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首页> 外文期刊>Antimicrobial agents and chemotherapy. >Evaluations of unformulated and formulated dendrimer-based microbicide candidates in mouse and Guinea pig models of genital herpes.
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Evaluations of unformulated and formulated dendrimer-based microbicide candidates in mouse and Guinea pig models of genital herpes.

机译:在生殖器疱疹的小鼠和豚鼠模型中评估未配制和配制的基于树状聚合物的杀微生物剂候选物。

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Prevention of sexually transmitted infections is a priority in developed and developing countries. One approach to prevention is the use of topical microbicides, and one promising approach is the use of dendrimers, highly branched macromolecules synthesized from a polyfunctional core. Three new dendrimer products developed to provide stable and cost-efficient microbicides were initially evaluated in vitro for anti-herpes simplex virus activity and then in vivo by using a mouse model of genital herpes. From these experiments one product, SPL7013, was chosen for further evaluation to define the dose and duration of protection. Unformulated SPL7013 provided significant protection from genital herpes disease and infection at concentrations as low as 1 mg/ml and for at least 1 h following topical (intravaginal) administration of 10 mg/ml. This compound was then formulated into three vehicles and further evaluated in mouse and guinea pig models of genital herpes infection. In the murine evaluations each of the formulations provided significant protection at concentrations of 10 and 50 mg/ml. Formulated compounds provided protection for at least 1 h at a concentration of 10 mg/ml. From these experiments formulation 2V was chosen for dose ranging experiments using the guinea pig model of genital herpes. The guinea pig evaluations suggested that doses of 30 to 50 mg/ml were required for optimal protection. From these studies a lead compound and formulation (2V of SPL7013) was chosen for ongoing evaluations in primate models of simian immunodeficiency virus and Chlamydia trachomatis infection.
机译:预防性传播感染是发达国家和发展中国家的当务之急。一种预防方法是使用局部杀菌剂,一种有前途的方法是使用树枝状聚合物,即由多官能核心合成的高度分支的大分子。最初在体外评估了三种提供稳定且具有成本效益的杀微生物剂的新的树状聚合物产品的抗单纯疱疹病毒活性,然后使用生殖器疱疹小鼠模型在体内进行了评估。从这些实验中,选择一种产品SPL7013进行进一步评估,以定义保护的剂量和持续时间。浓度低至1 mg / ml且局部(阴道内)给药10 mg / ml后,未配制的SPL7013可有效预防生殖器疱疹和感染。然后将该化合物配制成三种载体,并在生殖器疱疹感染的小鼠和豚鼠模型中进行进一步评估。在鼠类评估中,每种制剂在10和50 mg / ml的浓度下均提供了显着的保护作用。配制的化合物以10 mg / ml的浓度提供至少1小时的保护。从这些实验中,使用生殖器疱疹的豚鼠模型选择制剂2V进行剂量范围实验。豚鼠的评估表明,需要30至50 mg / ml的剂量才能达到最佳保护效果。从这些研究中,选择了先导化合物和制剂(SPL7013的2V)在猿猴免疫缺陷病毒和沙眼衣原体感染的灵长类动物模型中进行评估。

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