Literature DB >> 16950761

Hepatocyte NF-kappaB activation is hepatoprotective during ischemia-reperfusion injury and is augmented by ischemic hypothermia.

Satoshi Kuboki1, Tomohisa Okaya, Rebecca Schuster, John Blanchard, Alvin Denenberg, Hector R Wong, Alex B Lentsch.   

Abstract

The present study examined the role of hepatocyte NF-kappaB activation during ischemia-reperfusion injury. Second, we evaluated the effects of ischemic hypothermia on NF-kappaB activation and liver injury. C57BL/6 mice underwent 90 min of partial hepatic ischemia and up to 8 h of reperfusion. Body temperature was regulated during the ischemic period between 35 and 37 degrees C, 33 and 35 degrees C, 29 and 33 degrees C or unregulated, where temperature fell to <29 degrees C. Liver injury, as measured by serum alanine aminotransferase as well as liver histopathology, was inversely proportional to regulated body temperature, with the unregulated group (<29 degrees C) being highly protected and the normothermic group (35-37 degrees C) displaying the greatest injury. Inflammation, as measured by production of TNF-alpha and liver recruitment of neutrophils, was greatest in the normothermic groups and lowest in the ischemic hypothermia groups. Interestingly, hepatocyte NF-kappaB activation was highest in the hypothermic group and least in the normothermic group. Paradoxically, degradation of IkappaB proteins, IkappaB-alpha and IkappaB-beta, was greatest in the normothermic group, suggesting an alternate NF-kappaB regulatory mechanism during ischemia-reperfusion injury. Subsequently, we found that NF-kappaB p65 protein was increasingly degraded in normothermic versus hypothermic groups, and this degradation was specific for hepatocytes and was associated with decreased expression of the peptidyl-prolyl isomerase Pin1. The data suggest that NF-kappaB activation in hepatocytes is a protective response during ischemia-reperfusion and can be augmented by ischemic hypothermia. Furthermore, it appears that Pin1 promotes NF-kappaB p65 protein stability such that decreased expression of Pin1 during ischemia-reperfusion results in p65 degradation, reduced nuclear translocation of NF-kappaB, and enhanced hepatocellular injury.

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Year:  2006        PMID: 16950761     DOI: 10.1152/ajpgi.00186.2006

Source DB:  PubMed          Journal:  Am J Physiol Gastrointest Liver Physiol        ISSN: 0193-1857            Impact factor:   4.052


  32 in total

1.  Receptor activator of nuclear factor-κB ligand (RANKL) protects against hepatic ischemia/reperfusion injury in mice.

Authors:  Nozomu Sakai; Heather L Van Sweringen; Rebecca Schuster; John Blanchard; Justin M Burns; Amit D Tevar; Michael J Edwards; Alex B Lentsch
Journal:  Hepatology       Date:  2012-01-13       Impact factor: 17.425

Review 2.  Innate Immune Regulations and Liver Ischemia-Reperfusion Injury.

Authors:  Ling Lu; Haoming Zhou; Ming Ni; Xuehao Wang; Ronald Busuttil; Jerzy Kupiec-Weglinski; Yuan Zhai
Journal:  Transplantation       Date:  2016-12       Impact factor: 4.939

3.  Abnormal modulation of cell protective systems in response to ischemic/reperfusion injury is important in the development of mouse sickle cell hepatopathy.

Authors:  Angela Siciliano; Giorgio Malpeli; Orah S Platt; Christophe Lebouef; Anne Janin; Aldo Scarpa; Oliviero Olivieri; Eliana Amato; Roberto Corrocher; Yves Beuzard; Lucia De Franceschi
Journal:  Haematologica       Date:  2010-09-17       Impact factor: 9.941

4.  The peptidyl-prolyl isomerase, Pin1, facilitates NF-kappaB binding in hepatocytes and protects against hepatic ischemia/reperfusion injury.

Authors:  Satoshi Kuboki; Nozomu Sakai; Callisia Clarke; Rebecca Schuster; John Blanchard; Michael J Edwards; Alex B Lentsch
Journal:  J Hepatol       Date:  2009-05-24       Impact factor: 25.083

5.  Unique early gene expression patterns in human adult-to-adult living donor liver grafts compared to deceased donor grafts.

Authors:  J de Jonge; S Kurian; A Shaked; K R Reddy; W Hancock; D R Salomon; K M Olthoff
Journal:  Am J Transplant       Date:  2009-04       Impact factor: 8.086

Review 6.  CXC chemokines play a critical role in liver injury, recovery, and regeneration.

Authors:  Callisia N Clarke; Satoshi Kuboki; Amit Tevar; Alex B Lentsch; Michael Edwards
Journal:  Am J Surg       Date:  2009-09       Impact factor: 2.565

Review 7.  Genomics of liver transplant injury and regeneration.

Authors:  Sohaib Khalid Hashmi; Esther Baranov; Ana Gonzalez; Kim Olthoff; Abraham Shaked
Journal:  Transplant Rev (Orlando)       Date:  2014-03-04       Impact factor: 3.943

8.  Age-related decrease in proteasome expression contributes to defective nuclear factor-kappaB activation during hepatic ischemia/reperfusion.

Authors:  Nadine Huber; Nozomu Sakai; Thorsten Eismann; Thomas Shin; Satoshi Kuboki; John Blanchard; Rebecca Schuster; Michael J Edwards; Hector R Wong; Alex B Lentsch
Journal:  Hepatology       Date:  2009-05       Impact factor: 17.425

9.  Reactive oxygen species mediate liver injury through parenchymal nuclear factor-kappaB inactivation in prolonged ischemia/reperfusion.

Authors:  Laura Llacuna; Montserrat Marí; Josep M Lluis; Carmen García-Ruiz; José C Fernández-Checa; Albert Morales
Journal:  Am J Pathol       Date:  2009-04-06       Impact factor: 4.307

Review 10.  Hepatic Ischemia/Reperfusion: Mechanisms of Tissue Injury, Repair, and Regeneration.

Authors:  Takanori Konishi; Alex B Lentsch
Journal:  Gene Expr       Date:  2017-09-11
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