Emetine Inhibits Replication of RNA and DNA Viruses Without Generating Drug-resistant Virus Variants

Overview

Journal Antiviral Res

Publisher Elsevier

Date 2017 Jun 19

PMID 28624461

Citations 42

Authors

Nitin Khandelwal

Yogesh Chander

Krishan Dutt Rawat

Thachamvally Riyesh

Chikkahonnaiah Nishanth

Shalini Sharma

Naresh Jindal

Bhupendra N Tripathi

Sanjay Barua

Naveen Kumar

Affiliations

Soon will be listed here.

Abstract

At a noncytotoxic concentration, emetine was found to inhibit replication of DNA viruses [buffalopoxvirus (BPXV) and bovine herpesvirus 1 (BHV-1)] as well as RNA viruses [peste des petits ruminants virus (PPRV) and Newcastle disease virus (NDV)]. Using the time-of-addition and virus step-specific assays, we showed that emetine treatment resulted in reduced synthesis of viral RNA (PPRV and NDV) and DNA (BPXV and BHV-1) as well as inhibiting viral entry (NDV and BHV-1). In addition, emetine treatment also resulted in decreased synthesis of viral proteins. In a cell free endogenous viral polymerase assay, emetine was found to significantly inhibit replication of NDV, but not BPXV genome, suggesting that besides directly inhibiting specific viral polymerases, emetine may also target other factors essentially required for efficient replication of the viral genome. Moreover, emetine was found to significantly inhibit BPXV-induced pock lesions on chorioallantoic membrane (CAM) along with associated mortality of embryonated chicken eggs. At a lethal dose 50 (LD) of 126.49 ng/egg and at an effective concentration 50 (EC) of 3.03 ng/egg, the therapeutic index of the emetine against BPXV was determined to be 41.74. Emetine was also found to significantly delay NDV-induced mortality in chicken embryos associated with reduced viral titers. Further, emetine-resistant mutants were not observed upon long-term (P = 25) sequential passage of BPXV and NDV in cell culture. Collectively, we have extended the effective antiviral activity of emetine against diverse groups of DNA and RNA viruses and propose that emetine could provide significant therapeutic value against some of these viruses without inducing an antiviral drug-resistant phenotype.

Citing Articles

A Comprehensive Review of the Development and Therapeutic Use of Antivirals in Flavivirus Infection.

Tripathi A, Chauhan S, Khasa R Viruses. 2025; 17(1).

PMID: 39861863 PMC: 11769230. DOI: 10.3390/v17010074.

Dual effects of ipecac alkaloids with potent antiviral activity against foot-and-mouth disease virus as replicase inhibitors and direct virucides.

Pantanam A, Mana N, Semkum P, Lueangaramkul V, Phecharat N, Lekcharoensuk P Int J Vet Sci Med. 2024; 12(1):134-147.

PMID: 39359867 PMC: 11445910. DOI: 10.1080/23144599.2024.2408189.

Exploring Iguape Virus-A Lesser-Known Orthoflavivirus.

Saivish M, Nogueira M, Rossi S, Vasilakis N Viruses. 2024; 16(6).

PMID: 38932252 PMC: 11209261. DOI: 10.3390/v16060960.

Identification of miR-29a as a novel biomarker for lumpy skin disease virus exposure in cattle.

Kumar R, Kamboj H, Dhanda S, Verma A, Chander Y, Nehra K Virulence. 2024; 15(1):2324711.

PMID: 38527940 PMC: 10965105. DOI: 10.1080/21505594.2024.2324711.

Virus-like particles (VLPs): A promising platform for combating against Newcastle disease virus.

Taghizadeh M, Niazi A, Afsharifar A Vaccine X. 2024; 16:100440.

PMID: 38283623 PMC: 10811427. DOI: 10.1016/j.jvacx.2024.100440.