SLC30A3 responds to glucose- and zinc variations in beta-cells and is critical for insulin production and in vivo glucose-metabolism during beta-cell stress

Kamille Smidt; Niels Jessen; Andreas Brønden Petersen; Agnete Larsen; Nils Erik Magnusson; Johanne Bruun Jeppesen; Meredin Stoltenberg; Janetta G Culvenor; Andrew Tsatsanis; Birgitte Brock; Ole Schmitz; Lise Wogensen; Ashley I Bush; Jørgen Rungby

doi:10.1371/journal.pone.0005684

SLC30A3 responds to glucose- and zinc variations in beta-cells and is critical for insulin production and in vivo glucose-metabolism during beta-cell stress

Kamille Smidt, Niels Jessen, Andreas Brønden Petersen, Agnete Larsen, Nils Erik Magnusson, Johanne Bruun Jeppesen, Meredin Stoltenberg, Janetta G Culvenor, Andrew Tsatsanis, Birgitte Brock, Ole Schmitz, Lise Wogensen, Ashley I Bush, Jørgen Rungby

81 Citations (Scopus)

Abstract

BACKGROUND: Ion transporters of the Slc30A- (ZnT-) family regulate zinc fluxes into sub-cellular compartments. beta-cells depend on zinc for both insulin crystallization and regulation of cell mass.

METHODOLOGY/PRINCIPAL FINDINGS: This study examined: the effect of glucose and zinc chelation on ZnT gene and protein levels and apoptosis in beta-cells and pancreatic islets, the effects of ZnT-3 knock-down on insulin secretion in a beta-cell line and ZnT-3 knock-out on glucose metabolism in mice during streptozotocin-induced beta-cell stress. In INS-1E cells 2 mM glucose down-regulated ZnT-3 and up-regulated ZnT-5 expression relative to 5 mM. 16 mM glucose increased ZnT-3 and decreased ZnT-8 expression. Zinc chelation by DEDTC lowered INS-1E insulin content and insulin expression. Furthermore, zinc depletion increased ZnT-3- and decreased ZnT-8 gene expression whereas the amount of ZnT-3 protein in the cells was decreased. Zinc depletion and high glucose induced apoptosis and necrosis in INS-1E cells. The most responsive zinc transporter, ZnT-3, was investigated further; by immunohistochemistry and western blotting ZnT-3 was demonstrated in INS-1E cells. 44% knock-down of ZnT-3 by siRNA transfection in INS-1E cells decreased insulin expression and secretion. Streptozotocin-treated mice had higher glucose levels after ZnT-3 knock-out, particularly in overt diabetic animals.

CONCLUSION/SIGNIFICANCE: Zinc transporting proteins in beta-cells respond to variations in glucose and zinc levels. ZnT-3, which is pivotal in the development of cellular changes as also seen in type 2 diabetes (e.g. amyloidosis in Alzheimer's disease) but not previously described in beta-cells, is present in this cell type, up-regulated by glucose in a concentration dependent manner and up-regulated by zinc depletion which by contrast decreased ZnT-3 protein levels. Knock-down of the ZnT-3 gene lowers insulin secretion in vitro and affects in vivo glucose metabolism after streptozotocin treatment.

Original language	English
Journal	P L o S One
Volume	4
Issue number	5
Pages (from-to)	e5684
ISSN	1932-6203
DOIs	https://doi.org/10.1371/journal.pone.0005684
Publication status	Published - 25 May 2009
Externally published	Yes

Keywords

Animals
Blood Glucose
Carrier Proteins
Cation Transport Proteins
Cell Death
Cell Line
Chelating Agents
Dose-Response Relationship, Drug
Fasting
Gene Expression Regulation
Gene Knockdown Techniques
Glucose
Hyperglycemia
Insulin
Insulin-Secreting Cells
Membrane Proteins
Mice
Mice, Knockout
Rats
Streptozocin
Stress, Physiological
Zinc

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Smidt, K., Jessen, N., Petersen, A. B., Larsen, A., Magnusson, N. E., Jeppesen, J. B., Stoltenberg, M., Culvenor, J. G., Tsatsanis, A., Brock, B., Schmitz, O., Wogensen, L., Bush, A. I., & Rungby, J. (2009). SLC30A3 responds to glucose- and zinc variations in beta-cells and is critical for insulin production and in vivo glucose-metabolism during beta-cell stress. P L o S One, 4(5), e5684. https://doi.org/10.1371/journal.pone.0005684

Smidt, K, Jessen, N, Petersen, AB, Larsen, A, Magnusson, NE, Jeppesen, JB, Stoltenberg, M, Culvenor, JG, Tsatsanis, A, Brock, B, Schmitz, O, Wogensen, L, Bush, AI & Rungby, J 2009, 'SLC30A3 responds to glucose- and zinc variations in beta-cells and is critical for insulin production and in vivo glucose-metabolism during beta-cell stress', P L o S One, vol. 4, no. 5, pp. e5684. https://doi.org/10.1371/journal.pone.0005684

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title = "SLC30A3 responds to glucose- and zinc variations in beta-cells and is critical for insulin production and in vivo glucose-metabolism during beta-cell stress",

abstract = "BACKGROUND: Ion transporters of the Slc30A- (ZnT-) family regulate zinc fluxes into sub-cellular compartments. beta-cells depend on zinc for both insulin crystallization and regulation of cell mass.METHODOLOGY/PRINCIPAL FINDINGS: This study examined: the effect of glucose and zinc chelation on ZnT gene and protein levels and apoptosis in beta-cells and pancreatic islets, the effects of ZnT-3 knock-down on insulin secretion in a beta-cell line and ZnT-3 knock-out on glucose metabolism in mice during streptozotocin-induced beta-cell stress. In INS-1E cells 2 mM glucose down-regulated ZnT-3 and up-regulated ZnT-5 expression relative to 5 mM. 16 mM glucose increased ZnT-3 and decreased ZnT-8 expression. Zinc chelation by DEDTC lowered INS-1E insulin content and insulin expression. Furthermore, zinc depletion increased ZnT-3- and decreased ZnT-8 gene expression whereas the amount of ZnT-3 protein in the cells was decreased. Zinc depletion and high glucose induced apoptosis and necrosis in INS-1E cells. The most responsive zinc transporter, ZnT-3, was investigated further; by immunohistochemistry and western blotting ZnT-3 was demonstrated in INS-1E cells. 44\% knock-down of ZnT-3 by siRNA transfection in INS-1E cells decreased insulin expression and secretion. Streptozotocin-treated mice had higher glucose levels after ZnT-3 knock-out, particularly in overt diabetic animals.CONCLUSION/SIGNIFICANCE: Zinc transporting proteins in beta-cells respond to variations in glucose and zinc levels. ZnT-3, which is pivotal in the development of cellular changes as also seen in type 2 diabetes (e.g. amyloidosis in Alzheimer's disease) but not previously described in beta-cells, is present in this cell type, up-regulated by glucose in a concentration dependent manner and up-regulated by zinc depletion which by contrast decreased ZnT-3 protein levels. Knock-down of the ZnT-3 gene lowers insulin secretion in vitro and affects in vivo glucose metabolism after streptozotocin treatment.",

keywords = "Animals, Blood Glucose, Carrier Proteins, Cation Transport Proteins, Cell Death, Cell Line, Chelating Agents, Dose-Response Relationship, Drug, Fasting, Gene Expression Regulation, Gene Knockdown Techniques, Glucose, Hyperglycemia, Insulin, Insulin-Secreting Cells, Membrane Proteins, Mice, Mice, Knockout, Rats, Streptozocin, Stress, Physiological, Zinc",

author = "Kamille Smidt and Niels Jessen and Petersen, \{Andreas Br{\o}nden\} and Agnete Larsen and Magnusson, \{Nils Erik\} and Jeppesen, \{Johanne Bruun\} and Meredin Stoltenberg and Culvenor, \{Janetta G\} and Andrew Tsatsanis and Birgitte Brock and Ole Schmitz and Lise Wogensen and Bush, \{Ashley I\} and J{\o}rgen Rungby",

year = "2009",

month = may,

day = "25",

doi = "10.1371/journal.pone.0005684",

language = "English",

volume = "4",

pages = "e5684",

journal = "P L o S One",

issn = "1932-6203",

publisher = "Public Library of Science",

number = "5",

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TY - JOUR

T1 - SLC30A3 responds to glucose- and zinc variations in beta-cells and is critical for insulin production and in vivo glucose-metabolism during beta-cell stress

AU - Smidt, Kamille

AU - Jessen, Niels

AU - Petersen, Andreas Brønden

AU - Larsen, Agnete

AU - Magnusson, Nils Erik

AU - Jeppesen, Johanne Bruun

AU - Stoltenberg, Meredin

AU - Culvenor, Janetta G

AU - Tsatsanis, Andrew

AU - Brock, Birgitte

AU - Schmitz, Ole

AU - Wogensen, Lise

AU - Bush, Ashley I

AU - Rungby, Jørgen

PY - 2009/5/25

Y1 - 2009/5/25

N2 - BACKGROUND: Ion transporters of the Slc30A- (ZnT-) family regulate zinc fluxes into sub-cellular compartments. beta-cells depend on zinc for both insulin crystallization and regulation of cell mass.METHODOLOGY/PRINCIPAL FINDINGS: This study examined: the effect of glucose and zinc chelation on ZnT gene and protein levels and apoptosis in beta-cells and pancreatic islets, the effects of ZnT-3 knock-down on insulin secretion in a beta-cell line and ZnT-3 knock-out on glucose metabolism in mice during streptozotocin-induced beta-cell stress. In INS-1E cells 2 mM glucose down-regulated ZnT-3 and up-regulated ZnT-5 expression relative to 5 mM. 16 mM glucose increased ZnT-3 and decreased ZnT-8 expression. Zinc chelation by DEDTC lowered INS-1E insulin content and insulin expression. Furthermore, zinc depletion increased ZnT-3- and decreased ZnT-8 gene expression whereas the amount of ZnT-3 protein in the cells was decreased. Zinc depletion and high glucose induced apoptosis and necrosis in INS-1E cells. The most responsive zinc transporter, ZnT-3, was investigated further; by immunohistochemistry and western blotting ZnT-3 was demonstrated in INS-1E cells. 44% knock-down of ZnT-3 by siRNA transfection in INS-1E cells decreased insulin expression and secretion. Streptozotocin-treated mice had higher glucose levels after ZnT-3 knock-out, particularly in overt diabetic animals.CONCLUSION/SIGNIFICANCE: Zinc transporting proteins in beta-cells respond to variations in glucose and zinc levels. ZnT-3, which is pivotal in the development of cellular changes as also seen in type 2 diabetes (e.g. amyloidosis in Alzheimer's disease) but not previously described in beta-cells, is present in this cell type, up-regulated by glucose in a concentration dependent manner and up-regulated by zinc depletion which by contrast decreased ZnT-3 protein levels. Knock-down of the ZnT-3 gene lowers insulin secretion in vitro and affects in vivo glucose metabolism after streptozotocin treatment.

AB - BACKGROUND: Ion transporters of the Slc30A- (ZnT-) family regulate zinc fluxes into sub-cellular compartments. beta-cells depend on zinc for both insulin crystallization and regulation of cell mass.METHODOLOGY/PRINCIPAL FINDINGS: This study examined: the effect of glucose and zinc chelation on ZnT gene and protein levels and apoptosis in beta-cells and pancreatic islets, the effects of ZnT-3 knock-down on insulin secretion in a beta-cell line and ZnT-3 knock-out on glucose metabolism in mice during streptozotocin-induced beta-cell stress. In INS-1E cells 2 mM glucose down-regulated ZnT-3 and up-regulated ZnT-5 expression relative to 5 mM. 16 mM glucose increased ZnT-3 and decreased ZnT-8 expression. Zinc chelation by DEDTC lowered INS-1E insulin content and insulin expression. Furthermore, zinc depletion increased ZnT-3- and decreased ZnT-8 gene expression whereas the amount of ZnT-3 protein in the cells was decreased. Zinc depletion and high glucose induced apoptosis and necrosis in INS-1E cells. The most responsive zinc transporter, ZnT-3, was investigated further; by immunohistochemistry and western blotting ZnT-3 was demonstrated in INS-1E cells. 44% knock-down of ZnT-3 by siRNA transfection in INS-1E cells decreased insulin expression and secretion. Streptozotocin-treated mice had higher glucose levels after ZnT-3 knock-out, particularly in overt diabetic animals.CONCLUSION/SIGNIFICANCE: Zinc transporting proteins in beta-cells respond to variations in glucose and zinc levels. ZnT-3, which is pivotal in the development of cellular changes as also seen in type 2 diabetes (e.g. amyloidosis in Alzheimer's disease) but not previously described in beta-cells, is present in this cell type, up-regulated by glucose in a concentration dependent manner and up-regulated by zinc depletion which by contrast decreased ZnT-3 protein levels. Knock-down of the ZnT-3 gene lowers insulin secretion in vitro and affects in vivo glucose metabolism after streptozotocin treatment.

KW - Animals

KW - Blood Glucose

KW - Carrier Proteins

KW - Cation Transport Proteins

KW - Cell Death

KW - Cell Line

KW - Chelating Agents

KW - Dose-Response Relationship, Drug

KW - Fasting

KW - Gene Expression Regulation

KW - Gene Knockdown Techniques

KW - Glucose

KW - Hyperglycemia

KW - Insulin

KW - Insulin-Secreting Cells

KW - Membrane Proteins

KW - Mice

KW - Mice, Knockout

KW - Rats

KW - Streptozocin

KW - Stress, Physiological

KW - Zinc

UR - https://www.scopus.com/pages/publications/66249127252

U2 - 10.1371/journal.pone.0005684

DO - 10.1371/journal.pone.0005684

M3 - Journal article

C2 - 19492079

SN - 1932-6203

VL - 4

SP - e5684

JO - P L o S One

JF - P L o S One

IS - 5

ER -

SLC30A3 responds to glucose- and zinc variations in beta-cells and is critical for insulin production and in vivo glucose-metabolism during beta-cell stress

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