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环孢素对急性小鼠柯萨奇B3病毒性心肌炎的影响。

The effects of cyclosporine on acute murine Coxsackie B3 myocarditis.

作者信息

O'Connell J B, Reap E A, Robinson J A

出版信息

Circulation. 1986 Feb;73(2):353-9. doi: 10.1161/01.cir.73.2.353.

Abstract

The effects of the immunosuppressant drug cyclosporine were studied in the murine model of Coxsackie B3 myocarditis. Ten BALB/c mice, given daily cyclosporine (15 mg/kg) intraperitoneally but not infected, were normal in all respects after 2 weeks. All 32 BALB/c mice infected, but given no cyclosporine, survived and had moderate myocardial mononuclear infiltrates and minimal necrosis at 7 and 14 days. In contrast, 24 mice concurrently infected and given cyclosporine had a high mortality rate (75%) and a significantly attenuated mononuclear infiltrate in the presence of enhanced necrosis when compared with control infected mice. Sixteen mice started on the drug 1 week after infection had a lower mortality rate (55%), but very similar histologic abnormalities. In contrast to negligible or no virus in the hearts of infected mice that were not given cyclosporine, drug treated, infected groups had easily detectable virus in their hearts 14 days after infection. An identical study in Swiss ICR mice yielded similar results. Cyclosporine, when given early during acute murine Coxsackie B3 myocarditis, causes a significant increase in myocardial necrosis and mortality, possibly secondary to enhanced viral survival.

摘要

在柯萨奇B3型心肌炎的小鼠模型中研究了免疫抑制剂环孢素的作用。10只BALB/c小鼠每天腹腔注射环孢素(15毫克/千克)但未感染,2周后在各方面均正常。所有32只感染但未给予环孢素的BALB/c小鼠存活,在第7天和第14天有中度心肌单核细胞浸润和最小程度的坏死。相比之下,与对照感染小鼠相比,24只同时感染并给予环孢素的小鼠死亡率高(75%),在坏死增强的情况下单核细胞浸润明显减弱。16只在感染后1周开始用药的小鼠死亡率较低(55%),但组织学异常非常相似。与未给予环孢素的感染小鼠心脏中病毒可忽略不计或没有病毒不同,药物治疗的感染组在感染后14天心脏中病毒易于检测到。在瑞士ICR小鼠中进行的一项相同研究得出了类似结果。在急性小鼠柯萨奇B3型心肌炎早期给予环孢素会导致心肌坏死和死亡率显著增加,可能继发于病毒存活增强。

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