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严重慢性二尖瓣反流患者心肌钙处理蛋白表达降低。

Reduced myocardial expression of calcium handling protein in patients with severe chronic mitral regurgitation.

作者信息

Leszek Przemysław, Korewicki Jerzy, Klisiewicz Anna, Janas Jadwiga, Biederman Andrzej, Browarek Aldona, Charlemagne Danièle, Trouvé Pascal

机构信息

Institute of Cardiology, Alpejska 42 St., 04-628 Warsaw, Poland.

出版信息

Eur J Cardiothorac Surg. 2006 Nov;30(5):737-43. doi: 10.1016/j.ejcts.2006.07.008. Epub 2006 Sep 22.

Abstract

OBJECTIVE

Left ventricle (LV) function was shown to be a principal determinant of morbidity and mortality in both uncorrected and surgically corrected mitral regurgitation (MR). However, the cellular mechanisms that develop in the LV remodeling secondary to volume overload in chronic severe MR is still not well defined. In single ventricular myocyte, a reduced contraction and slowed relaxation have been mainly attributed to defective intracellular Ca2+ currents. Between several Ca2+ handling proteins, sarcoplasmic reticulum Ca2+-ATPase 2 (SERCA2) expression and activity determines not only the extent and rate of relaxation, but also the rate and amplitude of contraction. The aim of the study was to determine whether modifications of SERCA2 gene expression occurs in LV wall remodeling process secondary to chronic severe MR.

METHODS

The LV samples were obtained from 12 patients presented LV wall remodeling (LV: diastolic/systolic diameter-70+/-7 mm vs 46+/-10 mm; diastolic/systolic volume-260+/-65 ml vs 102+/-68 ml) due to chronic, severe MR. Expressions of SERCA2 isoforms-SERCA2a and 2b mRNAs were estimated by semiquantitative RT-PCR and normalized to GAPDH. The protein levels of SERCA2 were determined by Western blot after normalization to actin. Results were compared with samples from non-failing human hearts (NFH).

RESULTS

On SERCA2 mRNA levels, important reduction on both SERCA isoforms SERCA2a (-40%) and SERCA2b (-49%) compared to NFH, together with significant correlation between isoforms (r = 0.89; p = 0.01) were observed. SERCA2 protein levels were decreased (-38%) in MR compared to NFH. Also significant correlations between SERCA2a/2b and SERCA2 protein expression (r = 0.83, p = 0.017; r = 0.68, p = 0.05, respectively) were observed. Moreover, a negative correlation between protein levels of SERCA2 (r = -0.64, p = 0.053) and left ventricular diastolic diameter was observed.

CONCLUSIONS

In chronic volume overload the down-regulation of SERCA2a and 2b at the mRNA and SERCA2 protein levels exist. Moreover, protein levels of SERCA2 tend to correlate to the grade of left ventricular diastolic dilatation and suggest an important role LV remodeling.

摘要

目的

左心室(LV)功能被证明是未矫正和手术矫正二尖瓣反流(MR)患者发病率和死亡率的主要决定因素。然而,慢性重度MR容量超负荷继发左心室重构时所发生的细胞机制仍未完全明确。在单个心室肌细胞中,收缩减弱和舒张减慢主要归因于细胞内钙电流缺陷。在几种钙处理蛋白中,肌浆网钙ATP酶2(SERCA2)的表达和活性不仅决定舒张的程度和速率,还决定收缩的速率和幅度。本研究的目的是确定慢性重度MR继发左心室壁重构过程中是否发生SERCA2基因表达的改变。

方法

从12例因慢性重度MR出现左心室壁重构(左心室:舒张末期/收缩末期直径 - 70±7mm对46±10mm;舒张末期/收缩末期容积 - 260±65ml对102±68ml)的患者获取左心室样本。通过半定量逆转录聚合酶链反应(RT-PCR)评估SERCA2亚型(SERCA2a和2b mRNA)的表达,并以甘油醛-3-磷酸脱氢酶(GAPDH)进行标准化。以肌动蛋白进行标准化后,通过蛋白质印迹法测定SERCA2的蛋白水平。将结果与非衰竭人心脏(NFH)样本进行比较。

结果

在SERCA2 mRNA水平上,与NFH相比,两种SERCA亚型SERCA2a(-40%)和SERCA2b(-49%)均有显著降低,并且亚型之间存在显著相关性(r = 0.89;p = 0.01)。与NFH相比,MR中SERCA2蛋白水平降低(-38%)。还观察到SERCA2a/2b与SERCA2蛋白表达之间存在显著相关性(分别为r = 0.83,p = 0.017;r = 0.68,p = 0.05)。此外,观察到SERCA2蛋白水平与左心室舒张末期直径之间存在负相关(r = -0.64,p = 0.053)。

结论

在慢性容量超负荷时,存在SERCA2a和2b在mRNA及SERCA2蛋白水平的下调。此外,SERCA2蛋白水平倾向于与左心室舒张期扩张程度相关,并提示其在左心室重构中起重要作用。

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