DANGER Signals Activate G -Protein Receptor Kinases Suppressing Neutrophil Function and Predisposing to Infection After Tissue Trauma

Hyo In Kim; Jinbong Park; David Gallo; Sidharth Shankar; Barbora Konecna; Yohan Han; Valerie Banner-Goodspeed; Krystal R Capers; Seong-Gyu Ko; Leo E Otterbein; Kiyoshi Itagaki; Carl J Hauser

doi:10.1097/SLA.0000000000005898

DANGER Signals Activate G -Protein Receptor Kinases Suppressing Neutrophil Function and Predisposing to Infection After Tissue Trauma

Ann Surg. 2023 Dec 1;278(6):e1277-e1288. doi: 10.1097/SLA.0000000000005898. Epub 2023 May 8.

Authors

Affiliations

¹ Department of Surgery, Beth Israel Deaconess Medical Center, Harvard Medical School, Boston, MA.
² College of Korean Medicine, Kyung Hee University, Seoul, Republic of Korea.
³ Institute of Molecular Biomedicine, Faculty of Medicine, Comenius University, Bratislava, Slovakia.
⁴ Department of Anesthesia, Critical Care and Pain Medicine, Beth Israel Deaconess Medical Center, Harvard Medical School, Boston, MA.

PMID: 37154066
DOI: 10.1097/SLA.0000000000005898

Abstract

Objective: Injured tissue predisposes the subject to local and systemic infection. We studied injury-induced immune dysfunction seeking novel means to reverse such predisposition.

Background: Injury mobilizes primitive "DANGER signals" [danger-associated molecular patterns (DAMPs)] activating innate immunocyte (neutrophils, PMN) signaling and function. Mitochondrial formyl peptides activate G -protein coupled receptors (GPCR) like formyl peptide receptor-1. Mitochondrial DNA and heme activate toll-like receptors (TLR9 and TLR2/4). GPCR kinases (GRKs) can regulate GPCR activation.

Methods: We studied human and mouse PMN signaling elicited by mitochondrial DAMPs (GPCR surface expression; protein phosphorylation, or acetylation; Ca 2+ flux) and antimicrobial functions [cytoskeletal reorganization, chemotaxis (CTX), phagocytosis, bacterial killing] in cellular systems and clinical injury samples. Predicted rescue therapies were assessed in cell systems and mouse injury-dependent pneumonia models.

Results: Mitochondrial formyl peptides activate GRK2, internalizing GPCRs and suppressing CTX. Mitochondrial DNA suppresses CTX, phagocytosis, and killing through TLR9 through a novel noncanonical mechanism that lacks GPCR endocytosis. Heme also activates GRK2. GRK2 inhibitors like paroxetine restore functions. GRK2 activation through TLR9 prevented actin reorganization, implicating histone deacetylases (HDACs). Actin polymerization, CTX, bacterial phagocytosis, and killing were also rescued, therefore, by the HDAC inhibitor valproate. Trauma repository PMN showed GRK2 activation and cortactin deacetylation, which varied with severity and was most marked in patients developing infections. Either GRK2 or HDAC inhibition prevented loss of mouse lung bacterial clearance, but only the combination rescued clearance when given postinjury.

Conclusions: Tissue injury-derived DAMPs suppress antimicrobial immunity through canonical GRK2 activation and a novel TLR-activated GRK2-pathway impairing cytoskeletal organization. Simultaneous GRK2/HDAC inhibition rescues susceptibility to infection after tissue injury.

Publication types

Research Support, N.I.H., Extramural
Research Support, U.S. Gov't, Non-P.H.S.
Research Support, Non-U.S. Gov't

MeSH terms

Actins / metabolism
Animals
Anti-Infective Agents*
DNA, Mitochondrial / metabolism
Heme / metabolism
Humans
Mice
Neutrophils* / metabolism
Peptides / metabolism
Toll-Like Receptor 9 / metabolism

Substances

Actins
Toll-Like Receptor 9
DNA, Mitochondrial
Peptides
Anti-Infective Agents
Heme

Abstract

Publication types

MeSH terms

Substances

Grants and funding