FABP4 As a Therapeutic Host Target Controlling SARS-CoV-2 Infection

Overview

Journal EMBO Mol Med

Date 2025 Jan 22

PMID 39843629

Authors

Hatoon Baazim

Emre Koyuncu

Gurol Tuncman

M Furkan Burak

Lea Merkel

Nadine Bahour

Ezgi Simay Karabulut

Grace Yankun Lee

Alireza Hanifehnezhad

Zehra Firat Karagoz

Katalin Foldes

Ilayda Engin

Ayse Gokce Erman

Sidika Oztop

Nazlican Filazi

Buket Gul

Ahmet Ceylan

Ozge Ozgenc Cinar

Fusun Can

Hahn Kim

Ali Al-Hakeem

Hui Li

Fatih Semerci

Xihong Lin

Erkan Yilmaz

Onder Ergonul

Aykut Ozkul

Gokhan S Hotamisligil

Affiliations

Soon will be listed here.

Abstract

Host metabolic fitness is a critical determinant of infectious disease outcomes. Obesity, aging, and other related metabolic disorders are recognized as high-risk disease modifiers for respiratory infections, including coronavirus infections, though the underlying mechanisms remain unknown. Our study highlights fatty acid-binding protein 4 (FABP4), a key regulator of metabolic dysfunction and inflammation, as a modulator of SARS-CoV-2 pathogenesis, correlating strongly with disease severity in COVID-19 patients. We demonstrate that loss of FABP4 function, by genetic or pharmacological means, reduces SARS-CoV-2 replication and disrupts the formation of viral replication organelles in adipocytes and airway epithelial cells. Importantly, FABP4 inhibitor treatment of infected hamsters diminished lung viral titers, alleviated lung damage and reduced collagen deposition. These findings highlight the therapeutic potential of targeting host metabolism in limiting coronavirus replication and mitigating the pathogenesis of infection.

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