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Hypothermic Oxygenated Machine Perfusion Prevents Arteriolonecrosis of the Peribiliary Plexus in Pig Livers Donated after Circulatory Death: e88521
by
Gouw, Annette SH
, Leuvenink, Henri GD
, Dries, Sanna opden
, Lisman, Ton
, Sutton, Michael E
, Karimian, Negin
, Wiersema-Buist, Janneke
, Porte, Robert J
, Boer, Marieke Tde
2014
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Hypothermic Oxygenated Machine Perfusion Prevents Arteriolonecrosis of the Peribiliary Plexus in Pig Livers Donated after Circulatory Death: e88521
by
Gouw, Annette SH
, Leuvenink, Henri GD
, Dries, Sanna opden
, Lisman, Ton
, Sutton, Michael E
, Karimian, Negin
, Wiersema-Buist, Janneke
, Porte, Robert J
, Boer, Marieke Tde
in
2014
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Hypothermic Oxygenated Machine Perfusion Prevents Arteriolonecrosis of the Peribiliary Plexus in Pig Livers Donated after Circulatory Death: e88521
by
Gouw, Annette SH
, Leuvenink, Henri GD
, Dries, Sanna opden
, Lisman, Ton
, Sutton, Michael E
, Karimian, Negin
, Wiersema-Buist, Janneke
, Porte, Robert J
, Boer, Marieke Tde
2014
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Hypothermic Oxygenated Machine Perfusion Prevents Arteriolonecrosis of the Peribiliary Plexus in Pig Livers Donated after Circulatory Death: e88521
Journal Article
Hypothermic Oxygenated Machine Perfusion Prevents Arteriolonecrosis of the Peribiliary Plexus in Pig Livers Donated after Circulatory Death: e88521
2014
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Overview
Background Livers derived from donation after circulatory death (DCD) are increasingly accepted for transplantation. However, DCD livers suffer additional donor warm ischemia, leading to biliary injury and more biliary complications after transplantation. It is unknown whether oxygenated machine perfusion results in better preservation of biliary epithelium and the peribiliary vasculature. We compared oxygenated hypothermic machine perfusion (HMP) with static cold storage (SCS) in a porcine DCD model. Methods After 30 min of cardiac arrest, livers were perfused in situ with HTK solution (4 degree C) and preserved for 4 h by either SCS (n = 9) or oxygenated HMP (10 degree C; n = 9), using pressure-controlled arterial and portal venous perfusion. To simulate transplantation, livers were reperfused ex vivo at 37 degree C with oxygenated autologous blood. Bile duct injury and function were determined by biochemical and molecular markers, and a systematic histological scoring system. Results After reperfusion, arterial flow was higher in the HMP group, compared to SCS (251 plus or minus 28 vs 166 plus or minus 28 mL/min, respectively, after 1 hour of reperfusion; p = 0.003). Release of hepatocellular enzymes was significantly higher in the SCS group. Markers of biliary epithelial injury (biliary LDH, gamma-GT) and function (biliary pH and bicarbonate, and biliary transporter expression) were similar in the two groups. However, histology of bile ducts revealed significantly less arteriolonecrosis of the peribiliary vascular plexus in HMP preserved livers (>50% arteriolonecrosis was observed in 7 bile ducts of the SCS preserved livers versus only 1 bile duct of the HMP preserved livers; p = 0.024). Conclusions Oxygenated HMP prevents arteriolonecrosis of the peribiliary vascular plexus of the bile ducts of DCD pig livers and results in higher arterial flow after reperfusion. Together this may contribute to better perfusion of the bile ducts, providing a potential advantage in the post-ischemic recovery of bile ducts.
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