Literature DB >> 22037848

F18, a novel small-molecule nonnucleoside reverse transcriptase inhibitor, inhibits HIV-1 replication using distinct binding motifs as demonstrated by resistance selection and docking analysis.

Xiaofan Lu1, Li Liu, Xu Zhang, Terrence Chi Kong Lau, Stephen Kwok Wing Tsui, Yuanxi Kang, Purong Zheng, Bojian Zheng, Gang Liu, Zhiwei Chen.   

Abstract

Nonnucleoside reverse transcriptase inhibitors (NNRTIs) are one of the key components of antiretroviral therapy drug regimen against human immunodeficiency virus type 1 (HIV-1) replication. We previously described a newly synthesized small molecule, 10-chloromethyl-11-demethyl-12-oxo-calanolide A (F18), a (+)-calanolide A analog, as a novel anti-HIV-1 NNRTI (H. Xue et al., J. Med. Chem. 53:1397-1401, 2010). Here, we further investigated its antiviral range, drug resistance profile, and underlying mechanism of action. F18 consistently displayed potent activity against primary HIV-1 isolates, including various subtypes of group M, circulating recombinant form (CRF) 01_AE, and laboratory-adapted drug-resistant viruses. Moreover, F18 displayed distinct profiles against 17 NNRTI-resistant pseudoviruses, with an excellent potency especially against one of the most prevalent strains with the Y181C mutation (50% effective concentration, 1.0 nM), which was in stark contrast to the extensively used NNRTIs nevirapine and efavirenz. Moreover, we induced F18-resistant viruses by in vitro serial passages and found that the mutation L100I appeared to be the dominant contributor to F18 resistance, further suggesting a binding motif different from that of nevirapine and efavirenz. F18 was nonantagonistic when used in combination with other antiretrovirals against both wild-type and drug-resistant viruses in infected peripheral blood mononuclear cells. Interestingly, F18 displayed a highly synergistic antiviral effect with nevirapine against nevirapine-resistant virus (Y181C). Furthermore, in silico docking analysis suggested that F18 may bind to the HIV-1 reverse transcriptase differently from other NNRTIs. This study presents F18 as a new potential drug for clinical use and also presents a new mechanism-based design for future NNRTI.

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Year:  2011        PMID: 22037848      PMCID: PMC3256034          DOI: 10.1128/AAC.05537-11

Source DB:  PubMed          Journal:  Antimicrob Agents Chemother        ISSN: 0066-4804            Impact factor:   5.191


  46 in total

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3.  Highly suppressing wild-type HIV-1 and Y181C mutant HIV-1 strains by 10-chloromethyl-11-demethyl-12-oxo-calanolide A with druggable profile.

Authors:  Hai Xue; Xiaofan Lu; Purong Zheng; Li Liu; Chunyan Han; Jinping Hu; Zijie Liu; Tao Ma; Yan Li; Lin Wang; Zhiwei Chen; Gang Liu
Journal:  J Med Chem       Date:  2010-02-11       Impact factor: 7.446

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Authors:  Tao Ma; Li Liu; Hai Xue; Li Li; Chunyan Han; Lin Wang; Zhiwei Chen; Gang Liu
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10.  AutoDock4 and AutoDockTools4: Automated docking with selective receptor flexibility.

Authors:  Garrett M Morris; Ruth Huey; William Lindstrom; Michel F Sanner; Richard K Belew; David S Goodsell; Arthur J Olson
Journal:  J Comput Chem       Date:  2009-12       Impact factor: 3.376

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Review 9.  Computational drug design strategies applied to the modelling of human immunodeficiency virus-1 reverse transcriptase inhibitors.

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10.  Metabolism of F18, a Derivative of Calanolide A, in Human Liver Microsomes and Cytosol.

Authors:  Xiangmeng Wu; Qinghao Zhang; Jiamei Guo; Yufei Jia; Ziqian Zhang; Manman Zhao; Yakun Yang; Baolian Wang; Jinping Hu; Li Sheng; Yan Li
Journal:  Front Pharmacol       Date:  2017-07-19       Impact factor: 5.810

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