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Crosstalk between nonclassical monocytes and alveolar macrophages mediates transplant ischemia-reperfusion injury through classical monocyte recruitment

Authors :
G. R. Scott Budinger
Félix L. Núñez-Santana
Emilia Lecuona
Hiam Abdala-Valencia
Xianpeng Liu
Wenbin Yang
Haiying Sun
Ziyou Ren
Ali Shilatifard
Mahzad Akbarpour
Qiang Wu
Megan E Kelly
Melissa Querrey
Daniel Kreisel
Sowmya Ravi
Wenjun Li
Emily Cerier
Thalachallour Mohanakumar
Megan L Anderson
Chitaru Kurihara
Ankit Bharat
Source :
JCI Insight, Vol 6, Iss 6 (2021), JCI Insight
Publication Year :
2021
Publisher :
American Society for Clinical investigation, 2021.

Abstract

Primary graft dysfunction (PGD) is the predominant cause of early graft loss following lung transplantation. We recently demonstrated that donor pulmonary intravascular nonclassical monocytes (NCM) initiate neutrophil recruitment. Simultaneously, host-origin classical monocytes (CM) permeabilize the vascular endothelium to allow neutrophil extravasation necessary for PGD. Here, we show that a CCL2-CCR2 axis is necessary for CM recruitment. Surprisingly, although intravital imaging and multichannel flow cytometry revealed that depletion of donor NCM abrogated CM recruitment, single cell RNA sequencing identified donor alveolar macrophages (AM) as predominant CCL2 secretors. Unbiased transcriptomic analysis of murine tissues combined with murine KOs and chimeras indicated that IL-1β production by donor NCM was responsible for the early activation of AM and CCL2 release. IL-1β production by NCM was NLRP3 inflammasome dependent and inhibited by treatment with a clinically approved sulphonylurea. Production of CCL2 in the donor AM occurred through IL-1R-dependent activation of the PKC and NF-κB pathway. Accordingly, we show that IL-1β-dependent paracrine interaction between donor NCM and AM leads to recruitment of recipient CM necessary for PGD. Since depletion of donor NCM, IL-1β, or IL-1R antagonism and inflammasome inhibition abrogated recruitment of CM and PGD and are feasible using FDA-approved compounds, our findings may have potential for clinical translation.

Details

Language :
English
ISSN :
23793708
Volume :
6
Issue :
6
Database :
OpenAIRE
Journal :
JCI Insight
Accession number :
edsair.doi.dedup.....2734624eaa0a6b0a0c6ee04a597e05c3