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2'-去甲环鸟苷酸对豚鼠巨细胞病毒感染的影响。

Effect of 2'-nor-cyclic GMP against guinea pig cytomegalovirus infection.

作者信息

Yang Z H, Lucia H L, Tolman R L, Colonno R J, Hsiung G D

机构信息

Department of Laboratory Medicine, Yale University School of Medicine, New Haven, Connecticut 06510.

出版信息

Antimicrob Agents Chemother. 1989 Sep;33(9):1563-8. doi: 10.1128/AAC.33.9.1563.

Abstract

Cyclic phosphate derivative of DHPG, 2'-nor-cGMP [9-[(2-hydroxy-1,3,2-dioxaphosphorinan-5-yl)oxymethyl]-guani ne phosphate-oxide] was evaluated for activity against guinea pig cytomegalovirus (GPCMV) infection in cultured guinea pig embryo cells and in guinea pigs. By virus yield reduction and plaque reduction assays, 2'-nor-cGMP was demonstrated to be 15- to 20-fold more potent against GPCMV infection than its parental drug DHPG. The selectivity index of 2-nor-cGMP was 110, which was 10-fold higher than that of DHPG. In cultured cells, 2'-nor-cGMP attained maximal antiviral activity when added to the cells within 12 h postinfection. In the studies on GPCMV infection in guinea pigs, 2'-nor-cGMP administered subcutaneously once daily (5 mg/kg per day) for 8 days, starting 24 after virus inoculation, significantly suppressed GPCMV infectivity titers in the blood, spleen, lung, and salivary gland during acute infection (10 days postinfection) as compared with sham-treated infected animals. A greater reduction of GPCMV infectivity titers in the salivary gland was noted during chronic infection (i.e., 24 days postinfection). Clinically, splenomegaly and peripheral lymphocytosis were significantly modified as compared with the sham-treated animals (P less than 0.05). The drug, administered at this dosage, was reasonably tolerated by the guinea pigs and showed clinical benefit.

摘要

DHPG的环磷酸衍生物2'-去甲-cGMP [9-[(2-羟基-1,3,2-二氧磷杂环己烷-5-基)氧甲基]-鸟嘌呤磷酸氧化物] 在培养的豚鼠胚胎细胞和豚鼠体内进行了抗豚鼠巨细胞病毒 (GPCMV) 感染活性的评估。通过病毒产量降低和蚀斑减少试验表明,2'-去甲-cGMP对GPCMV感染的效力比其母体药物DHPG高15至20倍。2-去甲-cGMP 的选择性指数为110, 比DHPG高10倍. 在培养细胞中, 感染后12小时内加入2'-去甲-cGMP可获得最大抗病毒活性。在豚鼠GPCMV感染研究中, 从病毒接种后24小时开始, 每天皮下注射一次2'-去甲-cGMP (5mg/kg/天), 持续8天, 与假处理的感染动物相比, 在急性感染期间 (感染后10天),血液、脾脏、肺和唾液腺中的GPCMV感染性滴度显著降低, 在慢性感染期间 (即感染后24天), 唾液腺中的GPCMV感染性滴度降低更为明显。临床上,与假处理的动物相比,脾肿大和外周淋巴细胞增多症得到了显著改善 (P<0.05)。以该剂量给药的药物,豚鼠耐受性良好,并显示出临床益处。

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