Your search keyword '"Julie Kerr-Conte"' showing total 11 results

1. Neuromedin U uses Gαi2 and Gαo to suppress glucose-stimulated Ca2+ signaling and insulin secretion in pancreatic β cells.

Author

Weidong Zhang, Hideyuki Sakoda, Yuki Nakazato, Md Nurul Islam, François Pattou, Julie Kerr-Conte, and Masamitsu Nakazato

Subjects

Medicine, Science

Abstract

Neuromedin U (NMU), a highly conserved peptide in mammals, is involved in a wide variety of physiological processes, including impairment of pancreatic β-cell function via induction of mitochondrial dysfunction and endoplasmic reticulum (ER) stress, ultimately suppressing insulin secretion. NMU has two receptors, NMU receptor 1 (NMUR1) and NMUR2, both of which are G-protein-coupled receptors (GPCRs). Only NMUR1 is expressed in mouse islets and β cell-derived MIN6-K8 cells. The molecular mechanisms underlying the insulinostatic action mediated by NMUR1 in β cells have yet to be elucidated. In this study, we explored the molecular mechanism driving impairment of insulin secretion in β cells by the NMU-NMUR1 axis. Pretreatment with the Gαi/o inhibitor Bordetella pertussis toxin (PTX), but not the Gαq inhibitor YM254890, abolished NMU-induced suppression of glucose-stimulated insulin secretion and calcium response in β cells. Knockdown of Gαi2 and Gαo in β cells counteracted NMU-induced suppression of insulin secretion and gene alterations related to mitochondrial fusion (Mfn1, Mfn2), fission (Fis1, Drp1), mitophagy (Pink1, Park2), mitochondrial dynamics (Pgc-1α, Nrf1, and Tfam), ER stress (Chop, Atp2a3, Ryr2, and Itpr2), intracellular ATP level, and mitochondrial membrane potential. NMU decreased forskolin-stimulated intracellular cAMP in both mouse and human islets. We concluded that NMUR1 coupled to PTX-sensitive Gαi2 and Gαo proteins in β cells reduced intracellular Ca2+ influx and cAMP level, thereby causing β-cell dysfunction and impairment. These results highlight a novel signaling mechanism of NMU and provide valuable insights into the further investigation of NMU functions in β-cell biology.

Published

2021

2. Endoplasmic Reticulum Stress Links Oxidative Stress to Impaired Pancreatic Beta-Cell Function Caused by Human Oxidized LDL.

Author

Valérie Plaisance, Saška Brajkovic, Mathie Tenenbaum, Dimitri Favre, Hélène Ezanno, Amélie Bonnefond, Caroline Bonner, Valéry Gmyr, Julie Kerr-Conte, Benoit R Gauthier, Christian Widmann, Gérard Waeber, François Pattou, Philippe Froguel, and Amar Abderrahmani

Subjects

Medicine, Science

Abstract

Elevated plasma concentration of the pro-atherogenic oxidized low density lipoprotein cholesterol (LDL) triggers adverse effects in pancreatic beta-cells and is associated with type 2 diabetes. Here, we investigated whether the endoplasmic reticulum (ER) stress is a key player coupling oxidative stress to beta-cell dysfunction and death elicited by human oxidized LDL. We found that human oxidized LDL activates ER stress as evidenced by the activation of the inositol requiring 1α, and the elevated expression of both DDIT3 (also called CHOP) and DNAJC3 (also called P58IPK) ER stress markers in isolated human islets and the mouse insulin secreting MIN6 cells. Silencing of Chop and inhibition of ER stress markers by the chemical chaperone phenyl butyric acid (PBA) prevented cell death caused by oxidized LDL. Finally, we found that oxidative stress accounts for activation of ER stress markers induced by oxidized LDL. Induction of Chop/CHOP and p58IPK/P58IPK by oxidized LDL was mimicked by hydrogen peroxide and was blocked by co-treatment with the N-acetylcystein antioxidant. As a conclusion, the harmful effects of oxidized LDL in beta-cells requires ER stress activation in a manner that involves oxidative stress. This mechanism may account for impaired beta-cell function in diabetes and can be reversed by antioxidant treatment.

Published

2016

3. The temporal and hierarchical control of transcription factors-induced liver to pancreas transdifferentiation.

Author

Dana Berneman-Zeitouni, Kfir Molakandov, Marina Elgart, Eytan Mor, Alessia Fornoni, Miriam Ramírez Domínguez, Julie Kerr-Conte, Michael Ott, Irit Meivar-Levy, and Sarah Ferber

Subjects

Medicine, Science

Abstract

Lineage-specific transcription factors (TFs) display instructive roles in directly reprogramming adult cells into alternate developmental fates, in a process known as transdifferentiation. The present study analyses the hypothesis that despite being fast, transdifferentiation does not occur in one step but is rather a consecutive and hierarchical process. Using ectopic expression of Pdx1 in human liver cells, we demonstrate that while glucagon and somatostatin expression initiates within a day, insulin gene expression becomes evident only 2-3 days later. To both increase transdifferentiation efficiency and analyze whether the process indeed display consecutive and hierarchical characteristics, adult human liver cells were treated by three pancreatic transcription factors, Pdx1, Pax4 and Mafa (3pTFs) that control distinct hierarchical stages of pancreatic development in the embryo. Ectopic expression of the 3pTFs in human liver cells, increased the transdifferentiation yield, manifested by 300% increase in the number of insulin positive cells, compared to each of the ectopic factors alone. However, only when the 3pTFs were sequentially supplemented one day apart from each other in a direct hierarchical manner, the transdifferentiated cells displayed increased mature β-cell-like characteristics. Ectopic expression of Pdx1 followed by Pax4 on the 2(nd) day and concluded by Mafa on the 3(rd) day resulted in increased yield of transdifferentiation that was associated by increased glucose regulated c-peptide secretion. By contrast, concerted or sequential administration of the ectopic 3pTFs in an indirect hierarchical mode resulted in the generation of insulin and somatostatin co-producing cells and diminished glucose regulated processed insulin secretion. In conclusion transcription factors induced liver to pancreas transdifferentiation is a progressive and hierarchical process. It is reasonable to assume that this characteristic is general to wide ranges of tissues. Therefore, our findings could facilitate the development of cell replacement therapy modalities for many degenerative diseases including diabetes.

Published

2014

4. CpG methylation changes within the IL2RA promoter in type 1 diabetes of childhood onset.

Author

Marie-Pierre Belot, Delphine Fradin, Nga Mai, Sophie Le Fur, Diana Zélénika, Julie Kerr-Conte, François Pattou, Bruno Lucas, and Pierre Bougnères

Subjects

Medicine, Science

Abstract

None of the polymorphic variants of the IL2RA gene found associated with Type 1 Diabetes (T1D) was shown to have a functional effect. To test if the epigenetic variation could play a role at this locus, we studied the methylation of 6 CpGs located within the proximal promoter of IL2RA gene in 252 T1D patients compared with 286 age-matched controls. We found that DNA methylation at CpGs -373 and -456 was slightly but significantly higher in patients than in controls (40.4 ± 4.6 vs 38.3 ± 5.4, p=1.4E4; 91.4 ± 2.8 vs 89.5 ± 5.3, p=1.8E-6), while other CpG showed a strictly comparable methylation. Among 106 single nucleotide polymorphisms (SNPs) located in the neighboring 180 kb region, we found that 28 SNPs were associated with DNA methylation at CpG -373. Sixteen of these SNPs were known to be associated with T1D. Our findings suggest that the effect of IL2RA risk alleles on T1D may be partially mediated through epigenetic changes.

Published

2013

5. Both PAX4 and MAFA are expressed in a substantial proportion of normal human pancreatic alpha cells and deregulated in patients with type 2 diabetes.

Author

Rémy Bonnavion, Rami Jaafar, Julie Kerr-Conte, Fouzia Assade, Esther van Stralen, Emmanuelle Leteurtre, Célio Pouponnot, Sofia Gargani, François Pattou, Philippe Bertolino, Martine Cordier-Bussat, Jieli Lu, and Chang Xian Zhang

Subjects

Medicine, Science

Abstract

Pax4 and MafA (v-maf musculoaponeurotic fibrosarcoma oncogene homolog A) are two transcription factors crucial for normal functions of islet beta cells in the mouse. Intriguingly, recent studies indicate the existence of notable difference between human and rodent islet in terms of gene expression and functions. To better understand the biological role of human PAX4 and MAFA, we investigated their expression in normal and diseased human islets, using validated antibodies. PAX4 was detected in 43.0±5.0% and 39.1±4.0% of normal human alpha and beta cells respectively. We found that MAFA, detected in 88.3±6.3% insulin(+)cells as in the mouse, turned out to be also expressed in 61.2±6.4% of human glucagons(+) cells with less intensity than in insulin(+) cells, whereas MAFB expression was found not only in the majority of glucagon(+) cells (67.2±7.6%), but also in 53.6±10.5% of human insulin(+) cells. Interestingly, MAFA nuclear expression in both alpha and beta cells, and the percentage of alpha cells expressing PAX4 were found altered in a substantial proportion of patients with type 2 diabetes. Both MAFA and PAX4 display, therefore, a distinct expression pattern in human islet cells, suggesting more potential plasticity of human islets as compared with rodent islets.

Published

2013

6. Type 2 diabetes susceptibility gene expression in normal or diabetic sorted human alpha and beta cells: correlations with age or BMI of islet donors.

Author

Clare L Kirkpatrick, Piero Marchetti, Francesco Purrello, Salvatore Piro, Marco Bugliani, Domenico Bosco, Eelco J P de Koning, Marten A Engelse, Julie Kerr-Conte, François Pattou, and Claes B Wollheim

Subjects

Medicine, Science

Abstract

BackgroundGenome-wide association studies have identified susceptibility genes for development of type 2 diabetes. We aimed to examine whether a subset of these (comprising FTO, IDE, KCNJ11, PPARG and TCF7L2) were transcriptionally restricted to or enriched in human beta cells by sorting islet cells into alpha and beta - specific fractions. We also aimed to correlate expression of these transcripts in both alpha and beta cell types with phenotypic traits of the islet donors and to compare diabetic and non-diabetic cells.Methodology/principal findingsIslet cells were sorted using a previously published method and RNA was extracted, reverse transcribed and used as the template for quantitative PCR. Sorted cells were also analysed for insulin and glucagon immunostaining and insulin secretion from the beta cells as well as insulin, glucagon and GLP-1 content. All five genes were expressed in both alpha and beta cells, with significant enrichment of KCNJ11 in the beta cells and of TCF7L2 in the alpha cells. The ratio of KCNJ11 in beta to alpha cells was negatively correlated with BMI, while KCNJ11 expression in alpha cells was negatively correlated with age but not associated with BMI. Beta cell expression of glucagon, TCF7L2 and IDE was increased in cells from islets that had spent more time in culture prior to cell sorting. In beta cells, KCNJ11, FTO and insulin were positively correlated with each other. Diabetic alpha and beta cells had decreased expression of insulin, glucagon and FTO.Conclusions/significanceThis study has identified novel patterns of expression of type 2 diabetes susceptibility genes within sorted islet cells and suggested interactions of gene expression with age or BMI of the islet donors. However, expression of these genes in islets is less associated with BMI than has been found for other tissues.

Published

2010

7. Epithelial-mesenchymal transition in cells expanded in vitro from lineage-traced adult human pancreatic beta cells.

Author

Holger A Russ, Philippe Ravassard, Julie Kerr-Conte, Francois Pattou, and Shimon Efrat

Subjects

Medicine, Science

Abstract

BackgroundIn-vitro expansion of functional beta cells from adult human islets is an attractive approach for generating an abundant source of cells for beta-cell replacement therapy of diabetes. Using genetic cell-lineage tracing we have recently shown that beta cells cultured from adult human islets undergo rapid dedifferentiation and proliferate for up to 16 population doublings. These cells have raised interest as potential candidates for redifferentiation into functional insulin-producing cells. Previous work has associated dedifferentiation of cultured epithelial cells with epithelial-mesenchymal transition (EMT), and suggested that EMT generates cells with stem cell properties. Here we investigated the occurrence of EMT in these cultures and assessed their stem cell potential.Methodology/principal findingsUsing cell-lineage tracing we provide direct evidence for occurrence of EMT in cells originating from beta cells in cultures of adult human islet cells. These cells express multiple mesenchymal markers, as well as markers associated with mesenchymal stem cells (MSC). However, we do not find evidence for the ability of such cells, nor of cells in these cultures derived from a non-beta-cell origin, to significantly differentiate into mesodermal cell types.Conclusions/significanceThese findings constitute the first demonstration based on genetic lineage-tracing of EMT in cultured adult primary human cells, and show that EMT does not induce multipotency in cells derived from human beta cells.

Published

2009

8. Neuromedin U uses Gαi2 and Gαo to suppress glucose-stimulated Ca2+ signaling and insulin secretion in pancreatic β cells

Author

Masamitsu Nakazato, Yuki Nakazato, Nurul Islam, François Pattou, Weidong Zhang, Julie Kerr-Conte, and Hideyuki Sakoda

Subjects

Physiology, Peptide Hormones, Cell Membranes, MFN2, Mitochondrion, Biochemistry, Mice, Endocrinology, Insulin-Secreting Cells, Insulin Secretion, Medicine and Health Sciences, Energy-Producing Organelles, Membrane Potential, Mitochondrial, Multidisciplinary, biology, Organic Compounds, Chemistry, Monosaccharides, Small interfering RNA, Receptors, Neurotransmitter, Mitochondria, Cell biology, Nucleic acids, mitochondrial fusion, Physical Sciences, Medicine, Cellular Structures and Organelles, Somatostatin, Intracellular, Neuromedin U, Research Article, Signal Transduction, FIS1, Transmembrane Receptors, Science, Carbohydrates, Bioenergetics, Cell Line, GTP-Binding Proteins, Genetics, Animals, Humans, Calcium Signaling, Non-coding RNA, Endocrine Physiology, Neuropeptides, Organic Chemistry, Insulin Signaling, Chemical Compounds, Biology and Life Sciences, Proteins, Cell Biology, Intracellular Membranes, TFAM, Hormones, Gene regulation, Insulin receptor, Glucose, biology.protein, RNA, Gene expression, G Protein Coupled Receptors

Abstract

Neuromedin U (NMU), a highly conserved peptide in mammals, is involved in a wide variety of physiological processes, including impairment of pancreatic β-cell function via induction of mitochondrial dysfunction and endoplasmic reticulum (ER) stress, ultimately suppressing insulin secretion. NMU has two receptors, NMU receptor 1 (NMUR1) and NMUR2, both of which are G-protein–coupled receptors (GPCRs). Only NMUR1 is expressed in mouse islets and β cell–derived MIN6-K8 cells. The molecular mechanisms underlying the insulinostatic action mediated by NMUR1 in β cells have yet to be elucidated. In this study, we explored the molecular mechanism driving impairment of insulin secretion in β cells by the NMU–NMUR1 axis. Pretreatment with the Gαi/o inhibitor Bordetella pertussis toxin (PTX), but not the Gαq inhibitor YM254890, abolished NMU-induced suppression of glucose-stimulated insulin secretion and calcium response in β cells. Knockdown of Gαi2 and Gαo in β cells counteracted NMU-induced suppression of insulin secretion and gene alterations related to mitochondrial fusion (Mfn1, Mfn2), fission (Fis1, Drp1), mitophagy (Pink1, Park2), mitochondrial dynamics (Pgc-1α, Nrf1, and Tfam), ER stress (Chop, Atp2a3, Ryr2, and Itpr2), intracellular ATP level, and mitochondrial membrane potential. NMU decreased forskolin-stimulated intracellular cAMP in both mouse and human islets. We concluded that NMUR1 coupled to PTX-sensitive Gαi2 and Gαo proteins in β cells reduced intracellular Ca2+ influx and cAMP level, thereby causing β-cell dysfunction and impairment. These results highlight a novel signaling mechanism of NMU and provide valuable insights into the further investigation of NMU functions in β-cell biology.

Published

2021

9. Endoplasmic Reticulum Stress Links Oxidative Stress to Impaired Pancreatic Beta-Cell Function Caused by Human Oxidized LDL

Author

Gérard Waeber, Amar Abderrahmani, Philippe Froguel, Saška Brajkovic, Mathie Tenenbaum, Christian Widmann, Hélène Ezanno, Julie Kerr-Conte, François Pattou, Valery Gmyr, Benoit R. Gauthier, Dimitri Favre, Valérie Plaisance, Caroline Bonner, Amélie Bonnefond, Région Nord Pas de Calais, European Commission, [Plaisance, Valerie] Univ Lille, CNRS, Inst Pasteur Lille, UMR 8199 EGID, Lille, France, [Brajkovic, Saska] Univ Lille, CNRS, Inst Pasteur Lille, UMR 8199 EGID, Lille, France, [Tenenbaum, Mathie] Univ Lille, CNRS, Inst Pasteur Lille, UMR 8199 EGID, Lille, France, [Favre, Dimitri] Univ Lille, CNRS, Inst Pasteur Lille, UMR 8199 EGID, Lille, France, [Ezanno, Helene] Univ Lille, CNRS, Inst Pasteur Lille, UMR 8199 EGID, Lille, France, [Bonnefond, Amelie] Univ Lille, CNRS, Inst Pasteur Lille, UMR 8199 EGID, Lille, France, [Froguel, Philippe] Univ Lille, CNRS, Inst Pasteur Lille, UMR 8199 EGID, Lille, France, [Abderrahmani, Amar] Univ Lille, CNRS, Inst Pasteur Lille, UMR 8199 EGID, Lille, France, [Brajkovic, Saska] Univ Lausanne, Ctr Hosp Univ Vaudois, Serv Internal Med, Lausanne, Switzerland, [Favre, Dimitri] Univ Lausanne, Ctr Hosp Univ Vaudois, Serv Internal Med, Lausanne, Switzerland, [Waeber, Gerard] Univ Lausanne, Ctr Hosp Univ Vaudois, Serv Internal Med, Lausanne, Switzerland, [Bonner, Caroline] Univ Lille, INSERM, CHU Lille, U1190 EGID, Lille, France, [Gmyr, Valery] Univ Lille, INSERM, CHU Lille, U1190 EGID, Lille, France, [Kerr-Conte, Julie] Univ Lille, INSERM, CHU Lille, U1190 EGID, Lille, France, [Pattou, Francois] Univ Lille, INSERM, CHU Lille, U1190 EGID, Lille, France, [Gauthier, Benoit R.] Andalusian Ctr Mol Biol & Regenerat Med, Dept Stem Cells, Seville, Spain, [Widmann, Christian] Univ Lausanne, Dept Physiol, Lausanne, Switzerland, [Bonnefond, Amelie] Imperial Coll London, Dept Genom Common Dis, London, England, [Froguel, Philippe] Imperial Coll London, Dept Genom Common Dis, London, England, [Abderrahmani, Amar] Imperial Coll London, Dept Genom Common Dis, London, England, 'European Genomic Institute for Diabetes' (E.G.I.D.), Regional Council Nord Pas de Calais, and European Regional Development Fund

Subjects

0301 basic medicine, Density-lipoproteins, Physiology, lcsh:Medicine, Gene Expression, Expression, Apoptosis, 030204 cardiovascular system & hematology, CHOP, medicine.disease_cause, Endoplasmic Reticulum, Biochemistry, Antioxidants, Unfolded protein response, chemistry.chemical_compound, Mice, 0302 clinical medicine, Endocrinology, Insulin Secretion, Medicine and Health Sciences, Insulin, Inositol, lcsh:Science, Multidisciplinary, Secretory Pathway, Cell Death, Endoplasmic Reticulum Stress, Lipids, Lipoproteins, LDL, Cholesterol, Cell Processes, Er stress, Cellular Structures and Organelles, Research Article, medicine.medical_specialty, Programmed cell death, General Science & Technology, Activation, Protein Serine-Threonine Kinases, Cell Line, 03 medical and health sciences, Islets of Langerhans, Internal medicine, MD Multidisciplinary, Endoribonucleases, medicine, Genetics, Animals, Humans, Diabetic Endocrinology, Diabetes-mellitus, Endocrine Physiology, Macrophages, Endoplasmic reticulum, lcsh:R, Biology and Life Sciences, Hydrogen Peroxide, Cell Biology, Hormones, Acetylcysteine, Activating Transcription Factor 6, Oxidative Stress, Metabolism, 030104 developmental biology, chemistry, lcsh:Q, Oxidative stress, Biomarkers

Abstract

Plaisance, Valérie et al., Elevated plasma concentration of the pro-Atherogenic oxidized low density lipoprotein cholesterol (LDL) triggers adverse effects in pancreatic beta-cells and is associated with type 2 diabetes. Here, we investigated whether the endoplasmic reticulum (ER) stress is a key player coupling oxidative stress to beta-cell dysfunction and death elicited by human oxidized LDL. We found that human oxidized LDL activates ER stress as evidenced by the activation of the inositol requiring 1α, and the elevated expression of both DDIT3 (also called CHOP) and DNAJC3 (also called P58IPK) ER stress markers in isolated human islets and the mouse insulin secreting MIN6 cells. Silencing of Chop and inhibition of ER stress markers by the chemical chaperone phenyl butyric acid (PBA) prevented cell death caused by oxidized LDL. Finally, we found that oxidative stress accounts for activation of ER stress markers induced by oxidized LDL. Induction of Chop/CHOP and p58IPK/P58IPK by oxidized LDL was mimicked by hydrogen peroxide and was blocked by co-Treatment with the N-Acetylcystein antioxidant. As a conclusion, the harmful effects of oxidized LDL in beta-cells requires ER stress activation in a manner that involves oxidative stress. This mechanism may account for impaired beta-cell function in diabetes and can be reversed by antioxidant treatment., This work was supported by the “European Genomic Institute for Diabetes” (E.G.I.D., ANR-10-LABX-46), European Commission, the Regional Council Nord Pas de Calais and the European Regional Development Fund.

Published

2016

10. Both PAX4 and MAFA Are Expressed in a Substantial Proportion of Normal Human Pancreatic Alpha Cells and Deregulated in Patients with Type 2 Diabetes

Author

Celio Pouponnot, Martine Cordier-Bussat, Rémy Bonnavion, Fouzia Assade, Philippe Bertolino, Julie Kerr-Conte, François Pattou, Rami Jaafar, Jieli Lu, Sofia Gargani, Chang Xian Zhang, Esther van Stralen, and Emmanuelle Leteurtre

Subjects

Adult, Male, endocrine system, medicine.medical_specialty, Maf Transcription Factors, Large, Adolescent, lcsh:Medicine, Gene Expression, Alpha (ethology), Biology, Glucagon, Alpha cell, Mice, Insulin-Secreting Cells, Internal medicine, medicine, Animals, Humans, Paired Box Transcription Factors, Obesity, lcsh:Science, Pancreas, Cells, Cultured, Aged, Cell Nucleus, Homeodomain Proteins, Regulation of gene expression, geography, Multidisciplinary, geography.geographical_feature_category, lcsh:R, Middle Aged, Islet, Endocrinology, medicine.anatomical_structure, Diabetes Mellitus, Type 2, Gene Expression Regulation, Glucagon-Secreting Cells, MAFB, Case-Control Studies, PAX4, lcsh:Q, Female, Research Article

Abstract

Pax4 and MafA (v-maf musculoaponeurotic fibrosarcoma oncogene homolog A) are two transcription factors crucial for normal functions of islet beta cells in the mouse. Intriguingly, recent studies indicate the existence of notable difference between human and rodent islet in terms of gene expression and functions. To better understand the biological role of human PAX4 and MAFA, we investigated their expression in normal and diseased human islets, using validated antibodies. PAX4 was detected in 43.0±5.0% and 39.1±4.0% of normal human alpha and beta cells respectively. We found that MAFA, detected in 88.3±6.3% insulin(+)cells as in the mouse, turned out to be also expressed in 61.2±6.4% of human glucagons(+) cells with less intensity than in insulin(+) cells, whereas MAFB expression was found not only in the majority of glucagon(+) cells (67.2±7.6%), but also in 53.6±10.5% of human insulin(+) cells. Interestingly, MAFA nuclear expression in both alpha and beta cells, and the percentage of alpha cells expressing PAX4 were found altered in a substantial proportion of patients with type 2 diabetes. Both MAFA and PAX4 display, therefore, a distinct expression pattern in human islet cells, suggesting more potential plasticity of human islets as compared with rodent islets.

Published

2013

11. Epithelial-Mesenchymal Transition in Cells Expanded In Vitro from Lineage-Traced Adult Human Pancreatic Beta Cells

Author

Philippe Ravassard, Julie Kerr-Conte, Shimon Efrat, François Pattou, and Holger A. Russ

Subjects

Adult, Mesoderm, Science, Cellular differentiation, Population, Fluorescent Antibody Technique, In Vitro Techniques, Biology, Osteocytes, Islets of Langerhans, Adipocytes, medicine, Humans, Cell Lineage, Epithelial–mesenchymal transition, education, Cell Biology/Gene Expression, Cell Proliferation, DNA Primers, education.field_of_study, Multidisciplinary, Base Sequence, Cell growth, Mesenchymal stem cell, Cell Differentiation, Epithelial Cells, Flow Cytometry, Developmental Biology/Stem Cells, Cell biology, Diabetes and Endocrinology, medicine.anatomical_structure, Immunology, Medicine, Stem cell, Research Article, Adult stem cell

Abstract

BackgroundIn-vitro expansion of functional beta cells from adult human islets is an attractive approach for generating an abundant source of cells for beta-cell replacement therapy of diabetes. Using genetic cell-lineage tracing we have recently shown that beta cells cultured from adult human islets undergo rapid dedifferentiation and proliferate for up to 16 population doublings. These cells have raised interest as potential candidates for redifferentiation into functional insulin-producing cells. Previous work has associated dedifferentiation of cultured epithelial cells with epithelial-mesenchymal transition (EMT), and suggested that EMT generates cells with stem cell properties. Here we investigated the occurrence of EMT in these cultures and assessed their stem cell potential.Methodology/principal findingsUsing cell-lineage tracing we provide direct evidence for occurrence of EMT in cells originating from beta cells in cultures of adult human islet cells. These cells express multiple mesenchymal markers, as well as markers associated with mesenchymal stem cells (MSC). However, we do not find evidence for the ability of such cells, nor of cells in these cultures derived from a non-beta-cell origin, to significantly differentiate into mesodermal cell types.Conclusions/significanceThese findings constitute the first demonstration based on genetic lineage-tracing of EMT in cultured adult primary human cells, and show that EMT does not induce multipotency in cells derived from human beta cells.

Published

2009