Exploring Ugi-Azide Four-Component Reaction Products for Broad-Spectrum Influenza Antivirals with a High Genetic Barrier to Drug Resistance

Zhang, Jiantao; Hu, Yanmei; Foley, Christopher; Wang, Yuanxiang; Musharrafieh, Rami; Xu, Shuting; Zhang, Yongtao; Ma, Chunlong; Hulme, Christopher; Wang, Jun

doi:10.1038/s41598-018-22875-9

Cited by 27 publications

(38 citation statements)

References 41 publications

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“…During the preparation of this manuscript, a study reporting the identification of a new PA-PB1 inhibitor of influenza virus as well as the evaluation of the barrier to drug resistance of this compound was published (Zhang et al, 2018). In keeping with our findings, Zhang and coworkers showed that OST rapidly induced the selection of resistant viral variants, while no viruses with altered susceptibility to the PA-PB1 inhibitor were isolated.…”

Section: Discussionsupporting

confidence: 77%

“…In keeping with our findings, Zhang and coworkers showed that OST rapidly induced the selection of resistant viral variants, while no viruses with altered susceptibility to the PA-PB1 inhibitor were isolated. However, they stopped the selection process at P10 (Zhang et al, 2018), while we carried out a prolonged drug-resistance selection for a total of 20/30 viral passages. Altogether, our data and the results obtained by Zhang et al suggest that drug resistance in vitro to dissociative inhibitors targeting the PA-PB1 interactions of influenza virus RdRP appears hard to develop, differently from what happens with the current anti-influenza drugs such as adamantanes and neuraminidase inhibitors and also with PA and PB2 enzymatic inhibitors approved or under clinical development (Hay et al, 1985;Molla et al, 2002;McKimm-Breschkin et al, 2012;Byrn et al, 2015;Noshi et al, 2018).…”

Section: Discussionmentioning

confidence: 99%

“…To evaluate the barrier to drug resistance of selected cHTC compounds (29, 31, and 54) and OST as a reference compound, IAV PR/8 strain was serially passaged in the presence of increasing concentrations of test compounds following a procedure previously described (Zhang et al, 2018).…”

Section: In Vitro Serial Influenza Virus Passage Experimentsmentioning

confidence: 99%

“…To evaluate the propensity of this class of inhibitors to induce drug resistance, we tried to select in vitro influenza viruses resistant to the most promising compounds under drug selective pressure, following a procedure similar to that previously employed for other anti-influenza compounds, including PA-PB1 inhibitors (Molla et al, 2002;Shih et al, 2010;Ma et al, 2016;Hu et al, 2017;Zhang et al, 2018). The cHTC compounds that both inhibited the viral replication in PRAs with EC50 values ≤ 1 µM and disrupted specifically the PA-PB1 interaction in ELISA with IC50 values < 20 µM were selected for these studies.…”

Section: Selected Chtc Compounds Have a High Barrier To Drug Resistanmentioning

confidence: 99%

“…Since these interactions are essential for viral replication and their binding interfaces are highly conserved among IAV and IBV strains (Pérez and Donis, 1995;Ghanem et al, 2007;Stevaert and Naesens, 2016), the disruption of such interactions represents an attractive strategy for the development of anti-influenza drugs with broad activity (Loregian et al, 2002;Loregian and Palù, 2005;Palù and Loregian, 2013;Loregian et al, 2014;Stevaert and Naesens, 2016;Massari et al, 2016). The feasibility and the effectiveness of such an approach have been demonstrated by the increasing number of PA-PB1 dissociative inhibitors developed in the last decade (Wunderlich et al, 2009;Wunderlich et al, 2011;Muratore et al, 2012a;Muratore et al, 2012b;Fukuoka et al, 2012;Massari et al, 2013;Kessler et al, 2013;Lepri et al, 2014;Pagano et al, 2014;Tintori et al, 2014;Massari et al, 2015;Trist et al, 2016;Yuan et al, 2016;Desantis et al, 2017;Watanabe et al, 2017;Massari et al, 2017;Zhang et al, 2018;D'Agostino et al, 2018).…”

Section: Introductionmentioning

confidence: 99%

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Potent and broad-spectrum cycloheptathiophene-3-carboxamide compounds that target the PA-PB1 interaction of influenza virus RNA polymerase and possess a high barrier to drug resistance

et al. 2019

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Influenza viruses are major respiratory pathogens responsible for both seasonal epidemics and occasional pandemics worldwide. The current available treatment options have limited efficacy and thus the development of new antivirals is highly needed. We previously reported the identification of a series of cycloheptathiophene-3-carboxamide compounds as influenza A virus inhibitors that act by targeting the protein-protein interactions between the PA-PB1 subunits of the viral polymerase. In this study, we characterized the antiviral properties of the most promising compounds as well as investigated their propensity to induce drug resistance. Our results show that some of the selected compounds possess potent, broad-spectrum anti-influenza activity as they efficiently inhibited the replication of several strains of influenza A and B viruses, including an oseltamivir-resistant clinical isolate, with nanomolar or low-micromolar potency. The most promising compounds specifically inhibited the PA−PB1 binding in vitro and interfered with the influenza A virus polymerase activity in a cellular context, without showing cytotoxicity. The most active PA-PB1 inhibitors showed to possess a drug resistance barrier higher than that of oseltamivir. Indeed, no viral variants with reduced susceptibility to the selected compounds emerged after serial passages of influenza A virus under drug selective pressure. Overall, our studies identified potent PA-PB1 inhibitors as promising candidates for the development of new anti-influenza drugs.

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Section: Discussionsupporting

confidence: 77%

Section: Discussionmentioning

confidence: 99%

Section: In Vitro Serial Influenza Virus Passage Experimentsmentioning

confidence: 99%

Section: Selected Chtc Compounds Have a High Barrier To Drug Resistanmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

Potent and broad-spectrum cycloheptathiophene-3-carboxamide compounds that target the PA-PB1 interaction of influenza virus RNA polymerase and possess a high barrier to drug resistance

et al. 2019

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Six‐Component Reactions and Beyond: The Nuts and Bolts

Hooshmand

Yazdani²,

Hulme

2022

Eur J Org Chem

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The deployment of multicomponent reactions (MCRs), defined as containing three or more reactants, not only enjoys pot, atom, and step‐economy in the synthesis of novel complex molecules but also aligns with sustainable chemistry principles as a green symphony. Generally, more components lead to more complexity, and are taken to an extreme ‘‘higher‐order’’ MCRs, where six or even more components react in a one‐pot, have been developed, although they remain scarce compared to their 3, 4 and 5‐component relatives. On this topic, the rich footprint of isocyanides in MCRs has been fruitful in delivering higher order six to eight‐component reactions through mechanistically similar pathways. The present review encompasses a brief history of MCRs and their product utility, followed by a thorough discussion of the principles of reaction design that enabled the discovery of higher‐order MCRs, spanning 6 to 8‐components. Future challenges and opportunities will also be elaborated.

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Three Complementary One‐Pot Four‐Component Reaction Sequences for Rapid, General and Direct Spiropyran Synthesis

Hughes-Whiffing

Perry

2022

Eur J Org Chem

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Three one-pot three-step four-component reaction sequences for spiropyran synthesis have been developed, based around three different methods for in situ generation of 1,2,3trisubstituted indoles (indole N-alkylation, Fischer indolisation and indole C-alkylation). The reaction sequences give access to a broad swathe of spiropyran structures. Each sequence is operationally straightforward, rapid and high yielding. We have synthesized 58 structurally diverse spiropyrans bearing a wide range of useful functional groups, and their utility were demonstrated in the targeted synthesis of potential ratiometric fluorescence probes for metal ions and spiropyran-cholesterol conjugates. Finally, we showed that our one-pot N-alkylation-Calkylation-condensation sequence can underpin combinatorial spiropyran synthesis through generation of a 16-member spiropyran library.

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Exploring Ugi-Azide Four-Component Reaction Products for Broad-Spectrum Influenza Antivirals with a High Genetic Barrier to Drug Resistance

Cited by 27 publications

References 41 publications

Potent and broad-spectrum cycloheptathiophene-3-carboxamide compounds that target the PA-PB1 interaction of influenza virus RNA polymerase and possess a high barrier to drug resistance

Potent and broad-spectrum cycloheptathiophene-3-carboxamide compounds that target the PA-PB1 interaction of influenza virus RNA polymerase and possess a high barrier to drug resistance

Six‐Component Reactions and Beyond: The Nuts and Bolts

Three Complementary One‐Pot Four‐Component Reaction Sequences for Rapid, General and Direct Spiropyran Synthesis

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