Ischemia/reperfusion injury in the liver of BALB/c mice activates AP‐1 and nuclear factor κB independently of IκB degradation

Ralf M Zwacka; Yulong Zhang; Weihong Zhou; Jeff Halldorson; John F Engelhardt

doi:10.1002/hep.510280417

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Ischemia/reperfusion injury in the liver of BALB/c mice activates AP‐1 and nuclear factor κB independently of IκB degradation

Journal article

Peer reviewed

Ischemia/reperfusion injury in the liver of BALB/c mice activates AP‐1 and nuclear factor κB independently of IκB degradation

Ralf M Zwacka, Yulong Zhang, Weihong Zhou, Jeff Halldorson and John F Engelhardt

Hepatology (Baltimore, Md.), Vol.28(4), pp.1022-1030

10/1998

DOI: 10.1002/hep.510280417

PMID: 9755239

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Abstract

For many inherited and acquired hepatic diseases, liver transplantation is the only possible therapeutic strategy. Ischemia/reperfusion (I/R) damage to donor tissue is thought to be one component that may play a role in the decline of posttransplant tissue function and ultimately rejection. The transcription factors, AP‐1 and nuclear factor κB (NF‐κB), play important roles in the acute cellular responses to tissue damage, as well as the inflammatory phase following I/R. We have found that the DNA binding activity of AP‐1 was dramatically increased following warm ischemia at 1 to 3 hours postreperfusion. Induced DNA binding activity was composed of predominately c‐Jun and JunD hetero‐ and homodimers as determined by electrophoretic mobility supershift assays. This increase in AP‐1 activity occurred in the absence of significant changes in the steady‐state protein levels of c‐Jun and JunB. Maximal activation of Jun amino‐terminal kinase (JNK) occurred within the 25 to 30 minutes postreperfusion, just before the peak in AP‐1 DNA binding. These findings suggest that phosphorylation may play an important role in regulating AP‐1 transcriptional complexes. Furthermore, JunD protein levels slightly increased at 3 hours postreperfusion, concordant with changes in AP‐1 DNA binding activity. The activation of NF‐κB at 1 hour postreperfusion was independent of proteolytic degradation of IκB‐α or IκB‐β. This activation of NF‐κB DNA binding activity in the nucleus was preceded by an increase in tyrosine phosphorylation of IκB‐α. These studies suggest that JNK, IκB tyrosine kinase, and JunD are potential targets for therapeutic intervention during liver I/R injury.

Details

Title: Subtitle: Ischemia/reperfusion injury in the liver of BALB/c mice activates AP‐1 and nuclear factor κB independently of IκB degradation
Creators: Ralf M Zwacka
Yulong Zhang
Weihong Zhou
Jeff Halldorson
John F Engelhardt
Resource Type: Journal article
Publication Details: Hepatology (Baltimore, Md.), Vol.28(4), pp.1022-1030
DOI: 10.1002/hep.510280417
PMID: 9755239
NLM abbreviation: Hepatology
ISSN: 0270-9139
eISSN: 1527-3350
Publisher: W.B. Saunders; Philadelphia, PA
Number of pages: 9
Grant note: NIH NIDDK (to J.F.E.) (R01 DK51315)
Language: English
Date published: 10/1998
Academic Unit: Roy J. Carver Department of Biomedical Engineering; Anatomy and Cell Biology; Radiation Oncology; Internal Medicine
Record Identifier: 9984025340402771

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