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Molecular targets for human papillomaviruses: prospects for antiviral therapy.

机译:人类乳头瘤病毒的分子靶标:抗病毒治疗的前景。

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摘要

A substantial medical need exists for the development of antiviral medicines for the treatment of diseases associated with infection by human papillomaviruses (HPVs). HPVs are associated with various benign and malignant lesions including benign genital condyloma, common skin warts, laryngeal papillomas and anogenital cancer. Since treatment options are limited and typically not very satisfactory, the development of safe and effective antiviral drugs for HPV could have substantial clinical impact. In the last few years, exciting advances have been made in our understanding of papillomavirus replication and the effects that the virus has on growth of the host cell. Although still somewhat rudimentary, techniques have been developed for limited virion production in vitro offering the promise of more rapid advances in the dissection and understanding of the virus life cycle. Of the 8-10 HPV gene products that are made during infection, only one encodes enzymatic activities, the E1 helicase. Successful antiviral therapies have traditionally targeted viral enzymes such as polymerases, kinases and proteases. In contrast, macromolecular interactions which mediate the functions of E6, E7 and E2 are thought to be more difficult targets for small molecule therapy.
机译:迫切需要开发抗病毒药物来治疗与人类乳头瘤病毒(HPV)感染相关的疾病。 HPV与各种良性和恶性病变有关,包括良性生殖器尖锐湿疣,常见的皮肤疣,喉乳头状瘤和生殖器癌。由于治疗选择有限且通常不能令人满意,因此开发针对HPV的安全有效的抗病毒药物可能会对临床产生重大影响。在过去的几年中,我们对乳头瘤病毒复制以及该病毒对宿主细胞生长的影响的理解取得了令人激动的进展。尽管还很初级,但是已经开发出用于体外有限的病毒体生产的技术,有望在解剖和了解病毒的生命周期方面取得更快的进步。在感染过程中产生的8-10种HPV基因产物中,只有一种编码酶活性,即E1解旋酶。成功的抗病毒疗法传统上具有针对性的病毒酶,例如聚合酶,激酶和蛋白酶。相反,介导E6,E7和E2功能的大分子相互作用被认为是小分子治疗更困难的目标。

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