Transcriptional profiling of stress response in cultured porcine islets

C. M.T. Dvorak; M. Hårdstedt; H. Xie; M. Wang; K. K. Papas; B. J. Hering; M. P. Murtaugh; S. C. Fahrenkrug

doi:10.1016/j.bbrc.2007.03.101

Transcriptional profiling of stress response in cultured porcine islets

C. M.T. Dvorak, M. Hårdstedt, H. Xie, M. Wang, K. K. Papas, B. J. Hering, M. P. Murtaugh, S. C. Fahrenkrug

Research output: Contribution to journal › Article › peer-review

3 Scopus citations

Abstract

Cell-based diabetes therapy may be achieved through xenotransplantation of adult porcine islets, but tissue quality and immunoreactivity barriers need to be overcome. Early identification and exclusion of irreversibly stressed and dying islets may improve transplant outcomes. We used oligonucleotide microarray and quantitative RT-PCR to identify molecular markers of physiological and immunological stress in porcine islets cultured under stress conditions of elevated glucose (16.7 mM), inflammatory cytokine addition (IL-1β, TNF-α, and IFN-γ), or both, for 48 h. Hyperglycemic conditions were associated with increased thioredoxin interacting protein and metabolic process mRNAs, as observed in rodent and primate species. Cytokine treatment increased expression of JAK-STAT pathway components, oxidative stress (transglutaminase 2), and β cell dysfunction genes. Transglutaminase 2 induction is unique to porcine islets. Biomarkers involved in hyperglycemia and islet inflammation may serve as novel targets for improving and monitoring isolated porcine islet function and viability.

Original language	English (US)
Pages (from-to)	118-125
Number of pages	8
Journal	Biochemical and Biophysical Research Communications
Volume	357
Issue number	1
DOIs	https://doi.org/10.1016/j.bbrc.2007.03.101
State	Published - May 25 2007
Externally published	Yes

Keywords

Cytokines
Diabetes
Gene expression
Islet cells
Microarray
Swine

ASJC Scopus subject areas

Biophysics
Biochemistry
Molecular Biology
Cell Biology

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10.1016/j.bbrc.2007.03.101

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title = "Transcriptional profiling of stress response in cultured porcine islets",

abstract = "Cell-based diabetes therapy may be achieved through xenotransplantation of adult porcine islets, but tissue quality and immunoreactivity barriers need to be overcome. Early identification and exclusion of irreversibly stressed and dying islets may improve transplant outcomes. We used oligonucleotide microarray and quantitative RT-PCR to identify molecular markers of physiological and immunological stress in porcine islets cultured under stress conditions of elevated glucose (16.7 mM), inflammatory cytokine addition (IL-1β, TNF-α, and IFN-γ), or both, for 48 h. Hyperglycemic conditions were associated with increased thioredoxin interacting protein and metabolic process mRNAs, as observed in rodent and primate species. Cytokine treatment increased expression of JAK-STAT pathway components, oxidative stress (transglutaminase 2), and β cell dysfunction genes. Transglutaminase 2 induction is unique to porcine islets. Biomarkers involved in hyperglycemia and islet inflammation may serve as novel targets for improving and monitoring isolated porcine islet function and viability.",

keywords = "Cytokines, Diabetes, Gene expression, Islet cells, Microarray, Swine",

author = "Dvorak, {C. M.T.} and M. H{\aa}rdstedt and H. Xie and M. Wang and Papas, {K. K.} and Hering, {B. J.} and Murtaugh, {M. P.} and Fahrenkrug, {S. C.}",

note = "Funding Information: The authors wish to thank Jeffrey Ansite, Thomas Gilmore, Andrew Friberg, Andrea Bauer, and Dr. Hui-Jian Zhang of the Diabetes Institute for porcine islet isolation and culture, Dr. Zheng Jin Tu at the University of Minnesota Supercomputing Institute for computing support, and Mr. Bhupinder Juneja for technical assistance. Financial support was provided by the Eunice L. Dwan Diabetes Research Endowment, Iacocca Foundation, Children with Diabetes Foundation, and the Winston and Maxine Wallin Islet Xenotransplant Fund. ",

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doi = "10.1016/j.bbrc.2007.03.101",

language = "English (US)",

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T1 - Transcriptional profiling of stress response in cultured porcine islets

AU - Dvorak, C. M.T.

AU - Hårdstedt, M.

AU - Xie, H.

AU - Wang, M.

AU - Papas, K. K.

AU - Hering, B. J.

AU - Murtaugh, M. P.

AU - Fahrenkrug, S. C.

N1 - Funding Information: The authors wish to thank Jeffrey Ansite, Thomas Gilmore, Andrew Friberg, Andrea Bauer, and Dr. Hui-Jian Zhang of the Diabetes Institute for porcine islet isolation and culture, Dr. Zheng Jin Tu at the University of Minnesota Supercomputing Institute for computing support, and Mr. Bhupinder Juneja for technical assistance. Financial support was provided by the Eunice L. Dwan Diabetes Research Endowment, Iacocca Foundation, Children with Diabetes Foundation, and the Winston and Maxine Wallin Islet Xenotransplant Fund.

PY - 2007/5/25

Y1 - 2007/5/25

N2 - Cell-based diabetes therapy may be achieved through xenotransplantation of adult porcine islets, but tissue quality and immunoreactivity barriers need to be overcome. Early identification and exclusion of irreversibly stressed and dying islets may improve transplant outcomes. We used oligonucleotide microarray and quantitative RT-PCR to identify molecular markers of physiological and immunological stress in porcine islets cultured under stress conditions of elevated glucose (16.7 mM), inflammatory cytokine addition (IL-1β, TNF-α, and IFN-γ), or both, for 48 h. Hyperglycemic conditions were associated with increased thioredoxin interacting protein and metabolic process mRNAs, as observed in rodent and primate species. Cytokine treatment increased expression of JAK-STAT pathway components, oxidative stress (transglutaminase 2), and β cell dysfunction genes. Transglutaminase 2 induction is unique to porcine islets. Biomarkers involved in hyperglycemia and islet inflammation may serve as novel targets for improving and monitoring isolated porcine islet function and viability.

AB - Cell-based diabetes therapy may be achieved through xenotransplantation of adult porcine islets, but tissue quality and immunoreactivity barriers need to be overcome. Early identification and exclusion of irreversibly stressed and dying islets may improve transplant outcomes. We used oligonucleotide microarray and quantitative RT-PCR to identify molecular markers of physiological and immunological stress in porcine islets cultured under stress conditions of elevated glucose (16.7 mM), inflammatory cytokine addition (IL-1β, TNF-α, and IFN-γ), or both, for 48 h. Hyperglycemic conditions were associated with increased thioredoxin interacting protein and metabolic process mRNAs, as observed in rodent and primate species. Cytokine treatment increased expression of JAK-STAT pathway components, oxidative stress (transglutaminase 2), and β cell dysfunction genes. Transglutaminase 2 induction is unique to porcine islets. Biomarkers involved in hyperglycemia and islet inflammation may serve as novel targets for improving and monitoring isolated porcine islet function and viability.

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KW - Gene expression

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KW - Microarray

KW - Swine

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Transcriptional profiling of stress response in cultured porcine islets

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