Novel Small Molecule Targeting the Hemagglutinin Stalk of Influenza Viruses

Author:

Kim Jin Il1,Lee Sangmoo1,Lee Gong Yeal2,Park Sehee1,Bae Joon-Yong1,Heo Jun2,Kim Hong-Youb2,Woo Seok-Hun2,Lee Hae Un2,Ahn Chung Am2,Bang Hye Jin2,Ju Hyun Soo2,Ok Kiwon3,Byun Youngjoo3,Cho Dae-Jin2,Shin Jae Soo2,Kim Dong-Yeon2,Park Mee Sook1,Park Man-Seong1

Affiliation:

1. Department of Microbiology and Institute for Viral Diseases, College of Medicine, Korea University, Seoul, Republic of Korea

2. Il-Yang Pharmaceutical Co., Yongin, Republic of Korea

3. College of Pharmacy, Korea University, Sejong, Republic of Korea

Abstract

Anti-influenza drugs with broad-spectrum efficacy against antigenically diverse influenza viruses can be highly useful when no vaccines are available. To develop new anti-influenza drugs, we screened a number of small molecules and identified a strong candidate, IY7640. When added at the time of or after influenza virus infection, IY7640 was observed to successfully inhibit or reduce viral replication in cells. We subsequently discovered that IY7640 targets the stalk region of the influenza HA protein, which exhibits a relatively high degree of amino acid sequence conservation across various (sub)types of influenza viruses. Furthermore, IY7640 was observed to block HA-mediated membrane fusion of H1N1, H3N2, and influenza B viruses in cells. Although it appears less effective against strains other than H1N1 subtype viruses in a challenge study in mice, we suggest that the small molecule IY7640 has potential to be optimized as a new anti-influenza drug.

Funder

National Research Foundation of Korea

Publisher

American Society for Microbiology

Subject

Virology,Insect Science,Immunology,Microbiology

Reference59 articles.

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