Lysine deacetylase inhibition prevents diabetes by chromatin-independent immunoregulation and β-cell protection

Dan Ploug Christensen; Conny Gysemans; Morten Lundh; Mattias Salling Dahllöf; Daniel Noesgaard; Søren Fisker Schmidt; Susanne Mandrup; Nikolai Birkbak; Christopher Workman; Lorenzo Piemonti; Lykke Blaabjerg; Valmen Monzani; Gianluca Fossati; Paolo Mascagni; Steven Paraskevas; Reid A Aikin; Nils Billestrup; Lars Groth Grunnet; Charles A Dinarello; Chantal Mathieu; Thomas Mandrup-Poulsen

doi:10.1073/pnas.1320850111

Lysine deacetylase inhibition prevents diabetes by chromatin-independent immunoregulation and β-cell protection

Dan Ploug Christensen, Conny Gysemans, Morten Lundh, Mattias Salling Dahllöf, Daniel Noesgaard, Søren Fisker Schmidt, Susanne Mandrup, Nikolai Birkbak, Christopher Workman, Lorenzo Piemonti, Lykke Blaabjerg, Valmen Monzani, Gianluca Fossati, Paolo Mascagni, Steven Paraskevas, Reid A Aikin, Nils Billestrup, Lars Groth Grunnet, Charles A Dinarello, Chantal MathieuThomas Mandrup-Poulsen

42 Citationer (Scopus)

Abstract

Type 1 diabetes is due to destruction of pancreatic β-cells. Lysine deacetylase inhibitors (KDACi) protect β-cells from inflammatory destruction in vitro and are promising immunomodulators. Here we demonstrate that the clinically well-tolerated KDACi vorinostat and givinostat revert diabetes in the nonobese diabetic (NOD) mouse model of type 1 diabetes and counteract inflammatory target cell damage by a mechanism of action consistent with transcription factor-rather than global chromatin-hyperacetylation. Weaning NOD mice received low doses of vorinostat and givinostat in their drinking water until 100-120 d of age. Diabetes incidence was reduced by 38% and 45%, respectively, there was a 15% increase in the percentage of islets without infiltration, and pancreatic insulin content increased by 200%. Vorinostat treatment increased the frequency of functional regulatory T-cell subsets and their transcription factors Gata3 and FoxP3 in parallel to a decrease in inflammatory dendritic cell subsets and their cytokines IL-6, IL-12, and TNF-α. KDACi also inhibited LPS-induced Cox-2 expression in peritoneal macrophages from C57BL/6 and NOD mice. In insulin-producing β-cells, givinostat did not upregulate expression of the anti-inflammatory genes Socs1-3 or sirtuin-1 but reduced levels of IL-1β + IFN-γ-induced proinflammatory Il1a, Il1b, Tnfα, Fas, Cxcl2, and reduced cytokine-induced ERK phosphorylation. Further, NF-κB genomic iNos promoter binding was reduced by 50%, and NF-κB-dependent mRNA expression was blocked. These effects were associated with NF-κB subunit p65 hyperacetylation. Taken together, these data provide a rationale for clinical trials of safety and efficacy of KDACi in patients with autoimmune disease such as type 1 diabetes.

Originalsprog	Engelsk
Tidsskrift	Proceedings of the National Academy of Sciences of the United States of America
Vol/bind	111
Udgave nummer	3
Sider (fra-til)	1055-9
Antal sider	5
DOI	https://doi.org/10.1073/pnas.1320850111
Status	Udgivet - 21 jan. 2014

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10.1073/pnas.1320850111

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Christensen, D. P., Gysemans, C., Lundh, M., Dahllöf, M. S., Noesgaard, D., Schmidt, S. F., Mandrup, S., Birkbak, N., Workman, C., Piemonti, L., Blaabjerg, L., Monzani, V., Fossati, G., Mascagni, P., Paraskevas, S., Aikin, R. A., Billestrup, N., Grunnet, L. G., Dinarello, C. A., ... Mandrup-Poulsen, T. (2014). Lysine deacetylase inhibition prevents diabetes by chromatin-independent immunoregulation and β-cell protection. Proceedings of the National Academy of Sciences of the United States of America, 111(3), 1055-9. https://doi.org/10.1073/pnas.1320850111

Lysine deacetylase inhibition prevents diabetes by chromatin-independent immunoregulation and β-cell protection. / Christensen, Dan Ploug; Gysemans, Conny; Lundh, Morten et al.

I: Proceedings of the National Academy of Sciences of the United States of America, Bind 111, Nr. 3, 21.01.2014, s. 1055-9.

Publikation: Bidrag til tidsskrift › Tidsskriftartikel › Forskning › peer review

Christensen, DP, Gysemans, C, Lundh, M, Dahllöf, MS, Noesgaard, D, Schmidt, SF, Mandrup, S, Birkbak, N, Workman, C, Piemonti, L, Blaabjerg, L, Monzani, V, Fossati, G, Mascagni, P, Paraskevas, S, Aikin, RA, Billestrup, N, Grunnet, LG, Dinarello, CA, Mathieu, C & Mandrup-Poulsen, T 2014, 'Lysine deacetylase inhibition prevents diabetes by chromatin-independent immunoregulation and β-cell protection', Proceedings of the National Academy of Sciences of the United States of America, bind 111, nr. 3, s. 1055-9. https://doi.org/10.1073/pnas.1320850111

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title = "Lysine deacetylase inhibition prevents diabetes by chromatin-independent immunoregulation and β-cell protection",

abstract = "Type 1 diabetes is due to destruction of pancreatic β-cells. Lysine deacetylase inhibitors (KDACi) protect β-cells from inflammatory destruction in vitro and are promising immunomodulators. Here we demonstrate that the clinically well-tolerated KDACi vorinostat and givinostat revert diabetes in the nonobese diabetic (NOD) mouse model of type 1 diabetes and counteract inflammatory target cell damage by a mechanism of action consistent with transcription factor-rather than global chromatin-hyperacetylation. Weaning NOD mice received low doses of vorinostat and givinostat in their drinking water until 100-120 d of age. Diabetes incidence was reduced by 38% and 45%, respectively, there was a 15% increase in the percentage of islets without infiltration, and pancreatic insulin content increased by 200%. Vorinostat treatment increased the frequency of functional regulatory T-cell subsets and their transcription factors Gata3 and FoxP3 in parallel to a decrease in inflammatory dendritic cell subsets and their cytokines IL-6, IL-12, and TNF-α. KDACi also inhibited LPS-induced Cox-2 expression in peritoneal macrophages from C57BL/6 and NOD mice. In insulin-producing β-cells, givinostat did not upregulate expression of the anti-inflammatory genes Socs1-3 or sirtuin-1 but reduced levels of IL-1β + IFN-γ-induced proinflammatory Il1a, Il1b, Tnfα, Fas, Cxcl2, and reduced cytokine-induced ERK phosphorylation. Further, NF-κB genomic iNos promoter binding was reduced by 50%, and NF-κB-dependent mRNA expression was blocked. These effects were associated with NF-κB subunit p65 hyperacetylation. Taken together, these data provide a rationale for clinical trials of safety and efficacy of KDACi in patients with autoimmune disease such as type 1 diabetes.",

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T1 - Lysine deacetylase inhibition prevents diabetes by chromatin-independent immunoregulation and β-cell protection

AU - Christensen, Dan Ploug

AU - Gysemans, Conny

AU - Lundh, Morten

AU - Dahllöf, Mattias Salling

AU - Noesgaard, Daniel

AU - Schmidt, Søren Fisker

AU - Mandrup, Susanne

AU - Birkbak, Nikolai

AU - Workman, Christopher

AU - Piemonti, Lorenzo

AU - Blaabjerg, Lykke

AU - Monzani, Valmen

AU - Fossati, Gianluca

AU - Mascagni, Paolo

AU - Paraskevas, Steven

AU - Aikin, Reid A

AU - Billestrup, Nils

AU - Grunnet, Lars Groth

AU - Dinarello, Charles A

AU - Mathieu, Chantal

AU - Mandrup-Poulsen, Thomas

PY - 2014/1/21

Y1 - 2014/1/21

N2 - Type 1 diabetes is due to destruction of pancreatic β-cells. Lysine deacetylase inhibitors (KDACi) protect β-cells from inflammatory destruction in vitro and are promising immunomodulators. Here we demonstrate that the clinically well-tolerated KDACi vorinostat and givinostat revert diabetes in the nonobese diabetic (NOD) mouse model of type 1 diabetes and counteract inflammatory target cell damage by a mechanism of action consistent with transcription factor-rather than global chromatin-hyperacetylation. Weaning NOD mice received low doses of vorinostat and givinostat in their drinking water until 100-120 d of age. Diabetes incidence was reduced by 38% and 45%, respectively, there was a 15% increase in the percentage of islets without infiltration, and pancreatic insulin content increased by 200%. Vorinostat treatment increased the frequency of functional regulatory T-cell subsets and their transcription factors Gata3 and FoxP3 in parallel to a decrease in inflammatory dendritic cell subsets and their cytokines IL-6, IL-12, and TNF-α. KDACi also inhibited LPS-induced Cox-2 expression in peritoneal macrophages from C57BL/6 and NOD mice. In insulin-producing β-cells, givinostat did not upregulate expression of the anti-inflammatory genes Socs1-3 or sirtuin-1 but reduced levels of IL-1β + IFN-γ-induced proinflammatory Il1a, Il1b, Tnfα, Fas, Cxcl2, and reduced cytokine-induced ERK phosphorylation. Further, NF-κB genomic iNos promoter binding was reduced by 50%, and NF-κB-dependent mRNA expression was blocked. These effects were associated with NF-κB subunit p65 hyperacetylation. Taken together, these data provide a rationale for clinical trials of safety and efficacy of KDACi in patients with autoimmune disease such as type 1 diabetes.

AB - Type 1 diabetes is due to destruction of pancreatic β-cells. Lysine deacetylase inhibitors (KDACi) protect β-cells from inflammatory destruction in vitro and are promising immunomodulators. Here we demonstrate that the clinically well-tolerated KDACi vorinostat and givinostat revert diabetes in the nonobese diabetic (NOD) mouse model of type 1 diabetes and counteract inflammatory target cell damage by a mechanism of action consistent with transcription factor-rather than global chromatin-hyperacetylation. Weaning NOD mice received low doses of vorinostat and givinostat in their drinking water until 100-120 d of age. Diabetes incidence was reduced by 38% and 45%, respectively, there was a 15% increase in the percentage of islets without infiltration, and pancreatic insulin content increased by 200%. Vorinostat treatment increased the frequency of functional regulatory T-cell subsets and their transcription factors Gata3 and FoxP3 in parallel to a decrease in inflammatory dendritic cell subsets and their cytokines IL-6, IL-12, and TNF-α. KDACi also inhibited LPS-induced Cox-2 expression in peritoneal macrophages from C57BL/6 and NOD mice. In insulin-producing β-cells, givinostat did not upregulate expression of the anti-inflammatory genes Socs1-3 or sirtuin-1 but reduced levels of IL-1β + IFN-γ-induced proinflammatory Il1a, Il1b, Tnfα, Fas, Cxcl2, and reduced cytokine-induced ERK phosphorylation. Further, NF-κB genomic iNos promoter binding was reduced by 50%, and NF-κB-dependent mRNA expression was blocked. These effects were associated with NF-κB subunit p65 hyperacetylation. Taken together, these data provide a rationale for clinical trials of safety and efficacy of KDACi in patients with autoimmune disease such as type 1 diabetes.

U2 - 10.1073/pnas.1320850111

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JO - Proceedings of the National Academy of Sciences of the United States of America

JF - Proceedings of the National Academy of Sciences of the United States of America

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ER -

Lysine deacetylase inhibition prevents diabetes by chromatin-independent immunoregulation and β-cell protection

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