肠道病毒蛋白酶2A的诱导性心脏限制性表达足以诱发扩张型心肌病。

Inducible cardiac-restricted expression of enteroviral protease 2A is sufficient to induce dilated cardiomyopathy.

作者信息

Xiong Dingding, Yajima Toshitaka, Lim Byung-Kwan, Stenbit Antine, Dublin Andrew, Dalton Nancy D, Summers-Torres Daphne, Molkentin Jeffery D, Duplain Herve, Wessely Rainer, Chen Ju, Knowlton Kirk U

机构信息

University of California, San Diego, Department of Medicine, 9500 Gilman Dr, La Jolla, CA 92093, USA.

出版信息

Circulation. 2007 Jan 2;115(1):94-102. doi: 10.1161/CIRCULATIONAHA.106.631093. Epub 2006 Dec 26.

DOI:10.1161/CIRCULATIONAHA.106.631093

PMID:17190866

Abstract

BACKGROUND

Enterovirus infection is a cause of cardiomyopathy. We previously demonstrated that enteroviral protease 2A directly cleaves the cytoskeletal protein dystrophin. However, the direct effect of protease 2A in enteroviral cardiomyopathy is less clear because other viral proteins are also expressed with viral infection.

METHODS AND RESULTS

A transgenic mouse with inducible cardiac-restricted expression of enteroviral protease 2A was generated. In the transgenic mouse, a tamoxifen-regulated Cre-loxP system, MerCreMer (MCM), was used to induce genetic recombination in cardiac myocytes, which led to protease 2A expression. Protease 2A and MCM double transgenic (2AxMCM) mice were treated with tamoxifen; the controls included 2AxMCM mice treated with diluents for tamoxifen and tamoxifen-treated MCM littermates. Protease 2A activity was significantly induced after tamoxifen in the 2AxMCM mice compared with controls. Echocardiographic analysis demonstrated an increase in left ventricular end-diastolic and end-systolic chamber size, with decreased fractional shortening in tamoxifen-treated 2AxMCM mice. There was an increase in heart weight-to-body weight ratio in 2AxMCM mice treated with tamoxifen. Only a small increase in interstitial fibrosis and inflammation was found in tamoxifen-treated 2AxMCM mice; however, ultrastructural analysis demonstrated myofibrillar collapse with abnormalities of intercalated discs and sarcolemmal membranes. Evans blue dye-positive myocytes with disruption of dystrophin were present in 2AxMCM mice treated with tamoxifen. Disruption of dystrophin was also found in cultured myocytes isolated from 2AxMCM mice with Cre in the nucleus.

CONCLUSIONS

Protease 2A has a significant role in enteroviral cardiomyopathy and alone is sufficient to induce dilated cardiomyopathy, which is associated with disruption of the sarcolemmal membrane and cleavage of dystrophin with protease 2A expression.

摘要

背景

肠道病毒感染是心肌病的一个病因。我们之前证明肠道病毒蛋白酶2A可直接切割细胞骨架蛋白肌营养不良蛋白。然而，蛋白酶2A在肠道病毒性心肌病中的直接作用尚不清楚，因为病毒感染时其他病毒蛋白也会表达。

方法与结果

构建了一种可诱导心脏特异性表达肠道病毒蛋白酶2A的转基因小鼠。在转基因小鼠中，使用他莫昔芬调节的Cre-loxP系统MerCreMer（MCM）在心肌细胞中诱导基因重组，从而导致蛋白酶2A表达。对蛋白酶2A和MCM双转基因（2AxMCM）小鼠给予他莫昔芬治疗；对照组包括用他莫昔芬稀释剂治疗的2AxMCM小鼠和接受他莫昔芬治疗的MCM同窝小鼠。与对照组相比，他莫昔芬处理后2AxMCM小鼠的蛋白酶2A活性显著诱导。超声心动图分析显示，接受他莫昔芬治疗的2AxMCM小鼠左心室舒张末期和收缩末期内径增加，缩短分数降低。接受他莫昔芬治疗的2AxMCM小鼠心脏重量与体重之比增加。在接受他莫昔芬治疗的2AxMCM小鼠中仅发现间质纤维化和炎症有少量增加；然而，超微结构分析显示肌原纤维崩溃，伴有闰盘和肌膜异常。接受他莫昔芬治疗的2AxMCM小鼠中存在伊文思蓝染料阳性且肌营养不良蛋白破坏的心肌细胞。在细胞核中有Cre的2AxMCM小鼠分离的培养心肌细胞中也发现了肌营养不良蛋白的破坏。