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首页> 外文期刊>FEBS Letters >Structure to 1.9 Å resolution of a complex with herpes simplex virus type‐1 thymidine kinase of a novel, non‐substrate inhibitor: X‐ray crystallographic comparison with binding of aciclovir
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Structure to 1.9 Å resolution of a complex with herpes simplex virus type‐1 thymidine kinase of a novel, non‐substrate inhibitor: X‐ray crystallographic comparison with binding of aciclovir

机译:新型无底物抑制剂的单纯疱疹病毒1型胸苷激酶复合物的结构至1.9Å分辨率:X射线晶体学比较与阿昔洛韦的结合

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摘要

>Treatment of herpes infections with nucleoside analogues requires as an initial step the activation of the compounds by thymidine kinase. As an aid to developing more effective chemotherapy, both for treatment of recurrent herpes infection and in gene therapy systems where thymidine kinase is expressed, two high-resolution X-ray structures of thymidine kinase have been compared: one with the relatively poor substrate aciclovir (Zovirax), the other with a synthetic inhibitor having an N 2-substituted guanine. Both compounds have similar binding modes in spite of their size difference and apparently distinct ligand properties.
机译:>用核苷类似物治疗疱疹感染需要作为第一步,通过胸苷激酶激活化合物。为了开发更有效的化学疗法,无论是用于治疗复发性疱疹感染还是在表达胸苷激酶的基因治疗系统中,已经比较了胸苷激酶的两种高分辨率X射线结构:一种具有相对较差的底物阿昔洛韦( Zovirax),另一种是具有 N 2 取代鸟嘌呤的合成抑制剂。尽管这两种化合物的大小不同和明显不同的配体性质,但它们具有相似的结合模式。

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