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Fluoxetine can inhibit coxsackievirus-B4 E2 in vitro and in vivo

机译:氟西汀可以在体外和体内抑制Coxsackievirus-B4 e2

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Group B Coxsackieviruses (CV-B) are responsible for various acute human diseases, and they are involved in chronic diseases such as type 1 diabetes. It has been reported that fluoxetine (FLX) inhibited CV-B4E2 in human cell linesin vitro. In so far as CV-B4E2 can replicate in CD1 mice, it was investigated whether FLX could inhibit CV-B4E2in vitroandin vivoin mouse systems. When 5.5?μM FLX was added to CV-B4E2-infected Min-6?cell (murine pancreas beta cell line) cultures, the virus-induced cytopathic effect was inhibited. In this system and in CV-B4E2-infected CD1 mouse pancreatic organotypic cultures treated with FLX the levels of infectious particles in supernatant fluids were below the limit of detection of the assay. The administration of FLX (10?mg/kg/day) by intraperitoneal route resulted in significant reduced levels of infectious particles in heart and pancreas of mice inoculated with CV-B4E2 by the same route. In conclusion FLX can inhibit CV-B4in vitroandin vivoin mouse systems, additional studies are needed to investigate further the potential value of FLX to combat CV-B4 infections and to treat CV-B4-induced diseases.
机译:B组CoxSackeigiruses(CV-B)负责各种急性人类疾病,它们参与慢性疾病,如1型糖尿病。据报道,氟西汀(FLX)抑制人细胞系中的CV-B4E2。除了CV-B4E2可以在CD1小鼠中复制,研究了FLX是否可以抑制CV-B4E2IN VIVOIN小鼠系统。当加入5.5?μmflx到CV-B4E2感染的MIN-6?细胞(鼠胰腺β细胞系)培养物中,抑制病毒引起的细胞病变效应。在该系统中和在CV-B4E2感染的CD1小鼠胰腺有机型培养物中,用FLX处理的上清液中的传染性颗粒的水平低于测定的检测限。通过腹膜内途径给予FLX(10?Mg / kg /天)导致心脏病和用CV-B4E2接种的小鼠的感染性颗粒水平显着降低。总之,FLX可以抑制CV-B4IN VITRAANDIN小鼠体系,需要额外的研究来研究FLX对抗CV-B4感染和治疗CV-B4诱导疾病的潜在价值。

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