Kucerova Dana, Doka Gabriel, Kruzliak Peter, Turcekova Katarina, Kmecova Jana, Brnoliakova Zuzana, Kyselovic Jan, Kirchhefer Uwe, Müller Frank U, Krenek Peter, Boknik Peter, Klimas Jan
Department of Pharmacology and Toxicology, Faculty of Pharmacy, Comenius University Bratislava, Slovak Republic ; Institut für Pharmakologie und Toxikologie, Universitätsklinikum Münster Münster, Germany.
Department of Pharmacology and Toxicology, Faculty of Pharmacy, Comenius University Bratislava, Slovak Republic.
Am J Transl Res. 2015 Jul 15;7(7):1280-94. eCollection 2015.
Calcium release channel on the sarcoplasmic reticulum of cardiomyocytes (ryanodine receptor type 2, RyR2) plays a critical role in the regulation of calcium and was identified as a crucial factor for development of chronic anthracycline cardiomyopathy. Its early stages are less well described although these determine the later development. Hence, we tested the effect of repeated, short-term anthracycline (daunorubicin) administration on cardiac performance, cardiomyocyte function and accompanied changes in calcium regulating proteins expression. Ten-twelve weeks old male Wistar rats were administered with 6 doses of daunorubicin (DAU, 3 mg/kg, i.p., every 48 h), controls (CON) received vehicle. Left ventricular function (left ventricular pressure, LVP; rate of pressure development, +dP/dt and decline, -dP/dt) was measured using left ventricular catheterization under tribromethanol anaesthesia (15 ml/kg b.w.). Cell shortening was measured in enzymatically isolated cardiomyocytes. The expressions of RyR2 and associated intracellular calcium regulating proteins, cytoskeletal proteins (alpha-actinin, alpha-tubul in) as well as oxidative stress regulating enzymes (gp91phox, MnSOD) were detected in ventricular tissue samples using immunoblotting. mRNA expressions of cardiac damage markers (Nppa and Nppb, atrial and brain natriuretic peptides; Myh6, Myh7 and Myh7b, myosin heavy chain alpha and beta) were detected using RT-PCR. Thiobarbituric acid reactive substances concentration was measured to estimate oxidative stress. DAU rats exhibited significantly depressed left ventricular features (LVP by 14%, +dP/dt by 36% and -dP/dt by 30%; for all P<0.05), in line with concomitant increase in Nppa and Nppb gene expressions (3.23- and 2.18-fold, for both P<0.05), and a 4.34-fold increase in Myh7 (P<0.05). Controversially, we observed increased cell shortening of isolated cardiac cells by 31% (p<0.05). DAU administration was associated with a twofold upregulation of RyR2 (P<0.05), but not of other examined Ca(2+) regulating proteins remained. In addition, we observed a significant reduction in alpha-tubulin (by 46% when compared to CON P<0.05). Indicators of oxidative injury were unaffected. In conclusion, unbalanced RyR2 overexpression plays a particular role in early development of daunorubicin cardiomyopathy characterized by discrepant in situ versus in vitro cardiac performance.
心肌细胞肌浆网上的钙释放通道(2型兰尼碱受体,RyR2)在钙调节中起关键作用,并且被确定为慢性蒽环类药物性心肌病发展的关键因素。尽管其早期阶段决定了后期发展,但对其描述较少。因此,我们测试了重复短期给予蒽环类药物(柔红霉素)对心脏功能、心肌细胞功能以及钙调节蛋白表达伴随变化的影响。10 - 12周龄雄性Wistar大鼠接受6剂柔红霉素(DAU,3 mg/kg,腹腔注射,每48小时一次),对照组(CON)接受溶剂。在三溴乙醇麻醉(15 ml/kg体重)下通过左心室插管测量左心室功能(左心室压力,LVP;压力上升速率,+dP/dt和下降速率,-dP/dt)。在酶分离的心肌细胞中测量细胞缩短。使用免疫印迹法在心室组织样本中检测RyR2及相关细胞内钙调节蛋白、细胞骨架蛋白(α - 辅肌动蛋白、α - 微管蛋白)以及氧化应激调节酶(gp91phox、MnSOD)的表达。使用RT - PCR检测心脏损伤标志物(Nppa和Nppb,心房钠尿肽和脑钠尿肽;Myh6、Myh7和Myh7b,肌球蛋白重链α和β)的mRNA表达。测量硫代巴比妥酸反应性物质浓度以评估氧化应激。DAU大鼠表现出明显的左心室功能降低(LVP降低14%,+dP/dt降低36%,-dP/dt降低30%;所有P < 0.05),同时Nppa和Nppb基因表达增加(分别增加3.23倍和2.18倍,两者P < 0.05),Myh7增加4.34倍(P < 0.05)。与之相反,我们观察到分离的心肌细胞的细胞缩短增加了31%(p < 0.05)。给予DAU与RyR2上调两倍相关(P < 0.05),但其他检测的Ca(2+)调节蛋白未上调。此外,我们观察到α - 微管蛋白显著减少(与CON相比降低46%,P < 0.05)。氧化损伤指标未受影响。总之,RyR2表达失衡在柔红霉素心肌病的早期发展中起特殊作用,其特征是原位与体外心脏功能存在差异。
