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Polymorphic substitution E157Q in HIV-1 integrase increases R263K-mediated dolutegravir resistance and decreases DNA binding activity

机译：HIV-1整合酶中的多态性替换E157Q增加R263K介导的dolutegravir耐药性并降低DNA结合活性

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摘要

ObjectivesThe E157Q substitution in HIV-1 integrase (IN) is a relatively common natural polymorphism associated with HIV resistance to IN strand transfer inhibitors (INSTIs). Although R263K is the most common resistance substitution for the INSTI dolutegravir, an INSTI treatment-experienced individual recently failed dolutegravir-based therapy, with E157Q being the only resistance-associated change reported. Given that different resistance pathways can sometimes synergize to confer high levels of resistance to antiretroviral drugs, we studied the effects of E157Q in association with R263K. Because Glu157 is thought to lie within the binding site of HIV IN DNA binding inhibitors such as FZ41, we also evaluated DNA binding activity and resistance to IN inhibitors in the presence of E157Q.

机译：目的HIV-1整合酶（IN）中的E157Q取代是与HIV对IN链转移抑制剂（INSTI）的抗性相关的一种相对普遍的自然多态性。尽管R263K是INSTI dolutegravir的最常见抗药性替代品，但有INSTI治疗经验的个体最近失败了基于dolutegravir的疗法，据报道仅有E157Q发生了抗药性变化。考虑到不同的耐药途径有时可以协同作用，从而赋予抗逆转录病毒药物以高水平的耐药性，因此我们研究了E157Q与R263K的联合作用。因为Glu157被认为位于HIV IN DNA结合抑制剂（例如FZ41）的结合位点内，所以我们还评估了在E157Q存在下DNA结合活性和对IN抑制剂的抗性。

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期刊名称 Journal of Antimicrobial Chemotherapy
作者
Kaitlin Anstett; Vincent Cutillas; Robert Fusco; Thibault Mesplède; Mark A. Wainberg;
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作者单位

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年(卷),期 -1(71),8
年度 -1
页码 2083–2088
总页数 6
原文格式 PDF
正文语种
中图分类药学;微生物学;病毒传染病;
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专利

1. Polymorphic substitution E157Q in HIV-1 integrase increases R263K-mediated dolutegravir resistance and decreases DNA binding activity [J] . Anstett Kaitlin, Cutillas Vincent, Fusco Robert, The Journal of Antimicrobial Chemotherapy . 2016,第8期

机译：HIV-1整合酶中的多态性替换E157Q增加R263K介导的dolutegravir耐药性并降低DNA结合活性
2. The M50I polymorphic substitution in association with the R263K mutation in HIV-1 subtype B integrase increases drug resistance but does not restore viral replicative fitness [J] . Melissa Wares, Thibault Mesplède, Peter K Quashie, Retrovirology . 2014,第S1期

机译：与HIV-1亚型B整合酶中的R263K突变相关的M50I多态性置换可增加耐药性，但不能恢复病毒复制适应性
3. Increased adiposity in DNA binding-dependent androgen receptor knockout male mice associated with decreased voluntary activity and not insulin resistance. [J] . Rana K, Fam BC, Clarke MV, American Journal of Physiology . 2011,第5Parta1期

机译：在与胰岛素活性降低相关的DNA结合依赖性雄激素受体敲除阳小鼠中增加肥胖增加，而不是胰岛素抵抗力。
4. Docking Dinucleotides to HIV-1 Integrase Carboxyl-Terminal Domain for Finding Possible DNA Binding Sites [C] . H. M. Zhu, W. Z. Chen, C. X. Wang The 2nd World Congress for Chinese Biomedical Engineers . 2004

机译：将二核苷酸对接至HIV-1整合酶羧基末端结构域，以寻找可能的DNA结合位点
5. Green Chemical Synthesis of Amodiaquine, Purification, and Cocrystal Formation Studies of Piperine with HIV-1 Integrase Inhibitor: Dolutegravir [D] . Yeibyo, Woldegebriel G. 2020

机译：与HIV-1整合酶抑制剂的哌啶的绿色化学合成哌啶，纯化和哌啶的组合研究：DoluteGravir
6. The M50I polymorphic substitution in association with the R263K mutation in HIV-1 subtype B integrase increases drug resistance but does not restore viral replicative fitness [O] . Melissa Wares, Thibault Mesplède, Peter K Quashie, 2014

机译：M50I多态性替换与HIV-1 B亚型整合酶中的R263K突变相关可增加耐药性但无法恢复病毒复制适应性
7. The M50I polymorphic substitution in association with the R263K mutation in HIV-1 subtype B integrase increases drug resistance but does not restore viral replicative fitness [O] . Melissa Wares, Thibault Mesplède, Peter K Quashie, 2014

机译：M50I多态性替换与HIV-1 B亚型整合酶中的R263K突变相关，可增加耐药性，但无法恢复病毒复制适应性

Polymorphic substitution E157Q in HIV-1 integrase increases R263K-mediated dolutegravir resistance and decreases DNA binding activity

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