The evolution of nucleoside analogue antivirals: A review for chemists and non-chemists. Part 1: Early structural modifications to the nucleoside scaffold

Seley‐Radtke, Katherine L.; Yates, Mary K.

doi:10.1016/j.antiviral.2018.04.004

Cited by 415 publications

(378 citation statements)

References 329 publications

(495 reference statements)

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“…3,4 Dihydropyrimidinones (DHPMs) are implicated in a wide range of biological activities. Pyrimidone derivatives are already being used against viral infections (Phucho et al, 2009;Wierenga et al, 1985;Skulnick et al, 1985;Sharma et al, 2014;Seley-Radtke et al, 2018). The pyrimidone nucleus is a core component of many of the anti-retroviral drugs (Sharma et al, 2014).…”

Section: Identification Of the Top Hitsmentioning

confidence: 99%

In-silico homology assisted identification of inhibitor of RNA binding against 2019-nCoV N-protein (N terminal domain)

Sarma

Shekhar

Prajapat

et al. 2020

Journal of Biomolecular Structure and Dynamics

183

187

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The N terminal domain (NTD) of Nucleocapsid protein (N protein) of coronavirus (CoV) binds to the viral (þ) sense RNA and results in CoV ribonucleoprotien (CoV RNP) complex, essential for the virus replication. In this study, the RNA-binding N terminal domain (NTD) of the N protein was targeted for the identification of possible inhibitors of RNA binding. Two NTD structures of N proteins were selected (2OFZ and 1SSK, 92% homology) for virtual screening of 56,079 compounds from Asinex and Maybridge library to identify top 15 hits for each of the targets based on 'docking score'. These tophits were further screened for MM-GBSA binding free energy, pharmacokinetic properties (QikProp) and drug-likeness (SwissADME) and subjected to molecular dynamics (MD) studies. Two suitable binders (ZINC00003118440 and ZINC0000146942) against the target 2OFZ were identified. ZINC00003118440 is a theophylline derivative under the drug class 'bronchodilators' and further screening with approved bronchodilators was also studied to identify their ability to bind to the RNA binding region on the N protein. The other identified top hit is ZINC0000146942, which is a 3,4dihydropyrimidone class molecule. Hence this study suggests two important class of compounds, theophylline and pyrimidone derivaties as possible inhibitors of RNA binding to the N terminal domain of N protein of coronavirus, thus opening new avenues for in vitro validations.

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Section: Identification Of the Top Hitsmentioning

confidence: 99%

In-silico homology assisted identification of inhibitor of RNA binding against 2019-nCoV N-protein (N terminal domain)

Sarma

Shekhar

Prajapat

et al. 2020

Journal of Biomolecular Structure and Dynamics

183

187

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“…Nucleos(t)ide analogues are much more structurally diverse than their naturally occurring counterparts (Seley-Radtke and Yates, 2018;Yates and Seley-Radtke, 2019). Modifications may be introduced in the nucleobase, the sugar moiety or the phosphate residue.…”

Section: Introductionmentioning

confidence: 99%

Selected nucleos(t)ide-based prescribed drugs and their multi-target activity

Pastuch-Gawołek

Gillner

Król

et al. 2019

European Journal of Pharmacology

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A B S T R A C T Nucleos(t)ide analogues play pivotal roles as antiviral, cytotoxic or immunosuppressive agents. Here, we review recent reports of nucleoside analogues that exhibit broad-spectrum activity towards multiple life-threatening RNA and DNA viruses. We also present a discussion about nucleoside antimetabolites-approved antineoplastic agents-that have recently been shown to have antiviral and/or antibacterial activity. The approved drugs and drug combinations, as well as recently identified candidates for investigation and/or experimentation, are discussed. Several examples of repurposed drugs that have already been approved for use are presented. This strategy can be crucial for the first-line treatment of acute infections or coinfections and for the management of drug-resistant strains.T against viral infections of great medical importance (e.g., herpes simplex virus (HSV), varicella zoster virus (VZV), human immunodeficiency virus (HIV), hepatitis B virus (HBV) and hepatitis C virus (HCV)) and/or that are known antineoplastic agents used to treat cancer. Approved nucleos(t)ide-based drugs with multi-target activity and compounds being tested in clinical trials or evaluated in preclinical assays are listed in Table 1. In this paper, the term "approval date" means the date on which the drug was approved by the US Food and Drug Administration (FDA) unless otherwise stated. G. Pastuch-Gawołek, et al. Multi-target nucleos(t)ide-based drugs in the treatment and prophylaxis of HIV, HBV and HCV infections

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“…During the last decades, many nucleotide analogues have been synthesised and their biological activities tested . The main therapeutic application of this family of compounds is in the field of antiviral agents, counting at the present with more than 30 drugs approved for numerous targets such as hepatitis, HIV and herpes virus infections ,. Among these analogues, acyclic nucleosides (ANs) exhibit enhanced chemical and metabolic stability, acting mainly as chain terminators during DNA or RNA biosynthesis.…”

Section: Introductionmentioning

confidence: 99%

“…[1] The main therapeutic application of this family of compounds is in the field of antiviral agents, counting at the present with more than 30 drugs approved for numerous targets such as hepatitis, HIV and herpes virus infections. [2,3] Among these analogues, acyclic nucleosides (ANs) exhibit enhanced chemical and metabolic stability, acting mainly as chain terminators during DNA or RNA biosynthesis. The first known member of this family, acyclovir, displays extremely low toxicity for normal cells and a strong inhibitory activity against herpes simplex virus (HSV) being today the main drug for the treatment of this infection.…”

Section: Introductionmentioning

confidence: 99%

Keto‐Enol Tautomerism in Nucleobase‐Substituted Aldols

et al. 2018

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Acyclic nucleosides, which exhibit significant antiviral activity, are usually synthesised using traditional chemical strategies. However, the efficient and selective formation of carbon‐carbon bonds using small organic molecules as catalysts provides a promising alternative route for the sustainable synthesis of this family of compounds. Following this organocatalytic strategy, 5‐(adenyl, thyminyl and cytosyl)‐4‐hydroxy‐2‐pentanones were prepared by the pyrrolidine catalysed reaction between the 2‐oxoethyl derivative of the corresponding nucleobases and acetone. In order to investigate the keto‐enol equilibrium of these compounds in basic media, H‐D exchange studies were carried out by 1H and 13C NMR spectroscopy. The obtained results suggest that the mechanism by which this exchange occurs is of first order with respect to all the substrates, but of second order with regard to pyrrolidine in the case of the cytosine and adenine derivatives and of first order for the thymine analogue. Theoretical calculations of the structures involved in this equilibrium also suggest that the stability of the different ionic intermediates depends on the pKa of the corresponding nucleobases.

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The evolution of nucleoside analogue antivirals: A review for chemists and non-chemists. Part 1: Early structural modifications to the nucleoside scaffold

Cited by 415 publications

References 329 publications

In-silico homology assisted identification of inhibitor of RNA binding against 2019-nCoV N-protein (N terminal domain)

In-silico homology assisted identification of inhibitor of RNA binding against 2019-nCoV N-protein (N terminal domain)

Selected nucleos(t)ide-based prescribed drugs and their multi-target activity

Keto‐Enol Tautomerism in Nucleobase‐Substituted Aldols

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