Inhibition of de novo ceramide synthesis by sirtuin-1 improves beta-cell function and glucose metabolism in type 2 diabetes

Srividya Velagapudi; Gergely Karsai; Maria Karsai; Shafeeq A. Mohammed; Fabrizio Montecucco; Luca Liberale; Hwan Lee; Federico Carbone; Giovanni Francesco Adami; Kangmin Yang; Margot Crucet; Sokrates Stein; Franceso Paneni; Tetiana Lapikova-Bryhinska; Hyun Duk Jang; Simon Kraler; Daria Vdovenko; Richard Arnold Züllig; Giovanni G. Camici; Hyo Soo Kim; Reijo Laaksonen; Philipp A. Gerber; Thorsten Hornemann; Alexander Akhmedov; Thomas F. Lüscher

doi:10.1093/cvr/cvae100

Inhibition of de novo ceramide synthesis by sirtuin-1 improves beta-cell function and glucose metabolism in type 2 diabetes

Srividya Velagapudi, Gergely Karsai, Maria Karsai, Shafeeq A. Mohammed, Fabrizio Montecucco, Luca Liberale, Hwan Lee, Federico Carbone, Giovanni Francesco Adami, Kangmin Yang, Margot Crucet, Sokrates Stein, Franceso Paneni, Tetiana Lapikova-Bryhinska, Hyun Duk Jang, Simon Kraler, Daria Vdovenko, Richard Arnold Züllig, Giovanni G. Camici, Hyo Soo KimReijo Laaksonen, Philipp A. Gerber, Thorsten Hornemann, Alexander Akhmedov, Thomas F. Lüscher

Lapset ja naiset, diagnostiset alat, psykiatria

Tutkimustuotos: Artikkeli › Tieteellinen › vertaisarvioitu

3 Sitaatiot (Scopus)

Abstrakti

Aims: Obesity and type 2 diabetes (T2D) are major risk factors for cardiovascular (CV) diseases. Dysregulated pro-apoptotic ceramide synthesis reduces β-cell insulin secretion, thereby promoting hyperglycaemic states that may manifest as T2D. Pro-apoptotic ceramides modulate insulin sensitivity and glucose tolerance while being linked to poor CV outcomes. Sirtuin-1 (SIRT1) is a NAD ⁺ -dependent deacetylase that protects against pancreatic β-cell dysfunction; however, systemic levels are decreased in obese-T2D mice and may promote pro-apoptotic ceramide synthesis and hyperglycaemia. Herein, we aimed to assess the effects of restoring circulating SIRT1 levels to prevent metabolic imbalance in obese and diabetic mice. Methods and results: Circulating SIRT1 levels were reduced in obese-diabetic mice (db/db) as compared to age-matched non-diabetic db/+ controls. Restoration of SIRT1 plasma levels with recombinant murine SIRT1 for 4 weeks prevented body weight gain and improved glucose tolerance, insulin sensitivity, and vascular function in mice models of obesity and T2D. Untargeted lipidomics revealed that SIRT1 restored insulin secretory function of β-cells by reducing synthesis and accumulation of pro-apoptotic ceramides. Molecular mechanisms involved direct binding to and deacetylation of Toll-like receptor 4 (TLR4) by SIRT1 in β-cells, thereby decreasing the rate-limiting enzymes of sphingolipid synthesis SPTLC1/2 via AKT/NF-κB. Among patients with T2D, those with high baseline plasma levels of SIRT1 prior to metabolic surgery displayed restored β-cell function (HOMA2-β) and were more likely to have T2D remission during follow-up. Conclusion: Acetylation of TLR4 promotes β-cell dysfunction via ceramide synthesis in T2D, which is blunted by systemic SIRT1 replenishment. Hence, restoration of systemic SIRT1 may provide a novel therapeutic strategy to counteract toxic ceramide synthesis and mitigate CV complications of T2D.

Alkuperäiskieli	Englanti
Sivut	1265-1278
Sivumäärä	14
Julkaisu	CARDIOVASCULAR RESEARCH
Vuosikerta	120
Numero	11
DOI - pysyväislinkit	https://doi.org/10.1093/cvr/cvae100
Tila	Julkaistu - heinäk. 2024
OKM-julkaisutyyppi	A1 Alkuperäisartikkeli tieteellisessä aikakauslehdessä

Julkaisufoorumi-taso

Jufo-taso 2

!!ASJC Scopus subject areas

Yleinen lääketiede

YK:n kestävän kehityksen tavoitteet

Tämä tuotos edistää seuraavia kestävän kehityksen tavoitteita:

Pääsy asiakirjaan

10.1093/cvr/cvae100

Siteeraa tätä

Velagapudi, S., Karsai, G., Karsai, M., Mohammed, S. A., Montecucco, F., Liberale, L., Lee, H., Carbone, F., Adami, G. F., Yang, K., Crucet, M., Stein, S., Paneni, F., Lapikova-Bryhinska, T., Jang, H. D., Kraler, S., Vdovenko, D., Züllig, R. A., Camici, G. G., ... Lüscher, T. F. (2024). Inhibition of de novo ceramide synthesis by sirtuin-1 improves beta-cell function and glucose metabolism in type 2 diabetes. CARDIOVASCULAR RESEARCH, 120(11), 1265-1278. https://doi.org/10.1093/cvr/cvae100

@article{c1572c91d97b4c07a4e9aa6bcba1d005,

title = "Inhibition of de novo ceramide synthesis by sirtuin-1 improves beta-cell function and glucose metabolism in type 2 diabetes",

abstract = "Aims: Obesity and type 2 diabetes (T2D) are major risk factors for cardiovascular (CV) diseases. Dysregulated pro-apoptotic ceramide synthesis reduces β-cell insulin secretion, thereby promoting hyperglycaemic states that may manifest as T2D. Pro-apoptotic ceramides modulate insulin sensitivity and glucose tolerance while being linked to poor CV outcomes. Sirtuin-1 (SIRT1) is a NAD + -dependent deacetylase that protects against pancreatic β-cell dysfunction; however, systemic levels are decreased in obese-T2D mice and may promote pro-apoptotic ceramide synthesis and hyperglycaemia. Herein, we aimed to assess the effects of restoring circulating SIRT1 levels to prevent metabolic imbalance in obese and diabetic mice. Methods and results: Circulating SIRT1 levels were reduced in obese-diabetic mice (db/db) as compared to age-matched non-diabetic db/+ controls. Restoration of SIRT1 plasma levels with recombinant murine SIRT1 for 4 weeks prevented body weight gain and improved glucose tolerance, insulin sensitivity, and vascular function in mice models of obesity and T2D. Untargeted lipidomics revealed that SIRT1 restored insulin secretory function of β-cells by reducing synthesis and accumulation of pro-apoptotic ceramides. Molecular mechanisms involved direct binding to and deacetylation of Toll-like receptor 4 (TLR4) by SIRT1 in β-cells, thereby decreasing the rate-limiting enzymes of sphingolipid synthesis SPTLC1/2 via AKT/NF-κB. Among patients with T2D, those with high baseline plasma levels of SIRT1 prior to metabolic surgery displayed restored β-cell function (HOMA2-β) and were more likely to have T2D remission during follow-up. Conclusion: Acetylation of TLR4 promotes β-cell dysfunction via ceramide synthesis in T2D, which is blunted by systemic SIRT1 replenishment. Hence, restoration of systemic SIRT1 may provide a novel therapeutic strategy to counteract toxic ceramide synthesis and mitigate CV complications of T2D.",

keywords = "Cardiovascular disease, Ceramide synthesis, Post-translational modification, Sirtuin-1, Type 2 diabetes, Β-cell function",

author = "Srividya Velagapudi and Gergely Karsai and Maria Karsai and Mohammed, {Shafeeq A.} and Fabrizio Montecucco and Luca Liberale and Hwan Lee and Federico Carbone and Adami, {Giovanni Francesco} and Kangmin Yang and Margot Crucet and Sokrates Stein and Franceso Paneni and Tetiana Lapikova-Bryhinska and Jang, {Hyun Duk} and Simon Kraler and Daria Vdovenko and Z{\"u}llig, {Richard Arnold} and Camici, {Giovanni G.} and Kim, {Hyo Soo} and Reijo Laaksonen and Gerber, {Philipp A.} and Thorsten Hornemann and Alexander Akhmedov and L{\"u}scher, {Thomas F.}",

year = "2024",

month = jul,

doi = "10.1093/cvr/cvae100",

language = "English",

volume = "120",

pages = "1265--1278",

journal = "CARDIOVASCULAR RESEARCH",

issn = "0008-6363",

publisher = "Oxford University Press",

number = "11",

}

Velagapudi, S, Karsai, G, Karsai, M, Mohammed, SA, Montecucco, F, Liberale, L, Lee, H, Carbone, F, Adami, GF, Yang, K, Crucet, M, Stein, S, Paneni, F, Lapikova-Bryhinska, T, Jang, HD, Kraler, S, Vdovenko, D, Züllig, RA, Camici, GG, Kim, HS, Laaksonen, R, Gerber, PA, Hornemann, T, Akhmedov, A & Lüscher, TF 2024, 'Inhibition of de novo ceramide synthesis by sirtuin-1 improves beta-cell function and glucose metabolism in type 2 diabetes', CARDIOVASCULAR RESEARCH, Vuosikerta 120, Nro 11, Sivut 1265-1278. https://doi.org/10.1093/cvr/cvae100

TY - JOUR

T1 - Inhibition of de novo ceramide synthesis by sirtuin-1 improves beta-cell function and glucose metabolism in type 2 diabetes

AU - Velagapudi, Srividya

AU - Karsai, Gergely

AU - Karsai, Maria

AU - Mohammed, Shafeeq A.

AU - Montecucco, Fabrizio

AU - Liberale, Luca

AU - Lee, Hwan

AU - Carbone, Federico

AU - Adami, Giovanni Francesco

AU - Yang, Kangmin

AU - Crucet, Margot

AU - Stein, Sokrates

AU - Paneni, Franceso

AU - Lapikova-Bryhinska, Tetiana

AU - Jang, Hyun Duk

AU - Kraler, Simon

AU - Vdovenko, Daria

AU - Züllig, Richard Arnold

AU - Camici, Giovanni G.

AU - Kim, Hyo Soo

AU - Laaksonen, Reijo

AU - Gerber, Philipp A.

AU - Hornemann, Thorsten

AU - Akhmedov, Alexander

AU - Lüscher, Thomas F.

PY - 2024/7

Y1 - 2024/7

N2 - Aims: Obesity and type 2 diabetes (T2D) are major risk factors for cardiovascular (CV) diseases. Dysregulated pro-apoptotic ceramide synthesis reduces β-cell insulin secretion, thereby promoting hyperglycaemic states that may manifest as T2D. Pro-apoptotic ceramides modulate insulin sensitivity and glucose tolerance while being linked to poor CV outcomes. Sirtuin-1 (SIRT1) is a NAD + -dependent deacetylase that protects against pancreatic β-cell dysfunction; however, systemic levels are decreased in obese-T2D mice and may promote pro-apoptotic ceramide synthesis and hyperglycaemia. Herein, we aimed to assess the effects of restoring circulating SIRT1 levels to prevent metabolic imbalance in obese and diabetic mice. Methods and results: Circulating SIRT1 levels were reduced in obese-diabetic mice (db/db) as compared to age-matched non-diabetic db/+ controls. Restoration of SIRT1 plasma levels with recombinant murine SIRT1 for 4 weeks prevented body weight gain and improved glucose tolerance, insulin sensitivity, and vascular function in mice models of obesity and T2D. Untargeted lipidomics revealed that SIRT1 restored insulin secretory function of β-cells by reducing synthesis and accumulation of pro-apoptotic ceramides. Molecular mechanisms involved direct binding to and deacetylation of Toll-like receptor 4 (TLR4) by SIRT1 in β-cells, thereby decreasing the rate-limiting enzymes of sphingolipid synthesis SPTLC1/2 via AKT/NF-κB. Among patients with T2D, those with high baseline plasma levels of SIRT1 prior to metabolic surgery displayed restored β-cell function (HOMA2-β) and were more likely to have T2D remission during follow-up. Conclusion: Acetylation of TLR4 promotes β-cell dysfunction via ceramide synthesis in T2D, which is blunted by systemic SIRT1 replenishment. Hence, restoration of systemic SIRT1 may provide a novel therapeutic strategy to counteract toxic ceramide synthesis and mitigate CV complications of T2D.

AB - Aims: Obesity and type 2 diabetes (T2D) are major risk factors for cardiovascular (CV) diseases. Dysregulated pro-apoptotic ceramide synthesis reduces β-cell insulin secretion, thereby promoting hyperglycaemic states that may manifest as T2D. Pro-apoptotic ceramides modulate insulin sensitivity and glucose tolerance while being linked to poor CV outcomes. Sirtuin-1 (SIRT1) is a NAD + -dependent deacetylase that protects against pancreatic β-cell dysfunction; however, systemic levels are decreased in obese-T2D mice and may promote pro-apoptotic ceramide synthesis and hyperglycaemia. Herein, we aimed to assess the effects of restoring circulating SIRT1 levels to prevent metabolic imbalance in obese and diabetic mice. Methods and results: Circulating SIRT1 levels were reduced in obese-diabetic mice (db/db) as compared to age-matched non-diabetic db/+ controls. Restoration of SIRT1 plasma levels with recombinant murine SIRT1 for 4 weeks prevented body weight gain and improved glucose tolerance, insulin sensitivity, and vascular function in mice models of obesity and T2D. Untargeted lipidomics revealed that SIRT1 restored insulin secretory function of β-cells by reducing synthesis and accumulation of pro-apoptotic ceramides. Molecular mechanisms involved direct binding to and deacetylation of Toll-like receptor 4 (TLR4) by SIRT1 in β-cells, thereby decreasing the rate-limiting enzymes of sphingolipid synthesis SPTLC1/2 via AKT/NF-κB. Among patients with T2D, those with high baseline plasma levels of SIRT1 prior to metabolic surgery displayed restored β-cell function (HOMA2-β) and were more likely to have T2D remission during follow-up. Conclusion: Acetylation of TLR4 promotes β-cell dysfunction via ceramide synthesis in T2D, which is blunted by systemic SIRT1 replenishment. Hence, restoration of systemic SIRT1 may provide a novel therapeutic strategy to counteract toxic ceramide synthesis and mitigate CV complications of T2D.

KW - Cardiovascular disease

KW - Ceramide synthesis

KW - Post-translational modification

KW - Sirtuin-1

KW - Type 2 diabetes

KW - Β-cell function

U2 - 10.1093/cvr/cvae100

DO - 10.1093/cvr/cvae100

M3 - Article

C2 - 38739545

AN - SCOPUS:85204744562

SN - 0008-6363

VL - 120

SP - 1265

EP - 1278

JO - CARDIOVASCULAR RESEARCH

JF - CARDIOVASCULAR RESEARCH

IS - 11

ER -

Inhibition of de novo ceramide synthesis by sirtuin-1 improves beta-cell function and glucose metabolism in type 2 diabetes

Abstrakti

Julkaisufoorumi-taso

!!ASJC Scopus subject areas

YK:n kestävän kehityksen tavoitteet

Pääsy asiakirjaan

Sormenjälki

Siteeraa tätä