p16 Ink4a-induced senescence of pancreatic beta cells enhances insulin secretion

Aharon Helman; Agnes Klochendler; Narmen Azazmeh; Yael Gabai; Elad Horwitz; Shira Anzi; Avital Swisa; Reba Condiotti; Roy Z. Granit; Yuval Nevo; Yaakov Fixler; Dorin Shreibman; Amit Zamir; Sharona Tornovsky-Babeay; Chunhua Dai; Benjamin Glaser; Alvin C. Powers; A. M.James Shapiro; Mark A. Magnuson; Yuval Dor; Ittai Ben-Porath

doi:10.1038/nm.4054

p16 Ink4a-induced senescence of pancreatic beta cells enhances insulin secretion

Aharon Helman, Agnes Klochendler, Narmen Azazmeh, Yael Gabai, Elad Horwitz, Shira Anzi, Avital Swisa, Reba Condiotti, Roy Z. Granit, Yuval Nevo, Yaakov Fixler, Dorin Shreibman, Amit Zamir, Sharona Tornovsky-Babeay, Chunhua Dai, Benjamin Glaser, Alvin C. Powers, A. M.James Shapiro, Mark A. Magnuson, Yuval DorIttai Ben-Porath

The Hebrew University of Jerusalem

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

Abstract

Cellular senescence is thought to contribute to age-associated deterioration of tissue physiology. The senescence effector p16 Ink4a is expressed in pancreatic beta cells during aging and limits their proliferative potential; however, its effects on beta cell function are poorly characterized. We found that beta cell-specific activation of p16 Ink4a in transgenic mice enhances glucose-stimulated insulin secretion (GSIS). In mice with diabetes, this leads to improved glucose homeostasis, providing an unexpected functional benefit. Expression of p16 Ink4a in beta cells induces hallmarks of senescence - including cell enlargement, and greater glucose uptake and mitochondrial activity - which promote increased insulin secretion. GSIS increases during the normal aging of mice and is driven by elevated p16 Ink4a activity. We found that islets from human adults contain p16 Ink4a -expressing senescent beta cells and that senescence induced by p16 Ink4a in a human beta cell line increases insulin secretion in a manner dependent, in part, on the activity of the mechanistic target of rapamycin (mTOR) and the peroxisome proliferator-activated receptor (PPAR)- 3 proteins. Our findings reveal a novel role for p16 Ink4a and cellular senescence in promoting insulin secretion by beta cells and in regulating normal functional tissue maturation with age.

Original language	English
Pages (from-to)	412-420
Number of pages	9
Journal	Nature Medicine
Volume	22
Issue number	4
DOIs	https://doi.org/10.1038/nm.4054
State	Published - 1 Apr 2016

All Science Journal Classification (ASJC) codes

General Biochemistry,Genetics and Molecular Biology

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10.1038/nm.4054

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Helman, A., Klochendler, A., Azazmeh, N., Gabai, Y., Horwitz, E., Anzi, S., Swisa, A., Condiotti, R., Granit, R. Z., Nevo, Y., Fixler, Y., Shreibman, D., Zamir, A., Tornovsky-Babeay, S., Dai, C., Glaser, B., Powers, A. C., Shapiro, A. M. J., Magnuson, M. A., ... Ben-Porath, I. (2016). p16 Ink4a-induced senescence of pancreatic beta cells enhances insulin secretion. Nature Medicine, 22(4), 412-420. https://doi.org/10.1038/nm.4054

@article{2b34106fc22840cfa40bf1bceb612121,

title = "p16 Ink4a-induced senescence of pancreatic beta cells enhances insulin secretion",

abstract = "Cellular senescence is thought to contribute to age-associated deterioration of tissue physiology. The senescence effector p16 Ink4a is expressed in pancreatic beta cells during aging and limits their proliferative potential; however, its effects on beta cell function are poorly characterized. We found that beta cell-specific activation of p16 Ink4a in transgenic mice enhances glucose-stimulated insulin secretion (GSIS). In mice with diabetes, this leads to improved glucose homeostasis, providing an unexpected functional benefit. Expression of p16 Ink4a in beta cells induces hallmarks of senescence - including cell enlargement, and greater glucose uptake and mitochondrial activity - which promote increased insulin secretion. GSIS increases during the normal aging of mice and is driven by elevated p16 Ink4a activity. We found that islets from human adults contain p16 Ink4a -expressing senescent beta cells and that senescence induced by p16 Ink4a in a human beta cell line increases insulin secretion in a manner dependent, in part, on the activity of the mechanistic target of rapamycin (mTOR) and the peroxisome proliferator-activated receptor (PPAR)- 3 proteins. Our findings reveal a novel role for p16 Ink4a and cellular senescence in promoting insulin secretion by beta cells and in regulating normal functional tissue maturation with age.",

author = "Aharon Helman and Agnes Klochendler and Narmen Azazmeh and Yael Gabai and Elad Horwitz and Shira Anzi and Avital Swisa and Reba Condiotti and Granit, \{Roy Z.\} and Yuval Nevo and Yaakov Fixler and Dorin Shreibman and Amit Zamir and Sharona Tornovsky-Babeay and Chunhua Dai and Benjamin Glaser and Powers, \{Alvin C.\} and Shapiro, \{A. M.James\} and Magnuson, \{Mark A.\} and Yuval Dor and Ittai Ben-Porath",

note = "Funding Information: Acknowledgments We thank M. Barbacid for CDK4lsl-R24C mice, L. Philipson for MIP-CreER mice, R. Scharfmann for the EndoC-βH2 cells; S. Efrat for the pTRIPΔU3-CMV-nlsCre vector and C. Wright for the Pdx1-specific antibody. We thank N.E. Kidess-Bassir for histological preparation and T. Szoke for experimental assistance. This research was supported by a postdoctoral fellowship from the Juvenile Diabetes Research Foundation (A.H.) and by grants from Israel Science Foundation (grant no. 1009/13; I.B.-P.), the Jacob and Lena Joels Memorial Foundation Senior Lectureship for Excellence in the Life and Medical Sciences (I.B.-P.), Diabetes Onderzoek Nederland (Y.D. and I.B.-P.), the Alex U. Soyka program (Y.D. and I.B.-P.), the Juvenile Diabetes Research Foundation (Y.D. and A.C.P.), the US National Institutes of Health (NIH) Beta Cell Biology Consortium (Y.D.), the Leona M. and Harry B. Helmsley Charitable Trust (Y.D.), the Israeli Centers Of Research Excellence Program of the Planning and Budgeting Committee and the Israel Science Foundation (grant no. 41.11; Y.D.), the United States Agency for International Development's American Schools and Hospitals Abroad Program (Y.D. and I.B.-P.), the Network for Pancreatic Organ Donors with Diabetes (nPOD) (Y.D.), the US Department of Veterans Affairs (A.C.P.), the National Institute of Diabetes and Digestive and Kidney DiseasesNIH (grant no. DK089572 (A.C.P.), DK72473 (A.C.P.) and DK104211 (A.C.P.)), and the Vanderbilt Diabetes Research and Training Center (grant no. DK20593; A.C.P.). Organ procurement organizations partnering with nPOD are listed at http://www.jdrfnpod.org/our-partners.php.",

year = "2016",

month = apr,

day = "1",

doi = "10.1038/nm.4054",

language = "الإنجليزيّة",

volume = "22",

pages = "412--420",

journal = "Nature Medicine",

issn = "1078-8956",

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Helman, A , Klochendler, A, Azazmeh, N, Gabai, Y, Horwitz, E, Anzi, S, Swisa, A, Condiotti, R, Granit, RZ, Nevo, Y, Fixler, Y, Shreibman, D, Zamir, A, Tornovsky-Babeay, S, Dai, C, Glaser, B, Powers, AC, Shapiro, AMJ, Magnuson, MA, Dor, Y & Ben-Porath, I 2016, 'p16 Ink4a-induced senescence of pancreatic beta cells enhances insulin secretion', Nature Medicine, vol. 22, no. 4, pp. 412-420. https://doi.org/10.1038/nm.4054

TY - JOUR

T1 - p16 Ink4a-induced senescence of pancreatic beta cells enhances insulin secretion

AU - Helman, Aharon

AU - Klochendler, Agnes

AU - Azazmeh, Narmen

AU - Gabai, Yael

AU - Horwitz, Elad

AU - Anzi, Shira

AU - Swisa, Avital

AU - Condiotti, Reba

AU - Granit, Roy Z.

AU - Nevo, Yuval

AU - Fixler, Yaakov

AU - Shreibman, Dorin

AU - Zamir, Amit

AU - Tornovsky-Babeay, Sharona

AU - Dai, Chunhua

AU - Glaser, Benjamin

AU - Powers, Alvin C.

AU - Shapiro, A. M.James

AU - Magnuson, Mark A.

AU - Dor, Yuval

AU - Ben-Porath, Ittai

N1 - Funding Information: Acknowledgments We thank M. Barbacid for CDK4lsl-R24C mice, L. Philipson for MIP-CreER mice, R. Scharfmann for the EndoC-βH2 cells; S. Efrat for the pTRIPΔU3-CMV-nlsCre vector and C. Wright for the Pdx1-specific antibody. We thank N.E. Kidess-Bassir for histological preparation and T. Szoke for experimental assistance. This research was supported by a postdoctoral fellowship from the Juvenile Diabetes Research Foundation (A.H.) and by grants from Israel Science Foundation (grant no. 1009/13; I.B.-P.), the Jacob and Lena Joels Memorial Foundation Senior Lectureship for Excellence in the Life and Medical Sciences (I.B.-P.), Diabetes Onderzoek Nederland (Y.D. and I.B.-P.), the Alex U. Soyka program (Y.D. and I.B.-P.), the Juvenile Diabetes Research Foundation (Y.D. and A.C.P.), the US National Institutes of Health (NIH) Beta Cell Biology Consortium (Y.D.), the Leona M. and Harry B. Helmsley Charitable Trust (Y.D.), the Israeli Centers Of Research Excellence Program of the Planning and Budgeting Committee and the Israel Science Foundation (grant no. 41.11; Y.D.), the United States Agency for International Development's American Schools and Hospitals Abroad Program (Y.D. and I.B.-P.), the Network for Pancreatic Organ Donors with Diabetes (nPOD) (Y.D.), the US Department of Veterans Affairs (A.C.P.), the National Institute of Diabetes and Digestive and Kidney DiseasesNIH (grant no. DK089572 (A.C.P.), DK72473 (A.C.P.) and DK104211 (A.C.P.)), and the Vanderbilt Diabetes Research and Training Center (grant no. DK20593; A.C.P.). Organ procurement organizations partnering with nPOD are listed at http://www.jdrfnpod.org/our-partners.php.

PY - 2016/4/1

Y1 - 2016/4/1

N2 - Cellular senescence is thought to contribute to age-associated deterioration of tissue physiology. The senescence effector p16 Ink4a is expressed in pancreatic beta cells during aging and limits their proliferative potential; however, its effects on beta cell function are poorly characterized. We found that beta cell-specific activation of p16 Ink4a in transgenic mice enhances glucose-stimulated insulin secretion (GSIS). In mice with diabetes, this leads to improved glucose homeostasis, providing an unexpected functional benefit. Expression of p16 Ink4a in beta cells induces hallmarks of senescence - including cell enlargement, and greater glucose uptake and mitochondrial activity - which promote increased insulin secretion. GSIS increases during the normal aging of mice and is driven by elevated p16 Ink4a activity. We found that islets from human adults contain p16 Ink4a -expressing senescent beta cells and that senescence induced by p16 Ink4a in a human beta cell line increases insulin secretion in a manner dependent, in part, on the activity of the mechanistic target of rapamycin (mTOR) and the peroxisome proliferator-activated receptor (PPAR)- 3 proteins. Our findings reveal a novel role for p16 Ink4a and cellular senescence in promoting insulin secretion by beta cells and in regulating normal functional tissue maturation with age.

AB - Cellular senescence is thought to contribute to age-associated deterioration of tissue physiology. The senescence effector p16 Ink4a is expressed in pancreatic beta cells during aging and limits their proliferative potential; however, its effects on beta cell function are poorly characterized. We found that beta cell-specific activation of p16 Ink4a in transgenic mice enhances glucose-stimulated insulin secretion (GSIS). In mice with diabetes, this leads to improved glucose homeostasis, providing an unexpected functional benefit. Expression of p16 Ink4a in beta cells induces hallmarks of senescence - including cell enlargement, and greater glucose uptake and mitochondrial activity - which promote increased insulin secretion. GSIS increases during the normal aging of mice and is driven by elevated p16 Ink4a activity. We found that islets from human adults contain p16 Ink4a -expressing senescent beta cells and that senescence induced by p16 Ink4a in a human beta cell line increases insulin secretion in a manner dependent, in part, on the activity of the mechanistic target of rapamycin (mTOR) and the peroxisome proliferator-activated receptor (PPAR)- 3 proteins. Our findings reveal a novel role for p16 Ink4a and cellular senescence in promoting insulin secretion by beta cells and in regulating normal functional tissue maturation with age.

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U2 - 10.1038/nm.4054

DO - 10.1038/nm.4054

M3 - مقالة

C2 - 26950362

SN - 1078-8956

VL - 22

SP - 412

EP - 420

JO - Nature Medicine

JF - Nature Medicine

IS - 4

ER -

p16 Ink4a-induced senescence of pancreatic beta cells enhances insulin secretion

Abstract

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