK-B mRNA levels on Northern blots with specific cDNA probes showed that, in diabetic hearts, CK-B mRNA levels represent only 19.8% of control levels and are more markedly depressed than CK-M mRNA levels, which are 46.5% of control values. Acute injection of insulin led to a significant 1.6-fold increase in CK-M mRNA and a 2.2-fold increase of CK-B mRNA 5 h after insulin injection. CK-M mRNA levels were restored to normal within 12 h, but 48 h were required to restore CK-B mRNA levels to normal values. After 1 mo of insulin therapy, CK-B mRNA levels had risen 9.7-fold, exceeding normal values by 90%, whereas CK-M mRNA levels were at the normal level as previously shown. CK enzyme activity showed only a small response to insulin administration 48 h postinjection. Diabetes leads therefore to a marked lowering of CK-M and CK-B mRNA levels in the rat heart.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

心脏功能下降是糖尿病已知的并发症,但导致这种收缩异常的详细分子机制仅得到部分探索,且尚未描述具有明显且活跃的胰岛素反应性的已知功能的心脏基因产物。最近,我们发现实验性糖尿病大鼠心脏中的肌酸激酶(CK)酶活性和CK-M亚基mRNA水平降低。长期给予胰岛素可使这些异常恢复正常。CK-M和CK-B基因在心脏中表达,我们想确定糖尿病是否也会引起CK-B mRNA水平的变化。用特异性cDNA探针在Northern印迹上对CK-M和CK-B mRNA水平进行定量分析表明,在糖尿病心脏中,CK-B mRNA水平仅为对照水平的19.8%,且比CK-M mRNA水平(为对照值的46.5%)更显著降低。急性注射胰岛素导致注射后5小时CK-M mRNA显著增加1.6倍,CK-B mRNA增加2.2倍。CK-M mRNA水平在12小时内恢复正常,但CK-B mRNA水平恢复到正常水平需要48小时。胰岛素治疗1个月后,CK-B mRNA水平升高了9.7倍,超过正常值90%,而CK-M mRNA水平如前所示处于正常水平。注射后48小时,CK酶活性对胰岛素给药仅表现出轻微反应。因此,糖尿病导致大鼠心脏中CK-M和CK-B mRNA水平显著降低。(摘要截短于250字)

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Insulin responsiveness of CK-M and CK-B mRNA in the diabetic rat heart.糖尿病大鼠心脏中肌酸激酶-M和肌酸激酶-B mRNA的胰岛素反应性。
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