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Effect of glucagon-like peptide-1 gene expression on graft function in mouse islet transplantation

Authors
Chae, Hee YoungKang, Jun GooKim, Chul SikLee, Seong JinLee, MinhyungKang, DongchulJun, Hee-SookIhm, Sung-Hee
Issue Date
Feb-2012
Publisher
WILEY
Keywords
glucagon-like peptide-1 (GLP-1); islet; transplantation
Citation
TRANSPLANT INTERNATIONAL, v.25, no.2, pp.242 - 249
Journal Title
TRANSPLANT INTERNATIONAL
Volume
25
Number
2
Start Page
242
End Page
249
URI
https://scholarworks.bwise.kr/gachon/handle/2020.sw.gachon/16585
DOI
10.1111/j.1432-2277.2011.01394.x
ISSN
0934-0874
Abstract
This study investigated the effect of local glucagon-like peptide-1 (GLP-1) production within mouse islets on cytoprotection in vitro and in vivo by gene transfer of GLP-1. Transduction of recombinant adenovirus vector expressing GLP-1 (rAd-GLP-1) induced a significant increase in bioactive GLP-1 in the mouse islet culture, whereas transduction with adenovirus vector expressing beta-galactosidase (rAd-LacZ), as a control, had no effect on GLP-1 secretion. Islets transduced with rAd-GLP-1 were protected from H2O2-induced cell damage in vitro. In addition, glucose-stimulated insulin secretion was significantly increased in rAd-GLP-1-transduced islets. When transplanted under the kidney capsule of diabetic syngeneic mice, islet grafts retrieved 4 or 7 days after transplantation revealed that the rAd-GLP-1-transduced group had significantly more Ki67-positive cells as compared with the rAd-LacZ-transduced group. Regarding blood glucose control, diabetic mice transplanted with a marginal mass of rAd-GLP-1-transduced islets became normoglycemic more rapidly and 78% of the recipients were normoglycemic at 35 days post-transplant, whereas only 48% of the mice transplanted with rAd-LacZ-transduced islets were normoglycemic (P < 0.05). In conclusion, delivery of the GLP-1 gene to islets enhanced islet cell survival during the early post-transplant period, and preserved islet mass and functions over time in the transplants.
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