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游离或脂质体包裹的利巴韦林用于实验性诱导猫传染性腹膜炎抗病毒治疗的评估。

Evaluation of free or liposome-encapsulated ribavirin for antiviral therapy of experimentally induced feline infectious peritonitis.

作者信息

Weiss R C, Cox N R, Martinez M L

机构信息

Scott-Ritchey Research Center, College of Veterinary Medicine, Auburn University, Alabama 36849.

出版信息

Res Vet Sci. 1993 Sep;55(2):162-72. doi: 10.1016/0034-5288(93)90076-r.

DOI:10.1016/0034-5288(93)90076-r
PMID:8235082
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7131103/
Abstract

Ribavirin, either free in aqueous solution or incorporated into liposomes, was evaluated in 50 specific-pathogen-free kittens after experimental challenge exposure with feline infectious peritonitis virus (FIPV). Ribavirin was administered daily for 10 to 14 days at 16.5 mg kg-1 bodyweight given per os, intramuscularly or intravenously beginning 18 hours after kittens were challenge-exposed with FIPV. All kittens, including ribavirin-treated and untreated kittens, succumbed to FIP. Clinical signs of disease were more severe in the ribavirin-treated kittens and their mean survival times were shortened. The clinical efficacy of free ribavirin given intravenously at a reduced dosage (5.5 mg kg-1 bodyweight) was compared to that of ribavirin incorporated into lecithin-containing liposomes (5 mg kg-1) intravenously. Drugs were given once daily for three consecutive days of each week for three weeks, beginning 18 hours after virus challenge exposure. There was no significant difference either in survival rate or severity of disease between kittens given free ribavirin, liposomal ribavirin or saline only. Because of its intrinsic toxicity and low therapeutic index against FIPV and its marginal antiviral activities in vivo at maximal doses, ribavirin cannot presently be recommended as primary antiviral chemotherapy against FIP.

摘要

在50只无特定病原体的小猫经猫传染性腹膜炎病毒(FIPV)实验性攻击暴露后,对水溶液中游离的或包裹于脂质体中的利巴韦林进行了评估。利巴韦林在小猫经FIPV攻击暴露18小时后开始,以16.5毫克/千克体重的剂量口服、肌肉注射或静脉注射,每日给药10至14天。所有小猫,包括接受利巴韦林治疗和未治疗的小猫,均死于FIP。接受利巴韦林治疗的小猫疾病临床症状更严重,平均存活时间缩短。将静脉注射较低剂量(5.5毫克/千克体重)的游离利巴韦林的临床疗效与静脉注射包裹于含卵磷脂脂质体中的利巴韦林(5毫克/千克)的临床疗效进行了比较。在病毒攻击暴露18小时后开始,每周连续三天每天给药一次,共给药三周。接受游离利巴韦林、脂质体利巴韦林或仅接受生理盐水的小猫在存活率或疾病严重程度方面均无显著差异。由于利巴韦林具有内在毒性、对FIPV的治疗指数低以及在最大剂量下体内抗病毒活性有限,目前不能推荐将其作为抗FIP的主要抗病毒化疗药物。

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