HIF2α is a Direct Regulator of Neutrophil Motility

Sormendi, Sundary; Deygas, Mathieu; Sinha, Anupam; Krüger, Anja; Kourtzelis, Ioannis; Le Lay, Gregoire; Bernard, Mathilde; Sáez, Pablo J.; Gerlach, Michael; Franke, Kristin; Meneses, Ana; Kräter, Martin; Palladini, Allesandra; Guck, Jochen; Coskun, Ünal; Chavakis, Triantafyllos; Vargas, Pablo; Wielockx, Ben

doi:10.1182/blood.2020007505

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HIF2α is a Direct Regulator of Neutrophil Motility

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Kräter, Martin
Guck Division, Max Planck Institute for the Science of Light, Max Planck Society;

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Guck, Jochen
Technische Universität Dresden;
Guck Division, Max Planck Institute for the Science of Light, Max Planck Society;
Max-Planck-Zentrum für Physik und Medizin, Max Planck Institute for the Science of Light, Max Planck Society;

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2020.06.05.137133v1.full.pdf
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Zitation

Sormendi, S., Deygas, M., Sinha, A., Krüger, A., Kourtzelis, I., Le Lay, G., et al. (2021). HIF2α is a Direct Regulator of Neutrophil Motility. Blood. doi:10.1182/blood.2020007505.

Zitierlink: https://hdl.handle.net/21.11116/0000-0007-D708-E

Zusammenfassung

Orchestrated recruitment of neutrophils to inflamed tissue is essential during initiation of inflammation. Inflamed areas are usually hypoxic, and adaptation to reduced oxygen pressure is typically mediated by hypoxia pathway proteins. However, it is still unclear how these factors influence the migration of neutrophils to and at the site of inflammation either during their transmigration through the blood-endothelial cell barrier, or their motility in the interstitial space. Here, we reveal that activation of the Hypoxia Inducible Factor-2 (HIF2α) due to deficiency of HIF-prolyl hydroxylase domain protein-2 (PHD2) boosts neutrophil migration specifically through highly confined microenvironments. In vivo, the increased migratory capacity of PHD2-deficient neutrophils resulted in massive tissue accumulation in models of acute local inflammation. Using systematic RNAseq analyses and mechanistic approaches, we identified RhoA, a cytoskeleton organizer, as the central downstream factor that mediates HIF2α-dependent neutrophil motility. Thus, we propose that the here identified novel PHD2-HIF2α-RhoA axis is vital to the initial stages of inflammation as it promotes neutrophil movement through highly confined tissue landscapes.