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Antiviral activity of broad-spectrum and enterovirus-specific inhibitors against clinical isolates of enterovirus D68

机译：广谱和肠道病毒特异性抑制剂对肠道病毒D68临床分离株的抗病毒活性

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We investigated the susceptibility of 10 enterovirus D68 (EV-D68) isolates (belonging to clusters A, B, and C) to (entero)virus inhibitors with different mechanisms of action. The 3C-protease inhibitors proved to be more efficient than enviroxime and pleconaril, which in turn were more effective than vapendavir and pirodavir. Favipiravir proved to be a weak inhibitor. Resistance to pleconaril maps to V69A in the VP1 protein, and resistance to rupintrivir maps to V104I in the 3C protease. A structural explanation of why both substitutions may cause resistance is provided.

机译：我们调查了10种肠道病毒D68（EV-D68）分离株（属于簇A，B和C）对具有不同作用机制的（肠）病毒抑制剂的敏感性。事实证明，3C蛋白酶抑制剂比enviroxime和pleconaril更有效，而enviroxime和pleconaril则比vapendavir和pirodavir更有效。 Favipiravir被证明是一种弱抑制剂。对pleconaril的抗性对应于VP1蛋白中的V69A，对rupintrivir的抗性对应于3C蛋白酶中的V104I。提供了两个取代为什么会引起抗性的结构解释。

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Sun Liang; Meijer Adam; Froeyen Mathy; Zhang Linlin; Thibaut Hendrik Jan; Baggen Jim; George Shyla; Vernachio John; van Kuppeveld Frank J M; Leyssen Pieter; Hilgenfeld Rolf; Neyts Johan; Delang Leen;
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1. Antiviral Activity of Broad-Spectrum and Enterovirus-Specific Inhibitors against Clinical Isolates of Enterovirus D68 [J] . Sun Liang, Meijer Adam, Froeyen Mathy, Antimicrobial agents and chemotherapy. . 2015,第12期

机译：广谱和肠道病毒特异性抑制剂对肠道病毒D68临床分离株的抗病毒活性
2. The monoamine oxidase A inhibitor clorgyline is a broad-spectrum inhibitor of fungal ABC and MFS transporter efflux pump activities which reverses the azole resistance of Candida albicans and Candida glabrata clinical isolates [J] . HolmesA.R., KeniyaM.V., Ivnitski-SteeleI., Antimicrobial agents and chemotherapy. . 2012,第3期

机译：单胺氧化酶A抑制剂clorgyline是真菌ABC和MFS转运蛋白外排泵活动的广谱抑制剂，可逆转白色念珠菌和光滑念珠菌临床分离株的唑耐药性
3. Pyrrolobenzoxazepinone derivatives as non-nucleoside HIV-1 RT inhibitors: further structure-activity relationship studies and identification of more potent broad-spectrum HIV-1 RT inhibitors with antiviral activity. [J] . Campiani G, Morelli E, Fabbrini M, Journal of Medicinal Chemistry . 1999,第21期

机译：吡咯并苯并a庚酮衍生物作为非核苷HIV-1 RT抑制剂：进一步的结构活性关系研究和鉴定具有抗病毒活性的更有效的广谱HIV-1 RT抑制剂。
4. Design, synthesis, and activity evaluation of broad-spectrum small-molecule inhibitors of anti-apoptofic Bcl-2 family proteins: Characteristics of broad-spectrum protein binding and its effects on anti-tumor activity [C] . Can-Hui Zheng, Jia-Guo Lv, Ju Zhu, International conference of molecular simulations and applied informatics technologies . 2012

机译：抗凋亡Bcl-2家族蛋白的广谱小分子抑制剂的设计，合成和活性评估：广谱蛋白结合的特征及其对抗肿瘤活性的影响
5. Discovery and Design of Broad-spectrum Antiviral Peptides [D] . Hoffmann, Andrew Robert. 2020

机译：广谱抗病毒肽的发现与设计
6. Antiviral Activity of Broad-Spectrum and Enterovirus-Specific Inhibitors against Clinical Isolates of Enterovirus D68 [O] . Liang Sun, Adam Meijer, Mathy Froeyen, 2015

机译：广谱和肠道病毒特异性抑制剂对肠道病毒D68临床分离株的抗病毒活性
7. A Novel Capsid Binding Inhibitor Displays Potent Antiviral Activity against Enterovirus D68 [O] . Chunlong Ma, Yanmei Hu, Jiantao Zhang, 2019

机译：一种新型衣壳结合抑制剂对肠道病毒D68显示有效的抗病毒活性

Antiviral activity of broad-spectrum and enterovirus-specific inhibitors against clinical isolates of enterovirus D68

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