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Co-option of Neutrophil Fates by Tissue Environments

Overview
Journal Cell
Publisher Cell Press
Specialty Cell Biology
Date 2020 Oct 25
PMID 33098771
Citations 178
Authors
Ivan Ballesteros
Andrea Rubio-Ponce
Marco Genua
Eleonora Lusito
Immanuel Kwok
Gabriel Fernandez-Calvo
Tariq E Khoyratty
Erinke van Grinsven
Sara Gonzalez-Hernandez
Jose Angel Nicolas-Avila
Tommaso Vicanolo
Antonio Maccataio
Alberto Benguria
Jackson LiangYao Li
Jose M Adrover
Alejandra Aroca-Crevillen
Juan A Quintana
Sandra Martin-Salamanca
Francisco Mayo
Stefanie Ascher
Giulia Barbiera
Oliver Soehnlein
Matthias Gunzer
Florent Ginhoux
Fatima Sanchez-Cabo
Estanislao Nistal-Villan
Christian Schulz
Ana Dopazo
Christoph Reinhardt
Irina A Udalova
Lai Guan Ng
Renato Ostuni
Andres Hidalgo
Affiliations
Soon will be listed here.
Abstract

Classically considered short-lived and purely defensive leukocytes, neutrophils are unique in their fast and moldable response to stimulation. This plastic behavior may underlie variable and even antagonistic functions during inflammation or cancer, yet the full spectrum of neutrophil properties as they enter healthy tissues remains unexplored. Using a new model to track neutrophil fates, we found short but variable lifetimes across multiple tissues. Through analysis of the receptor, transcriptional, and chromatin accessibility landscapes, we identify varying neutrophil states and assign non-canonical functions, including vascular repair and hematopoietic homeostasis. Accordingly, depletion of neutrophils compromised angiogenesis during early age, genotoxic injury, and viral infection, and impaired hematopoietic recovery after irradiation. Neutrophils acquired these properties in target tissues, a process that, in the lungs, occurred in CXCL12-rich areas and relied on CXCR4. Our results reveal that tissues co-opt neutrophils en route for elimination to induce programs that support their physiological demands.

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