Activation of c-Jun NH₂-terminal kinase (JNK) pathway during islet transplantation and prevention of islet graft loss by intraportal injection of JNK inhibitor

H. Noguchi, Y. Nakai, M. Ueda, Y. Masui, S. Futaki, N. Kobayashi, S. Hayashi and S. Matsumoto

View Related Documents

Journal Article
The c-Jun N-terminal kinase JNK participates in cytokine- and isolation stress-induced rat pancreatic islet apoptosis
S. Abdelli, A. Abderrahmani, B. J. Hering, J. S. Beckmann and C. Bonny
Diabetologia, 2007, Volume 50, Number 8, Pages 1660-1669
- Download PDF (437.4 KB)
- View HTML
Journal Article
Changes in gene expression in beta cells after islet isolation and transplantation using laser-capture microdissection
Y. B. Ahn, G. Xu, L. Marselli, E. Toschi and A. Sharma, et al.
Diabetologia, 2007, Volume 50, Number 2, Pages 334-342
Journal Article
Inhibition of c-jun N terminal kinase (JNK) improves functional beta cell mass in human islets and leads to AKT and glycogen synthase kinase-3 (GSK-3) phosphorylation
A. Fornoni, A. Pileggi, R. D. Molano, N. Y. Sanabria and T. Tejada, et al.
Diabetologia, 2008, Volume 51, Number 2, Pages 298-308
Journal Article
Exendin-4 treatment improves metabolic control after rat islet transplantation to athymic mice with streptozotocin-induced diabetes
A. Sharma, A. Sörenby, A. Wernerson, S. Efendic and M. Kumagai-Braesch, et al.
Diabetologia, 2006, Volume 49, Number 6, Pages 1247-1253
- Download PDF (195.5 KB)
- View HTML
Journal Article
Improving islet transplantation by gene delivery of hepatocyte growth factor (HGF) and its downstream target, protein kinase B (PKB)/Akt
Nathalie Fiaschi-Taesch, Andrew F. Stewart and Adolfo Garcia-Ocaña
Cell Biochemistry and Biophysics, 2007, Volume 48, Numbers 2-3, Pages 191-199
- Download PDF (304.9 KB)
- View HTML
Journal Article
Protein transduction technology offers a novel therapeutic approach for diabetes
Hirofumi Noguchi and Shinichi Matsumoto
Journal of Hepato-Biliary-Pancreatic Surgery, 2006, Volume 13, Number 4, Pages 306-313
- Download PDF (263.7 KB)
Journal Article
Islet transplantation at the Diabetes Research Institute Japan
Hirofumi Noguchi and Shinichi Matsumoto
Journal of Hepato-Biliary-Pancreatic Surgery, 2008, Volume 15, Number 3, Pages 278-283
- Download PDF (155.7 KB)
Journal Article
Current Status and Prospects for Gene and Cell Therapeutics for Type 1 Diabetes Mellitus
Nick Giannoukakis and Massimo Trucco
Reviews in Endocrine & Metabolic Disorders, 2003, Volume 4, Number 4, Pages 369-380
- Download PDF (4.2 KB)
Journal Article
Glucose- and Metabolically Regulated Hepatic Insulin Gene Therapy for Diabetes
Paul Yueh-Jen Hsu, Robert M. Kotin and Ya-Wun Yang
Pharmaceutical Research, 2008, Volume 25, Number 6, Pages 1460-1468
- Download PDF (305.8 KB)
- View HTML
Journal Article
The altered expression of glucose-regulated proteins 78 in different phase of streptozotocin-affected pancreatic beta-cells
Min Wang, Ping Wang, Ji-Lin Peng, Sha Wu and Xiao-Ping Zhao, et al.
Cell Stress and Chaperones, 2009, Volume 14, Number 1, Pages 43-48
- Download PDF (297.8 KB)
- View HTML

Abstract

Aims/hypothesis

Although application of the Edmonton protocol has markedly improved the outcome for pancreatic islet transplantation, the insulin independence rate after islet transplantation from one donor pancreas has remained low. During the isolation process and subsequent clinical transplantation, islets are subjected to severe adverse conditions that impair survival and ultimately contribute to graft failure. The aim of this study was to map the c-Jun NH₂-terminal kinase (JNK) pathway that mediates islet loss during islet transplantation and to clarify whether intraportal injection with JNK inhibitor during islet transplantation can prevent islet graft loss.

Methods

We measured JNK activity in the liver, fat and muscle of diabetic mice and in the liver immediately after islet transplantation. We examined the effect of intraportal injection of JNK inhibitory peptide at islet transplantation.

Results

JNK activity became progressively higher at least until 24 h after transplantation. The cell-permeable peptide of JNK inhibitor was delivered not only in the liver but also in other insulin target organs, preventing JNK activation in the liver at least until 24 h after transplantation and reducing JNK activity in these insulin target organs. Moreover, the peptide inhibitor prevented islet graft loss immediately after transplantation and improved islet transplant outcome.

Conclusions/interpretation

These findings suggest that control of the JNK pathway is extremely important in islet transplantation and that intraportal injection of JNK inhibitor during islet transplantation (addition of JNK inhibitor to transplant media) could prevent the impairment of islet cells, leading to improved outcome for pancreatic islet transplantation.

Keywords Cell-permeable peptide - Islet transplantation - JNK inhibitory peptide - c-Jun NH₂-terminal kinase

Fulltext Preview

Image of the first page of the fulltext document

Frequently asked questions General info on journals and books Send us your feedback Impressum Contact us

SpringerLink

Activation of c-Jun NH2-terminal kinase (JNK) pathway during islet transplantation and prevention of islet graft loss by intraportal injection of JNK inhibitor