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Development of new antivirals for herpesviruses.

机译:开发用于疱疹病毒的新型抗病毒药。

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The long-term treatment of herpesvirus infections with current antivirals in immunocompromised hosts leads to the development of drug-resistant viruses. Because nearly all currently available antivirals finally target viral DNA polymerase, virus resistant to one drug often shows cross-resistance to other drugs. In addition, nearly all the antivirals show various kinds of side effects or poor bioavailability. This evidence highlights the need for developing new antivirals for herpesviruses that have the different viral targets. Recently, high-throughput screening of large compound collections for inhibiting specific viral enzymes, or in vitro cell culture assay, has identified several new antivirals that target different viral proteins. These include the inhibitors of helicase/primase complex, terminase complex, portal protein and UL97 protein kinase. In addition, non-nucleoside inhibitors for viral DNA polymerase have been also developed. This review will focus on these new compounds that directly inhibit viral replication.
机译:在免疫功能低下的宿主中用当前的抗病毒剂长期治疗疱疹病毒感染导致了耐药性病毒的发展。因为几乎所有当前可用的抗病毒剂最终都靶向病毒DNA聚合酶,所以对一种药物具有抗药性的病毒通常表现出与其他药物的交叉抗性。此外,几乎所有抗病毒药都显示出各种副作用或不良的生物利用度。该证据突出表明,需要为具有不同病毒靶标的疱疹病毒开发新的抗病毒药。近来,用于抑制特定病毒酶的大型化合物集合的高通量筛选或体外细胞培养测定法已经鉴定出了针对不同病毒蛋白的几种新型抗病毒剂。这些包括解旋酶/引发酶复合物,末端酶复合物,门禁蛋白和UL97蛋白激酶的抑制剂。另外,还开发了用于病毒DNA聚合酶的非核苷抑制剂。这篇综述将集中在直接抑制病毒复制的这些新化合物上。

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