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EFFECT OF VERAPAMIL ONCa^(2+) INFLUX ANDCVB3-RNA REPLICATION IN CULTURED NEONATALRAT HEART CELLS INFECTED WITH CVB3

EFFECT OF VERAPAMIL ON Ca ̄(2+) INFLUX AND CVB3-RNA REPLICATION IN CULTURED NEONATAL RAT HEART CELLS INFECTED WITH CVB3
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摘要 The effect of verapamil on Ca2+ influx across the myocardial plasma membrane and coxsackie virus B3 ( CVB3)-RNA replication in cultured neonatal rat heart cells infected with CVB3 was investigated. It was found that the Ca2+ influx could be inhibited significantly (P<O. 01) by verapamil (1 μmol/L) after infection of heart cells for 48h. However, when the cultured heart cells infected with CVB3 and treated with verapamil (Iμmol/L and 10 nmo/L) at the same time for 48h, the amounts of CVB3-RNA in myocytes were significantly higher than that in infected control group (P<O. 05). These phenomena suggest that the increase of Ca2+ influx of cultured heart cells infected with CVB3 could be inhibited by some calcium antagonists, e. g. verapamil at the early stage. On the other hand, verapamil might accelerate viral replication in myocardium. Thus, although verapamil could be beneficial for decreasing the secondary Ca2+ damages and improve the myocardial electric activity, it isn’t a sensible choice for therapy in early stage of virus infection with cardiac symptoms.
出处 《Chinese Medical Sciences Journal》 CAS CSCD 1996年第2期89-92,共4页 中国医学科学杂志(英文版)
关键词 coxsackie virus B_3 VERAPAMIL Ca ̄(2+) influx 异博定 钙离子 细胞培养 柯萨奇病毒B3 新生儿感染 动物实验
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