| Literature DB >> 34115982 |
Sebastian Baasch1, Piero Giansanti2, Julia Kolter1, André Riedl3, Aaron James Forde4, Solveig Runge4, Simon Zenke4, Roland Elling5, Anne Halenius6, Simone Brabletz7, Hartmut Hengel6, Bernhard Kuster8, Thomas Brabletz7, Luka Cicin-Sain9, Ramon Arens10, Andreas Vlachos11, Jan Christopher Rohr5, Marc Philippe Stemmler7, Manfred Kopf12, Zsolt Ruzsics6, Philipp Henneke13.
Abstract
Cytomegaloviruses (CMVs) have co-evolved with their mammalian hosts for millions of years, leading to remarkable host specificity and high infection prevalence. Macrophages, which already populate barrier tissues in the embryo, are the predominant immune cells at potential CMV entry sites. Here we show that, upon CMV infection, macrophages undergo a morphological, immunophenotypic, and metabolic transformation process with features of stemness, altered migration, enhanced invasiveness, and provision of the cell cycle machinery for viral proliferation. This complex process depends on Wnt signaling and the transcription factor ZEB1. In pulmonary infection, mouse CMV primarily targets and reprograms alveolar macrophages, which alters lung physiology and facilitates primary CMV and secondary bacterial infection by attenuating the inflammatory response. Thus, CMV profoundly perturbs macrophage identity beyond established limits of plasticity and rewires specific differentiation processes, allowing viral spread and impairing innate tissue immunity.Entities:
Keywords: CMV; EMT; Legionella pneumophila; alveolar macrophage; co-evolution; cytomegalovirus; epithelial-mesenchymal transition; host-pathogen interaction; macrophage; myeloid cell differentiation; respiratory tract infection
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Year: 2021 PMID: 34115982 DOI: 10.1016/j.cell.2021.05.009
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 41.582