The Discovery and Development of Daclatasvir: An Inhibitor of the Hepatitis C Virus NS5A Replication Complex

Meanwell, Nicholas A.; Belema, Makonen

doi:10.1007/7355_2018_47

Cited by 7 publications

(7 citation statements)

References 137 publications

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“…To determine the effect of Huh7 hepatoma cells on HCV clearance in vitro, we measured the half-life of HCV virions at 37°C in cell culture medium in the absence and presence of chronically infected Huh7 cells by monitoring the decrease of HCV RNA over time ( Figure 4 ). To measure HCV half-life in cell culture medium in the presence of chronically HCV-infected cells, we established a steady-state chronic infection in Huh7 cells, and then inhibited the secretion of HCV from the cells using 1 nM of the NS5a inhibitor daclatasvir to block HCV replication and secretion ( Meanwell and Belema, 2019 ) or 200 µM naringenin to block HCV secretion ( Goldwasser et al, 2011 ). In the absence of cells, the HCV half-life observed was 112 hr ( Figure 4a ).…”

Section: Resultsmentioning

confidence: 99%

Modeling hepatitis C virus kinetics during liver transplantation reveals the role of the liver in virus clearance

Shekhtman

Navasa

Sansone

et al. 2021

eLife

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While the liver, specifically hepatocytes, are widely accepted as the main source of hepatitis C virus (HCV) production, the role of the liver/hepatocytes in clearance of circulating HCV remains unknown. Frequent HCV kinetic data were recorded and mathematically modeled from five liver transplant patients throughout the anhepatic (absence of liver) phase and for 4 hr post-reperfusion. During the anhepatic phase, HCV remained at pre-anhepatic levels (n = 3) or declined (n = 2) with t1/2~1 hr. Immediately post-reperfusion, virus declined in a biphasic manner in four patients consisting of a rapid decline (t1/2 = 5 min) followed by a slower decline (t1/2 = 67 min). Consistent with the majority of patients in the anhepatic phase, when we monitored HCV clearance at 37°C from culture medium in the absence/presence of chronically infected hepatoma cells that were inhibited from secreting HCV, the HCV t1/2 in cell culture was longer in the absence of chronically HCV-infected cells. The results suggest that the liver plays a major role in the clearance of circulating HCV and that hepatocytes may be involved.

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Section: Resultsmentioning

confidence: 99%

Modeling hepatitis C virus kinetics during liver transplantation reveals the role of the liver in virus clearance

Shekhtman

Navasa

Sansone

et al. 2021

eLife

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“…Due to the presence of substituted biphenyl increases the polarity of the heterocyclic skeleton which might be the reason for high antitubercular (anti-TB) activities via interacting with the MurB inhibitors 186 Treatment of heart failure with a combination of valsartan Neprilysin inhibitor 186,187 Antihypertensive Since inhibition of angiotensin II type 1 (AT1) receptor reduces chronic inammation associated with hypertension, we evaluated the anti-inammatory potential and the underlying mechanism of masartan 188 Anti-inammatory 188 Antiviral As a result of sp 2 hybridization of CNTs between the drug and target protein sequence, leads to improving the uorescence reactivity. Because the conjugated system of biphenyl and the presence of Cs/CNT can increase the electroactive surface area of the electrode, leading to an increase in the number of structural aws 189 Treatment selections for hepatitis C virus 189,190 Active for the AT1 receptor [191][192][193] Lung-selective muscarinic cholinergic receptor (mAChR) antagonist…”

Section: Biphenyl Atropisomerismmentioning

confidence: 99%

A fruitful century for the scalable synthesis and reactions of biphenyl derivatives: applications and biological aspects

et al. 2023

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“…Successful drug, daclatasvir 3) was approved in 2014 by the European Medicine Agency and in 2016 by the FDA, under the brand name Daklinza. It is usually coadministered with sofosbuvir [158]. It was proposed that daclatasvir blocks the transport of viral RNAs to the assembly sites and thus inhibits viral particle assembly [159].…”

Section: Hepatitis C Virus Assembly Inhibitorsmentioning

confidence: 99%

Targeting the Virus Capsid as a Tool to Fight RNA Viruses

Hozáková

Vokatá

Ruml

et al. 2022

Viruses

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Several strategies have been developed to fight viral infections, not only in humans but also in animals and plants. Some of them are based on the development of efficient vaccines, to target the virus by developed antibodies, others focus on finding antiviral compounds with activities that inhibit selected virus replication steps. Currently, there is an increasing number of antiviral drugs on the market; however, some have unpleasant side effects, are toxic to cells, or the viruses quickly develop resistance to them. As the current situation shows, the combination of multiple antiviral strategies or the combination of the use of various compounds within one strategy is very important. The most desirable are combinations of drugs that inhibit different steps in the virus life cycle. This is an important issue especially for RNA viruses, which replicate their genomes using error-prone RNA polymerases and rapidly develop mutants resistant to applied antiviral compounds. Here, we focus on compounds targeting viral structural capsid proteins, thereby inhibiting virus assembly or disassembly, virus binding to cellular receptors, or acting by inhibiting other virus replication mechanisms. This review is an update of existing papers on a similar topic, by focusing on the most recent advances in the rapidly evolving research of compounds targeting capsid proteins of RNA viruses.

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The Discovery and Development of Daclatasvir: An Inhibitor of the Hepatitis C Virus NS5A Replication Complex

Cited by 7 publications

References 137 publications

Modeling hepatitis C virus kinetics during liver transplantation reveals the role of the liver in virus clearance

Modeling hepatitis C virus kinetics during liver transplantation reveals the role of the liver in virus clearance

A fruitful century for the scalable synthesis and reactions of biphenyl derivatives: applications and biological aspects

Targeting the Virus Capsid as a Tool to Fight RNA Viruses

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