Hypothermic oxygenated perfusion protects from mitochondrial injury before liver transplantation

Autor:	Philipp Kron, Matteo Mueller, Olivier de Rougemont, David Meierhofer, Philipp Dutkowski, Paolo Muiesan, Anna Stepanova, Xavier Muller, Andrea Schlegel, Alexander Galkin, Pierre-Alain Clavien
Přispěvatelé:	University of Zurich, Dutkowski, Philipp
Rok vydání:	2020
Předmět:	DWIT Donor warm ischemia time SDH Succinate dehydrogenase Transplantation Conditioning medicine.medical_treatment DBD Donation after brain death Liver transplantation Pharmacology OLT Orthotopic liver transplantation AS Anastomotic strictures 0302 clinical medicine FAD Flavin adenine dinucleotide DCD Donation after circulatory death D-HOPE Dual hypothermic oxygenated perfusion Normothermic oxygenated perfusion General Medicine IMP Inosine monophosphate Perfusion 030220 oncology & carcinogenesis AST Aspartate aminotransferase DBQ Decylubiquinone lcsh:Medicine (General) HAT Hepatic artery thrombosis Inosine monophosphate AMP Adenosine monophosphate MELD Model of end stage liver disease General Biochemistry Genetics and Molecular Biology RET Reverse electron flow Structure-Activity Relationship 03 medical and health sciences CD-68 Cluster of differentiation 68 IC Ischemic cholangiopathy 1300 General Biochemistry Genetics and Molecular Biology Complex I DAMP`s Danger associated molecular pattern`s Humans LDH Lactate dehydrogenase CS cold storage lcsh:R NAD medicine.disease FMN flavin mononucleotide Oxygen LT Liver transplantation 030104 developmental biology NMP Normothermic machine perfusion Hypothermic oxygenated perfusion HOPE Hypothermic oxygenated perfusion Biomarkers NADP ROS Reactive oxygen species 0301 basic medicine 8-OHdG 8-hydroxy-2-deoxy guanosine PV portal vein lcsh:Medicine EAD Early allograft dysfunction Liver Function Tests Hypothermia Induced HAR Hexaammineruthenium GSH Glutathione lcsh:R5-920 Chemistry Temperature PNF Primary non function HMGB-1 High mobility group box-1 protein Cellular Reprogramming NAD/NADH Nicotine adenine dinucleotide (oxidized/ reduced) Mitochondria ICU Intensive care unit Liver ECMO Extracorporeal membrane oxygenation Reperfusion Injury H&E Hematoxylin and eosin Models Animal KC`s Kupffer cells MPT pore Mitochondria permeability transition pore Research Paper ATP adenosine triphosphate MPS Machine perfusion solution Cold storage 610 Medicine & health ADP Adenosine diphosphate HMP Hypothermic machine perfusion ICAM-1 Intercellular adhesion molecule-1 SEC Sinusoidal endothelial cells NRP Normothermic regional perfusion medicine Animals FMN TLR-4 Toll-like-receptor-4 10217 Clinic for Visceral and Transplantation Surgery Machine perfusion OAA Oxaloacetate ALT Alanine aminotransferase Rats Transplantation HA Hepatic artery NAS Non-anastomotic strictures Electron Transport Chain Complex Proteins Mitochondrial permeability transition pore ECD Extended criteria donor Liver function Energy Metabolism Reperfusion injury
Zdroj:	EBioMedicine EBioMedicine, Vol 60, Iss, Pp 103014-(2020)
ISSN:	2352-3964
DOI:	10.1016/j.ebiom.2020.103014
Popis:	Background Mitochondrial succinate accumulation has been suggested as key event for ischemia reperfusion injury in mice. No specific data are however available on behavior of liver mitochondria during ex situ machine perfusion in clinical transplant models. Methods We investigated mitochondrial metabolism of isolated perfused rat livers before transplantation. Livers were exposed to warm and cold ischemia to simulate donation after circulatory death (DCD) and organ transport. Subsequently, livers were perfused with oxygenated Belzer-MPS for 1h, at hypothermic or normothermic conditions. Various experiments were performed with supplemented succinate and/or mitochondrial inhibitors. The perfusate, liver tissues, and isolated mitochondria were analyzed by mass-spectroscopy and fluorimetry. Additionally, rat DCD livers were transplanted after 1h hypothermic or normothermic oxygenated perfusion. In parallel, perfusate samples were analysed during HOPE-treatment of human DCD livers before transplantation. Findings Succinate exposure during rat liver perfusion triggered a dose-dependent release of mitochondrial Flavin-Mononucleotide (FMN) and NADH in perfusates under normothermic conditions. In contrast, perfusate FMN was 3-8 fold lower under hypothermic conditions, suggesting less mitochondrial injury during cold re-oxygenation compared to normothermic conditions. HOPE-treatment induced a mitochondrial reprogramming with uploading of the nucleotide pool and effective succinate metabolism. This resulted in a clear superiority after liver transplantation compared to normothermic perfusion. Finally, the degree of mitochondrial injury during HOPE of human DCD livers, quantified by perfusate FMN and NADH, was predictive for liver function. Interpretation Mitochondrial injury determines outcome of transplanted rodent and human livers. Hypothermic oxygenated perfusion improves mitochondrial function, and allows viability assessment of liver grafts before implantation. Funding detailed information can be found in Acknowledgments. Graphical Abstract Image, graphical abstract
Databáze:	OpenAIRE
Externí odkaz:	https://explore.openaire.eu/search/publication?articleId=doi_dedup___::66b9e911eda3c09d19bbb520f7b49a76 https://doi.org/10.1016/j.ebiom.2020.103014 Zobrazit plný text záznamu