Identification of 2,4-Diaminoquinazoline Derivative as a Potential Small-Molecule Inhibitor against Chikungunya and Ross River Viruses

Author:

Saha Amrita12,Acharya Badri Narayan3,Parida Manmohan1,Saxena Nandita4,Rajaiya Jaya2,Dash Paban Kumar1

Affiliation:

1. Virology Division, Defence Research & Development Establishment, Gwalior 474002, India

2. Department of Molecular Genetics and Microbiology, University of New Mexico Health Sciences Center, Albuquerque, NM 87131, USA

3. Synthetic Chemistry Division, Defence Research & Development Establishment, Gwalior 474002, India

4. Pharmacology & Toxicology Division, Defence Research & Development Establishment, Gwalior 474002, India

Abstract

Alphaviruses are serious zoonotic threats responsible for significant morbidity, causing arthritis or encephalitis. So far, no licensed drugs or vaccines are available to combat alphaviral infections. About 300,000 chikungunya virus (CHIKV) infections have been reported in 2023, with more than 300 deaths, including reports of a few cases in the USA as well. The discovery and development of small-molecule drugs have been revolutionized over the last decade. Here, we employed a cell-based screening approach using a series of in-house small-molecule libraries to test for their ability to inhibit CHIKV replication. DCR 137, a quinazoline derivative, was found to be the most potent inhibitor of CHIKV replication in our screening assay. Both, the cytopathic effect, and immunofluorescence of infected cells were reduced in a dose-dependent manner with DCR 137 post-treatment. Most importantly, DCR 137 was more protective than the traditional ribavirin drug and reduced CHIKV plaque-forming units by several log units. CHIKV-E2 protein levels were also reduced in a dose-dependent manner. Further, DCR 137 was probed for its antiviral activity against another alphavirus, the Ross River virus, which revealed effective inhibition of viral replication. These results led to the identification of a potential quinazoline candidate for future optimization that might act as a pan-alphavirus inhibitor.

Funder

Defence Research and Development Organization (DRDO), Ministry of Defence, Govt of India

NIH

Publisher

MDPI AG

Subject

Virology,Infectious Diseases

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