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This research aims to synthesize and evaluate novel flexible nucleoside analogues as potential treatments for H1N1 influenza virus.

March 29, 2026Open Access

Synthesis and evaluation of novel flexible nucleoside analogues against H1N1 influenza virus

Key Points

This research aims to synthesize and evaluate novel flexible nucleoside analogues as potential treatments for H1N1 influenza virus.
Chemically synthesized a series of flexible nucleoside analogues with a specific base moiety and pentose sugar ring.
Tested antiviral activity against H1N1 influenza virus in vitro.
Assessed safety profiles including cytotoxicity and in vivo toxicity.
The most potent analogue, 7c, showed an EC50 of 1.371 μM against H1N1.
Compound 7c had excellent safety with a CC50 >200 μM and an in vivo LD50 >2000 mg/kg.
The novel analogues exhibit low micromolar levels of antiviral activity.

Abstract

Flexible nucleoside analogues (fleximers) are viewed as a new class of inhibitors against numerous highly lethal RNA virus infections and pandemics. In this work, we chemically synthesized a series of novel fleximers featuring a flexible base moiety connected to a pentose sugar ring and tested them for activity against H1N1 influenza virus. The novel flexible nucleoside analogues exhibit low micromolar levels of antiviral activity. The most potent 7c is able to potently inhibit the multiplication of the H1N1 influenza strains with an in vitro anti-H1N1 EC 50 of 1.371 μM. Most importantly, 7c demonstrated an excellent safety profile with cytotoxicity CC 50 >200μM and an in vivo mouse LD 50 > 2000 mg/kg. As such, 7c could serve as a novel lead compound for the further development of antiviral drug candidate.

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Synthesis and evaluation of novel flexible nucleoside analogues against H1N1 influenza virus

Key Points

Abstract

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