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GRK2 Mediates β-Arrestin Interactions with 5-HT <sub>2</sub> Receptors for JC Polyomavirus Endocytosis

Colleen L. Mayberry, Michael Wilczek, Tristan M. Fong, Sarah L. Nichols, Melissa S. Maginnis

2021Journal of Virology16 citationsDOIOpen Access PDF

Abstract

As intracellular parasites, viruses require a host cell to replicate and cause disease. Therefore, virus-host interactions contribute to viral pathogenesis. JC polyomavirus (JCPyV) infects most of the population, establishing a lifelong asymptomatic infection within the kidney. Under conditions of severe immunosuppression JCPyV may spread to the central nervous system, causing the fatal demyelinating disease progressive multifocal leukoencephalopathy (PML). Individuals living with HIV or undergoing immunomodulatory therapies are at risk for developing PML. The mechanisms of how JCPyV uses specific receptors on the surface of host cells to initiate internalization and infection is a poorly understood process. We have further identified cellular proteins involved in JCPyV internalization and infection and elucidated their specific interactions that are responsible for activation of receptors. Collectively, these findings illuminate how viruses usurp cellular receptors during infection, contributing to current development efforts for therapeutic options for the treatment or prevention of PML.

Topics & Concepts

BiologyInternalizationArrestinClathrinEndocytosisDynaminCell biologyReceptorVirologyG protein-coupled receptorGeneticsSignal transductionPolyomavirus and related diseasesPlant Virus Research StudiesFull-Duplex Wireless Communications
GRK2 Mediates β-Arrestin Interactions with 5-HT <sub>2</sub> Receptors for JC Polyomavirus Endocytosis | Litcius