Your search keyword '"Bonner-Weir S"' showing total 572 results

201. Subpopulations of GFP-marked mouse pancreatic β-cells differ in size, granularity, and insulin secretion.

Author

Katsuta H, Aguayo-Mazzucato C, Katsuta R, Akashi T, Hollister-Lock J, Sharma AJ, Bonner-Weir S, and Weir GC

Subjects

Animals, Flow Cytometry, Insulin Secretion, Insulin-Secreting Cells metabolism, Mice, Mice, Transgenic, Promoter Regions, Genetic, Cell Size, Green Fluorescent Proteins genetics, Insulin metabolism, Insulin-Secreting Cells cytology

Abstract

There is growing information about the heterogeneity of pancreatic β-cells and how it relates to insulin secretion. This study used the approach of flow cytometry to sort and analyze β-cells from transgenic mice expressing green fluorescent protein (GFP) under the control of the mouse insulin I gene promoter. Three populations of β-cells with differing GFP brightness could be identified, which were classified as GFP-low, GFP-medium, and GFP-bright. The GFP-medium population comprised about 70% of the total. The GFP-low population had less insulin secretion as determined by the reverse hemolytic plaque assay and reduced insulin gene expression. Additionally, all three subpopulations of β-cells were found in mice of varying ages (embryonic d 15.5 and postnatal wk 1-9). The three populations from the youngest had larger cells (forward scatter) and less granularity (side scatter) than those from the adults. This approach opens up new ways to advance knowledge about β-cell heterogeneity.

Published

2012

202. New clues to bariatric surgery's benefits.

Author

Sarruf DA, Bonner-Weir S, and Schwartz MW

Subjects

Animals, Diabetes Mellitus, Type 1 surgery, Diabetes Mellitus, Type 2 surgery, Humans, Obesity surgery, Rats, Bariatric Surgery

Published

2012

203. Concise review: pancreas regeneration: recent advances and perspectives.

Author

Lysy PA, Weir GC, and Bonner-Weir S

Subjects

Acinar Cells cytology, Acinar Cells physiology, Acinar Cells transplantation, Animals, Cell Culture Techniques methods, Cell Proliferation, Cell Transplantation methods, Cell- and Tissue-Based Therapy methods, Diabetes Mellitus therapy, Embryonic Stem Cells physiology, Embryonic Stem Cells transplantation, Epithelial Cells cytology, Epithelial Cells physiology, Epithelial Cells transplantation, Humans, Immunomodulation, Induced Pluripotent Stem Cells cytology, Induced Pluripotent Stem Cells physiology, Induced Pluripotent Stem Cells transplantation, Insulin-Secreting Cells physiology, Insulin-Secreting Cells transplantation, Pancreas physiology, Cell Differentiation, Insulin-Secreting Cells cytology, Pancreas cytology, Regeneration

Abstract

The replacement of functional pancreatic β-cells is seen as an attractive potential therapy for diabetes, because diabetes results from an inadequate β-cell mass. Inducing replication of the remaining β-cells and new islet formation from progenitors within the pancreas (neogenesis) are the most direct ways to increase the β-cell mass. Stimulation of both replication and neogenesis have been reported in rodents, but their clinical significance must still be shown. Because human islet transplantation is limited by the scarcity of donors and graft failure within a few years, efforts have recently concentrated on the use of stem cells to replace the deficient β-cells. Currently, embryonic stem cells and induced pluripotent stem cells achieve high levels of β-cell differentiation, but their clinical use is still hampered by ethical issues and/or the risk of developing tumors after transplantation. Pancreatic epithelial cells (duct, acinar, or α-cells) represent an appealing alternative to stem cells because they demonstrate β-cell differentiation capacities. Yet translation of such capacity to human cells after significant in vitro expansion has yet to be achieved. Besides providing new β-cells, cell therapy also has to address the question on how to protect the transplanted cells from destruction by the immune system via either allo- or autoimmunity. Encouraging developments have been made in encapsulation and immunomodulation techniques, but many challenges still remain. Herein, we discuss recent advances in the search for β-cell replacement therapies, current strategies for circumventing the immune system, and mandatory steps for new techniques to be translated from bench to clinics.

Published

2012

204. Stem cell approaches for diabetes: towards beta cell replacement.

Author

Weir GC, Cavelti-Weder C, and Bonner-Weir S

Abstract

Stem cells hold great promise for pancreatic beta cell replacement therapy for diabetes. In type 1 diabetes, beta cells are mostly destroyed, and in type 2 diabetes beta cell numbers are reduced by 40% to 60%. The proof-of-principle that cellular transplants of pancreatic islets, which contain insulin-secreting beta cells, can reverse the hyperglycemia of type 1 diabetes has been established, and there is now a need to find an adequate source of islet cells. Human embryonic stem cells can be directed to become fully developed beta cells and there is expectation that induced pluripotent stem (iPS) cells can be similarly directed. iPS cells can also be generated from patients with diabetes to allow studies of the genomics and pathogenesis of the disease. Some alternative approaches for replacing beta cells include finding ways to enhance the replication of existing beta cells, stimulating neogenesis (the formation of new islets in postnatal life), and reprogramming of pancreatic exocrine cells to insulin-producing cells. Stem-cell-based approaches could also be used for modulation of the immune system in type 1 diabetes, or to address the problems of obesity and insulin resistance in type 2 diabetes. Herein, we review recent advances in our understanding of diabetes and beta cell biology at the genomic level, and we discuss how stem-cell-based approaches might be used for replacing beta cells and for treating diabetes.

Published

2011

205. Finally! A human pancreatic β cell line.

Author

Weir GC and Bonner-Weir S

Subjects

Animals, Humans, Insulin Secretion, Male, Cell Line, Glucose pharmacology, Insulin metabolism, Insulin-Secreting Cells cytology, Insulin-Secreting Cells drug effects, Insulin-Secreting Cells metabolism

Abstract

For decades, investigators have made numerous attempts to generate human pancreatic β cell lines that could be used to advance β cell biology, facilitate drug discovery, and provide a pathway to β cell replacement therapy for the treatment of diabetes. In this issue of the JCI, Ravassard and colleagues report that this has finally been achieved successfully with a multistep process that led to the generation of cells, which they termed EndoC-βH1 cells, that secreted insulin in response to glucose challenge.

Published

2011

206. Quantitative assessment of islets of Langerhans encapsulated in alginate.

Author

Johnson AS, O'Sullivan E, D'Aoust LN, Omer A, Bonner-Weir S, Fisher RJ, Weir GC, and Colton CK

Subjects

Animals, Biological Assay, Capsules, Cell Nucleus drug effects, Cell Nucleus metabolism, DNA metabolism, Diffusion drug effects, Edetic Acid pharmacology, Fluorocarbons pharmacology, Glucuronic Acid pharmacology, Hexuronic Acids pharmacology, Humans, Materials Testing, Octoxynol pharmacology, Oxygen Consumption drug effects, Rats, Rats, Sprague-Dawley, Static Electricity, Alginates pharmacology, Islets of Langerhans cytology, Islets of Langerhans drug effects, Tissue Engineering methods

Abstract

Improved methods have recently been developed for assessing islet viability and quantity in human islet preparations for transplantation, and these measurements have proven useful for predicting transplantation outcome. The objectives of this study were to adapt these methods for use with microencapsulated islets, to verify that they provide meaningful quantitative measurements, and to test them with two model systems: (1) barium alginate and (2) barium alginate containing a 70% (w/v) perfluorocarbon (PFC) emulsion, which presents challenges to use of these assays and is of interest in its own right as a means for reducing oxygen supply limitations to encapsulated tissue. Mitochondrial function was assessed by oxygen consumption rate measurements, and the analysis of data was modified to account for the increased solubility of oxygen in the PFC-alginate capsules. Capsules were dissolved and tissue recovered for nuclei counting to measure the number of cells. Capsule volume was determined from alginate or PFC content and used to normalize measurements. After low oxygen culture for 2 days, islets in normal alginate lost substantial viable tissue and displayed necrotic cores, whereas most of the original oxygen consumption rate was recovered with PFC alginate, and little necrosis was observed. All nuclei were recovered with normal alginate, but some nuclei from nonrespiring cells were lost with PFC alginate. Biocompatibility tests revealed toxicity at the islet periphery associated with the lipid emulsion used to provide surfactants during the emulsification process. We conclude that these new assay methods can be applied to islets encapsulated in materials as complex as PFC-alginate. Measurements made with these materials revealed that enhancement of oxygen permeability of the encapsulating material with a concentrated PFC emulsion improves survival of encapsulated islets under hypoxic conditions, but reformulation of the PFC emulsion is needed to reduce toxicity.

Published

2011

207. Rat neonatal beta cells lack the specialised metabolic phenotype of mature beta cells.

Author

Jermendy A, Toschi E, Aye T, Koh A, Aguayo-Mazzucato C, Sharma A, Weir GC, Sgroi D, and Bonner-Weir S

Subjects

Animals, Animals, Newborn, Aspartate Aminotransferases genetics, Expressed Sequence Tags, Female, Glycerolphosphate Dehydrogenase genetics, In Vitro Techniques, Islets of Langerhans cytology, Islets of Langerhans metabolism, Malate Dehydrogenase genetics, Male, Microdissection, Oligonucleotide Array Sequence Analysis, Rats, Rats, Sprague-Dawley, Reverse Transcriptase Polymerase Chain Reaction, Insulin-Secreting Cells metabolism

Abstract

Aims/hypothesis: Fetal and neonatal beta cells have poor glucose-induced insulin secretion and only gain robust glucose responsiveness several weeks after birth. We hypothesise that this unresponsiveness is due to a generalised immaturity of the metabolic pathways normally found in beta cells rather than to a specific defect., Methods: Using laser-capture microdissection we excised beta cell-enriched cores of pancreatic islets from day 1 (P1) neonatal and young adult Sprague-Dawley rats in order to compare their gene-expression profiles using Affymetrix U34A microarrays (neonatal, n = 4; adult, n = 3)., Results: Using dChip software for analysis, 217 probe sets for genes/38 expressed sequence tags (ESTs) were significantly higher and 345 probe sets for genes/33 ESTs significantly lower in beta cell-enriched cores of neonatal islets compared with those of adult islets. Among the genes lower in the neonatal beta cells were key metabolic genes including mitochondrial shuttles (malate dehydrogenase, glycerol-3-phosphate dehydrogenase and glutamate oxalacetate transaminase), pyruvate carboxylase and carnitine palmitoyl transferase 2. Differential expression of these enzyme genes was confirmed by quantitative PCR on RNA from isolated neonatal (P2 until P28) and adult islets and with immunostaining of pancreas. Even by 28 days of age some of these genes were still expressed at lower levels than in adults., Conclusions/interpretation: The lack of glucose responsiveness in neonatal islets is likely to be due to a generalised immaturity of the metabolic specialisation of pancreatic beta cells.

Published

2011

208. Mafa expression enhances glucose-responsive insulin secretion in neonatal rat beta cells.

Author

Aguayo-Mazzucato C, Koh A, El Khattabi I, Li WC, Toschi E, Jermendy A, Juhl K, Mao K, Weir GC, Sharma A, and Bonner-Weir S

Subjects

Animals, Blotting, Western, Female, Humans, In Vitro Techniques, Insulin metabolism, Maf Transcription Factors, Large genetics, Rats, Rats, Sprague-Dawley, Reverse Transcriptase Polymerase Chain Reaction, Insulin-Secreting Cells metabolism, Maf Transcription Factors, Large metabolism

Abstract

Aim/hypothesis: Neonatal beta cells lack glucose-stimulated insulin secretion and are thus functionally immature. We hypothesised that this lack of glucose responsiveness results from a generalised low expression of genes characteristic of mature functional beta cells. Important glucose-responsive transcription factors, Mafa and Pdx1, regulate genes involved in insulin synthesis and secretion, and have been implicated in late beta cell development. The aim of this study was to assess whether Mafa and/or Pdx1 regulates the postnatal functional maturation of beta cells., Methods: By quantitative PCR we evaluated expression of these and other beta cell genes over the first month compared with adult. After infection with adenovirus expressing MAFA, Pdx1 or green fluorescent protein (Gfp), P2 rat islets were evaluated by RT-PCR and insulin secretion with static incubation and reverse haemolytic plaque assay (RHPA)., Results: At P2 most beta cell genes were expressed at about 10% of adult, but by P7 Pdx1 and Neurod1 no longer differ from adult; by contrast, Mafa expression remained significantly lower than adult through P21. Overexpression of Pdx1 increased Mafa, Neurod1, glucokinase (Gck) mRNA and insulin content but failed to enhance glucose responsiveness. Similar overexpression of MAFA resulted in increased Neurod1, Nkx6-1, Gck and Glp1r mRNAs and no change in insulin content but, importantly, acquisition of glucose-responsive insulin secretion. Both the percentage of secreting beta cells and the amount of insulin secreted per beta cell increased, approaching that of adult beta cells., Conclusions/interpretation: In the process of functional maturation acquiring glucose-responsive insulin secretion, neonatal beta cells undergo a coordinated gene expression programme in which Mafa plays a crucial role.

Published

2011

209. Tissue-specific disallowance of housekeeping genes: the other face of cell differentiation.

Author

Thorrez L, Laudadio I, Van Deun K, Quintens R, Hendrickx N, Granvik M, Lemaire K, Schraenen A, Van Lommel L, Lehnert S, Aguayo-Mazzucato C, Cheng-Xue R, Gilon P, Van Mechelen I, Bonner-Weir S, Lemaigre F, and Schuit F

Subjects

Animals, Epigenomics, Female, Islets of Langerhans cytology, Islets of Langerhans metabolism, Lactate Dehydrogenases genetics, Lactate Dehydrogenases metabolism, Liver cytology, Male, Mice, Mice, Inbred C57BL, MicroRNAs genetics, MicroRNAs metabolism, Monocarboxylic Acid Transporters genetics, Monocarboxylic Acid Transporters metabolism, Oligonucleotide Array Sequence Analysis, Organ Specificity, Pancreas cytology, RNA, Messenger genetics, RNA, Messenger metabolism, Rats, Symporters genetics, Symporters metabolism, Cell Differentiation, Gene Expression Regulation, Developmental, Liver metabolism, Pancreas metabolism

Abstract

We report on a hitherto poorly characterized class of genes that are expressed in all tissues, except in one. Often, these genes have been classified as housekeeping genes, based on their nearly ubiquitous expression. However, the specific repression in one tissue defines a special class of "disallowed genes." In this paper, we used the intersection-union test to screen for such genes in a multi-tissue panel of genome-wide mRNA expression data. We propose that disallowed genes need to be repressed in the specific target tissue to ensure correct tissue function. We provide mechanistic data of repression with two metabolic examples, exercise-induced inappropriate insulin release and interference with ketogenesis in liver. Developmentally, this repression is established during tissue maturation in the early postnatal period involving epigenetic changes in histone methylation. In addition, tissue-specific expression of microRNAs can further diminish these repressed mRNAs. Together, we provide a systematic analysis of tissue-specific repression of housekeeping genes, a phenomenon that has not been studied so far on a genome-wide basis and, when perturbed, can lead to human disease.

Published

2011

210. Mice with a targeted deletion of the type 2 deiodinase are insulin resistant and susceptible to diet induced obesity.

Author

Marsili A, Aguayo-Mazzucato C, Chen T, Kumar A, Chung M, Lunsford EP, Harney JW, Van-Tran T, Gianetti E, Ramadan W, Chou C, Bonner-Weir S, Larsen PR, Silva JE, and Zavacki AM

Subjects

Adipose Tissue metabolism, Animals, Gene Expression Profiling, Glucose Tolerance Test, Iodide Peroxidase genetics, Liver metabolism, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Muscles metabolism, Obesity genetics, Reverse Transcriptase Polymerase Chain Reaction, Iodothyronine Deiodinase Type II, Diet, Insulin Resistance, Iodide Peroxidase metabolism, Obesity etiology

Abstract

Background: The type 2 iodothyronine deiodinase (D2) converts the pro-hormone thyroxine into T3 within target tissues. D2 is essential for a full thermogenic response of brown adipose tissue (BAT), and mice with a disrupted Dio2 gene (D2KO) have an impaired response to cold. BAT is also activated by overfeeding., Methodology/principal Findings: After 6-weeks of HFD feeding D2KO mice gained 5.6% more body weight and had 28% more adipose tissue. Oxygen consumption (V0(2)) was not different between genotypes, but D2KO mice had an increased respiratory exchange ratio (RER), suggesting preferential use of carbohydrates. Consistent with this, serum free fatty acids and β-hydroxybutyrate were lower in D2KO mice on a HFD, while hepatic triglycerides were increased and glycogen content decreased. Neither genotype showed glucose intolerance, but D2KO mice had significantly higher insulin levels during GTT independent of diet. Accordingly, during ITT testing D2KO mice had a significantly reduced glucose uptake, consistent with insulin resistance. Gene expression levels in liver, muscle, and brown and white adipose tissue showed no differences that could account for the increased weight gain in D2KO mice. However, D2KO mice have higher PEPCK mRNA in liver suggesting increased gluconeogenesis, which could also contribute to their apparent insulin resistance., Conclusions/significance: We conclude that the loss of the Dio2 gene has significant metabolic consequences. D2KO mice gain more weight on a HFD, suggesting a role for D2 in protection from diet-induced obesity. Further, D2KO mice appear to have a greater reliance on carbohydrates as a fuel source, and limited ability to mobilize and to burn fat. This results in increased fat storage in adipose tissue, hepatic steatosis, and depletion of liver glycogen in spite of increased gluconeogenesis. D2KO mice are also less responsive to insulin, independent of diet-induced obesity.

Published

2011

211. Residual insulin production and pancreatic ß-cell turnover after 50 years of diabetes: Joslin Medalist Study.

Author

Keenan HA, Sun JK, Levine J, Doria A, Aiello LP, Eisenbarth G, Bonner-Weir S, and King GL

Subjects

Aged, C-Peptide blood, Cohort Studies, Diabetes Mellitus, Type 1 drug therapy, Diabetes Mellitus, Type 1 genetics, Female, HLA-DQ Antigens genetics, HLA-DQ beta-Chains, HLA-DR Antigens genetics, HLA-DRB1 Chains, Humans, Insulin analysis, Insulin therapeutic use, Insulin-Secreting Cells metabolism, Insulin-Secreting Cells pathology, Male, Middle Aged, Numismatics, Phenotype, Time Factors, Tissue and Organ Procurement, Awards and Prizes, Diabetes Mellitus, Type 1 physiopathology, Insulin biosynthesis, Insulin-Secreting Cells physiology

Abstract

Objective: To evaluate the extent of pancreatic β-cell function in a large number of insulin-dependent diabetic patients with a disease duration of 50 years or longer (Medalists)., Research Design and Methods: Characterization of clinical and biochemical parameters and β-cell function of 411 Medalists with correlation with postmortem morphologic findings of 9 Medalists., Results: The Medalist cohort, with a mean ± SD disease duration and age of 56.2 ± 5.8 and 67.2 ± 7.5 years, respectively, has a clinical phenotype similar to type 1 diabetes (type 1 diabetes): mean ± SD onset at 11.0 ± 6.4 years, BMI at 26.0 ± 5.1 kg/m(2), insulin dose of 0.46 ± 0.2 u/kg, ∼94% positive for DR3 and/or DR4, and 29.5% positive for either IA2 or glutamic acid decarboxylase (GAD) autoantibodies. Random serum C-peptide levels showed that more than 67.4% of the participants had levels in the minimal (0.03-0.2 nmol/l) or sustained range (≥ 0.2 nmol/l). Parameters associated with higher random C-peptide were lower hemoglobin A1C, older age of onset, higher frequency of HLA DR3 genotype, and responsiveness to a mixed-meal tolerance test (MMTT). Over half of the Medalists with fasting C-peptide > 0.17 nmol/l responded in MMTT by a twofold or greater rise over the course of the test compared to fasting. Postmortem examination of pancreases from nine Medalists showed that all had insulin+ β-cells with some positive for TUNEL staining, indicating apoptosis., Conclusions: Demonstration of persistence and function of insulin-producing pancreatic cells suggests the possibility of a steady state of turnover in which stimuli to enhance endogenous β cells could be a viable therapeutic approach in a significant number of patients with type 1 diabetes, even for those with chronic duration.

Published

2010

212. Quantitative analysis of cell composition and purity of human pancreatic islet preparations.

Author

Pisania A, Weir GC, O'Neil JJ, Omer A, Tchipashvili V, Lei J, Colton CK, and Bonner-Weir S

Subjects

Adult, Aged, Cell Count, Cell Size, Dithizone, Humans, Islets of Langerhans ultrastructure, Microscopy, Microscopy, Electron, Middle Aged, Islets of Langerhans cytology

Abstract

Despite improvements in outcomes for human islet transplantation, characterization of islet preparations remains poorly defined. This study used both light microscopy (LM) and electron microscopy (EM) to characterize 33 islet preparations used for clinical transplants. EM allowed an accurate identification and quantification of cell types with measured cell number fractions (mean±s.e.m.) of 35.6±2.1% β-cells, 12.6±1.0% non-β-islet cells (48.3±2.6% total islet cells), 22.7±1.5% duct cells, and 25.3±1.8% acinar cells. Of the islet cells, 73.6±1.7% were β-cells. For comparison with the literature, estimates of cell number fraction, cell volume, and extracellular volume were combined to convert number fraction data to volume fractions applicable to cells, islets, and the entire preparation. The mathematical framework for this conversion was developed. By volume, β-cells were 86.5±1.1% of the total islet cell volume and 61.2±0.8% of intact islets (including the extracellular volume), which is similar to that of islets in the pancreas. Our estimates produced 1560±20 cells in an islet equivalent (volume of 150-μm diameter sphere), of which 1140±15 were β-cells. To test whether LM analysis of the same tissue samples could provide reasonable estimates of purity of the islet preparations, volume fraction of the islet tissue was measured on thin sections available from 27 of the clinical preparations by point counting morphometrics. Islet purity (islet volume fraction) of individual preparations determined by LM and EM analyses correlated linearly with excellent agreement (R²=0.95). However, islet purity by conventional dithizone staining was substantially higher with a 20-30% overestimation. Thus, both EM and LM provide accurate methods to determine the cell composition of human islet preparations and can help us understand many of the discrepancies of islet composition in the literature.

Published

2010

213. Enumeration of islets by nuclei counting and light microscopic analysis.

Author

Pisania A, Papas KK, Powers DE, Rappel MJ, Omer A, Bonner-Weir S, Weir GC, and Colton CK

Subjects

Animals, Cell Count, Cell Line, Tumor, DNA analysis, Humans, Islets of Langerhans ultrastructure, Mice, Microscopy, Rats, Cell Nucleus ultrastructure, Islets of Langerhans cytology

Abstract

Islet enumeration in impure preparations by conventional dithizone staining and visual counting is inaccurate and operator dependent. We examined nuclei counting for measuring the total number of cells in islet preparations, and we combined it with morphological analysis by light microscopy (LM) for estimating the volume fraction of islets in impure preparations. Cells and islets were disrupted with lysis solution and shear, and accuracy of counting successively diluted nuclei suspensions was verified with (1) visual counting in a hemocytometer after staining with crystal violet, and automatic counting by (2) aperture electrical resistance measurement and (3) flow cytometer measurement after staining with 7-aminoactinomycin-D. DNA content averaged 6.5 and 6.9 pg of DNA per cell for rat and human islets, respectively, in agreement with literature estimates. With pure rat islet preparations, precision improved with increasing counts, and samples with about ≥160 islets provided a coefficient of variation of about 6%. Aliquots of human islet preparations were processed for LM analysis by stereological point counting. Total nuclei counts and islet volume fraction from LM analysis were combined to obtain the number of islet equivalents (IEs). Total number of IE by the standard method of dithizone staining/manual counting was overestimated by about 90% compared with LM/nuclei counting for 12 freshly isolated human islet research preparations. Nuclei counting combined with islet volume fraction measurements from LM is a novel method for achieving accurate islet enumeration.

Published

2010

214. Beta-cell growth and regeneration: replication is only part of the story.

Author

Bonner-Weir S, Li WC, Ouziel-Yahalom L, Guo L, Weir GC, and Sharma A

Subjects

Adult, Animals, Cell Division, Cell Proliferation, Humans, Insulin-Secreting Cells physiology, Mice, Pancreas cytology, Pancreas physiology, Rats, Regeneration, Swine, Insulin-Secreting Cells cytology

Published

2010

215. Activation of pancreatic-duct-derived progenitor cells during pancreas regeneration in adult rats.

Author

Li WC, Rukstalis JM, Nishimura W, Tchipashvili V, Habener JF, Sharma A, and Bonner-Weir S

Subjects

Animals, Basic Helix-Loop-Helix Transcription Factors metabolism, Cell Differentiation physiology, Cell Growth Processes physiology, Embryonic Stem Cells cytology, Embryonic Stem Cells metabolism, Hepatocyte Nuclear Factor 6 deficiency, Hepatocyte Nuclear Factor 6 metabolism, Islets of Langerhans cytology, Islets of Langerhans metabolism, Male, Nerve Tissue Proteins metabolism, Pancreas cytology, Pancreas metabolism, Pancreatectomy, Pancreatic Ducts cytology, Pancreatic Ducts metabolism, Rats, Rats, Sprague-Dawley, Transcription Factors deficiency, Transcription Factors metabolism, Embryonic Stem Cells physiology, Islets of Langerhans physiology, Pancreas physiology, Pancreatic Ducts physiology, Regeneration physiology

Abstract

The adult pancreas has considerable capacity to regenerate in response to injury. We hypothesized that after partial pancreatectomy (Px) in adult rats, pancreatic-duct cells serve as a source of regeneration by undergoing a reproducible dedifferentiation and redifferentiation. We support this hypothesis by the detection of an early loss of the ductal differentiation marker Hnf6 in the mature ducts, followed by the transient appearance of areas composed of proliferating ductules, called foci of regeneration, which subsequently form new pancreatic lobes. In young foci, ductules express markers of the embryonic pancreatic epithelium - Pdx1, Tcf2 and Sox9 - suggesting that these cells act as progenitors of the regenerating pancreas. The endocrine-lineage-specific transcription factor Neurogenin3, which is found in the developing embryonic pancreas, was transiently detected in the foci. Islets in foci initially resemble embryonic islets in their lack of MafA expression and lower percentage of beta-cells, but with increasing maturation have increasing numbers of MafA(+) insulin(+) cells. Taken together, we provide a mechanism by which adult pancreatic duct cells recapitulate aspects of embryonic pancreas differentiation in response to injury, and contribute to regeneration of the pancreas. This mechanism of regeneration relies mainly on the plasticity of the differentiated cells within the pancreas.

Published

2010

216. Gene expression profiles of Beta-cell enriched tissue obtained by laser capture microdissection from subjects with type 2 diabetes.

Author

Marselli L, Thorne J, Dahiya S, Sgroi DC, Sharma A, Bonner-Weir S, Marchetti P, and Weir GC

Subjects

Aged, Apoptosis genetics, Cell Cycle genetics, Diabetes Mellitus, Type 2 pathology, Endoplasmic Reticulum pathology, Female, Gene Expression Profiling, Humans, In Vitro Techniques, Male, Matrix Metalloproteinase 7 genetics, Microdissection, Middle Aged, Oligonucleotide Array Sequence Analysis, Diabetes Mellitus, Type 2 metabolism, Insulin-Secreting Cells metabolism, Lasers

Abstract

Background: Changes in gene expression in pancreatic beta-cells from type 2 diabetes (T2D) should provide insights into their abnormal insulin secretion and turnover., Methodology/principal Findings: Frozen sections were obtained from cadaver pancreases of 10 control and 10 T2D human subjects. Beta-cell enriched samples were obtained by laser capture microdissection (LCM). RNA was extracted, amplified and subjected to microarray analysis. Further analysis was performed with DNA-Chip Analyzer (dChip) and Gene Set Enrichment Analysis (GSEA) software. There were changes in expression of genes linked to glucotoxicity. Evidence of oxidative stress was provided by upregulation of several metallothionein genes. There were few changes in the major genes associated with cell cycle, apoptosis or endoplasmic reticulum stress. There was differential expression of genes associated with pancreatic regeneration, most notably upregulation of members of the regenerating islet gene (REG) family and metalloproteinase 7 (MMP7). Some of the genes found in GWAS studies to be related to T2D were also found to be differentially expressed. IGF2BP2, TSPAN8, and HNF1B (TCF2) were upregulated while JAZF1 and SLC30A8 were downregulated., Conclusions/significance: This study made possible by LCM has identified many novel changes in gene expression that enhance understanding of the pathogenesis of T2D.

Published

2010

217. Dreams for type 1 diabetes: shutting off autoimmunity and stimulating beta-cell regeneration.

Author

Weir GC and Bonner-Weir S

Subjects

Animals, Diabetes Mellitus, Type 1 blood, Dipeptidyl-Peptidase IV Inhibitors pharmacology, Female, Insulin-Secreting Cells immunology, Mice, Mice, Inbred NOD, Nitriles pharmacology, Pyrrolidines pharmacology, T-Lymphocytes, Regulatory drug effects, T-Lymphocytes, Regulatory immunology, Diabetes Mellitus, Type 1 drug therapy, Diabetes Mellitus, Type 1 immunology, Dipeptidyl-Peptidase IV Inhibitors therapeutic use, Insulin-Secreting Cells cytology, Insulin-Secreting Cells drug effects, Nitriles therapeutic use, Pyrrolidines therapeutic use

Published

2010

218. Protective unfolded protein response in human pancreatic beta cells transplanted into mice.

Author

Kennedy J, Katsuta H, Jung MH, Marselli L, Goldfine AB, Balis UJ, Sgroi D, Bonner-Weir S, and Weir GC

Subjects

Animals, Apoptosis, Blood Glucose metabolism, Endoplasmic Reticulum metabolism, Humans, Islets of Langerhans cytology, Mice, Mice, SCID, Islets of Langerhans metabolism, Islets of Langerhans Transplantation, Mice, Inbred ICR, Protein Denaturation

Abstract

Background: There is great interest about the possible contribution of ER stress to the apoptosis of pancreatic beta cells in the diabetic state and with islet transplantation., Methods and Findings: Expression of genes involved in ER stress were examined in beta cell enriched tissue obtained with laser capture microdissection (LCM) from frozen sections of pancreases obtained from non-diabetic subjects at surgery and from human islets transplanted into ICR-SCID mice for 4 wk. Because mice have higher glucose levels than humans, the transplanted beta cells were exposed to mild hyperglycemia and the abnormal environment of the transplant site. RNA was extracted from the LCM specimens, amplified and then subjected to microarray analysis. The transplanted beta cells showed an unfolded protein response (UPR). There was activation of many genes of the IRE-1 pathway that provide protection against the deleterious effects of ER stress, increased expression of ER chaperones and ERAD (ER-associated protein degradation) proteins. The other two arms of ER stress, PERK and ATF-6, had many down regulated genes. Downregulation of EIF2A could protect by inhibiting protein synthesis. Two genes known to contribute to apoptosis, CHOP and JNK, were downregulated., Conclusions: Human beta cells in a transplant site had UPR changes in gene expression that protect against the proapoptotic effects of unfolded proteins.

Published

2010

219. Rat islet cell aggregates are superior to islets for transplantation in microcapsules.

Author

O'Sullivan ES, Johnson AS, Omer A, Hollister-Lock J, Bonner-Weir S, Colton CK, and Weir GC

Subjects

Analysis of Variance, Animals, Capsules metabolism, Cell Count, Cell Culture Techniques, Cells, Cultured, Islets of Langerhans metabolism, Male, Mice, Mice, Inbred BALB C, Necrosis metabolism, Rats, Rats, Sprague-Dawley, Transplantation, Heterologous, Cell Aggregation, Diabetes Mellitus, Experimental surgery, Islets of Langerhans cytology, Islets of Langerhans Transplantation methods

Abstract

Aims/hypothesis: Islet transplantation is a promising treatment for type 1 diabetes but is hampered by a shortage of donor human tissue and early failure. Research on islet cell transplantation includes finding new sources of cells and immunoisolation to protect from immune assault and tumourigenic potential. Small islet cell aggregates were studied to determine if their survival and function were superior to intact islets within microcapsules because of reduced oxygen transport limitation and inflammatory mediators., Methods: Islet cell aggregates were generated by dispersing rat islets into single cells and allowing them to re-aggregate in culture. Rat islets and islet cell aggregates were encapsulated in barium alginate capsules and studied when cultured in low (0.5% or 2%) or normal (20%) oxygen, or transplanted into mice., Results: Encapsulated islet cell aggregates were able to survive and function better than intact islets in terms of oxygen-consumption rate, nuclei counts, insulin-to-DNA ratio and glucose-stimulated insulin secretion. They also had reduced expression of pro-inflammatory genes. Islet cell aggregates showed reduced tissue necrosis in an immunodeficient transplant model and a much greater proportion of diabetic xenogeneic transplant recipients receiving islet cell aggregates (tissue volume of only 85 islet equivalents) had reversal of hyperglycaemia than recipients receiving intact islets., Conclusions/interpretation: These aggregates were superior to intact islets in terms of survival and function in low-oxygen culture and during transplantation and are likely to provide more efficient utilisation of islet tissue, a finding of importance for the future of cell therapy for diabetes.

Published

2010

220. Accurate control of oxygen level in cells during culture on silicone rubber membranes with application to stem cell differentiation.

Author

Powers DE, Millman JR, Bonner-Weir S, Rappel MJ, and Colton CK

Subjects

Animals, Cell Adhesion, Cell Count, Collagen metabolism, Drug Combinations, Fibronectins metabolism, Finite Element Analysis, Kinetics, Laminin metabolism, Linear Models, Mice, Models, Biological, Myocytes, Cardiac cytology, Partial Pressure, Polystyrenes, Proteoglycans metabolism, Cell Culture Techniques methods, Cell Differentiation physiology, Embryonic Stem Cells cytology, Oxygen metabolism, Silicon chemistry

Abstract

Oxygen level in mammalian cell culture is often controlled by placing culture vessels in humidified incubators with a defined gas phase partial pressure of oxygen (pO(2gas)). Because the cells are consuming oxygen supplied by diffusion, a difference between pO(2gas) and that experienced by the cells (pO(2cell)) arises, which is maximal when cells are cultured in vessels with little or no oxygen permeability. Here, we demonstrate theoretically that highly oxygen-permeable silicone rubber membranes can be used to control pO(2cell) during culture of cells in monolayers and aggregates much more accurately and can achieve more rapid transient response following a disturbance than on polystyrene and fluorinated ethylene-propylene copolymer membranes. Cell attachment on silicone rubber was achieved by physical adsorption of fibronectin or Matrigel. We use these membranes for the differentiation of mouse embryonic stem cells to cardiomyocytes and compare the results with culture on polystyrene or on silicone rubber on top of polystyrene. The fraction of cells that are cardiomyocyte-like increases with decreasing pO(2) only when using oxygen-permeable silicone membrane-based dishs, which contract on silicone rubber but not polystyrene. The high permeability of silicone rubber results in pO(2cell) being equal to pO(2gas) at the tissue-membrane interface. This, together with geometric information from histological sections, facilitates development of a model from which the pO(2) distribution within the resulting aggregates is computed. Silicone rubber membranes have significant advantages over polystyrene in controlling pO(2cell), and these results suggest they are a valuable tool for investigating pO(2) effects in many applications, such as stem cell differentiation., (Copyright 2009 American Institute of Chemical Engineers)

Published

2010

221. Dimorphic histopathology of long-standing childhood-onset diabetes.

Author

Gianani R, Campbell-Thompson M, Sarkar SA, Wasserfall C, Pugliese A, Solis JM, Kent SC, Hering BJ, West E, Steck A, Bonner-Weir S, Atkinson MA, Coppieters K, von Herrath M, and Eisenbarth GS

Subjects

Adolescent, Adult, Age of Onset, Autoantibodies blood, C-Peptide blood, Child, Child, Preschool, Diabetes Mellitus, Type 1 immunology, Female, HLA-DR Antigens, Histocompatibility Testing, Humans, Hyperinsulinism pathology, Male, Middle Aged, Tissue Donors, Diabetes Mellitus, Type 1 pathology, Insulin-Secreting Cells pathology, Pancreas pathology, Sex Characteristics

Abstract

Aims/hypothesis: Childhood diabetes is thought to usually result from autoimmune beta cell destruction (type 1A) with eventual total loss of beta cells. Analysis of C-peptide in children characterised at diabetes onset for autoantibodies shows heterogeneous preservation of insulin secretion in long-standing diabetes. The aim of this study was to characterise the pancreases of childhood-onset diabetes in order to define the pathological basis of this heterogeneity., Methods: We evaluated 20 cadaveric organ donor pancreases of childhood-onset long-term patients for disease heterogeneity and obtained corresponding C-peptide measurements., Results: Pancreases from the majority of cadaveric donors contained only insulin-deficient islets (14 of 20). The remaining six patients (30%) had numerous insulin-positive cells within at least some islets, with two different histological patterns. Pattern A (which we would associate with type 1A diabetes) had lobular retention of areas with 'abnormal' beta cells producing the apoptosis inhibitor survivin and HLA class I. In pattern B, 100% of all islets contained normal-appearing but quantitatively reduced beta cells without survivin or HLA class I., Conclusions/interpretation: Our data demonstrate that C-peptide secretion in long-standing diabetic patients can be explained by two different patterns of beta cell survival,possibly reflecting different subsets of type 1 diabetes.

Published

2010

222. Identification of markers for newly formed beta-cells in the perinatal period: a time of recognized beta-cell immaturity.

Author

Aye T, Toschi E, Sharma A, Sgroi D, and Bonner-Weir S

Subjects

Animals, Animals, Newborn, Biomarkers metabolism, Insulin-Secreting Cells metabolism, Keratin-19 genetics, Matrix Metalloproteinase 2 genetics, Pancreas cytology, Pancreas embryology, Pancreas growth & development, Pulmonary Surfactant-Associated Protein D genetics, RNA, Messenger biosynthesis, Rats, Rats, Sprague-Dawley, Time Factors, Insulin-Secreting Cells cytology, Keratin-19 biosynthesis, Matrix Metalloproteinase 2 biosynthesis, Pulmonary Surfactant-Associated Protein D biosynthesis

Abstract

Markers of beta-cell maturity would be useful in staging the differentiation of stem/progenitor cells to beta-cells whether in vivo or in vitro. We previously identified markers for newly formed beta-cells in regenerating rat pancreases after 90% partial pancreatectomy. To test the generality of these markers of newly formed beta-cells, we examined their expression during the perinatal period, a time of recognized beta-cell immaturity. We show by semiquantitative RT-PCR and immunostaining over the time course from embryonic day 18/20 to birth, 1 day, 2 days, 3 days, 7 days, and adult that MMP-2, CK-19, and SPD are truly markers of new and immature beta-cells and that their expression transiently peaks in the perinatal period and is not entirely synchronous. The shared expression of these markers among fetal, newborn, and newly regenerated beta-cells, but not adult, strongly supports their use as potential markers for new beta-cells in the assessment of both the maturity of stem cell-derived insulin-producing cells and the presence of newly formed islets (neogenesis) in the adult pancreas.

Published

2010

223. Stem cell therapy for type 1 diabetes mellitus.

Author

Aguayo-Mazzucato C and Bonner-Weir S

Subjects

Cell Differentiation physiology, Humans, Insulin-Secreting Cells cytology, Models, Biological, Signal Transduction, Stem Cells cytology, Diabetes Mellitus, Type 1 therapy, Stem Cell Transplantation methods

Abstract

The use of stem cells in regenerative medicine holds great promise for the cure of many diseases, including type 1 diabetes mellitus (T1DM). Any potential stem-cell-based cure for T1DM should address the need for beta-cell replacement, as well as control of the autoimmune response to cells which express insulin. The ex vivo generation of beta cells suitable for transplantation to reconstitute a functional beta-cell mass has used pluripotent cells from diverse sources, as well as organ-specific facultative progenitor cells from the liver and the pancreas. The most effective protocols to date have produced cells that express insulin and have molecular characteristics that closely resemble bona fide insulin-secreting cells; however, these cells are often unresponsive to glucose, a characteristic that should be addressed in future protocols. The use of mesenchymal stromal cells or umbilical cord blood to modulate the immune response is already in clinical trials; however, definitive results are still pending. This Review focuses on current strategies to obtain cells which express insulin from different progenitor sources and highlights the main pathways and genes involved, as well as the different approaches for the modulation of the immune response in patients with T1DM.

Published

2010

224. Regenerating pancreatic beta-cells: plasticity of adult pancreatic cells and the feasibility of in-vivo neogenesis.

Author

Juhl K, Bonner-Weir S, and Sharma A

Subjects

Adult, Animals, Diabetes Mellitus genetics, Diabetes Mellitus metabolism, Diabetes Mellitus pathology, Embryonic Stem Cells transplantation, Genetic Therapy, Humans, Insulin-Secreting Cells metabolism, Insulin-Secreting Cells transplantation, Pancreas, Exocrine metabolism, Transcription Factors metabolism, Cell Lineage, Cell Proliferation, Cell Transdifferentiation, Diabetes Mellitus therapy, Insulin-Secreting Cells pathology, Pancreas, Exocrine pathology, Regeneration, Tissue Engineering

Abstract

Purpose of Review: Diabetes results from inadequate functional mass of pancreatic beta-cells and therefore replenishing with new glucose-responsive beta-cells is an important therapeutic option. In addition to replication of pre-existing beta-cells, new beta-cells can be produced from differentiated adult cells using in-vitro or in-vivo approaches. This review will summarize recent advances in in-vivo generation of beta-cells from cells that are not beta-cells (neogenesis) and discuss ways to overcome the limitations of this process., Recent Findings: Multiple groups have shown that adult pancreatic ducts, acinar and even endocrine cells exhibit cellular plasticity and can differentiate into beta-cells in vivo. Several different approaches, including misexpression of transcription factors and tissue injury, have induced neogenesis of insulin-expressing cells in vivo and ameliorated diabetes., Summary: Recent breakthroughs demonstrating cellular plasticity of adult pancreatic cells to form new beta-cells are a positive first step towards developing in-vivo regeneration-based therapy for diabetes. Currently, neogenesis processes are inefficient and do not generate sufficient amounts of beta-cells required to normalize hyperglycemia. However, an improved understanding of mechanisms regulating neogenesis of beta-cells from adult pancreatic cells and of their maturation into functional glucose-responsive beta-cells can make therapies based on in-vivo regeneration a reality.

Published

2010

225. Ductal origin hypothesis of pancreatic regeneration under attack.

Author

Kushner JA, Weir GC, and Bonner-Weir S

Subjects

Animals, Cell Lineage, Mice, Stem Cells physiology, Insulin-Secreting Cells physiology, Pancreatic Ducts physiology, Regeneration

Published

2010

226. Single pancreatic beta cells co-express multiple islet hormone genes in mice.

Author

Katsuta H, Akashi T, Katsuta R, Nagaya M, Kim D, Arinobu Y, Hara M, Bonner-Weir S, Sharma AJ, Akashi K, and Weir GC

Subjects

Aging physiology, Animals, Animals, Newborn, B-Lymphocytes cytology, B-Lymphocytes physiology, Cell Differentiation, Cell Size, Cell Survival, Collagenases, Genes, Reporter, Glucagon genetics, Green Fluorescent Proteins genetics, Insulin-Secreting Cells cytology, Islets of Langerhans embryology, Islets of Langerhans growth & development, Islets of Langerhans physiology, Mice, Pancreatic Polypeptide genetics, Reverse Transcriptase Polymerase Chain Reaction, Somatostatin genetics, Gene Expression Regulation, Insulin genetics, Insulin-Secreting Cells physiology

Abstract

Aims/hypothesis: It is widely accepted that production of insulin, glucagon, somatostatin and pancreatic polypeptide in islet cells is specific to beta, alpha, delta and pancreatic polypeptide cells, respectively. We examined whether beta cells express other genes encoding islet hormones., Methods: Nested RT-PCR was performed on single beta cells of transgenic mice with green fluorescent protein (GFP) driven by mouse insulin I promoter (MIP-GFP)., Results: Only 55% of adult beta cells expressed the insulin gene alone, while others expressed two or more islet hormone genes; 4% expressed all four hormone genes. In embryonic and neonatal cells, 60% to 80% of GFP(+) cells co-expressed pancreatic polypeptide and insulin genes in contrast to 29% in adult. To clarify cell fate, we conducted lineage tracing using rat insulin II promoter-cre mice crossed with reporter mice Gt(ROSA)26Sor-loxP-flanked STOP-cassette-GFP. All GFP(+) cells expressed insulin I and II genes, and showed similar heterogeneity of co-expression to that seen in MIP-GFP mice. Although we report expression of other hormone genes in a significant proportion of beta cells, our lineage tracing results demonstrate that after inducing InsII (also known as Ins2) expression, beta cell progenitors do not redifferentiate to non-beta cells., Conclusions/interpretation: This study shows co-expression of multiple hormone genes in beta cells of adult mice as well as in embryos and neonates. This finding could: (1) represent residual expression from beta cell precursors; (2) result from alternative developmental pathways for beta cells; or (3) denote the differentiation potential of these cells. It may be linked to functional heterogeneity. This heterogeneity in gene expression may provide a means to characterise the functional, cellular and developmental heterogeneity seen in beta cells.

Published

2010

227. OVO homologue-like 1 (Ovol1) transcription factor: a novel target of neurogenin-3 in rodent pancreas.

Author

Vetere A, Li WC, Paroni F, Juhl K, Guo L, Nishimura W, Dai X, Bonner-Weir S, and Sharma A

Subjects

Animals, Cell Differentiation, Cell Division, Cell Line, Cell Proliferation, Cloning, Molecular, DNA Primers genetics, DNA-Binding Proteins metabolism, Exons, Mice, Mice, Inbred C57BL, Pancreas cytology, Pancreas pathology, Pancreatectomy, Rats, Rats, Sprague-Dawley, Regeneration, Reverse Transcriptase Polymerase Chain Reaction, Transcription Factors metabolism, Basic Helix-Loop-Helix Transcription Factors metabolism, DNA-Binding Proteins genetics, Gene Expression Regulation, Nerve Tissue Proteins metabolism, Transcription Factors genetics

Abstract

Aims/hypothesis: The basic helix-loop-helix transcription factor neurogenin-3 (NGN3) commits the fates of pancreatic progenitors to endocrine cell types, but knowledge of the mechanisms regulating the choice between proliferation and differentiation of these progenitors is limited., Methods: Using a chromatin immunoprecipitation cloning approach, we searched for direct targets of NGN3 and identified a zinc-finger transcription factor, OVO homologue-like 1 (OVOL1). Transactivation experiments were carried out to elucidate the functional role of NGN3 in Ovol1 gene expression. Embryonic and adult rodents pancreases were immunostained for OVOL1, Ki67 and NGN3., Results: We showed that NGN3 negatively regulates transcription of Ovol1 in an E-box-dependent fashion. The presence of either NGN3 or NEUROD1, but not MYOD, reduced endogenous Ovol1 mRNA. OVOL1 was detected in pancreatic tissue around embryonic day 15.5, after which OVOL1 levels dramatically increased. In embryonic pancreas, OVOL1 protein levels were low in NGN3(+) or Ki67(+) cells, but high in quiescent differentiated cells. OVOL1 presence was maintained in adult pancreas, where it was detected in islets, pancreatic ducts and some acinar cells. Additionally OVOL1 presence was lacking in proliferating ductules in regenerating pancreas and induced in cells as they began to acquire their differentiated phenotype., Conclusions/interpretation: The timing of OVOL1 appearance in pancreas and its increased levels in differentiated cells suggest that OVOL1 promotes the transition of cells from a proliferating, less-differentiated state to a quiescent more-differentiated state. We conclude that OVOL1, a downstream target of NGN3, may play an important role in regulating the balance between proliferation and differentiation of pancreatic cells.

Published

2010

228. Lack of evidence for recipient precursor cells replenishing β-cells in transplanted islets.

Author

Hamamoto Y, Akashi T, Inada A, Bonner-Weir S, and Weir GC

Subjects

Actins metabolism, Animals, Cell Separation methods, Chickens, Female, Glucagon genetics, Glucagon metabolism, Insulin genetics, Insulin metabolism, Insulin-Secreting Cells cytology, Male, Mice, Mice, Inbred C57BL, Recombinant Fusion Proteins genetics, Recombinant Fusion Proteins metabolism, Stem Cells cytology, Insulin-Secreting Cells physiology, Islets of Langerhans cytology, Islets of Langerhans physiology, Islets of Langerhans Transplantation, Stem Cells physiology

Abstract

Bone marrow and tissue precursor cells have been postulated to replenish grafts of transplanted islets. Several investigators have reported that bone marrow cells can promote the regeneration of injured islets. In this study, we investigated the potential of recipient-derived precursor cells to form new pancreatic endocrine cells in islet grafts transplanted under the kidney capsule. Mouse insulin promoter (MIP)-green fluorescence protein (GFP) mice, which express GFP only in β-cells, or β-actin GFP mice, which express GFP ubiquitously, were used to determine if the recipient-derived cells differentiate into β-cells or other types of endocrine cells. We transplanted MIP-GFP islets into wild-type mice, wild-type islets into MIP-GFP mice, β-actin GFP islets into wild-type mice, and wild-type islets into β-actin GFP mice. β-Actin GFP bone marrow cells were then injected into wild-type mice to evaluate the potential role of bone marrow stem cells to provide new islet cells to the graft. No β-cells with green fluorescence were seen in the graft when wild-type islets were transplanted into MIP-GFP mice. When wild-type islets were transplanted into β-actin GFP mice, no β-cells with GFP staining could be identified in the grafts. Similarly, no endocrine cells with GFP staining could be identified in the grafts after injection of β-actin GFP bone marrow cells into wild-type islet-transplanted wild-type mice. This study provides further support for the concept that recipient precursor cells do not produce new β-cells in grafts of transplanted islets.

Published

2010

229. Towards better understanding of the contributions of overwork and glucotoxicity to the beta-cell inadequacy of type 2 diabetes.

Author

Weir GC, Marselli L, Marchetti P, Katsuta H, Jung MH, and Bonner-Weir S

Subjects

Autophagy, Cadaver, Diabetes Mellitus, Type 2 genetics, Disease Progression, Gene Expression Profiling, Humans, Hyperglycemia physiopathology, Insulin metabolism, Insulin Secretion, Insulin-Secreting Cells pathology, Microdissection, Oxidative Stress genetics, Diabetes Mellitus, Type 2 pathology, Hyperglycemia pathology, Insulin Resistance physiology, Insulin-Secreting Cells physiology, Oxidative Stress physiology, Pancreas pathology

Abstract

Type 2 diabetes (T2D) is characterized by reduction of beta-cell mass and dysfunctional insulin secretion. Understanding beta-cell phenotype changes as T2D progresses should help explain these abnormalities. The normal phenotype should differ from the state of overwork when beta-cells compensate for insulin resistance to keep glucose levels normal. When only mild hyperglycaemia develops, beta-cells are subjected to glucotoxicity. As hyperglycaemia becomes more severe, so does glucotoxicity. beta-Cells in all four of these situations should have separate phenotypes. When assessing phenotype with gene expression, isolated islets have artefacts resulting from the trauma of isolation and hypoxia of islet cores. An advantage comes from laser capture microdissection (LCM), which obtains beta-cell-rich tissue from pancreatic frozen sections. Valuable data can be obtained from animal models, but the real goal is human beta-cells. Our experience with LCM and gene arrays on frozen pancreatic sections from cadaver donors with T2D and controls is described. Although valuable data was obtained, we predict that the approach of taking fresh samples at the time of surgery is an even greater opportunity to markedly advance our understanding of how beta-cell phenotype evolves as T2D develops and progresses.

Published

2009

230. Expression of MafA in pancreatic progenitors is detrimental for pancreatic development.

Author

Nishimura W, Bonner-Weir S, and Sharma A

Subjects

Animals, Cell Proliferation, Endocrine Cells metabolism, Maf Transcription Factors, Large genetics, Mice, Mice, Transgenic, Pancreas embryology, Stem Cells metabolism, Cell Differentiation physiology, Endocrine Cells cytology, Maf Transcription Factors, Large biosynthesis, Pancreas metabolism, Stem Cells cytology

Abstract

The transcription factor MafA regulates glucose-responsive expression of insulin. MafA-deficient mice have a normal proportion of insulin+ cells at birth but develop diabetes gradually with age, suggesting that MafA is required for maturation and not specification of pancreatic beta-cells. However, several studies show that ectopic expression of MafA may have a role in specification as it induces insulin+ cells in chicken gut epithelium, reprograms adult murine acinar cells into insulin+ cells in combination with Ngn3 and Pdx1, and triggers the lens differentiation. Hence, we examined whether MafA can induce specification of beta-cells during pancreatic development. When the MafA transgene is expressed in Pdx1+ pancreatic progenitors, both pancreatic mass and proliferation of progenitors are reduced, at least partially due to induction of cyclin kinase inhibitors p27 and p57. Expression of MafA in Pdx1+ cells until E12.5 was sufficient to cause these effects and to disproportionately inhibit the formation of endocrine cells in the remnant pancreas. Thus, in mice, MafA expression in Pdx1+ pancreatic progenitors is not sufficient to specify insulin+ cells but in fact deters pancreatic development and the differentiation of endocrine cells. These findings imply that MafA should be used to enhance maturation, rather than specification, of beta-cells from stem/progenitor cells.

Published

2009

231. Mutations at the BLK locus linked to maturity onset diabetes of the young and beta-cell dysfunction.

Author

Borowiec M, Liew CW, Thompson R, Boonyasrisawat W, Hu J, Mlynarski WM, El Khattabi I, Kim SH, Marselli L, Rich SS, Krolewski AS, Bonner-Weir S, Sharma A, Sale M, Mychaleckyj JC, Kulkarni RN, and Doria A

Subjects

Adolescent, Adult, Animals, Blotting, Western, Cell Line, Tumor, DNA Mutational Analysis, Diabetes Mellitus, Type 2 metabolism, Diabetes Mellitus, Type 2 physiopathology, Family Health, Female, Genetic Predisposition to Disease, Humans, Insulin metabolism, Insulin Secretion, Insulin-Secreting Cells pathology, Luciferases genetics, Luciferases metabolism, Male, Microscopy, Confocal, Middle Aged, Pedigree, RNA Interference, Recombinant Fusion Proteins genetics, Recombinant Fusion Proteins metabolism, Reverse Transcriptase Polymerase Chain Reaction, Young Adult, src-Family Kinases metabolism, Diabetes Mellitus, Type 2 genetics, Insulin-Secreting Cells metabolism, Mutation, src-Family Kinases genetics

Abstract

Maturity-onset diabetes of the young (MODY) is a subtype of diabetes defined by an autosomal pattern of inheritance and a young age at onset, often before age 25. MODY is genetically heterogeneous, with 8 distinct MODY genes identified to date and more believed to exist. We resequenced 732 kb of genomic sequence at 8p23 in 6 MODY families unlinked to known MODY genes that showed evidence of linkage at that location. Of the 410 sequence differences that we identified, 5 had a frequency <1% in the general population and segregated with diabetes in 3 of the families, including the 2 showing the strongest support for linkage at this location. The 5 mutations were all placed within 100 kb corresponding to the BLK gene. One resulted in an Ala71Thr substitution; the other 4 were noncoding and determined decreased in vitro promoter activity in reporter gene experiments. We found that BLK--a nonreceptor tyrosine-kinase of the src family of proto-oncogenes--is expressed in beta-cells where it enhances insulin synthesis and secretion in response to glucose by up-regulating transcription factors Pdx1 and Nkx6.1. These actions are greatly attenuated by the Ala71Thr mutation. These findings point to BLK as a previously unrecognized modulator of beta-cell function, the deficit of which may lead to the development of diabetes.

Published

2009

232. p38 MAPK is a major regulator of MafA protein stability under oxidative stress.

Author

Kondo T, El Khattabi I, Nishimura W, Laybutt DR, Geraldes P, Shah S, King G, Bonner-Weir S, Weir G, and Sharma A

Subjects

Animals, Glucose metabolism, Glycogen Synthase Kinase 3 metabolism, Hyperglycemia metabolism, Insulin-Secreting Cells metabolism, Male, Mice, Models, Biological, Protein Structure, Tertiary, Rats, Rats, Sprague-Dawley, p38 Mitogen-Activated Protein Kinases metabolism, Gene Expression Regulation, Enzymologic, Maf Transcription Factors, Large metabolism, Oxidative Stress, p38 Mitogen-Activated Protein Kinases physiology

Abstract

Mammalian MafA/RIPE3b1 is an important glucose-responsive transcription factor that regulates function, maturation, and survival of beta-cells. Increased expression of MafA results in improved glucose-stimulated insulin secretion and beta-cell function. Because MafA is a highly phosphorylated protein, we examined whether regulating activity of protein kinases can increase MafA expression by enhancing its stability. We demonstrate that MafA protein stability in MIN6 cells and isolated mouse islets is regulated by both p38 MAPK and glycogen synthase kinase 3. Inhibiting p38 MAPK enhanced MafA stability in cells grown under both low and high concentrations of glucose. We also show that the N-terminal domain of MafA plays a major role in p38 MAPK-mediated degradation; simultaneous mutation of both threonines 57 and 134 into alanines in MafA was sufficient to prevent this degradation. Under oxidative stress, a condition detrimental to beta-cell function, a decrease in MafA stability was associated with a concomitant increase in active p38 MAPK. Interestingly, inhibiting p38 MAPK but not glycogen synthase kinase 3 prevented oxidative stress-dependent degradation of MafA. These results suggest that the p38 MAPK pathway may represent a common mechanism for regulating MafA levels under oxidative stress and basal and stimulatory glucose concentrations. Therefore, preventing p38 MAPK-mediated degradation of MafA represents a novel approach to improve beta-cell function.

Published

2009

233. Porcine marginal mass islet autografts resist metabolic failure over time and are enhanced by early treatment with liraglutide.

Author

Emamaullee JA, Merani S, Toso C, Kin T, Al-Saif F, Truong W, Pawlick R, Davis J, Edgar R, Lock J, Bonner-Weir S, Knudsen LB, and Shapiro AM

Subjects

Animals, Apoptosis drug effects, Cells, Cultured, Dose-Response Relationship, Drug, Female, Glucagon-Like Peptide 1 pharmacology, Glucagon-Like Peptide 1 therapeutic use, Glucose metabolism, Graft Survival physiology, Insulin-Secreting Cells drug effects, Insulin-Secreting Cells metabolism, Insulin-Secreting Cells physiology, Insulin-Secreting Cells transplantation, Islets of Langerhans Transplantation rehabilitation, Islets of Langerhans Transplantation veterinary, Liraglutide, Swine, Swine, Miniature, Time Factors, Transplantation, Autologous, Glucagon-Like Peptide 1 analogs & derivatives, Graft Survival drug effects, Islets of Langerhans Transplantation methods, Metabolic Diseases prevention & control

Abstract

Although insulin independence is maintained in most islet recipients at 1 yr after transplant, extended follow-up has revealed that many patients will eventually require insulin therapy. Previous studies have shown that islet autografts are prone to chronic failure in large animals and humans, suggesting that nonimmunological events contribute to islet graft functional decay. Early intervention with therapies that promote graft stability should provide a measurable benefit over time. In this study, the efficacy of the long-acting glucagon-like peptide-1 analog liraglutide was explored in a porcine marginal mass islet autograft transplant model. Incubation with liraglutide enhanced porcine islet survival and function after prolonged culture. Most vehicle-treated (83%) and liraglutide-treated (80%) animals became insulin independent after islet autotransplantation. Although liraglutide therapy did not improve insulin independence rates or blood glucose levels after transplant, a significant increase in insulin secretion and acute-phase insulin response was observed in treated animals. Surprisingly, no evidence for deterioration of graft function was observed in any of the transplanted animals over more than 18 months of follow-up despite significant weight gain; in fact, an enhanced response to glucose developed over time even in control animals. Histological analysis showed that intraportally transplanted islets remained highly insulin positive, retained alpha-cells, and did not form amyloid deposits. This study demonstrates that marginal mass porcine islet autografts have stable long-term function, even in the presence of an increasing metabolic demand. These results are discrepant with previous large animal studies and suggest that porcine islets may be resistant to metabolic failure.

Published

2009

234. Differentiation of COPAS-sorted non-endocrine pancreatic cells into insulin-positive cells in the mouse.

Author

Kikugawa R, Katsuta H, Akashi T, Yatoh S, Weir GC, Sharma A, and Bonner-Weir S

Subjects

Animals, Cell Culture Techniques, Diabetes Mellitus, Type 1 surgery, Flow Cytometry, Genes, Reporter, Green Fluorescent Proteins genetics, Insulin genetics, Insulin-Secreting Cells physiology, Insulin-Secreting Cells transplantation, Mice, Mice, Inbred C57BL, Mice, Transgenic, Pancreas cytology, Pancreas physiology, Pancreatic Ducts cytology, Promoter Regions, Genetic, RNA, Messenger analysis, RNA, Messenger genetics, Reverse Transcriptase Polymerase Chain Reaction, Cell Separation methods, Insulin-Secreting Cells cytology, Islets of Langerhans cytology

Abstract

Aims/hypothesis: The regenerative process in the pancreas is of particular interest, since insulin-producing beta cells are lost in diabetes. Differentiation of new beta cells from pancreatic non-endocrine cells has been reported in vivo and in vitro, a finding that implies the existence of pancreatic stem/progenitor cells. However, while tissue-specific stem cells are well documented in skin, intestine and testis, pancreatic stem cells have been elusive. We hypothesised that pancreatic stem/progenitor cells within the non-endocrine fraction could be a source of new islets in vitro., Methods: To test if there were such cells within the pancreas, we generated pancreatic cell aggregates from tissue remaining after islet isolation from mouse insulin promoter 1-green fluorescent protein (MIP-GFP) mice. To eliminate any contamination of insulin-positive cells, we deleted all GFP-positive aggregates using COPAS Select and cultured with Matrigel. Immunohistochemistry, quantitative real-time PCR and single-cell nested RT-PCR were performed to confirm formation of insulin-producing cells., Results: The GFP-negative cells were expanded as monolayers and then differentiated into three-dimensional cystic structures. After 1 week of culture, GFP-positive cells were found as clusters or single cells. By quantitative real-time PCR, no insulin mRNA was detected immediately after COPAS sorting, but after differentiation insulin mRNA of the whole preparation was 1.91 +/- 0.31% that of purified MIP-GFP beta cells. All GFP-positive cells expressed insulin 1; most expressed insulin 2, pancreas duodenum homeobox-1 and cytokeratin 19 by single cell nested RT-PCR., Conclusions/interpretation: Our data support the concept that within the exocrine (acinar and ductal) pancreas of the adult mouse there are cells that can give rise to insulin-positive cells in vitro.

Published

2009

235. Adult mouse intrahepatic biliary epithelial cells induced in vitro to become insulin-producing cells.

Author

Nagaya M, Katsuta H, Kaneto H, Bonner-Weir S, and Weir GC

Subjects

Adenoviridae genetics, Age Factors, Animals, Basic Helix-Loop-Helix Transcription Factors genetics, Basic Helix-Loop-Helix Transcription Factors metabolism, Bile Ducts, Intrahepatic cytology, Bile Ducts, Intrahepatic metabolism, Cells, Cultured, Epithelial Cells metabolism, Gene Expression Profiling, Herpes Simplex Virus Protein Vmw65 genetics, Homeodomain Proteins genetics, Homeodomain Proteins metabolism, Insulin metabolism, Insulin-Secreting Cells metabolism, Male, Mice, Mice, Inbred C57BL, Nerve Tissue Proteins genetics, Nerve Tissue Proteins metabolism, Trans-Activators genetics, Trans-Activators metabolism, Bile Ducts, Intrahepatic physiology, Cell Transdifferentiation genetics, Epithelial Cells physiology, Insulin-Secreting Cells physiology, Transduction, Genetic

Abstract

Transdifferentiation of cells from a patient's own liver into pancreatic beta-cells could be useful for beta-cell replacement. We hypothesized that intrahepatic biliary epithelial cells (IHBECs) could become a new source of insulin-producing cells. IHBECs isolated from adult mice were expanded using our novel culture method termed, collagen-embedded floating culture method (CEFCM). With CEFCM, IHBECs formed three-dimensional ductal cysts and rapidly expanded their number by about 15-fold within 2 weeks. Over 90% of cells were positive for cytokeratin 7 and 19. At day 14, IHBECs were transfected with adenoviral (Ad)- pancreas duodenum homeobox 1 (Pdx-1), NeuroD or Pdx-1/VP16. After 7 additional days in serum- and insulin-free differentiation medium (DM), cell phenotypes were determined by RT-PCR, immunostaining and ELISA for insulin. In DM control IHBECs started to express some endocrine progenitor genes (Neurog3, NeuroD, Nkx6.1, and Pdx-1) but lacked insulin gene (Ins) mRNA. Transduced expression of PDX-1, NEUROD or PDX-1/VP16 led to expression of not only INS but also GLUT2 and prohormone convertase 1 and 2. About 3% of 4000 cells counted in PDX-1/VP16 transduced cultures stained strongly for C-peptide suggesting that a subpopulation may have the capacity for differentiation. Transduced cells released insulin (Ad-PDX-1 0.08+/-0.05, Ad-NEUROD 0.33+/-0.09, Ad-PDX-1/VP16 0.37+/-0.14 ng/1x10(5) cells after 48 h in culture). IHBECs can be markedly expanded, and then with molecular manipulation a subpopulation of these cells can differentiate towards a beta-cell phenotype. This approach may lead to a new source of beta-cells that can be used for transplantation in diabetes.

Published

2009

236. Developmental pathways during in vitro progression of human islet neogenesis.

Author

Dodge R, Loomans C, Sharma A, and Bonner-Weir S

Subjects

Animals, Calcium-Binding Proteins, Cell Proliferation, DNA-Binding Proteins, Down-Regulation, Gene Expression Profiling, Humans, Immunohistochemistry, Insulin-Secreting Cells cytology, Islets of Langerhans metabolism, Oligonucleotide Array Sequence Analysis, Rats, Receptors, Cell Surface genetics, Receptors, Cell Surface metabolism, Reverse Transcriptase Polymerase Chain Reaction, Signal Transduction, Tumor Suppressor Proteins, Ubiquitin Thiolesterase genetics, Ubiquitin Thiolesterase metabolism, Up-Regulation, Cell Differentiation, Insulin-Secreting Cells metabolism, Islets of Langerhans cytology

Abstract

Islet neogenesis, or the differentiation of islet cells from precursor cells, is seen in vitro and in vivo both embryonically and after birth. However, little is known about the differentiation pathways during embryonic development for human pancreas. Our previously reported in vitro generation of islets from human pancreatic tissue provides a unique system to identify potential markers of neogenesis and to determine the molecular mechanisms underlying this process. To this end, we analyzed the gene expression profiles of three different stages during in vitro islet generation: the Initially Adherent, Expanded, and Differentiated stages. Samples from four human pancreases were hybridized to Affymetrix U95A GeneChips, and data analyzed using GeneSpring 7.0/9.0 software. Using scatter plots we selected genes with a 2-fold or greater differential expression. Of the 12,000 genes/ESTs present on these arrays, 295 genes including 38 acinar-enriched genes were selectively lost during the progression from the Initially Adherent stage to the Expanded stage; 468 genes were increased in this progression to Expanded tissue; and 529 genes had a two-fold greater expression in the Differentiated stage than in the Expanded tissue. Besides the expected increases in insulin, glucagon, and duct markers (mucin 6, aquaporin 1 and 5), the beta cell auto-antigen IA-2/phogrin was increased 5-fold in Differentiated. In addition, developmentally important pathways, including notch/jagged, Wnt/frizzled, TGFbeta superfamily (follistatin, BMPs, and SMADs), and retinoic acid (COUP-TFI, CRABP1, 2, and RAIG1) were differentially regulated during the expansion/differentiation. Two putative markers for islet precursor cells, UCHL1/PGP9.5 and DMBT1, were enhanced during the progression to differentiated cells, but only the latter could be a marker of islet precursor cells. We suggest that appropriate manipulation of these differentiation-associated pathways will enhance the efficiency of differentiation of insulin-producing beta-cells in this in vitro model.

Published

2009

237. Laser capture microdissection of human pancreatic beta-cells and RNA preparation for gene expression profiling.

Author

Marselli L, Sgroi DC, Bonner-Weir S, and Weir GC

Subjects

Humans, Microdissection instrumentation, RNA isolation & purification, Tissue Preservation, Gene Expression Profiling methods, Insulin-Secreting Cells metabolism, Microdissection methods

Abstract

Human beta-cell gene profiling is a powerful tool for understanding beta-cell biology in normal and pathological conditions. The assessment is complicated when isolated islets are studied because of contamination by non-beta-cells and the exposure to the trauma of isolation that causes changes in gene expression. These limitations can be overcome by dissecting the beta-cells from the pancreatic tissue directly using the laser capture microdissection (LCM) technique. LCM allows the sampling of specific cell types from tissue sections. The technique requires morphological criteria or specific stains for targeted cells, and the protocols must preserve the condition of the sought-after macromolecules. We have developed a protocol of rapid tissue dehydration followed by identification of human beta-cells by their intrinsic autofluorescence, which allows laser microdissection for gene-profiling studies.

Published

2009

238. Carbonic anhydrase II-positive pancreatic cells are progenitors for both endocrine and exocrine pancreas after birth.

Author

Inada A, Nienaber C, Katsuta H, Fujitani Y, Levine J, Morita R, Sharma A, and Bonner-Weir S

Subjects

Animals, Carbonic Anhydrase II genetics, Epithelial Cells cytology, Epithelial Cells enzymology, Genes, Reporter, Humans, Mice, Mice, Transgenic, Pancreatic Ducts enzymology, Stem Cell Transplantation, Stem Cells cytology, Transgenes, beta-Galactosidase genetics, Carbonic Anhydrase II biosynthesis, Islets of Langerhans physiology, Pancreas, Exocrine physiology, Pancreatic Ducts cytology, Regeneration, Stem Cells enzymology

Abstract

The regenerative process in the pancreas is of particular interest because diabetes results from an inadequate number of insulin-producing beta cells and pancreatic cancer may arise from the uncontrolled growth of progenitor/stem cells. Continued and substantial growth of islet tissue occurs after birth in rodents and humans, with additional compensatory growth in response to increased demand. In rodents there is clear evidence of pancreatic regeneration after some types of injury, with proliferation of preexisting differentiated cell types accounting for some replacement. Additionally, neogenesis or the budding of new islet cells from pancreatic ducts has been reported, but the existence and identity of a progenitor cell have been debated. We hypothesized that the progenitor cells are duct epithelial cells that after replication undergo a regression to a less differentiated state and then can form new endocrine and exocrine pancreas. To directly test whether ductal cells serve as pancreatic progenitors after birth and give rise to new islets, we generated transgenic mice expressing human carbonic anhydrase II (CAII) promoter: Cre recombinase (Cre) or inducible CreER(TM) to cross with ROSA26 loxP-Stop-loxP LacZ reporter mice. We show that CAII-expressing cells within the pancreas act as progenitors that give rise to both new islets and acini normally after birth and after injury (ductal ligation). This identification of a differentiated pancreatic cell type as an in vivo progenitor of all differentiated pancreatic cell types has implications for a potential expandable source for new islets for replenishment therapy for diabetes.

Published

2008

239. Islets in type 2 diabetes: in honor of Dr. Robert C. Turner.

Author

Bonner-Weir S and O'Brien TD

Subjects

Amyloid metabolism, Amyloidosis physiopathology, Biomedical Research methods, Biomedical Research organization & administration, Diabetes Mellitus, Type 2 blood, Diabetes Mellitus, Type 2 history, History, 20th Century, Humans, Islets of Langerhans metabolism, Biomedical Research history, Diabetes Mellitus, Type 2 prevention & control, Islets of Langerhans pathology

Published

2008

240. Loss of Ncb5or results in impaired fatty acid desaturation, lipoatrophy, and diabetes.

Author

Larade K, Jiang Z, Zhang Y, Wang W, Bonner-Weir S, Zhu H, and Bunn HF

Subjects

Animals, Apoptosis, Cell Survival, Fatty Acids, Monounsaturated metabolism, Hepatocytes metabolism, Islets of Langerhans Transplantation, Lipids chemistry, Mice, Mice, Knockout, Models, Biological, Oleic Acid chemistry, Oleic Acid metabolism, Palmitic Acid metabolism, Cytochrome-B(5) Reductase metabolism, Diabetes Mellitus, Experimental metabolism, Fatty Acids metabolism

Abstract

Targeted ablation of the novel flavoheme reductase Ncb5or knock-out (KO) results in progressive loss of pancreatic beta-cells and white adipose tissue over time. Lipoatrophy persisted in KO animals in which the confounding metabolic effects of diabetes were eliminated by islet transplantation (transplanted knockout (TKO)). Lipid profiles in livers prepared from TKO animals were markedly deficient in triglycerides and diacylglycerides. Despite enhanced expression of stearoyl-Co-A desaturase-1, levels of palmitoleic and oleic acids (Delta9 fatty acid desaturation) were decreased in TKO relative to wild type controls. Treatment of KO hepatocytes with palmitic acid reduced cell viability and increased apoptosis, a response blunted by co-incubation with oleic acid. The results presented here support the hypothesis that Ncb5or supplies electrons for fatty acid desaturation, offer new insight into the regulation of a crucial step in fatty acid biosynthesis, and provide a plausible explanation for both the diabetic and the lipoatrophic phenotype in Ncb5or(-/-) mice.

Published

2008

241. Curative and beta cell regenerative effects of alpha1-antitrypsin treatment in autoimmune diabetic NOD mice.

Author

Koulmanda M, Bhasin M, Hoffman L, Fan Z, Qipo A, Shi H, Bonner-Weir S, Putheti P, Degauque N, Libermann TA, Auchincloss H Jr, Flier JS, and Strom TB

Subjects

Age of Onset, Animals, Diabetes Mellitus, Type 1 immunology, Female, Immune Tolerance drug effects, Immune Tolerance immunology, Inflammation immunology, Insulin metabolism, Insulin Resistance, Lymph Nodes drug effects, Lymph Nodes immunology, Lymphocyte Activation drug effects, Lymphocyte Activation immunology, Mice, Mice, Inbred NOD, Oligonucleotide Array Sequence Analysis, Signal Transduction drug effects, T-Lymphocytes drug effects, T-Lymphocytes immunology, Time Factors, Cell Differentiation drug effects, Insulin-Secreting Cells cytology, Insulin-Secreting Cells drug effects, alpha 1-Antitrypsin pharmacology

Abstract

Invasive insulitis is a destructive T cell-dependent autoimmune process directed against insulin-producing beta cells that is central to the pathogenesis of type 1 diabetes mellitus (T1DM) in humans and the clinically relevant nonobese diabetic (NOD) mouse model. Few therapies have succeeded in restoring long-term, drug-free euglycemia and immune tolerance to beta cells in overtly diabetic NOD mice, and none have demonstrably enabled enlargement of the functional beta cell mass. Recent studies have emphasized the impact of inflammatory cytokines on the commitment of antigen-activated T cells to various effector or regulatory T cell phenotypes and insulin resistance and defective insulin signaling. Hence, we tested the hypothesis that inflammatory mechanisms trigger insulitis, insulin resistance, faulty insulin signaling, and the loss of immune tolerance to islets. We demonstrate that treatment with alpha1-antitrypsin (AAT), an agent that dampens inflammation, does not directly inhibit T cell activation, ablates invasive insulitis, and restores euglycemia, immune tolerance to beta cells, normal insulin signaling, and insulin responsiveness in NOD mice with recent-onset T1DM through favorable changes in the inflammation milieu. Indeed, the functional mass of beta cells expands in AAT-treated diabetic NOD mice.

Published

2008

242. Bone marrow or foetal liver cells fail to induce islet regeneration in diabetic Akita mice.

Author

Akashi T, Shigematsu H, Hamamoto Y, Iwasaki H, Yatoh S, Bonner-Weir S, Akashi K, and Weir GC

Subjects

Animals, Disease Models, Animal, Mice, Regeneration, Bone Marrow Transplantation, Cell Transplantation, Diabetes Mellitus, Experimental therapy, Diabetes Mellitus, Type 1 therapy, Islets of Langerhans physiology, Liver cytology, Liver embryology

Abstract

Background: In this study, we carried out bone marrow and foetal liver cell transplantation to determine if these cells could differentiate into pancreatic beta-cells or promote regeneration., Methods: To exclude an artificial or immunological influence for induction of diabetes to recipients, Akita mice, which develop diabetes spontaneously,were used. In addition, we used mice harbouring the transgenic green fluorescent protein (GFP) reporter for insulin 1 gene as donors to mark donor-derived beta-cells., Results: All transplanted Akita mice after intravenous injection showed full donor chimerism in peripheral blood analysis. Their diabetic state represented by blood glucose levels did not change after transplantation. In spite of examination of more than 200 islets in each group, we could not find GFP-positive cells in any of the recipients., Conclusions: Bone marrow cells or foetal liver cells do not differentiate to new pancreatic beta-cells or promote regeneration in Akita mice, a non-chemical or non-immune model of diabetes., (Copyright (c) 2008 John Wiley & Sons, Ltd.)

Published

2008

243. Transdifferentiation of pancreatic ductal cells to endocrine beta-cells.

Author

Bonner-Weir S, Inada A, Yatoh S, Li WC, Aye T, Toschi E, and Sharma A

Subjects

Animals, Cell Lineage, Humans, Mice, Models, Biological, Rats, Stem Cells cytology, Cell Transdifferentiation, Insulin-Secreting Cells cytology, Pancreatic Ducts cytology

Abstract

The regenerative process in the pancreas is of particular interest, since diabetes, whether Type 1 or Type 2, results from an inadequate amount of insulin-producing beta-cells. Islet neogenesis, or the formation of new islets, seen as budding of hormone-positive cells from the ductal epithelium, has long been considered to be one of the mechanisms of normal islet growth after birth and in regeneration, and suggested the presence of pancreatic stem cells. Results from the rat regeneration model of partial pancreatectomy led us to hypothesize that differentiated pancreatic ductal cells were the pancreatic progenitors after birth, and that with replication they regressed to a less differentiated phenotype and then could differentiate to form new acini and islets. There are numerous supportive results for this hypothesis of neogenesis, including the ability of purified primary human ducts to form insulin-positive cells budding from ducts. However, to rigorously test this hypothesis, we took a direct approach of genetically marking ductal cells using CAII (carbonic anhydrase II) as a duct-cell-specific promoter to drive Cre recombinase in lineage-tracing experiments using the Cre-Lox system. We show that CAII-expressing pancreatic cells act as progenitors that give rise to both new islets and acini after birth and after injury (ductal ligation). This identification of a differentiated pancreatic cell type as an in vivo progenitor for all differentiated pancreatic cell types has implications for a potential expandable source for new islets for replenishment therapy for diabetes either in vivo or ex vivo.

Published

2008

244. Preservation of beta-cell function by targeting beta-cell mass.

Author

de Koning EJ, Bonner-Weir S, and Rabelink TJ

Subjects

Animals, Cytokines antagonists & inhibitors, Cytoprotection, Diabetes Mellitus, Type 2 pathology, Diabetes Mellitus, Type 2 physiopathology, Glucagon-Like Peptide-1 Receptor, Humans, Hypoglycemic Agents pharmacology, Insulin-Secreting Cells pathology, Insulin-Secreting Cells physiology, NF-kappa B antagonists & inhibitors, Obesity pathology, Receptors, Glucagon agonists, Renin-Angiotensin System drug effects, Diabetes Mellitus, Type 2 drug therapy, Insulin-Secreting Cells drug effects

Abstract

Type 2 diabetes is characterized by progressive beta-cell dysfunction and a reduction in beta-cell mass. Pancreatic islets are a target for adverse effectors such as high concentrations of glucose, pro-inflammatory cytokines and increased free fatty acid concentrations - which are associated with adiposity, insulin resistance and the induction of beta-cell apoptosis. If the beta-cell mass is already below the threshold for maintaining normoglycemia, the expansion of beta-cell mass is the only option for achieving normoglycemia without the use of additional glucose-lowering agents. Therapies based on glucagon-like peptide-1 and combinations of growth factors such as epidermal growth factor and gastrin are promising new strategies for beta-cell preservation. In this review, we address the mechanisms involved in beta-cell dysfunction and beta-cell loss, and provide a rationale for pharmacological intervention for the preservation and/or expansion of beta-cell mass in type 2 diabetes.

Published

2008

245. Gene expression of purified beta-cell tissue obtained from human pancreas with laser capture microdissection.

Author

Marselli L, Thorne J, Ahn YB, Omer A, Sgroi DC, Libermann T, Otu HH, Sharma A, Bonner-Weir S, and Weir GC

Subjects

Humans, Lasers, Mitogen-Activated Protein Kinases genetics, Oligonucleotide Array Sequence Analysis, Oxidative Stress, RNA analysis, Gene Expression Profiling, Insulin-Secreting Cells metabolism, Microdissection methods

Abstract

Context: Human beta-cell gene profiling is a powerful tool for understanding beta-cell biology in normal and pathological conditions. Assessment is complicated when isolated islets are studied because of contamination by non-beta-cells and the trauma of the isolation procedure., Objective: The objective was to use laser capture microdissection (LCM) of human beta-cells from pancreases of cadaver donors and compare their gene expression with that of handpicked isolated islets., Design: Endogenous autofluorescence of beta-cells facilitated procurement of purified beta-cell tissue from frozen pancreatic sections with LCM. Gene expression profiles of three microdissected beta-cell samples and three isolated islet preparations were obtained. The array data were normalized using DNA-Chip Analyzer software (Harvard School of Public Health, Boston, MA), and the lower confidence bound evaluated differentially expressed genes. Real-time PCR was performed on selected acinar genes and on the duct cell markers, carbonic anhydrase II and keratin 19., Results: Endogenous autofluorescence facilitates the microdissection of beta-cell rich tissue in human pancreas. When compared with array profiles of purified beta-cell tissue, with lower confidence bound set at 1.2, there were 4560 genes up-regulated and 1226 genes down-regulated in the isolated islets. Among the genes up-regulated in isolated islets were pancreatic acinar and duct genes, chemokine genes, and genes associated with hypoxia, apoptosis, and stress. Quantitative RT-PCR confirmed the differential expression of acinar gene transcripts and the duct marker carbonic anhydrase II in isolated islets., Conclusion: LCM makes it possible to obtain beta-cell enriched tissue from human pancreas sections without the trauma and ischemia of islet isolation.

Published

2008

246. Preferential reduction of beta cells derived from Pax6-MafB pathway in MafB deficient mice.

Author

Nishimura W, Rowan S, Salameh T, Maas RL, Bonner-Weir S, Sell SM, and Sharma A

Subjects

Animals, Embryo, Mammalian physiology, Eye Proteins genetics, Gene Expression Regulation, Developmental, Genes, Reporter, Homeodomain Proteins genetics, Insulin deficiency, Insulin genetics, Luciferases genetics, MafB Transcription Factor genetics, Mice, Mice, Knockout, Mutagenesis, PAX6 Transcription Factor, Paired Box Transcription Factors deficiency, Paired Box Transcription Factors genetics, Repressor Proteins genetics, Eye Proteins physiology, Homeodomain Proteins physiology, Insulin-Secreting Cells physiology, MafB Transcription Factor deficiency, MafB Transcription Factor physiology, Paired Box Transcription Factors physiology, Repressor Proteins physiology

Abstract

During pancreatic development insulin(+) cells co-express the transcription factors MafB and Pax6, and transition from a MafA(-) to MafA(+) state. To examine the role of Pax6 and MafB in the development of beta-cells, we analyzed embryonic pancreata from Pax6- and MafB-deficient mice. Pax6 deficiency, as manifest in the Pax6(Sey-Neu) allele, reduced not only the number of cells expressing insulin or glucagon, but also the number of MafB, PDX-1 and MafA expressing cells. We show that MafB can directly activate expression of insulin and glucagon, and a MafB protein engineered to contain N248S mutation in the MafB (kr(ENU)) results in significantly reduced activation. Furthermore, pancreata from MafB deficient (kr(ENU)/kr(ENU)) mice exhibited reduced number of cells expressing insulin, glucagon, PDX-1 and MafA, with only a minor reduction in MafB expressing cells. MafB deficiency does not affect endocrine specification but does affect the lineage commitment of the endocrine cells and their maturation. Similar to Pax6 deficient mice, MafB deficient mice showed reductions both in insulin and glucagon expressing cells and in the ability of MafB and PDX-1 expressing cells to activate expression of these hormones. However, MafB deficient mice exhibited no effect on Pax6 expression. These results suggest that MafB may function as a downstream mediator of Pax6 in regulating the specification of insulin and glucagon expressing cells. Interestingly, the remaining insulin(+) cells in these knockouts preferentially express Hb9, suggesting the existence of an alternate pathway for the generation of insulin expressing cells, even in the absence of Pax6 and MafB function. Thus, Pax6 acts upstream of MafB, which in turn may trigger the expression of insulin and regulate the PDX-1 and MafA expression required for beta-cell maturation.

Published

2008

247. Influence of diabetes on the loss of beta cell differentiation after islet transplantation in rats.

Author

Laybutt DR, Hawkins YC, Lock J, Lebet J, Sharma A, Bonner-Weir S, and Weir GC

Subjects

Animals, Blood Glucose metabolism, Diabetes Mellitus, Experimental genetics, Disease Models, Animal, Insulin blood, Male, Potassium Channels, Inwardly Rectifying genetics, RNA, Messenger genetics, Rats, Rats, Inbred Lew, Reverse Transcriptase Polymerase Chain Reaction, Time Factors, Transplantation, Homologous, Diabetes Mellitus, Experimental pathology, Diabetes Mellitus, Experimental surgery, Gene Expression Regulation, Insulin-Secreting Cells pathology, Islets of Langerhans Transplantation

Abstract

Aims/hypothesis: Hyperglycaemia can impair beta cell function after islet transplantation. Appropriate glucose-induced insulin secretion is dependent on a unique expression pattern of genes. Here we examined the effects of diabetes on gene expression in transplanted islets., Materials and Methods: Streptozotocin-induced diabetic or control non-diabetic Lewis rats were transplanted under the kidney capsule with an insufficient number (2,000) of syngeneic islets to normalise blood glucose levels in diabetic rats. Eighteen days after transplantation, islet grafts were retrieved and RT-PCR used to assess expression of selected genes critical for beta cell function. Islet grafts from diabetic rats transplanted with a sufficient number of islets (3,000) to normalise hyperglycaemia were used to assess the effects of correcting blood glucose levels. Additionally, gene expression of transplanted islets from non-diabetic rats was compared with freshly isolated islets., Results: In islet grafts from diabetic rats, mRNA levels of several transcription factors important for the maintenance of beta cell differentiation were reduced (pancreatic and duodenal homeobox 1 [Pdx1], neurogenic differentiation 1 [Neurod1], NK6 transcription factor related, locus 1 [Nkx6.1], paired box gene 6 [Pax6]), as were genes implicated in beta cell function (Glut2 [also known as solute carrier family 2 [facilitated glucose transporter], member 2 [Slc2a2], glucokinase, insulin, islet amyloid polypeptide [Iapp]). Conversely, mRNA levels of lactate dehydrogenase, which is normally suppressed in beta cells, were increased. The majority of the changes in gene expression were normalised after correction of hyperglycaemia, indicating that the severe loss of beta cell differentiation correlates with continuous exposure to diabetes. Even islet grafts from non-diabetic rats showed a few alterations in beta cell gene expression in comparison with fresh islets., Conclusions/interpretation: Chronic hyperglycaemia contributes to the deterioration of beta cell differentiation after islet transplantation.

Published

2007

248. Protein-tyrosine phosphatase 1B deficiency reduces insulin resistance and the diabetic phenotype in mice with polygenic insulin resistance.

Author

Xue B, Kim YB, Lee A, Toschi E, Bonner-Weir S, Kahn CR, Neel BG, and Kahn BB

Subjects

Animals, Diabetes Mellitus, Type 2 therapy, Glucose Intolerance, Insulin Receptor Substrate Proteins, Islets of Langerhans pathology, Liver metabolism, Male, Mice, Muscles metabolism, Phosphoproteins deficiency, Phosphoproteins genetics, Phosphorylation, Protein Tyrosine Phosphatase, Non-Receptor Type 1, Receptor, Insulin deficiency, Receptor, Insulin genetics, Diabetes Mellitus, Experimental therapy, Insulin Resistance genetics, Multifactorial Inheritance, Protein Tyrosine Phosphatases deficiency

Abstract

Mice heterozygous for insulin receptor (IR) and IR substrate (IRS)-1 deficiency provide a model of polygenic type 2 diabetes in which early-onset, genetically programmed insulin resistance leads to diabetes. Protein-tyrosine phosphatase 1B (PTP1B) dephosphorylates tyrosine residues in IR and possibly IRS proteins, thereby inhibiting insulin signaling. Mice lacking PTP1B are lean and have increased insulin sensitivity. To determine whether PTP1B can modify polygenic insulin resistance, we crossed PTP1B-/- mice with mice with a double heterozygous deficiency of IR and IRS-1 alleles (DHet). DHet mice weighed slightly less than wild-type mice and exhibited severe insulin resistance and hyperglycemia, with approximately 35% of DHet males developing diabetes by 9-10 weeks of age. Body weight in DHet mice with PTP1B deficiency was similar to that in DHet mice. However, absence of PTP1B in DHet mice markedly improved glucose tolerance and insulin sensitivity at 10-11 weeks of age and reduced the incidence of diabetes and hyperplastic pancreatic islets at 6 months of age. Insulin-stimulated phosphorylation of IR, IRS proteins, Akt/protein kinase B, glycogen synthase kinase 3beta, and p70(S6K) was impaired in DHet mouse muscle and liver and was differentially improved by PTP1B deficiency. In addition, increased phosphoenolpyruvate carboxykinase expression in DHet mouse liver was reversed by PTP1B deficiency. In summary, PTP1B deficiency reduces insulin resistance and hyperglycemia without altering body weight in a model of polygenic type 2 diabetes. Thus, even in the setting of high genetic risk for diabetes, reducing PTP1B is partially protective, further demonstrating its attractiveness as a target for prevention and treatment of type 2 diabetes.

Published

2007

249. Modification of adverse inflammation is required to cure new-onset type 1 diabetic hosts.

Author

Koulmanda M, Budo E, Bonner-Weir S, Qipo A, Putheti P, Degauque N, Shi H, Fan Z, Flier JS, Auchincloss H Jr, Zheng XX, and Strom TB

Subjects

Animals, Autoimmunity, Diabetes Mellitus, Type 1 immunology, Diabetes Mellitus, Type 1 pathology, Female, Immune Tolerance, Insulin blood, Insulin Resistance, Insulin-Secreting Cells immunology, Insulin-Secreting Cells pathology, Interleukin-15 administration & dosage, Interleukin-2 administration & dosage, Mice, Mice, Inbred NOD, Sirolimus administration & dosage, Diabetes Mellitus, Type 1 drug therapy, Inflammation drug therapy

Abstract

In nonobese diabetic (NOD) mice with overt new-onset type 1 diabetes mellitus (T1DM), short-term treatment with a "triple-therapy" regimen [rapamycin plus agonist IL-2-related and antagonist-type, mutant IL-15-related Ig fusion proteins (IL-2.Ig and mutIL-15.Ig)] halts autoimmune destruction of insulin-producing beta cells and restores both euglycemia and immune tolerance to beta cells. Increases in the mass of insulin-producing beta cells or circulating insulin levels were not linked to the restoration of euglycemia. Instead, the restoration of euglycemia was linked to relief from an inflammatory state that impaired the host's response to insulin. Both restoration of immune tolerance to beta cells and relief from the adverse metabolic effects of an inflammatory state in insulin-sensitive tissues appear essential for permanent restoration of normoglycemia in this T1DM model. Thus, this triple-therapy regimen, possessing both tolerance-inducing and select antiinflammatory properties, may represent a prototype for therapies able to restore euglycemia and self-tolerance in T1DM.

Published

2007

250. Differentiation of affinity-purified human pancreatic duct cells to beta-cells.

Author

Yatoh S, Dodge R, Akashi T, Omer A, Sharma A, Weir GC, and Bonner-Weir S

Subjects

Adult, CA-19-9 Antigen, Cell Differentiation, Humans, Insulin-Secreting Cells cytology, Insulin-Secreting Cells transplantation, Pancreatic Ducts cytology, Insulin-Secreting Cells physiology, Pancreatic Ducts physiology, Stem Cells physiology

Abstract

To test whether pancreatic duct cells are in vitro progenitors, they were purified from dispersed islet-depleted human pancreatic tissue using CA19-9 antibody. The purified fraction was almost entirely CK19+ with no insulin+ cells, whereas the unpurified cells (crude duct) were 56% CK19+ and 0.4% insulin+ of total cells (0.7% of CK19+ cells). These cells were expanded as monolayers, aggregated under serum-free conditions, and transplanted into normoglycemic NOD/SCID mice. In crude duct grafts, insulin+ cells increased to 6.1% of CK19+ cells. Purified duct cells had slow expansion and poor aggregation, as well as engraftment. The addition of 0.1% cultured stromal cells improved these parameters. These stromal cells contained no CK19+ cells and no insulin by either quantitative RT-PCR or immunohistochemistry; stromal cell aggregates and grafts contained no insulin+ cells. Aggregation of purified duct plus stromal preparations induced insulin+ cells (0.1% of CK19+ cells), with further increase to 1.1% in grafts. Insulin mRNA mirrored these changes. In these grafts, all insulin+ cells were in duct-like structures, while in crude duct grafts, 85% were. Some insulin+ cells coexpressed duct markers (CK19 and CA19-9) and heat shock protein (HSP)27, a marker of nonislet cells, suggesting the transition from duct. Thus, purified duct cells from adult human pancreas can differentiate to insulin-producing cells.

Published

2007