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Role of ARP2/3 Complex-Driven Actin Polymerization in RSV Infection

Autumn Paluck, Jaspreet Osan, Lauren Hollingsworth, Sattya N. Talukdar, Ali Al Saegh, Masfique Mehedi

2021Pathogens24 citationsDOIOpen Access PDF

Abstract

Respiratory syncytial virus (RSV) is the leading viral agent causing bronchiolitis and pneumonia in children under five years old worldwide. The RSV infection cycle starts with macropinocytosis-based entry into the host airway epithelial cell membrane, followed by virus transcription, replication, assembly, budding, and spread. It is not surprising that the host actin cytoskeleton contributes to different stages of the RSV replication cycle. RSV modulates actin-related protein 2/3 (ARP2/3) complex-driven actin polymerization for a robust filopodia induction on the infected lung epithelial A549 cells, which contributes to the virus's budding, and cell-to-cell spread. Thus, a comprehensive understanding of RSV-induced cytoskeletal modulation and its role in lung pathobiology may identify novel intervention strategies. This review will focus on the role of the ARP2/3 complex in RSV's pathogenesis and possible therapeutic targets to the ARP2/3 complex for RSV.

Topics & Concepts

PolymerizationActinMaterials scienceCell biologyBiologyComposite materialPolymerVirus-based gene therapy researchRespiratory viral infections researchViral Infections and Immunology Research