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Mitochondrial damage–associated molecular patterns released by lung transplants are associated with primary graft dysfunction
Journal article   Peer reviewed

Mitochondrial damage–associated molecular patterns released by lung transplants are associated with primary graft dysfunction

Davide Scozzi, Mohsen Ibrahim, Fuyi Liao, Xue Lin, Hsi-Min Hsiao, Ramsey Hachem, Laneshia K. Tague, Alberto Ricci, Hrishikesh S. Kulkarni, Howard J. Huang, …
American Journal of Transplantation, Vol.19(5)
2019

Abstract

Aged Alarmins Animals Cell Separation DNA, Mitochondrial Female Flow Cytometry Graft Survival Humans Lung Lung Diseases Lung Transplantation Male Mice Mice, Inbred C57BL Middle Aged Mitochondria Neutrophils Primary Graft Dysfunction Pulmonary Edema Reactive Oxygen Species Receptors, Formyl Peptide Reperfusion Injury Retrospective Studies Tissue Donors cyclosporine formylated peptide receptor 1 mitochondrial damage associated molecular pattern mitochondrial DNA mitochondrial protein peptide reactive oxygen metabolite unclassified drug alarmin formylpeptide receptor FPR1 protein, human mitochondrial DNA reactive oxygen metabolite adult aged airway cell animal tissue Article controlled study disease severity female gene deletion histopathology human lung transplantation major clinical study male middle aged mitochondrion mouse neutrophil neutrophil chemotaxis neutrophilia nonhuman peripheral circulation primary graft dysfunction priority journal reperfusion injury retrospective study transendothelial and transepithelial migration adverse event animal blood C57BL mouse cell separation complication donor flow cytometry graft survival immunology lung lung disease lung edema lung transplantation metabolism mitochondrion primary graft dysfunction

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