Impact of an SLC30A8 loss-of-function variant on the pancreatic distribution of zinc and manganese: laser ablation-ICP-MS and positron emission tomography studies in mice

INTRODUCTION: Common variants in the SLC30A8 gene, encoding the secretory granule zinc transporter ZnT8 (expressed largely in pancreatic islet alpha and beta cells), are associated with altered risk of type 2 diabetes. Unexpectedly, rare loss-of-function (LoF) variants in the gene, described in hete...

Descripción completa

Detalles Bibliográficos
Autores principales: Firth, George, Georgiadou, Eleni, Griffiths, Alexander, Amrahli, Maral, Kim, Jana, Yu, Zilin, Hu, Ming, Stewart, Theodora J., Leclerc, Isabelle, Okamoto, Haruka, Gomez, Daniel, Blower, Philip J., Rutter, Guy A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2023
Materias:
Endocrinology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10313231/
https://www.ncbi.nlm.nih.gov/pubmed/37396167
http://dx.doi.org/10.3389/fendo.2023.1171933
_version_ 1785067081659580416
author Firth, George
Georgiadou, Eleni
Griffiths, Alexander
Amrahli, Maral
Kim, Jana
Yu, Zilin
Hu, Ming
Stewart, Theodora J.
Leclerc, Isabelle
Okamoto, Haruka
Gomez, Daniel
Blower, Philip J.
Rutter, Guy A.
author_facet Firth, George
Georgiadou, Eleni
Griffiths, Alexander
Amrahli, Maral
Kim, Jana
Yu, Zilin
Hu, Ming
Stewart, Theodora J.
Leclerc, Isabelle
Okamoto, Haruka
Gomez, Daniel
Blower, Philip J.
Rutter, Guy A.
author_sort Firth, George
collection PubMed
description INTRODUCTION: Common variants in the SLC30A8 gene, encoding the secretory granule zinc transporter ZnT8 (expressed largely in pancreatic islet alpha and beta cells), are associated with altered risk of type 2 diabetes. Unexpectedly, rare loss-of-function (LoF) variants in the gene, described in heterozygous individuals only, are protective against the disease, even though knockout of the homologous SLC30A8 gene in mice leads to unchanged or impaired glucose tolerance. Here, we aimed to determine how one or two copies of the mutant R138X allele in the mouse SLC30A8 gene impacts the homeostasis of zinc at a whole-body (using non-invasive (62)Zn PET imaging to assess the acute dynamics of zinc handling) and tissue/cell level [using laser ablation inductively coupled plasma mass spectrometry (LA-ICP-MS) to map the long-term distribution of zinc and manganese in the pancreas]. METHODS: Following intravenous administration of [(62)Zn]Zn-citrate (~7 MBq, 150 μl) in wild-type (WT), heterozygous (R138X(+/−)), and homozygous (R138X(+/+)) mutant mice (14–15 weeks old, n = 4 per genotype), zinc dynamics were measured over 60 min using PET. Histological, islet hormone immunohistochemistry, and elemental analysis with LA-ICP-MS (Zn, Mn, P) were performed on sequential pancreas sections. Bulk Zn and Mn concentration in the pancreas was determined by solution ICP-MS. RESULTS: Our findings reveal that whereas uptake into organs, assessed using PET imaging of (62)Zn, is largely unaffected by the R138X variant, mice homozygous of the mutant allele show a substantial lowering (to 40% of WT) of total islet zinc, as anticipated. In contrast, mice heterozygous for this allele, thus mimicking human carriers of LoF alleles, show markedly increased endocrine and exocrine zinc content (1.6-fold increase for both compared to WT), as measured by LA-ICP-MS. Both endocrine and exocrine manganese contents were also sharply increased in R138X(+/−) mice, with smaller increases observed in R138X(+/+) mice. DISCUSSION: These data challenge the view that zinc depletion from the beta cell is the likely underlying driver for protection from type 2 diabetes development in carriers of LoF alleles. Instead, they suggest that heterozygous LoF may paradoxically increase pancreatic β-cell zinc and manganese content and impact the levels of these metals in the exocrine pancreas to improve insulin secretion.
format Online
Article
Text
id pubmed-10313231
institution National Center for Biotechnology Information
language English
publishDate 2023
publisher Frontiers Media S.A.
record_format MEDLINE/PubMed
spelling pubmed-103132312023-07-01 Impact of an SLC30A8 loss-of-function variant on the pancreatic distribution of zinc and manganese: laser ablation-ICP-MS and positron emission tomography studies in mice Firth, George Georgiadou, Eleni Griffiths, Alexander Amrahli, Maral Kim, Jana Yu, Zilin Hu, Ming Stewart, Theodora J. Leclerc, Isabelle Okamoto, Haruka Gomez, Daniel Blower, Philip J. Rutter, Guy A. Front Endocrinol (Lausanne) Endocrinology INTRODUCTION: Common variants in the SLC30A8 gene, encoding the secretory granule zinc transporter ZnT8 (expressed largely in pancreatic islet alpha and beta cells), are associated with altered risk of type 2 diabetes. Unexpectedly, rare loss-of-function (LoF) variants in the gene, described in heterozygous individuals only, are protective against the disease, even though knockout of the homologous SLC30A8 gene in mice leads to unchanged or impaired glucose tolerance. Here, we aimed to determine how one or two copies of the mutant R138X allele in the mouse SLC30A8 gene impacts the homeostasis of zinc at a whole-body (using non-invasive (62)Zn PET imaging to assess the acute dynamics of zinc handling) and tissue/cell level [using laser ablation inductively coupled plasma mass spectrometry (LA-ICP-MS) to map the long-term distribution of zinc and manganese in the pancreas]. METHODS: Following intravenous administration of [(62)Zn]Zn-citrate (~7 MBq, 150 μl) in wild-type (WT), heterozygous (R138X(+/−)), and homozygous (R138X(+/+)) mutant mice (14–15 weeks old, n = 4 per genotype), zinc dynamics were measured over 60 min using PET. Histological, islet hormone immunohistochemistry, and elemental analysis with LA-ICP-MS (Zn, Mn, P) were performed on sequential pancreas sections. Bulk Zn and Mn concentration in the pancreas was determined by solution ICP-MS. RESULTS: Our findings reveal that whereas uptake into organs, assessed using PET imaging of (62)Zn, is largely unaffected by the R138X variant, mice homozygous of the mutant allele show a substantial lowering (to 40% of WT) of total islet zinc, as anticipated. In contrast, mice heterozygous for this allele, thus mimicking human carriers of LoF alleles, show markedly increased endocrine and exocrine zinc content (1.6-fold increase for both compared to WT), as measured by LA-ICP-MS. Both endocrine and exocrine manganese contents were also sharply increased in R138X(+/−) mice, with smaller increases observed in R138X(+/+) mice. DISCUSSION: These data challenge the view that zinc depletion from the beta cell is the likely underlying driver for protection from type 2 diabetes development in carriers of LoF alleles. Instead, they suggest that heterozygous LoF may paradoxically increase pancreatic β-cell zinc and manganese content and impact the levels of these metals in the exocrine pancreas to improve insulin secretion. Frontiers Media S.A. 2023-06-16 /pmc/articles/PMC10313231/ /pubmed/37396167 http://dx.doi.org/10.3389/fendo.2023.1171933 Text en Copyright © 2023 Firth, Georgiadou, Griffiths, Amrahli, Kim, Yu, Hu, Stewart, Leclerc, Okamoto, Gomez, Blower and Rutter https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Endocrinology
Firth, George
Georgiadou, Eleni
Griffiths, Alexander
Amrahli, Maral
Kim, Jana
Yu, Zilin
Hu, Ming
Stewart, Theodora J.
Leclerc, Isabelle
Okamoto, Haruka
Gomez, Daniel
Blower, Philip J.
Rutter, Guy A.
Impact of an SLC30A8 loss-of-function variant on the pancreatic distribution of zinc and manganese: laser ablation-ICP-MS and positron emission tomography studies in mice
title Impact of an SLC30A8 loss-of-function variant on the pancreatic distribution of zinc and manganese: laser ablation-ICP-MS and positron emission tomography studies in mice
title_full Impact of an SLC30A8 loss-of-function variant on the pancreatic distribution of zinc and manganese: laser ablation-ICP-MS and positron emission tomography studies in mice
title_fullStr Impact of an SLC30A8 loss-of-function variant on the pancreatic distribution of zinc and manganese: laser ablation-ICP-MS and positron emission tomography studies in mice
title_full_unstemmed Impact of an SLC30A8 loss-of-function variant on the pancreatic distribution of zinc and manganese: laser ablation-ICP-MS and positron emission tomography studies in mice
title_short Impact of an SLC30A8 loss-of-function variant on the pancreatic distribution of zinc and manganese: laser ablation-ICP-MS and positron emission tomography studies in mice
title_sort impact of an slc30a8 loss-of-function variant on the pancreatic distribution of zinc and manganese: laser ablation-icp-ms and positron emission tomography studies in mice
topic Endocrinology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10313231/
https://www.ncbi.nlm.nih.gov/pubmed/37396167
http://dx.doi.org/10.3389/fendo.2023.1171933
work_keys_str_mv AT firthgeorge impactofanslc30a8lossoffunctionvariantonthepancreaticdistributionofzincandmanganeselaserablationicpmsandpositronemissiontomographystudiesinmice
AT georgiadoueleni impactofanslc30a8lossoffunctionvariantonthepancreaticdistributionofzincandmanganeselaserablationicpmsandpositronemissiontomographystudiesinmice
AT griffithsalexander impactofanslc30a8lossoffunctionvariantonthepancreaticdistributionofzincandmanganeselaserablationicpmsandpositronemissiontomographystudiesinmice
AT amrahlimaral impactofanslc30a8lossoffunctionvariantonthepancreaticdistributionofzincandmanganeselaserablationicpmsandpositronemissiontomographystudiesinmice
AT kimjana impactofanslc30a8lossoffunctionvariantonthepancreaticdistributionofzincandmanganeselaserablationicpmsandpositronemissiontomographystudiesinmice
AT yuzilin impactofanslc30a8lossoffunctionvariantonthepancreaticdistributionofzincandmanganeselaserablationicpmsandpositronemissiontomographystudiesinmice
AT huming impactofanslc30a8lossoffunctionvariantonthepancreaticdistributionofzincandmanganeselaserablationicpmsandpositronemissiontomographystudiesinmice
AT stewarttheodoraj impactofanslc30a8lossoffunctionvariantonthepancreaticdistributionofzincandmanganeselaserablationicpmsandpositronemissiontomographystudiesinmice
AT leclercisabelle impactofanslc30a8lossoffunctionvariantonthepancreaticdistributionofzincandmanganeselaserablationicpmsandpositronemissiontomographystudiesinmice
AT okamotoharuka impactofanslc30a8lossoffunctionvariantonthepancreaticdistributionofzincandmanganeselaserablationicpmsandpositronemissiontomographystudiesinmice
AT gomezdaniel impactofanslc30a8lossoffunctionvariantonthepancreaticdistributionofzincandmanganeselaserablationicpmsandpositronemissiontomographystudiesinmice
AT blowerphilipj impactofanslc30a8lossoffunctionvariantonthepancreaticdistributionofzincandmanganeselaserablationicpmsandpositronemissiontomographystudiesinmice
AT rutterguya impactofanslc30a8lossoffunctionvariantonthepancreaticdistributionofzincandmanganeselaserablationicpmsandpositronemissiontomographystudiesinmice

Ejemplares similares