PERK EIF2AK3 control of pancreatic β cell differentiation and proliferation is required for postnatal glucose homeostasis

Wei Zhang; Daorong Feng; Yulin Li; Kaori Iida; Barbara McGrath; Douglas R. Cavener

doi:10.1016/j.cmet.2006.11.002

PERK EIF2AK3 control of pancreatic β cell differentiation and proliferation is required for postnatal glucose homeostasis

Wei Zhang, Daorong Feng, Yulin Li, Kaori Iida, Barbara McGrath, Douglas R. Cavener

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

223 Scopus citations

Abstract

Mutations in PERK (EIF2AK3) result in permanent neonatal diabetes as well as several other anomalies that underlie the human Wolcott-Rallison syndrome, and these anomalies are mirrored in Perk knockout mice. To identify the cause of diabetes in PERK-deficient mice, we generated a series of tissue- and cell-specific knockouts of the Perk gene and performed a developmental analysis of the progression to overt diabetes. We discovered that PERK is specifically required in the insulin-secreting β cells during the fetal and early neonatal period as a prerequisite for postnatal glucose homeostasis. However, PERK expression in β cells is not required at the adult stage to maintain β cell functions and glucose homeostasis. We show that PERK-deficient mice exhibit severe defects in fetal/neonatal β cell proliferation and differentiation, resulting in low β cell mass, defects in proinsulin trafficking, and abrogation of insulin secretion that culminate in permanent neonatal diabetes.

Original language	English (US)
Pages (from-to)	491-497
Number of pages	7
Journal	Cell Metabolism
Volume	4
Issue number	6
DOIs	https://doi.org/10.1016/j.cmet.2006.11.002
State	Published - Dec 2006

Keywords

HUMDISEASE

ASJC Scopus subject areas

Physiology
Molecular Biology
Cell Biology

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10.1016/j.cmet.2006.11.002

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title = "PERK EIF2AK3 control of pancreatic β cell differentiation and proliferation is required for postnatal glucose homeostasis",

abstract = "Mutations in PERK (EIF2AK3) result in permanent neonatal diabetes as well as several other anomalies that underlie the human Wolcott-Rallison syndrome, and these anomalies are mirrored in Perk knockout mice. To identify the cause of diabetes in PERK-deficient mice, we generated a series of tissue- and cell-specific knockouts of the Perk gene and performed a developmental analysis of the progression to overt diabetes. We discovered that PERK is specifically required in the insulin-secreting β cells during the fetal and early neonatal period as a prerequisite for postnatal glucose homeostasis. However, PERK expression in β cells is not required at the adult stage to maintain β cell functions and glucose homeostasis. We show that PERK-deficient mice exhibit severe defects in fetal/neonatal β cell proliferation and differentiation, resulting in low β cell mass, defects in proinsulin trafficking, and abrogation of insulin secretion that culminate in permanent neonatal diabetes.",

keywords = "HUMDISEASE",

author = "Wei Zhang and Daorong Feng and Yulin Li and Kaori Iida and Barbara McGrath and Cavener, {Douglas R.}",

note = "Funding Information: We thank Monica Teta and Hanna Xu for technical assistance, Dr. Douglas Melton (Harvard University) for the Ngn3-Cre and Pdx-1-Cre strains, Dr. Manami Hara (University of Chicago) for the MIP-GFP strain, Dr. Craig Praul for assistance with the microarray experiments, and Elaine Kunze and Susan Magargee (Pennsylvania State University) for assistance with FACS isolation of β cells. This work was supported by NIH grants DK062049 and GM56957 and the Pennsylvania Department of Health TSF (D.R.C.). ",

year = "2006",

month = dec,

doi = "10.1016/j.cmet.2006.11.002",

language = "English (US)",

volume = "4",

pages = "491--497",

journal = "Cell Metabolism",

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AU - Zhang, Wei

AU - Feng, Daorong

AU - Li, Yulin

AU - Iida, Kaori

AU - McGrath, Barbara

AU - Cavener, Douglas R.

N1 - Funding Information: We thank Monica Teta and Hanna Xu for technical assistance, Dr. Douglas Melton (Harvard University) for the Ngn3-Cre and Pdx-1-Cre strains, Dr. Manami Hara (University of Chicago) for the MIP-GFP strain, Dr. Craig Praul for assistance with the microarray experiments, and Elaine Kunze and Susan Magargee (Pennsylvania State University) for assistance with FACS isolation of β cells. This work was supported by NIH grants DK062049 and GM56957 and the Pennsylvania Department of Health TSF (D.R.C.).

PY - 2006/12

Y1 - 2006/12

N2 - Mutations in PERK (EIF2AK3) result in permanent neonatal diabetes as well as several other anomalies that underlie the human Wolcott-Rallison syndrome, and these anomalies are mirrored in Perk knockout mice. To identify the cause of diabetes in PERK-deficient mice, we generated a series of tissue- and cell-specific knockouts of the Perk gene and performed a developmental analysis of the progression to overt diabetes. We discovered that PERK is specifically required in the insulin-secreting β cells during the fetal and early neonatal period as a prerequisite for postnatal glucose homeostasis. However, PERK expression in β cells is not required at the adult stage to maintain β cell functions and glucose homeostasis. We show that PERK-deficient mice exhibit severe defects in fetal/neonatal β cell proliferation and differentiation, resulting in low β cell mass, defects in proinsulin trafficking, and abrogation of insulin secretion that culminate in permanent neonatal diabetes.

AB - Mutations in PERK (EIF2AK3) result in permanent neonatal diabetes as well as several other anomalies that underlie the human Wolcott-Rallison syndrome, and these anomalies are mirrored in Perk knockout mice. To identify the cause of diabetes in PERK-deficient mice, we generated a series of tissue- and cell-specific knockouts of the Perk gene and performed a developmental analysis of the progression to overt diabetes. We discovered that PERK is specifically required in the insulin-secreting β cells during the fetal and early neonatal period as a prerequisite for postnatal glucose homeostasis. However, PERK expression in β cells is not required at the adult stage to maintain β cell functions and glucose homeostasis. We show that PERK-deficient mice exhibit severe defects in fetal/neonatal β cell proliferation and differentiation, resulting in low β cell mass, defects in proinsulin trafficking, and abrogation of insulin secretion that culminate in permanent neonatal diabetes.

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PERK EIF2AK3 control of pancreatic β cell differentiation and proliferation is required for postnatal glucose homeostasis

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