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In Vivo Anti-Herpes Simplex Virus Activity of a Sulfated Derivative of Agaricus brasiliensis Mycelial Polysaccharide

机译:巴西姬松茸菌丝体多糖硫酸盐衍生物的体内抗疱疹单纯疱疹病毒活性

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摘要

Agaricus brasiliensis (syn. A. subrufescens), a basidiomycete fungus native to the Atlantic forest in Brazil, contains cell walls rich in glucomannan polysaccharides. The β-(1→2)-gluco-β-(1→3)-mannan was isolated from A. brasiliensis mycelium, chemically modified by sulfation, and named MI-S. MI-S has multiple mechanisms of action, including inhibition of herpes simplex virus (HSV) attachment, entry, and cell-to-cell spread (F. T. G. S. Cardozo, C. M. Camelini, A. Mascarello, M. J. Rossi, R. J. Nunes, C. R. Barardi, M. M. de Mendonça, and C. M. O. Simões, Antiviral Res. 92:108–114, 2011). The antiherpetic efficacy of MI-S was assessed in murine ocular, cutaneous, and genital infection models of HSV. Groups of 10 mice were infected with HSV-1 (strain KOS) or HSV-2 (strain 333). MI-S was given either topically or by oral gavage under various pre- and posttreatment regimens, and the severity of disease and viral titers in ocular and vaginal samples were determined. No toxicity was observed in the uninfected groups treated with MI-S. The topical and oral treatments with MI-S were not effective in reducing ocular disease. Topical application of MI-S on skin lesions was also not effective, but cutaneously infected mice treated orally with MI-S had significantly reduced disease scores (P < 0.05) after day 9, suggesting that healing was accelerated. Vaginal administration of MI-S 20 min before viral challenge reduced the mean disease scores on days 5 to 9 (P < 0.05), viral titers on day 1 (P < 0.05), and mortality (P < 0.0001) in comparison to the control groups (untreated and vehicle treated). These results show that MI-S may be useful as an oral agent to reduce the severity of HSV cutaneous and mucosal lesions and, more importantly, as a microbicide to block sexual transmission of HSV-2 genital infections.
机译:巴西姬松茸(A. subrufescens)是一种原产于巴西大西洋森林的担子菌真菌,其细胞壁富含葡甘露聚糖。 β-(1→2)-葡萄糖-β-(1→3)-甘露聚糖是从巴西曲霉菌丝体中分离出来的,经硫酸化化学修饰后命名为MI-S。 MI-S具有多种作用机制,包括抑制单纯疱疹病毒(HSV)附着,进入和细胞间扩散(FTGS Cardozo,CM Camelini,A。Mascarello,MJ Rossi,RJ Nunes,CR Barardi,MM deMendonça和CMOSimões,Antiviral Res。92:108–114,2011年)。在HSV的鼠眼,皮肤和生殖器感染模型中评估了MI-S的抗疱疹功效。将每组10只小鼠感染HSV-1(KOS株)或HSV-2(333株)。在不同的治疗前和治疗后,通过局部或口服强饲法给予MI-S,并测定眼和阴道样品中疾病的严重程度和病毒滴度。在用MI-S治疗的未感染组中未观察到毒性。 MI-S的局部和口服治疗在减少眼部疾病方面无效。 MI-S在皮肤病变上的局部应用也不有效,但是口服MI-S治疗的皮肤感染小鼠在第9天后的疾病评分显着降低(P <0.05),表明加速了愈合。与对照组相比,在病毒攻击前20分钟阴道给予MI-S降低了第5至9天的平均疾病评分(P <0.05),第1天的病毒滴度(P <0.05)和死亡率(P <0.0001)组(未治疗和媒介治疗)。这些结果表明,MI-S可以作为口服剂以降低HSV皮肤和粘膜病变的严重程度,更重要的是,可以用作杀菌剂来阻止HSV-2生殖器感染的性传播。

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