外用R-837治疗生殖器HSV-2感染期间免疫反应和临床疾病的改变。
Modification of immunological responses and clinical disease during topical R-837 treatment of genital HSV-2 infection.
作者信息
Harrison C J, Jenski L, Voychehovski T, Bernstein D I
机构信息
Children's Hospital Research Foundation, Children's Hospital Medical Center, Cincinnati, Ohio 45229-2899.
出版信息
Antiviral Res. 1988 Dec 1;10(4-5):209-23. doi: 10.1016/0166-3542(88)90032-0.
R-837, a compound with no in vitro anti-HSV activity, was administered intravaginally to guinea pigs (5 mg/kg every 12 h) for five days beginning 12 h after genital HSV-2 inoculation. Drug treatment reduced vaginal viral replication (P less than 0.0001), completely protected against primary disease and reduced recurrent genital HSV disease (P less than 0.0001). Drug treatment also induced mild fever, weight loss, and decreased water intake. R-837 was a potent interferon inducer, which also induced variable enhancement of cell-mediated cytolytic activity against HSV-2 targets. Less than 36 h of vaginal HSV shedding was observed in animals with R-837 induced early enhancement of HSV-target cytolysis. Compared to placebo, R-837 decreased ELISA and ADCC antibody to HSV-2, but accelerated HSV-2 specific in vitro IL-2 production and peripheral blood mononuclear cell (PBMC) proliferation. R-837 exhibited potent anti-HSV activity in vivo apparently due to cytokine induction and enhancement of cell-mediated responses.
R - 837是一种在体外无抗单纯疱疹病毒(HSV)活性的化合物,在豚鼠生殖器接种HSV - 2后12小时开始,连续五天经阴道给予豚鼠(每12小时5毫克/千克)。药物治疗减少了阴道病毒复制(P小于0.0001),完全预防了原发性疾病,并减少了复发性生殖器HSV疾病(P小于0.0001)。药物治疗还引起了轻度发热、体重减轻和饮水量减少。R - 837是一种有效的干扰素诱导剂,它还能不同程度地增强针对HSV - 2靶标的细胞介导的细胞溶解活性。在R - 837诱导HSV靶标细胞溶解早期增强的动物中,观察到阴道HSV脱落少于36小时。与安慰剂相比,R - 837降低了针对HSV - 2的ELISA和ADCC抗体,但加速了HSV - 2特异性体外白细胞介素 - 2的产生和外周血单核细胞(PBMC)的增殖。R - 837在体内表现出强大的抗HSV活性,这显然归因于细胞因子诱导和细胞介导反应的增强。
Zotero 插件