Abstract

The influenza virus is a constantly evolving pathogen that challenges medical and public health systems. Traditionally, curcumin has been used to treat airway inflammatory diseases, such as bronchitis and pneumonia. To elucidate common targets of curcumin and influenza infection and underlying mechanisms, we employed network pharmacology and molecular docking approaches and confirmed results using in vitro experiments. Biological targets of curcumin and influenza were collected, and potential targets were identified by constructing compound–disease target (C-D) and protein–protein interaction (PPI) networks. The ligand–target interaction was determined using the molecular docking method, and in vitro antiviral experiments and target confirmation were conducted to evaluate curcumin’s effects on influenza. Our network and pathway analyses implicated the four targets of AKT1, RELA, MAPK1, and TP53 that could be involved in the inhibitory effects of curcumin on influenza. The binding energy calculations of each ligand–target interaction in the molecular docking showed that curcumin bound to AKT1 with the highest affinity among the four targets. In vitro experiments, in which influenza virus-infected MDCK cells were pre-, co-, or post-treated with curcumin, confirmed curcumin’s prophylactic and therapeutic effects. Influenza virus induction increased the level of mRNA expression of AKT in MDCK cells, and the level was attenuated by curcumin treatment. Collectively, our findings identified potential targets of curcumin against influenza and suggest curcumin as a potential therapy for influenza infection.

Highlights

  • Seasonal influenza A virus (IAV) is an infectious, enveloped, negative-sense, singlestrand RNA virus that is the most common cause of pneumonia-related deaths [1]

  • H. sapiens genes associated with curcumin were retrieved

  • DrugBank, GeneCards, and NCBI databases, and 1317 targets associated with influenza virus were identified from and NCBIand databases

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Summary

Introduction

Seasonal influenza A virus (IAV) is an infectious, enveloped, negative-sense, singlestrand RNA virus that is the most common cause of pneumonia-related deaths [1]. A mild respiratory infection targets the upper respiratory tract, characterized by fever, cough, muscle pain, and fatigue, IAV can lead to severe lethal pneumonia owing to secondary bacterial infection of the lower respiratory tract [2]. Antiviral drugs are used for both treating patients and preventing infection in individuals who have been exposed [2]. The emergence of drug-resistant viruses is a major challenge in using antiviral drugs; it is still necessary to explore alternative therapeutic approaches for treating influenza infection [4].

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