Kühl Uwe, Pauschinger Matthias, Schwimmbeck Peter Lothar, Seeberg Bettina, Lober Conny, Noutsias Michel, Poller Wolfgang, Schultheiss Heinz-Peter
Department of Cardiology and Pneumology, University Hospital Benjamin-Franklin, Freie Universität Berlin, Germany.
Circulation. 2003 Jun 10;107(22):2793-8. doi: 10.1161/01.CIR.0000072766.67150.51. Epub 2003 May 27.
Viral infections are important causes of myocarditis and may induce cardiac dysfunction and finally lead to dilated cardiomyopathy. We investigated whether interferon (IFN)-beta therapy is safe and may achieve virus clearance and prevent deterioration of left ventricular (LV) function in patients with myocardial virus persistence.
In this phase II study, 22 consecutive patients with persistence of LV dysfunction (history of symptoms, 44+/-27 months) and polymerase chain reaction-proven enteroviral or adenoviral genomes were treated with 18x10(6) IU/week IFN-beta (Beneferon) subcutaneously for 24 weeks. Histological and immunohistological analysis of endomyocardial biopsies was used to characterize myocardial inflammation. LV diameters and ejection fraction were assessed by echocardiography and angiography, respectively. During the treatment period, IFN-beta was well tolerated by all patients. No patient deteriorated. Clearance of viral genomes was observed in 22 of 22 of patients after antiviral therapy. Virus clearance was paralleled by a significant decrease of LV end diastolic and end systolic diameters, decreasing from 59.7+/-11.1 to 56.5+/-10.0 mm (P<0.001) and 43.2+/-13.6 to 39.4+/-12.1 mm (P<0.001), respectively. LV ejection fraction increased from 44.6+/-15.5% to 53.1+/-16.8% (P<0.001).
A 6 months, IFN-beta treatment was safe in patients with myocardial enteroviral or adenoviral persistence and LV dysfunction and resulted in elimination of viral genomes (22 of 22 patients) and improved LV function (15 of 22 patients).
病毒感染是心肌炎的重要病因,可诱发心脏功能障碍并最终导致扩张型心肌病。我们研究了干扰素(IFN)-β治疗对于心肌病毒持续存在的患者是否安全,以及是否能实现病毒清除并预防左心室(LV)功能恶化。
在这项II期研究中,22例连续的左心室功能障碍持续存在(症状病史为44±27个月)且经聚合酶链反应证实存在肠道病毒或腺病毒基因组的患者,接受皮下注射18×10⁶IU/周的IFN-β(倍泰龙)治疗24周。采用心内膜心肌活检的组织学和免疫组织学分析来表征心肌炎症。分别通过超声心动图和血管造影评估左心室直径和射血分数。在治疗期间,所有患者对IFN-β耐受性良好。无患者病情恶化。抗病毒治疗后,22例患者中有22例病毒基因组被清除。病毒清除同时左心室舒张末期和收缩末期直径显著减小,分别从59.7±11.1mm降至56.5±10.0mm(P<0.001)和从43.2±13.6mm降至39.4±12.1mm(P<0.001)。左心室射血分数从44.6±15.5%增至53.1±16.8%(P<0.001)。
对于心肌肠道病毒或腺病毒持续存在且左心室功能障碍的患者,6个月的IFN-β治疗是安全的,可清除病毒基因组(22例患者中有22例)并改善左心室功能(22例患者中有15例)。
