Synthesis, Biological Evaluation and Molecular Docking of Calix[4]arene-Based beta-Diketo Derivatives as HIV-1 Integrase Inhibitors

Luo Zaigang; Zhao Yu; Ma Chao; Li Zhipeng; Xu Xuemei; Hu Liming; Huang Nianyu; He Hongqiu

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Synthesis, Biological Evaluation and Molecular Docking of Calix[4]arene-Based beta-Diketo Derivatives as HIV-1 Integrase Inhibitors

机译：杯[4]芳烃基β-二酮衍生物作为HIV-1整合酶抑制剂的合成，生物学评价和分子对接

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In this publication, we design and report the synthesis of calix[4]arene-based -diketo derivatives as novel HIV-1 integrase (IN) inhibitors. The target compounds were obtained using Claisen condensation, and their structures were characterized by NMR and ESI-MS. Preliminary bioassays showed that calix[4]arene-based -diketo derivatives inhibit strand transfer (ST) with IC50 values between 5.9 and 21.2 mu M. Docking studies revealed the predominant binding modes that were distinct from the binding modes of raltegravir, which suggests a novel binding region in the IN active site. Moreover, these compounds are predicted not to interact with some of the key amino acids (GLN148 and ASN155) implicated in viral resistance. Therefore, this series of compounds can further be investigated for a possible chemotype to circumvent resistance to clinical HIV-1 IN inhibitors.

机译：在本出版物中，我们设计并报告了基于杯[4]芳烃的二酮衍生物作为新型HIV-1整合酶（IN）抑制剂的合成。使用克莱森缩合获得目标化合物，并通过NMR和ESI-MS对其结构进行表征。初步的生物测定表明，杯[4]芳烃基-二酮衍生物抑制链转移（ST），IC50值在5.9至21.2μM之间。对接研究表明，主要的结合方式与拉格韦的结合方式不同。 IN活性位点中的新结合区。此外，预计这些化合物不会与某些与病毒抗性有关的关键氨基酸（GLN148和ASN155）相互作用。因此，可以进一步研究该系列化合物的化学型，以规避对临床HIV-1 IN抑制剂的耐药性。

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来源
《Archiv der Pharmazie》 |2015年第3期|共8页
作者
Luo Zaigang; Zhao Yu; Ma Chao; Li Zhipeng; Xu Xuemei; Hu Liming; Huang Nianyu; He Hongqiu;
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中图分类药学;
关键词
Calix4arene; -Diketo derivatives; HIV-1 integrase inhibitors; Molecular docking; Synthesis;

机译：杯[4]芳烃;-二酮衍生物;HIV-1整合酶抑制剂;分子对接;合成;

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1. Synthesis, Biological Evaluation and Molecular Docking of Calix[4]arene-Based beta-Diketo Derivatives as HIV-1 Integrase Inhibitors [J] . Luo Zaigang, Zhao Yu, Ma Chao, Archiv der Pharmazie . 2015,第3期

机译：杯[4]芳烃基β-二酮衍生物作为HIV-1整合酶抑制剂的合成，生物学评价和分子对接
2. Docking, Synthesis and Biological Evaluation of Novel Diketoquinoline Analogues as HIV-1 Integrase Inhibitor [J] . Kishore D. Deo, I.J. Singhvi, S.R. Patil Asian Journal of Chemistry: An International Quarterly Research Journal of Chemistry . 2019,第9期

机译：新型二氧化喹啉类似物的对接，合成和生物学评价为HIV-1整合酶抑制剂
3. Design and synthesis of novel indole beta-diketo acid derivatives as HIV-1 integrase inhibitors [J] . Sechi M, Derudas M, Dallocchio R, Journal of Medicinal Chemistry . 2004,第21期

机译：新型吲哚β-二酮酸衍生物作为HIV-1整合酶抑制剂的设计与合成
4. Synthesis and Biological Evaluation of Quinolone Acid Derivatives Having Polyhydroxylated Aromatics as HIV-1 Integrase Inhibitions [C] . Xuemei Xu, Zaigang Luo, Kuai He, ICCMME 2012 . 2013

机译：喹啉酸衍生物作为HIV-1整合酶抑制的喹啉酸衍生物的合成与生物学评价
5. Design and synthesis of molecular probes to modulate cell membrane permeation: I. Design, synthesis, and biological evaluation of novel chicoric acid analogues as inhibitors of HIV-1 integrase. II. Design, synthesis, and biological evaluation of novel estradiol analogues targeting the membrane estrogen receptor. [D] . Charvat, Trevor Thomas. 2004

机译：设计和合成的分子探针，可调节细胞膜的渗透性：I.设计，合成和生物评价作为抗HIV-1整合酶抑制剂的新型菊苣酸类似物。二。针对膜雌激素受体的新型雌二醇类似物的设计，合成和生物学评估。
6. Design Practical Synthesis and Biological Evaluation of Novel 6-(Pyrazolylmethyl)-4-quinoline-3-carboxylic Acid Derivatives as HIV-1 Integrase Inhibitors [O] . Liming Hu, Song Yan, Zaigang Luo, 2012

机译：新型6-（吡唑基甲基）-4-喹啉-3-羧酸衍生物作为HIV-1整合酶抑制剂的设计实用合成和生物学评价
7. Molecular Docking Study of Four Chromene Derivatives as Novel HIV-1 Integrase Inhibitors [O] . Nevin Arslan 2019

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Synthesis, Biological Evaluation and Molecular Docking of Calix[4]arene-Based beta-Diketo Derivatives as HIV-1 Integrase Inhibitors

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