Literature DB >> 17542054

A novel way of liver preservation improves rat liver viability upon reperfusion.

Anton Kebis1, Marián Kukan, Peter Grancic, Ján Jakubovský.   

Abstract

BACKGROUND/AIM: Currently, the liver is cold-preserved at 0 approximately 4 degrees C for experimental and clinical purposes. Here, we investigated whether milder hypothermia during the initial phase of the preservation period was beneficial for liver viability upon reperfusion.
METHODS: In the first set of experiments, rat livers were preserved either conventionally in clinically used histidine-trypthopan-ketoglutarate (HTK) solution (Group A: 45 min and Group B: 24 h) or by slow cooling HTK solution (from 13 degrees C to 3 degrees C) during the initial 45 min of preservation (Group C: 24 h). In the second set of experiments, additional groups of livers were evaluated: Group BB--preservation according to Group B and Group CC--preservation according to Group C. Further, some livers were preserved at 13 degrees C for 24 h. Livers were then reperfused using a blood-free perfusion model.
RESULTS: Bile production was approximately 2-fold greater in Group C compared to Group B. Alanine transaminase (ALT) and aspartate transaminase (AST) release into perfusate were 2 approximately 3-fold higher in Group B compared to Group C. No significant differences were found in ALT and AST release between Group C and Group A. Livers in Group CC compared to Group BB exhibited significantly lower portal resistance, greater oxygen consumption and bromosulfophthalein excretion into bile and lower lactate dehydrogenase (LDH) release into perfusate. Histological evaluation of tissue sections in Group BB showed parenchymal dystrophy of hepatocytes, while dystrophy of hepatocytes was absent in Group CC. Livers preserved at 13 degrees C for 24 h exhibited severe ischemic injury.
CONCLUSION: These results suggest that the conventional way of liver preservation is not suitable at least for rat livers and that slow cooling of HTK solution during the initial phase of cold storage can improve liver viability during reperfusion.

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Year:  2007        PMID: 17542054      PMCID: PMC1859871          DOI: 10.1631/jzus.2007.B0289

Source DB:  PubMed          Journal:  J Zhejiang Univ Sci B        ISSN: 1673-1581            Impact factor:   3.066


  12 in total

1.  Protection of the rat liver against rewarming ischemic injury by University of Wisconsin solution.

Authors:  M Lutterová; M Kukan; K Vajdová; D Kuba; C Mislanová; A Kebis; F Danninger; P Mráz
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2.  Apoptosis after ischemia-reperfusion in human liver allografts.

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3.  Changes in liver core temperature during preservation and rewarming in human and porcine liver allografts.

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Review 5.  Reperfusion injury after liver preservation for transplantation.

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Authors:  A Kebis; M Kukan; D Kuba
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Review 7.  Role of hepatocytes and bile duct cells in preservation-reperfusion injury of liver grafts.

Authors:  M Kukan; P S Haddad
Journal:  Liver Transpl       Date:  2001-05       Impact factor: 5.799

8.  Isolated perfusion of rat livers: effect of temperature on O2 consumption, enzyme release, energy store, and morphology.

Authors:  S Fujita; I Hamamoto; K Nakamura; K Tanaka; K Ozawa
Journal:  Nihon Geka Hokan       Date:  1993-03-01

9.  Bile flow--an index of ischemic injury.

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10.  The effects of hepatic preservation at 0 degrees C compared to 5 degrees C: influence of antiproteases and periodic flushing.

Authors:  M Hertl; P B Chartrand; D D West; P R Harvey; S M Strasberg
Journal:  Cryobiology       Date:  1994-10       Impact factor: 2.487

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  2 in total

1.  Evaluation of hepatic CYP2D1 activity and hepatic clearance in type I and type II diabetic rat models, before and after treatment with insulin and metformin.

Authors:  Navid Neyshaburinezhad; Maryam Seidabadi; Mohammadreza Rouini; Hoda Lavasani; Alireza Foroumadi; Yalda H Ardakani
Journal:  Daru       Date:  2020-05-06       Impact factor: 3.117

2.  Can combination therapy with insulin and metformin improve metabolic function of the liver, in type I diabetic patients? An animal model study on CYP2D1 activity.

Authors:  Sara Rezai; Navid Neyshaburinezhad; Mohammadreza Rouini; Hoda Lavasani; Yalda H Ardakani
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  2 in total

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