Your search keyword '"Robert N. Bone"' showing total 34 results

1. A discovery-based proteomics approach identifies protein disulphide isomerase (PDIA1) as a biomarker of β cell stress in type 1 diabetesResearch in context

Author

Farooq Syed, Divya Singhal, Koen Raedschelders, Preethi Krishnan, Robert N. Bone, Madeline R. McLaughlin, Jennifer E. Van Eyk, Raghavendra G. Mirmira, Mei-Ling Yang, Mark J. Mamula, Huanmei Wu, Xiaowen Liu, and Carmella Evans-Molina

Subjects

β Cell stress, Type 1 diabetes, Protein disulphide isomerase A1, Proteomics, Biomarkers, Medicine, Medicine (General), R5-920

Abstract

Summary: Background: Stress responses within the β cell have been linked with both increased β cell death and accelerated immune activation in type 1 diabetes (T1D). At present, information on the timing and scope of these responses as well as disease-related changes in islet β cell protein expression during T1D development is lacking. Methods: Data independent acquisition-mass spectrometry was performed on islets collected longitudinally from NOD mice and NOD-SCID mice rendered diabetic through T cell adoptive transfer. Findings: In islets collected from female NOD mice at 10, 12, and 14 weeks of age, we found a time-restricted upregulation of proteins involved in stress mitigation and maintenance of β cell function, followed by loss of expression of protective proteins that heralded diabetes onset. EIF2 signalling and the unfolded protein response, mTOR signalling, mitochondrial function, and oxidative phosphorylation were commonly modulated pathways in both NOD mice and NOD-SCID mice rendered acutely diabetic by T cell adoptive transfer. Protein disulphide isomerase A1 (PDIA1) was upregulated in NOD islets and pancreatic sections from human organ donors with autoantibody positivity or T1D. Moreover, PDIA1 plasma levels were increased in pre-diabetic NOD mice and in the serum of children with recent-onset T1D compared to non-diabetic controls. Interpretation: We identified a core set of modulated pathways across distinct mouse models of T1D and identified PDIA1 as a potential human biomarker of β cell stress in T1D. Funding: NIH (R01DK093954, DK127308, U01DK127786, UC4DK104166, R01DK060581, R01GM118470, and 5T32DK101001-09). VA Merit Award I01BX001733. JDRF (2-SRA-2019-834-S-B, 2-SRA-2018-493-A-B, 3-PDF-20016-199-A-N, 5-CDA-2022-1176-A-N, and 3-PDF-2017-385-A-N).

Published

2023

2. Offspring of Obese Dams Exhibit Sex-Differences in Pancreatic Heparan Sulfate Glycosaminoglycans and Islet Insulin Secretion

Author

Jose Casasnovas, Christopher Luke Damron, James Jarrell, Kara S. Orr, Robert N. Bone, Stephanie Archer-Hartmann, Parastoo Azadi, and Kok Lim Kua

Subjects

islet insulin secretion, offspring of obese mothers, developmental origin of adult health and diseases, maternal obesity, heparan sulfate glycosaminoglycan, Diseases of the endocrine glands. Clinical endocrinology, RC648-665

Abstract

Offspring of obese mothers suffer higher risks of type 2 diabetes due to increased adiposity and decreased β cell function. To date, the sex-differences in offspring islet insulin secretion during early life has not been evaluated extensively, particularly prior to weaning at postnatal day 21 (P21). To determine the role of maternal obesity on offspring islet insulin secretion, C57BL/6J female dams were fed chow or western diet from 4 weeks prior to mating to induce maternal obesity. First, offspring of chow-fed and obese dams were evaluated on postnatal day 21 (P21) prior to weaning for body composition, glucose and insulin tolerance, and islet phasic insulin-secretion. Compared to same-sex controls, both male and female P21 offspring born to obese dams (MatOb) had higher body adiposity and exhibited sex-specific differences in glucose tolerance and insulin secretion. The male MatOb offspring developed the highest extent of glucose intolerance and lowest glucose-induced insulin secretion. In contrast, P21 female offspring of obese dams had unimpaired insulin secretion. Using SAX-HPLC, we found that male MatOb had a decrease in pancreatic heparan sulfate glycosaminoglycan, which is a macromolecule critical for islet health. Notably, 8-weeks-old offspring of obese dams continued to exhibit a similar pattern of sex-differences in glucose intolerance and decreased islet insulin secretion. Overall, our study suggests that maternal obesity induces sex-specific changes to pancreatic HSG in offspring and a lasting effect on offspring insulin secretion, leading to the sex-differences in glucose intolerance.

Published

2021

3. Lipid mediators and biomarkers associated with type 1 diabetes development

Author

Alexander J. Nelson, Daniel J. Stephenson, Robert N. Bone, Christopher L. Cardona, Margaret A. Park, Ying G. Tusing, Xiaoyong Lei, George Kokotos, Christina L. Graves, Clayton E. Mathews, Joanna Kramer, Martin J. Hessner, Charles E. Chalfant, and Sasanka Ramanadham

Subjects

Endocrinology, Inflammation, Medicine

Abstract

Type 1 diabetes (T1D) is a consequence of autoimmune β cell destruction, but the role of lipids in this process is unknown. We previously reported that activation of Ca2+-independent phospholipase A2β (iPLA2β) modulates polarization of macrophages (MΦ). Hydrolysis of the sn-2 substituent of glycerophospholipids by iPLA2β can lead to the generation of oxidized lipids (eicosanoids), pro- and antiinflammatory, which can initiate and amplify immune responses triggering β cell death. As MΦ are early triggers of immune responses in islets, we examined the impact of iPLA2β-derived lipids (iDLs) in spontaneous-T1D prone nonobese diabetic mice (NOD), in the context of MΦ production and plasma abundances of eicosanoids and sphingolipids. We find that (a) MΦNOD exhibit a proinflammatory lipid landscape during the prediabetic phase; (b) early inhibition or genetic reduction of iPLA2β reduces production of select proinflammatory lipids, promotes antiinflammatory MΦ phenotype, and reduces T1D incidence; (c) such lipid changes are reflected in NOD plasma during the prediabetic phase and at T1D onset; and (d) importantly, similar lipid signatures are evidenced in plasma of human subjects at high risk for developing T1D. These findings suggest that iDLs contribute to T1D onset and identify select lipids that could be targeted for therapeutics and, in conjunction with autoantibodies, serve as early biomarkers of pre-T1D.

Published

2020

4. Cigarette smoke exposure impairs β-cell function through activation of oxidative stress and ceramide accumulation

Author

Xin Tong, Zunaira Chaudhry, Chih-Chun Lee, Robert N. Bone, Sukrati Kanojia, Judith Maddatu, Paul Sohn, Staci A. Weaver, Morgan A. Robertson, Irina Petrache, Carmella Evans-Molina, and Tatsuyoshi Kono

Subjects

Ceramide, Smoking, Insulin secretion, Oxidative stress, β-cell, Type 2 diabetes, Internal medicine, RC31-1245

Abstract

Objectives: Epidemiological studies indicate that first- and second-hand cigarette smoke (CS) exposure are important risk factors for the development of type 2 diabetes (T2D). Additionally, elevated diabetes risk has been reported to occur within a short period of time after smoking cessation, and health risks associated with smoking are increased when combined with obesity. At present, the mechanisms underlying these associations remain incompletely understood. The objective of this study was to test the impact of CS exposure on pancreatic β-cell function using rodent and in vitro models. Methods: Beginning at 8 weeks of age, C57BL/6 J mice were concurrently fed a high-fat diet (HFD) and exposed to CS for 11 weeks, followed by an additional 11 weeks of smoking cessation with continued HFD. Glucose tolerance testing was performed during CS exposure and during the cessation period. Cultured INS-1 β-cells and primary islets were exposed ex vivo to CS extract (CSE), and β-cell function and viability were tested. Since CS increases ceramide accumulation in the lung and these bioactive sphingolipids have been implicated in pancreatic β-cell dysfunction in diabetes, islet and β-cell sphingolipid levels were measured in islets from CS-exposed mice and in CSE-treated islets and INS-1 cells using liquid chromatography-tandem mass spectrometry. Results: Compared to HFD-fed, ambient air-exposed mice, HFD-fed and CS-exposed mice had reduced weight gain and better glucose tolerance during the active smoking period. Following smoking cessation, CS-mice exhibited rapid weight gain and had accelerated worsening of their glucose tolerance. CS-exposed mice had higher serum proinsulin/insulin ratios, indicative of β-cell dysfunction, significantly lower β-cell mass (p = 0.017), reduced β-cell proliferation (p = 0.006), and increased islet ceramide content compared to non-smoking control mice. Ex vivo exposure of isolated islets to CSE was sufficient to increase islet ceramide levels, which was correlated with reduced insulin gene expression and glucose-stimulated insulin secretion, and increased β-cell oxidative and endoplasmic reticulum (ER) stress. Treatment with the antioxidant N-acetylcysteine markedly attenuated the effects of CSE on ceramide levels, restored β-cell function and survival, and increased cyclin D2 expression, while also reducing activation of β-cell ER and oxidative stress. Conclusions: Our results indicate that CS exposure leads to impaired insulin production, processing, secretion and reduced β-cell viability and proliferation. These effects were linked to increased β-cell oxidative and ER stress and ceramide accumulation. Mice fed HFD continued to experience detrimental effects of CS exposure even during smoking cessation. Elucidation of the mechanisms by which CS exposure impairs β-cell function in synergy with obesity will help design therapeutic and preventive interventions for both active and former smokers.

Published

2020

5. Calcium-independent phospholipases A2 and their roles in biological processes and diseases

Author

Sasanka Ramanadham, Tomader Ali, Jason W. Ashley, Robert N. Bone, William D. Hancock, and Xiaoyong Lei

Subjects

signaling, membrane homeostasis, arachidonic acid, eicosanoids, docosahexaenoic acid, inflammation, Biochemistry, QD415-436

Abstract

Among the family of phospholipases A2 (PLA2s) are the Ca2+-independent PLA2s (iPLA2s) and they are designated group VI iPLA2s. In relation to secretory and cytosolic PLA2s, the iPLA2s are more recently described and details of their expression and roles in biological functions are rapidly emerging. The iPLA2s or patatin-like phospholipases (PNPLAs) are intracellular enzymes that do not require Ca2+ for activity, and contain lipase (GXSXG) and nucleotide-binding (GXGXXG) consensus sequences. Though nine PNPLAs have been recognized, PNPLA8 (membrane-associated iPLA2γ) and PNPLA9 (cytosol-associated iPLA2β) are the most widely studied and understood. The iPLA2s manifest a variety of activities in addition to phospholipase, are ubiquitously expressed, and participate in a multitude of biological processes, including fat catabolism, cell differentiation, maintenance of mitochondrial integrity, phospholipid remodeling, cell proliferation, signal transduction, and cell death. As might be expected, increased or decreased expression of iPLA2s can have profound effects on the metabolic state, CNS function, cardiovascular performance, and cell survival; therefore, dysregulation of iPLA2s can be a critical factor in the development of many diseases. This review is aimed at providing a general framework of the current understanding of the iPLA2s and discussion of the potential mechanisms of action of the iPLA2s and related involved lipid mediators.

Published

2015

6. The Chd4 helicase regulates chromatin accessibility and gene expression critical for β-cell function in vivo

Author

Rebecca K. Davidson, Sukrati Kanojia, Wenting Wu, Tatsuyoshi Kono, Jerry Xu, Meredith Osmulski, Robert N. Bone, Nolan Casey, Carmella Evans-Molina, Emily K. Sims, and Jason M. Spaeth

Subjects

Endocrinology, Diabetes and Metabolism, Internal Medicine

Abstract

The transcriptional activity of Pdx1 is modulated by a diverse array of coregulatory factors that govern chromatin accessibility, histone modifications, and nucleosome distribution. We previously identified the Chd4 subunit of the nucleosome remodeling and deacetylase complex as a Pdx1-interacting factor. To identify how loss of Chd4 impacts glucose homeostasis and gene expression programs in β-cells in vivo, we generated an inducible β-cell–specific Chd4 knockout mouse model. Removal of Chd4 from mature islet β-cells rendered mutant animals glucose intolerant, in part due to defects in insulin secretion. We observed an increased ratio of immature-to-mature insulin granules in Chd4-deficient β-cells that correlated with elevated levels of proinsulin both within isolated islets and from plasma following glucose stimulation in vivo. RNA sequencing and assay for transposase-accessible chromatin with sequencing showed that lineage-labeled Chd4-deficient β-cells have alterations in chromatin accessibility and altered expression of genes critical for β-cell function, including MafA, Slc2a2, Chga, and Chgb. Knockdown of CHD4 from a human β-cell line revealed similar defects in insulin secretion and alterations in several β-cell–enriched gene targets. These results illustrate how critical Chd4 activities are in controlling genes essential for maintaining β-cell function. Article Highlights Pdx1–Chd4 interactions were previously shown to be compromised in β-cells from human donors with type 2 diabetes. β-Cell–specific removal of Chd4 impairs insulin secretion and leads to glucose intolerance in mice. Expression of key β-cell functional genes and chromatin accessibility are compromised in Chd4-deficient β-cells. Chromatin remodeling activities enacted by Chd4 are essential for β-cell function under normal physiological conditions.

Published

2023

7. The Determination Trial Impact on Upfront (vs Delayed) Autologous Stem Cell Transplantation for Transplant-Eligible Newly Diagnosed Multiple Myeloma

Author

Brooke Dulka, Robert N. Bone, Yolaine Jeune-Smith, Muhamed Baljevic, and Bruce A. Feinberg

Subjects

Immunology, Cell Biology, Hematology, Biochemistry

Published

2022

8. Provider Perceptions of Shine and Ibrutinib, Bendamustine, and Rituximab in the First-Line Setting

Author

Samuel C. Baird, Robert N. Bone, Yolaine Jeune-Smith, Bruce A. Feinberg, and Muhamed Baljevic

Subjects

Immunology, Cell Biology, Hematology, Biochemistry

Published

2022

9. SERCA2 regulates proinsulin processing and processing enzyme maturation in the pancreatic β cell

Author

Hitoshi Iida, Tatsuyoshi Kono, Chih-Chun Lee, Preethi Krishnan, Matthew C. Arvin, Staci A. Weaver, Timothy S. Jarvela, Robert N. Bone, Xin Tong, Peter Arvan, Iris Lindberg, and Carmella Evans-Molina

Abstract

Increased circulating levels of incompletely processed insulin (i.e. proinsulin) are observed clinically in both type 1 and type 2 diabetes; however, the mechanisms underlying impaired proinsulin processing remain incompletely understood. Here, we identify the sarcoendoplasmic reticulum Ca2+ ATPase-2 (SERCA2) pump and β cell ER Ca2+ as key regulators of systemic glucose tolerance and proinsulin processing. We generated mice with a β cell-specific SERCA2 deletion (βS2KO) and SERCA2 deficient INS-1 cells to show that SERCA2 loss increases systemic and pancreatic levels of proinsulin protein and leads to aberrant localization of proinsulin within the proximal β cell secretory pathway. These defects in proinsulin processing were linked to reduced maturation of the proinsulin processing enzymes PC1/3 and PC2, suggesting a model whereby chronic ER Ca2+ depletion in the β cell, which is observed in many pathological conditions, impairs the spatial regulation of prohormone trafficking, processing, and maturation within the β cell secretory pathway.

Published

2022

10. A Computational Approach for Defining a Signature of β-Cell Golgi Stress in Diabetes

Author

Farooq Syed, Huanmei Wu, Olufunmilola Oyebamiji, Carmella Evans-Molina, Robert N. Bone, Preethi Krishnan, Sayali Talware, and Sharmila Selvaraj

Subjects

0301 basic medicine, endocrine system diseases, Microarray, Endocrinology, Diabetes and Metabolism, Cell, Protein Array Analysis, Golgi Apparatus, 030209 endocrinology & metabolism, Computational biology, Biology, Models, Biological, Islets of Langerhans, 03 medical and health sciences, symbols.namesake, chemistry.chemical_compound, 0302 clinical medicine, Stress, Physiological, Organelle, Internal Medicine, medicine, Humans, Computer Simulation, Gene, RNA, Golgi apparatus, Brefeldin A, Diabetes Mellitus, Type 1, 030104 developmental biology, medicine.anatomical_structure, Diabetes Mellitus, Type 2, Gene Expression Regulation, Islet Studies, chemistry, symbols, Insulin processing

Abstract

The Golgi apparatus (GA) is an important site of insulin processing and granule maturation, but whether GA organelle dysfunction and GA stress are present in the diabetic β-cell has not been tested. We used an informatics-based approach to develop a transcriptional signature of β-cell GA stress using existing RNA sequencing and microarray data sets generated using human islets from donors with diabetes and islets where type 1 (T1D) and type 2 (T2D) diabetes had been modeled ex vivo. To narrow our results to GA-specific genes, we applied a filter set of 1,030 genes accepted as GA associated. In parallel, we generated an RNA-sequencing data set from human islets treated with brefeldin A (BFA), a known GA stress inducer. Overlapping the T1D and T2D groups with the BFA data set, we identified 120 and 204 differentially expressed genes, respectively. In both the T1D and T2D models, pathway analyses revealed that the top pathways were associated with GA integrity, organization, and trafficking. Quantitative RT-PCR was used to validate a common signature of GA stress that included ATF3, ARF4, CREB3, and COG6. Taken together, these data indicate that GA-associated genes are dysregulated in diabetes and identify putative markers of β-cell GA stress.

Published

2020

11. Loss of Secretory Pathway Ca2+ ATPase (SPCA1) Impairs Insulin Secretion and Reduces Autophagy in the Pancreatic Islet

Author

Charanya Muralidharan, Tatsuyoshi Kono, Xin Tong, Staci A. Weaver, Robert N. Bone, Preethi Krishnan, and Carmella Evans-Molina

Subjects

Autophagosome, Chemistry, Insulin, medicine.medical_treatment, Autophagy, Golgi apparatus, Cell biology, symbols.namesake, medicine, symbols, Intracellular, Secretory pathway, Homeostasis, Proinsulin

Abstract

The β cell Golgi apparatus serves as a significant store of intracellular Ca2+ and an important site of proinsulin maturation. However, the contribution of Golgi Ca2+ to diabetes pathophysiology is unknown. The Golgi primarily utilizes the Secretory Pathway Ca2+ ATPase (SPCA1) to maintain intraluminal Ca2+ stores, and loss of SPCA1 has been linked to impaired Golgi function in other cell types. Here, we demonstrated that SPCA1 expression is decreased in islets from diabetic mice and human organ donors with type 2 diabetes, suggesting SPCA1 may impact diabetes development. INS-1 β cells lacking SPCA1 (SPCA1KO) showed reduced intraluminal Golgi Ca2+ levels, reduced glucose-stimulated insulin secretion (GSIS), and increased insulin content. Islets from SPCA1 haploinsufficient mice (SPCA1+/-) exhibited reduced GSIS, altered glucose-induced Ca2+ oscillations, and altered insulin granule maturation. Autophagy can regulate granule homeostasis, therefore we induced autophagy with Torin1 and found that SPCA1KO cells and SPCA1+/- islets had reduced levels of the autophagosome marker LC3-II. Furthermore, SPCA1KO LC3-II were unchanged after blocking autophagy initiation or autophagolysosome fusion and acidification. Thus, we concluded that β cell SPCA1 plays an important role in the maintenance of Golgi Ca2+ homeostasis and reduced Golgi Ca2+ impairs autophagy initiation and may impact insulin granule homeostasis.

Published

2021

12. Endoplasmic reticulum stress alters ryanodine receptor function in the murine pancreatic β cell

Author

Tatsuyoshi Kono, Paul Sohn, Xin Tong, Carmella Evans-Molina, Farooq Syed, Wataru Yamamoto, Aruna B. Wijeratne, Amber L. Mosley, Jason D. True, Robert N. Bone, and Christopher A. Reissaus

Subjects

Male, 0301 basic medicine, Macrocyclic Compounds, Biochemistry, Cell Line, Mice, 03 medical and health sciences, chemistry.chemical_compound, Insulin-Secreting Cells, Diabetes Mellitus, Animals, Inositol, Calcium Signaling, Receptor, Oxazoles, Molecular Biology, Calcium signaling, 030102 biochemistry & molecular biology, Ryanodine receptor, Tunicamycin, Endoplasmic reticulum, Ryanodine Receptor Calcium Release Channel, Depolarization, Cell Biology, Endoplasmic Reticulum Stress, Mice, Mutant Strains, Cell biology, Metabolism, 030104 developmental biology, chemistry, Unfolded Protein Response, Unfolded protein response, Intracellular

Abstract

Alterations in endoplasmic reticulum (ER) calcium (Ca(2+)) levels diminish insulin secretion and reduce β-cell survival in both major forms of diabetes. The mechanisms responsible for ER Ca(2+) loss in β cells remain incompletely understood. Moreover, a specific role for either ryanodine receptor (RyR) or inositol 1,4,5-triphosphate receptor (IP(3)R) dysfunction in the pathophysiology of diabetes remains largely untested. To this end, here we applied intracellular and ER Ca(2+) imaging techniques in INS-1 β cells and isolated islets to determine whether diabetogenic stressors alter RyR or IP(3)R function. Our results revealed that the RyR is sensitive mainly to ER stress–induced dysfunction, whereas cytokine stress specifically alters IP(3)R activity. Consistent with this observation, pharmacological inhibition of the RyR with ryanodine and inhibition of the IP(3)R with xestospongin C prevented ER Ca(2+) loss under ER and cytokine stress conditions, respectively. However, RyR blockade distinctly prevented β-cell death, propagation of the unfolded protein response (UPR), and dysfunctional glucose-induced Ca(2+) oscillations in tunicamycin-treated INS-1 β cells and mouse islets and Akita islets. Monitoring at the single-cell level revealed that ER stress acutely increases the frequency of intracellular Ca(2+) transients that depend on both ER Ca(2+) leakage from the RyR and plasma membrane depolarization. Collectively, these findings indicate that RyR dysfunction shapes ER Ca(2+) dynamics in β cells and regulates both UPR activation and cell death, suggesting that RyR-mediated loss of ER Ca(2+) may be an early pathogenic event in diabetes.

Published

2019

13. 1240-P: Changes in Protein Expression during Islet Regeneration in a Cystic Fibrosis-Related Diabetes (CFRD) Ferret Model

Author

Carmella Evans-Molina, Robert N. Bone, Heba M. Ismail, and Raghavendra G. Mirmira

Subjects

medicine.medical_specialty, geography, geography.geographical_feature_category, biology, business.industry, Endocrinology, Diabetes and Metabolism, Insulin, medicine.medical_treatment, Cystic fibrosis-related diabetes, medicine.disease, Islet, Glucagon, Cystic fibrosis, Cystic fibrosis transmembrane conductance regulator, Endocrinology, Diabetes mellitus, Internal medicine, Internal Medicine, medicine, biology.protein, business, Hormone

Abstract

Diabetes is a common complication among persons with cystic fibrosis (CF), affecting nearly 20% of adolescents and 50% of all adults with CF. The Cystic Fibrosis Transmembrane Conductance Regulator (CFTR) knockout (KO) ferret is a well-characterized animal model of CF that exhibits distinct periods of dysglycemia and pancreatic remodeling that are similar to patterns observed in humans. After the first month of life (normoglycemia/Phase I), hyperglycemia develops during the second month of life (Phase II) with reduced islet mass, followed by a period of near normoglycemia (Phase III) during which the islet mass regenerates, followed by persistent hyperglycemia/CFRD at the 4th month of life (Phase IV). While dynamic changes in islet hormone mRNA levels have been described across these phases, changes in protein expression patterns have not been characterized. To this end, immunofluorescence was performed to characterize islet hormone expression patterns in age-matched CFTR KO and wild type (WT) ferrets, focusing on the regenerative Phase III. The relative intensity of immunofluorescent staining per islet area was calculated. Compared to WT ferrets, the relative staining intensity of insulin and glucagon increased (4.687 vs. 3.228, p Disclosure H. M. Ismail: None. R. G. Mirmira: Advisory Panel; Self; Hibercell Inc., Sigilon Therapeutics, Inc., Veralox Therapeutics, Employee; Spouse/Partner; Beta Bionics, Inc. C. Evans-molina: Advisory Panel; Self; Provention Bio, Inc., Consultant; Self; Dompe, Other Relationship; Self; Bristol-Myers Squibb Company, Nimbus Pharmaceuticals, Pfizer Inc. R. N. Bone: None.

Published

2021

14. 288-OR: Role of Endoplasmic Reticulum (ER) Calcium in ß-Cell Senescence and Type 1 Diabetes Pathophysiology

Author

Tatsuyoshi Kono, Staci A. Weaver, Robert N. Bone, Farooq Syed, and Carmella Evans-Molina

Subjects

Senescence, Type 1 diabetes, Endocrinology, Diabetes and Metabolism, Endoplasmic reticulum, chemistry.chemical_element, Calcium, Biology, medicine.disease, S cell, Pathophysiology, Cell biology, chemistry, Internal Medicine, medicine

Abstract

Type 1 diabetes (T1D) results from immune-mediated destruction of pancreatic β cells. Recent data suggest that activation of senescence and acquisition of a senescence-associated secretory phenotype (SASP) by β cells may contribute to T1D pathogenesis; however, the molecular mechanisms responsible for this phenotype are not well understood. Our previous work has linked loss of β cell ER Ca2+ with diabetes pathophysiology and demonstrated accelerated onset of hyperglycemia in non-obese diabetic (NOD) mice with haploinsufficiency of the SERCA2 pump (NOD-S2+/-). Therefore, we hypothesized that loss of ER Ca2+ via reduced SERCA2 activity may drive β cell senescence, SASP, mitochondrial dysfunction and T1D development. To test this hypothesis, SERCA2 KO INS-1 β cells (S2KO) and islets from NOD-S2+/- mice were assessed for senescence associated β-galactosidase staining (SA-β-gal), mRNA expression of senescence markers cdkn1a and cdkn2a, mitochondrial membrane potential and function (TMRM, Seahorse) as well as mitochondrial DNA copy number. S2KO β cells displayed increased SA-β-gal staining as well as increased mitochondrial coupling efficiency and baseline mitochondrial copy number compared to WT β cells, suggesting a senescence phenotype, and altered mitochondrial function. Pancreatic islets isolated from NOD-S2+/- mice show increased mRNA expression of the senescence marker cdkn2a at 12wks compared to age matched control mice (p Disclosure S. A. Weaver: None. T. Kono: None. F. Syed: None. R. N. Bone: None. C. Evans-molina: Advisory Panel; Self; Provention Bio, Inc., Consultant; Self; Dompe, Other Relationship; Self; Bristol-Myers Squibb Company, Nimbus Pharmaceuticals, Pfizer Inc. Funding Indiana Clinical and Translational Sciences Institute (UL1TR002529)

Published

2021

15. Offspring of Obese Dams Exhibit Sex-Differences in Pancreatic Heparan Sulfate Glycosaminoglycans and Islet Insulin Secretion

Author

Christopher Luke Damron, Kara S. Orr, Stephanie A. Archer-Hartmann, Parastoo Azadi, Kok Lim Kua, Robert N. Bone, James Jarrell, and Jose Casasnovas

Subjects

0301 basic medicine, Male, Endocrinology, Diabetes and Metabolism, Type 2 diabetes, Glycosaminoglycan, Obesity, Maternal, chemistry.chemical_compound, 0302 clinical medicine, Endocrinology, Pregnancy, Insulin Secretion, Insulin, heparan sulfate glycosaminoglycan, Adiposity, Glycosaminoglycans, Original Research, geography.geographical_feature_category, Heparan sulfate, Islet, maternal obesity, Prenatal Exposure Delayed Effects, Female, medicine.medical_specialty, Offspring, offspring of obese mothers, 030209 endocrinology & metabolism, Diet, High-Fat, Diseases of the endocrine glands. Clinical endocrinology, 03 medical and health sciences, Islets of Langerhans, Sex Factors, Internal medicine, Glucose Intolerance, medicine, Weaning, Animals, Humans, Insulin secretion, developmental origin of adult health and diseases, Pancreas, geography, islet insulin secretion, business.industry, medicine.disease, RC648-665, Obesity, Mice, Inbred C57BL, 030104 developmental biology, Glucose, chemistry, Heparitin Sulfate, business

Abstract

Offspring of obese mothers suffer higher risks of type 2 diabetes due to increased adiposity and decreased β cell function. To date, the sex-differences in offspring islet insulin secretion during early life has not been evaluated extensively, particularly prior to weaning at postnatal day 21 (P21). To determine the role of maternal obesity on offspring islet insulin secretion, C57BL/6J female dams were fed chow or western diet from 4 weeks prior to mating to induce maternal obesity. First, offspring of chow-fed and obese dams were evaluated on postnatal day 21 (P21) prior to weaning for body composition, glucose and insulin tolerance, and islet phasic insulin-secretion. Compared to same-sex controls, both male and female P21 offspring born to obese dams (MatOb) had higher body adiposity and exhibited sex-specific differences in glucose tolerance and insulin secretion. The male MatOb offspring developed the highest extent of glucose intolerance and lowest glucose-induced insulin secretion. In contrast, P21 female offspring of obese dams had unimpaired insulin secretion. Using SAX-HPLC, we found that male MatOb had a decrease in pancreatic heparan sulfate glycosaminoglycan, which is a macromolecule critical for islet health. Notably, 8-weeks-old offspring of obese dams continued to exhibit a similar pattern of sex-differences in glucose intolerance and decreased islet insulin secretion. Overall, our study suggests that maternal obesity induces sex-specific changes to pancreatic HSG in offspring and a lasting effect on offspring insulin secretion, leading to the sex-differences in glucose intolerance.

Published

2021

16. Nmp4, a Regulator of Induced Osteoanabolism, Also Influences Insulin Secretion and Sensitivity

Author

Emily G. Atkinson, Ronald C. Wek, Amy Creecy, Angela Klunk, Joseph P. Bidwell, Sarah A. Tersey, Michele Adaway, Alexander G. Robling, Carmella Evans-Molina, Robert N. Bone, and Joseph M. Wallace

Subjects

Male, medicine.medical_specialty, Anabolism, Normal diet, Endocrinology, Diabetes and Metabolism, Glucose uptake, Osteoporosis, Type 2 diabetes, Diet, High-Fat, Article, Mice, Endocrinology, Nuclear Matrix-Associated Proteins, Internal medicine, Insulin Secretion, medicine, Animals, Humans, Insulin, Orthopedics and Sports Medicine, Glycolysis, Mice, Knockout, business.industry, medicine.disease, Obesity, Mice, Inbred C57BL, Diabetes Mellitus, Type 2, Parathyroid Hormone, medicine.symptom, Insulin Resistance, business, Weight gain, Transcription Factors

Abstract

A bidirectional and complex relationship exists between bone and glycemia. Persons with type 2 diabetes (T2D) are at risk for bone loss and fracture, however, heightened osteoanabolism may ameliorate T2D-induced deficits in glycemia as bone-forming osteoblasts contribute to energy metabolism via increased glucose uptake and cellular glycolysis. Mice globally lacking Nuclear Matrix Protein 4 (Nmp4), a transcription factor expressed in all tissues and conserved between humans and rodents, are healthy and exhibit enhanced bone formation in response to anabolic osteoporosis therapies. To test whether loss of Nmp4 similarly impacted bone deficits caused by diet induced obesity, male wild type (WT) and Nmp4(−/−) mice (8wks) were fed either low-fat diet (LFD) or high-fat diet (HFD) for 12wks. Endpoint parameters included bone architecture, structural and estimated tissue level mechanical properties, body weight/composition, glucose-stimulated insulin secretion, glucose tolerance, insulin tolerance and metabolic cage analysis. HFD diminished bone architecture and ultimate force and stiffness equally in both genotypes. Unexpectedly, the Nmp4(−/−) mice exhibited deficits in pancreatic β-cell function and were modestly glucose intolerant under normal diet conditions. Despite the β-cell deficits, the Nmp4(−/−) mice were less sensitive to HFD-induced weight gain, increases in % fat mass, and decreases in glucose tolerance and insulin sensitivity. We conclude that Nmp4 supports pancreatic β-cell function but suppresses peripheral glucose utilization, perhaps contributing to its suppression of induced skeletal anabolism. Selective disruption of Nmp4 in peripheral tissues may provide a strategy for improving both induced osteoanabolism and energy metabolism in comorbid patients.

Published

2021

17. 2112-P: Sarco/Endoplasmic Reticulum ATPase (SERCA2) Deficiency in the Nonobese Diabetic (NOD) Mouse Accelerates Type 1 Diabetes Development

Author

Robert N. Bone, Carmella Evans-Molina, Tatsuyoshi Kono, and Christopher A. Reissaus

Subjects

0301 basic medicine, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, ATPase, Cell, 030209 endocrinology & metabolism, Nod, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Diabetes mellitus, Internal Medicine, medicine, geography, geography.geographical_feature_category, biology, Chemistry, Endoplasmic reticulum, Wild type, Islet, medicine.disease, 030104 developmental biology, Endocrinology, medicine.anatomical_structure, biology.protein, Unfolded protein response

Abstract

Recent evidence has implicated pathways intrinsic to the β cell, such as endoplasmic reticulum (ER) stress, as potential triggers of T1D. ER stress is increased by the loss of ER Ca2+, leading to decreased β cell function and increased β cell apoptosis. Maintenance of intraluminal ER Ca2+ stores is primarily regulated by the sarco/endoplasmic reticulum Ca2+ ATPase (SERCA2) pump, and we have shown that β cell SERCA2 expression is reduced in islets from mouse models of T1D prior to, and after, disease onset. Thus, we hypothesized that SERCA2-mediated ER Ca2+ dyshomeostasis could be a major contributor to T1D development. To test this, we generated a mouse model haploinsufficient for SERCA2 on the NOD background (NOD-S2+/-). Compared to wild type littermates (NOD-WT), NOD-S2+/- mice had a higher incidence of diabetes (p Disclosure R.N. Bone: None. C.A. Reissaus: None. T. Kono: None. C. Evans-Molina: Consultant; Self; Bristol-Myers Squibb.

Published

2020

18. Lipid mediators and biomarkers associated with type 1 diabetes development

Author

Joanna Kramer, George Kokotos, Charles E. Chalfant, Sasanka Ramanadham, Martin J. Hessner, Alexander J. Nelson, Christopher L. Cardona, Clayton E. Mathews, Margaret A. Park, Daniel J. Stephenson, Xiaoyong Lei, Robert N. Bone, Ying Gai Tusing, and Christina L. Graves

Subjects

0301 basic medicine, Male, endocrine system diseases, Adolescent, Autoimmune diseases, Inflammation, Nod, Phospholipase, Naphthalenes, Proinflammatory cytokine, 03 medical and health sciences, 0302 clinical medicine, Immune system, Endocrinology, Mice, Inbred NOD, medicine, Animals, Humans, Child, Chemistry, Group IV Phospholipases A2, Macrophages, Fatty Acids, Diabetes, Autoantibody, General Medicine, Lipid signaling, Ketones, Lipid Metabolism, Sphingolipid, Lipids, Mice, Inbred C57BL, 030104 developmental biology, Diabetes Mellitus, Type 1, 030220 oncology & carcinogenesis, Immunology, Macrophages, Peritoneal, Medicine, Eicosanoids, lipids (amino acids, peptides, and proteins), Female, medicine.symptom, Biomarkers, Research Article

Abstract

Type 1 diabetes (T1D) is a consequence of autoimmune β cell destruction, but the role of lipids in this process is unknown. We previously reported that activation of Ca2+-independent phospholipase A2β (iPLA2β) modulates polarization of macrophages (MΦ). Hydrolysis of the sn-2 substituent of glycerophospholipids by iPLA2β can lead to the generation of oxidized lipids (eicosanoids), pro- and antiinflammatory, which can initiate and amplify immune responses triggering β cell death. As MΦ are early triggers of immune responses in islets, we examined the impact of iPLA2β-derived lipids (iDLs) in spontaneous-T1D prone nonobese diabetic mice (NOD), in the context of MΦ production and plasma abundances of eicosanoids and sphingolipids. We find that (a) MΦNOD exhibit a proinflammatory lipid landscape during the prediabetic phase; (b) early inhibition or genetic reduction of iPLA2β reduces production of select proinflammatory lipids, promotes antiinflammatory MΦ phenotype, and reduces T1D incidence; (c) such lipid changes are reflected in NOD plasma during the prediabetic phase and at T1D onset; and (d) importantly, similar lipid signatures are evidenced in plasma of human subjects at high risk for developing T1D. These findings suggest that iDLs contribute to T1D onset and identify select lipids that could be targeted for therapeutics and, in conjunction with autoantibodies, serve as early biomarkers of pre-T1D., Lipid signaling contributes to type 1 diabetes onset and may provide therapeutic targets and biomarkers for disease.

Published

2020

19. A high-fat diet catalyzes progression to hyperglycemia in mice with selective impairment of insulin action in Glut4-expressing tissues

Author

Daniel J. Horan, Hyun Cheol Roh, Aaron C. Ericsson, Surabhi D. Abhyankar, Natalie D. Stull, Xiaocheng C. Dong, Alexander G. Robling, Hongxia Ren, Robert N. Bone, Austin M. Reilly, Shijun Yan, Jason M. Conley, Carmella Evans-Molina, and Menghao Huang

Subjects

insulin receptor (INSR), HFD, high-fat diet, OGTT, oral glucose tolerance test, medicine.medical_treatment, Glucose uptake, ROI, region of interest, Type 2 diabetes, Biochemistry, type 2 diabetes (T2DM), Insr, insulin receptor, Mice, insulin resistance, Hyperinsulinemia, Insulin, glucose transporter type 4 (GLUT4), Mice, Knockout, Glucose Transporter Type 4, diabetes, biology, GLUT4, glucose transporter type 4, GIRKO, GLUT4 promoter-driven insulin receptor knockout, FFPE, formalin-fixed paraffin-embedded, IPGTT, intraperitoneal glucose tolerance test, LPS, lipopolysaccharide, MIRKO, muscle-Insr-KO, Research Article, medicine.medical_specialty, glucose metabolism, T2D, type 2 diabetes, Diet, High-Fat, GSIS, glucose-stimulated insulin secretion, Insulin resistance, Diabetes mellitus, Internal medicine, Glucose Intolerance, medicine, Animals, Molecular Biology, micro-CT, micro-computed tomography, NCD, normal chow diet, business.industry, VLDL, very-low-density lipoprotein, nutritional and metabolic diseases, DIO, diet-induced obesity, Cell Biology, medicine.disease, Mice, Inbred C57BL, FIRKO, fat-Insr-KO, Insulin receptor, Endocrinology, Diabetes Mellitus, Type 2, Hyperglycemia, biology.protein, diet, business, metabolism, GLUT4

Abstract

Insulin resistance impairs postprandial glucose uptake through glucose transporter type 4 (GLUT4) and is the primary defect preceding type 2 diabetes. We previously generated an insulin-resistant mouse model with human GLUT4 promoter-driven insulin receptor knockout (GIRKO) in the muscle, adipose, and neuronal subpopulations. However, the rate of diabetes in GIRKO mice remained low prior to 6 months of age on normal chow diet (NCD), suggesting that additional factors/mechanisms are responsible for adverse metabolic effects driving the ultimate progression of overt diabetes. In this study, we characterized the metabolic phenotypes of the adult GIRKO mice acutely switched to high-fat diet (HFD) feeding in order to identify additional metabolic challenges required for disease progression. Distinct from other diet-induced obesity (DIO) and genetic models (e.g., db/db mice), GIRKO mice remained leaner on HFD feeding, but developed other cardinal features of insulin resistance syndrome. GIRKO mice rapidly developed hyperglycemia despite compensatory increases in β-cell mass and hyperinsulinemia. Furthermore, GIRKO mice also had impaired oral glucose tolerance and a limited glucose-lowering benefit from exendin-4, suggesting that the blunted incretin effect contributed to hyperglycemia. Secondly, GIRKO mice manifested severe dyslipidemia while on HFD due to elevated hepatic lipid secretion, serum triglyceride concentration, and lipid droplet accumulation in hepatocytes. Thirdly, GIRKO mice on HFD had increased inflammatory cues in the gut, which were associated with the HFD-induced microbiome alterations and increased serum lipopolysaccharide (LPS). In conclusion, our studies identified important gene/diet interactions contributing to diabetes progression, which might be leveraged to develop more efficacious therapies.

Published

2022

20. Impaired Store-Operated Calcium Entry and STIM1 Loss Lead to Reduced Insulin Secretion and Increased Endoplasmic Reticulum Stress in the Diabetic β-Cell

Author

Chih-Chun Lee, Michael W. Roe, Tatsuyoshi Kono, Paul Sohn, Xin Tong, Hitoshi Iida, Patrick Gilon, Solaema Taleb, Carmella Evans-Molina, and Robert N. Bone

Subjects

0301 basic medicine, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, Type 2 diabetes, Cell Line, Diabetes Mellitus, Experimental, Proinflammatory cytokine, Mice, 03 medical and health sciences, Insulin-Secreting Cells, Internal medicine, Internal Medicine, medicine, Animals, Humans, Insulin, Stromal Interaction Molecule 1, Calcium metabolism, geography, geography.geographical_feature_category, Chemistry, Endoplasmic reticulum, STIM1, Endoplasmic Reticulum Stress, Islet, medicine.disease, Store-operated calcium entry, Rats, Glucose, 030104 developmental biology, Endocrinology, Islet Studies, Unfolded protein response, Calcium

Abstract

Store-operated Ca2+ entry (SOCE) is a dynamic process that leads to refilling of endoplasmic reticulum (ER) Ca2+ stores through reversible gating of plasma membrane Ca2+ channels by the ER Ca2+ sensor Stromal Interaction Molecule 1 (STIM1). Pathogenic reductions in β-cell ER Ca2+ have been observed in diabetes. However, a role for impaired SOCE in this phenotype has not been tested. We measured the expression of SOCE molecular components in human and rodent models of diabetes and found a specific reduction in STIM1 mRNA and protein levels in human islets from donors with type 2 diabetes (T2D), islets from hyperglycemic streptozotocin-treated mice, and INS-1 cells (rat insulinoma cells) treated with proinflammatory cytokines and palmitate. Pharmacologic SOCE inhibitors led to impaired islet Ca2+ oscillations and insulin secretion, and these effects were phenocopied by β-cell STIM1 deletion. STIM1 deletion also led to reduced ER Ca2+ storage and increased ER stress, whereas STIM1 gain of function rescued β-cell survival under proinflammatory conditions and improved insulin secretion in human islets from donors with T2D. Taken together, these data suggest that the loss of STIM1 and impaired SOCE contribute to ER Ca2+ dyshomeostasis under diabetic conditions, whereas efforts to restore SOCE-mediated Ca2+ transients may have the potential to improve β-cell health and function.

Published

2018

21. 68722 Role of ER calcium in beta cell senescence and diabetes pathophysiology

Author

Staci A. Weaver, Robert N. Bone, Farooq Syed, Carmella Evans-Molina, and Tatsuyoshi Kono

Subjects

Senescence, geography, geography.geographical_feature_category, Cell, General Medicine, Biology, Islet, Phenotype, Cell biology, Pathogenesis, medicine.anatomical_structure, CDKN2A, medicine, Beta cell, Haploinsufficiency

Abstract

IMPACT: The proposed study has the potential to inform new paradigms of type 1 diabetes prevention and therapy with the overall goal of improving β cell health during autoimmunity. OBJECTIVES/GOALS: Type 1 diabetes (T1D) results from immune-mediated destruction of pancreatic βcells. Recent data suggest that activation of senescence and acquisition of a senescence associated secretory phenotype (SASP) by βcells may contribute to T1D pathogenesis. However, the molecular mechanisms responsible for this phenotype are not well understood. METHODS/STUDY POPULATION: We hypothesize that loss of endoplasmic reticulum (ER) Ca2+ induces βcell senescence, SASP as well as mitochondrial dysfunction which drive T1D development. The current study utilizes SERCA2 KO INS-1 βcells (S2KO) exhibiting loss of ER Ca2+ and a SERCA2 haploinsufficient mice on a non-obese diabetic background (NOD-S2+/-) to test the role of ER Ca2+ loss during T1D development. Senescence associated βgalactosidase staining (SA-βgal), expression of senescence markers (RT-qPCR), mitochondrial function (Seahorse, TMRM) and mitochondrial copy number (qPCR) were all measured in S2KO versus WT βcells and are currently being measured in the NOD-S2+/- mouse model at 6, 8, 12, 14, and 16wks of age. RESULTS/ANTICIPATED RESULTS: RT-qPCR assays detecting senescence markers cdkn1a and cdkn2a and mitochondrial specific genes cox1 and nd1 were developed and validated in both INS-1 βcells and mouse islets. Mitochondrial function assay (Seahorse) was optimized for use in INS-1 βcells and is currently under development for use in intact mouse islets. S2KO βcells displayed increased SA- βgal staining as well as increased mitochondrial coupling efficiency (p=0.0146) and baseline mitochondrial copy number (p=0.0053) compared to WT βcells, suggesting a senescence phenotype and altered mitochondrial function. NOD-S2+/- mice exhibited increased expression of the senescence marker cdkn2a in the islet at 12wks (p=0.0117) compared to control mice, whereas cdkn1a remained unchanged across all timepoints tested. DISCUSSION/SIGNIFICANCE OF FINDINGS: Our results suggest that loss of SERCA2 and reduced ER Ca2+ alter βcell mitochondrial function and are associated with features of senescence. Future studies will test whether SERCA2 activation and/or senolytic/senomorphic drugs are able to prevent or delay diabetes onset in NOD-S2+/- mice.

Published

2021

22. Cigarette Smoke Exposure Impairs β-Cell Function Through Activation of Oxidative Stress and Ceramide Accumulation

Author

Judith Maddatu, Sukrati Kanojia, Morgan A. Robertson, Tatsuyoshi Kono, Xin Tong, Paul Sohn, Robert N. Bone, Zunaira Chaudhry, Carmella Evans-Molina, Irina Petrache, and Chih-Chun Lee

Subjects

0303 health sciences, medicine.medical_specialty, Ceramide, Diabetes risk, Chemistry, Insulin, medicine.medical_treatment, 030209 endocrinology & metabolism, Type 2 diabetes, medicine.disease, medicine.disease_cause, 3. Good health, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Endocrinology, Diabetes mellitus, Internal medicine, medicine, Beta (finance), Oxidative stress, 030304 developmental biology, Proinsulin

Abstract

ObjectivesEpidemiological studies indicate that first- and second-hand cigarette smoke (CS) exposure are important risk factors for the development of type 2 diabetes (T2D). Additionally, elevated diabetes risk has been reported to occur within a short period of time after smoking cessation, and health risks associated with smoking are increased when combined with obesity. At present, the mechanisms underlying these associations remain incompletely understood. The objective of this study was to test the impact of CS exposure on pancreatic β-cell function using rodent and in vitro models.MethodsBeginning at 8 weeks of age, C57BL/6J mice were concurrently fed high fat-diet (HFD) and exposed to CS for 11 weeks, followed by an additional 11 weeks of smoking cessation with continued HFD exposure. Glucose tolerance testing was performed during CS exposure and during the cessation period. Cultured β-cells (INS-1) and primary islets were exposed ex vivo to CS extract (CSE), and β-cell function and viability were tested. Since CS increases ceramide in lungs cells and these bioactive sphingolipids have been implicated in pancreatic β-cell dysfunction in diabetes, islet and β-cell sphingolipid levels were measured in islets from CS-exposed mice and in CSE-treated islets and INS-1 cells using liquid chromatography-tandem mass spectrometry.ResultsCompared to HFD-fed ambient air-exposed mice, HFD-fed and CS- exposed mice had reduced weight gain and better glucose tolerance during the active smoking period. Following smoking cessation, CS-mice exhibited rapid weight gain and a significantly greater increase in glucose intolerance compared to non-smoking control mice. CS-exposed mice had higher serum proinsulin/insulin ratios, indicative of β-cell dysfunction, significantly lower β-cell mass (p=0.02), and reduced β-cell proliferation (p=0.006), and increased islet ceramide accumulation. Ex vivo exposure of isolated islets to CSE was sufficient to increase islet ceramide accumulation, reduce insulin gene expression and glucose-stimulated insulin secretion, and increase β-cell oxidative and ER stress. Treatment with the antioxidant N-acetylcysteine, markedly attenuated the effects of CSE on ceramide levels, restored β-cell function and survival, and increased cyclin D2 expression, while also reducing activation of β-cell ER and oxidative stress.ConclusionsOur results indicate that CS exposure inhibits insulin production, processing, and secretion and reduced β-cell viability and proliferation. These effects were linked to increased β-cell oxidative and ER stress and ceramide accumulation. Mice fed HFD continued to experience detrimental effects of CS exposure even during smoking cessation. Elucidation of mechanisms by which CS exposure impairs β-cell function in synergy with obesity will help design therapeutic and preventive interventions for both active and former smokers.

Published

2019

23. Reduced ß Cell SPCA1 Leads to Impaired Calcium Oscillations and Decreased Autophagy

Author

Robert N. Bone, Tatsuyoshi Kono, and Carmella Evans-Molina

Subjects

0301 basic medicine, medicine.medical_specialty, Programmed cell death, Chemistry, Endocrinology, Diabetes and Metabolism, Insulin, medicine.medical_treatment, ATG5, Autophagy, Golgi apparatus, 03 medical and health sciences, symbols.namesake, 030104 developmental biology, Endocrinology, Internal medicine, Internal Medicine, medicine, symbols, Secretory pathway, Homeostasis, Proinsulin

Abstract

The β-cell Golgi, an important site of proinsulin maturation, is a significant store of intracellular Ca2+. However, the contribution of Golgi Ca2+ to diabetes pathophysiology is unknown. The Golgi primarily utilizes the Secretory Pathway Ca2+ ATPase (SPCA1) to maintain intra-Golgi Ca2+ stores. SPCA1 expression was measured in islets from Akita and db/db mice and cadaveric human islets from donors with T1D and T2D. In all cases, SPCA1 levels were significantly lower compared to nondiabetic controls. Proteomics and Reverse Phase Protein Array performed in INS-1 β-cells lacking SPCA1 (SPCA1KO) indicated dysregulated cell death, cell growth, and proliferation pathways compared to WT INS-1 cells. Consistent with this, SPCA1KO cells exhibited increased caspase-3/7 following tunicamycin treatment. SPCA1KO cells also had elevated basal cytosolic Ca2+ levels, decreased organelle Ca2+ reuptake following organelle Ca2+ store depletion, and accelerated Golgi collapse. Despite a significant reduction in GSIS, SPCA1KO cells exhibited a 12-fold insulin content increase. Autophagy has been reported as a key regulator in maintaining β-cell insulin homeostasis. Immunoblot revealed reduced expression of the autophagy marker LC3-II and the autophagosome Atg5/Atg12 complex in SPCA1KO cells, following autophagy induction with Torin. Islets from mice haploinsufficient for SPCA1 (SPCA1+/-) exhibited elevated cytosolic Ca2+ levels and impaired Ca2+ oscillations as reflected by increased phase 1 amplitude and period, compared to WT littermates. In islets, restoration of SPCA1 to normal levels rescued the oscillatory defect. Interestingly, islets from SPCA1+/- mice did not exhibit increased insulin content, however, SPCA1+/- islets had decreased insulin secretion and increased numbers of immature insulin granules. Taken together, we find that β-cell SPCA1 plays an important role in the maintenance of Golgi Ca2+ levels, while loss of SPCA1 led to dysregulated β-cell Ca2+ homeostasis. Disclosure R.N. Bone: None. T. Kono: None. C. Evans-Molina: None.

Published

2018

24. Calcium-independent phospholipases A2 and their roles in biological processes and diseases

Author

Xiaoyong Lei, Tomader Ali, Jason W. Ashley, Sasanka Ramanadham, William D. Hancock, and Robert N. Bone

Subjects

Cellular differentiation, Amino Acid Motifs, QD415-436, Biology, Phospholipase, Biochemistry, eicosanoids, Endocrinology, Central Nervous System Diseases, Neoplasms, arachidonic acid, Humans, membrane homeostasis, Catabolism, Cell growth, Thematic Review Series, Lipase, Cell Biology, Lipid signaling, docosahexaenoic acid, Cell biology, Alternative Splicing, Cytosol, inflammation, Phospholipases A2, Calcium-Independent, Calcium, Signal transduction, signaling, Intracellular, Signal Transduction

Abstract

Among the family of phospholipases A2 (PLA2s) are the Ca(2+)-independent PLA2s (iPLA2s) and they are designated group VI iPLA2s. In relation to secretory and cytosolic PLA2s, the iPLA2s are more recently described and details of their expression and roles in biological functions are rapidly emerging. The iPLA2s or patatin-like phospholipases (PNPLAs) are intracellular enzymes that do not require Ca(2+) for activity, and contain lipase (GXSXG) and nucleotide-binding (GXGXXG) consensus sequences. Though nine PNPLAs have been recognized, PNPLA8 (membrane-associated iPLA2γ) and PNPLA9 (cytosol-associated iPLA2β) are the most widely studied and understood. The iPLA2s manifest a variety of activities in addition to phospholipase, are ubiquitously expressed, and participate in a multitude of biological processes, including fat catabolism, cell differentiation, maintenance of mitochondrial integrity, phospholipid remodeling, cell proliferation, signal transduction, and cell death. As might be expected, increased or decreased expression of iPLA2s can have profound effects on the metabolic state, CNS function, cardiovascular performance, and cell survival; therefore, dysregulation of iPLA2s can be a critical factor in the development of many diseases. This review is aimed at providing a general framework of the current understanding of the iPLA2s and discussion of the potential mechanisms of action of the iPLA2s and related involved lipid mediators.

Published

2015

25. Combination Immunotherapy for Type 1 Diabetes

Author

Carmella Evans-Molina and Robert N. Bone

Subjects

0301 basic medicine, Regulatory T cell, Endocrinology, Diabetes and Metabolism, T cell, medicine.medical_treatment, 030209 endocrinology & metabolism, medicine.disease_cause, Article, Autoimmunity, 03 medical and health sciences, 0302 clinical medicine, Immune system, Insulin Secretion, Internal Medicine, medicine, Animals, Humans, Insulin, Autoimmune disease, Clinical Trials as Topic, Type 1 diabetes, business.industry, Immunotherapy, medicine.disease, Immunity, Innate, Transplantation, Diabetes Mellitus, Type 1, 030104 developmental biology, medicine.anatomical_structure, Immunology, business

Abstract

Type 1 diabetes (T1D) is an autoimmune disease marked by β-cell destruction. Immunotherapies for T1D have been investigated since the 1980s and have focused on restoration of tolerance, T cell or B cell inhibition, regulatory T cell (Treg) induction, suppression of innate immunity and inflammation, immune system reset, and islet transplantation. The purpose of this review is to provide an overview and lessons learned from single immunotherapy trials, describe recent and ongoing combination immunotherapy trials, and provide perspectives on strategies for future combination clinical interventions aimed at preserving insulin secretion in T1D. Combination immunotherapies have had mixed results in improving short-term glycemic control and insulin secretion in recent-onset T1D. A handful of studies have successfully reached their primary end-point of improved insulin secretion in recent-onset T1D. However, long-term improvements glycemic control and the restoration of insulin independence remain elusive. Future interventions should focus on strategies that combine immunomodulation with efforts to alleviate β-cell stress and address the formation of antigens that activate autoimmunity.

Published

2017

26. Inhibition of Ca2+-Independent Phospholipase A2β (iPLA2β) Ameliorates Islet Infiltration and Incidence of Diabetes in NOD Mice

Author

Ying Gai, Hubert M. Tse, Sasanka Ramanadham, Xiaoyong Lei, Maroula G. Kokotou, Tomader Ali, George Kokotos, Victoria Magrioti, and Robert N. Bone

Subjects

CD4-Positive T-Lymphocytes, medicine.medical_specialty, Adoptive cell transfer, Endocrinology, Diabetes and Metabolism, Biological Availability, Nod, Naphthalenes, Biology, Gene Expression Regulation, Enzymologic, Group VI Phospholipases A2, Mice, 03 medical and health sciences, 0302 clinical medicine, Immune system, Mice, Inbred NOD, Insulin-Secreting Cells, Internal medicine, Internal Medicine, medicine, Animals, Homeostasis, Insulin, Protein Isoforms, Glucose homeostasis, 030304 developmental biology, NOD mice, B-Lymphocytes, 0303 health sciences, Type 1 diabetes, Molecular Structure, Ketones, medicine.disease, 3. Good health, Diabetes Mellitus, Type 1, Glucose, Endocrinology, Islet Studies, Calcium, Female, Tumor necrosis factor alpha, Insulitis, 030217 neurology & neurosurgery

Abstract

Autoimmune β-cell death leads to type 1 diabetes, and with findings that Ca2+-independent phospholipase A2β (iPLA2β) activation contributes to β-cell death, we assessed the effects of iPLA2β inhibition on diabetes development. Administration of FKGK18, a reversible iPLA2β inhibitor, to NOD female mice significantly reduced diabetes incidence in association with 1) reduced insulitis, reflected by reductions in CD4+ T cells and B cells; 2) improved glucose homeostasis; 3) higher circulating insulin; and 4) β-cell preservation. Furthermore, FKGK18 inhibited production of tumor necrosis factor-α (TNF-α) from CD4+ T cells and antibodies from B cells, suggesting modulation of immune cell responses by iPLA2β-derived products. Consistent with this, 1) adoptive transfer of diabetes by CD4+ T cells to immunodeficient and diabetes-resistant NOD.scid mice was mitigated by FKGK18 pretreatment and 2) TNF-α production from CD4+ T cells was reduced by inhibitors of cyclooxygenase and 12-lipoxygenase, which metabolize arachidonic acid to generate bioactive inflammatory eicosanoids. However, adoptive transfer of diabetes was not prevented when mice were administered FKGK18-pretreated T cells or when FKGK18 administration was initiated with T-cell transfer. The present observations suggest that iPLA2β-derived lipid signals modulate immune cell responses, raising the possibility that early inhibition of iPLA2β may be beneficial in ameliorating autoimmune destruction of β-cells and mitigating type 1 diabetes development.

Published

2014

27. Polarization of Macrophages toward M2 Phenotype Is Favored by Reduction in iPLA2β (Group VIA Phospholipase A2)

Author

Alexander J. Nelson, Sasanka Ramanadham, Hubert M. Tse, John Turk, William D. Hancock, Robert N. Bone, Jason W. Ashley, and Mary Wohltmann

Subjects

0301 basic medicine, Male, Inflammation, Biochemistry, Proinflammatory cytokine, Group VI Phospholipases A2, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, Phospholipase A2, Lysophosphatidic acid, medicine, Animals, Humans, Molecular Biology, Mice, Knockout, NADPH oxidase, biology, Macrophages, NOX4, Cell Polarity, NADPH Oxidases, Cell Biology, Molecular biology, Lipids, Mice, Inbred C57BL, 030104 developmental biology, Lysophosphatidylcholine, chemistry, Eicosanoid, Cyclooxygenase 2, NADPH Oxidase 4, biology.protein, Female, medicine.symptom, 030217 neurology & neurosurgery

Abstract

Macrophages are important in innate and adaptive immunity. Macrophage participation in inflammation or tissue repair is directed by various extracellular signals and mediated by multiple intracellular pathways. Activation of group VIA phospholipase A2 (iPLA2β) causes accumulation of arachidonic acid, lysophospholipids, and eicosanoids that can promote inflammation and pathologic states. We examined the role of iPLA2β in peritoneal macrophage immune function by comparing wild type (WT) and iPLA2β−/− mouse macrophages. Compared with WT, iPLA2β−/− macrophages exhibited reduced proinflammatory M1 markers when classically activated. In contrast, anti-inflammatory M2 markers were elevated under naive conditions and induced to higher levels by alternative activation in iPLA2β−/− macrophages compared with WT. Induction of eicosanoid (12-lipoxygenase (12-LO) and cyclooxygenase 2 (COX2))- and reactive oxygen species (NADPH oxidase 4 (NOX4))-generating enzymes by classical activation pathways was also blunted in iPLA2β−/− macrophages compared with WT. The effects of inhibitors of iPLA2β, COX2, or 12-LO to reduce M1 polarization were greater than those to enhance M2 polarization. Certain lipids (lysophosphatidylcholine, lysophosphatidic acid, and prostaglandin E2) recapitulated M1 phenotype in iPLA2β−/− macrophages, but none tested promoted M2 phenotype. These findings suggest that (a) lipids generated by iPLA2β and subsequently oxidized by cyclooxygenase and 12-LO favor macrophage inflammatory M1 polarization, and (b) the absence of iPLA2β promotes macrophage M2 polarization. Reducing macrophage iPLA2β activity and thereby attenuating macrophage M1 polarization might cause a shift from an inflammatory to a recovery/repair milieu.

Published

2016

28. Evidence of contribution of iPLA2β-mediated events during islet β-cell apoptosis due to proinflammatory cytokines suggests a role for iPLA2β in T1D development

Author

Tomader Ali, Keshore R. Bidasee, Sheng Zhang, Robert N. Bone, Xiaoyong Lei, Alan Bohrer, Hubert M. Tse, and Sasanka Ramanadham

Subjects

Adult, Male, medicine.medical_specialty, Ceramide, medicine.medical_treatment, Interleukin-1beta, Apoptosis, Biology, Proinflammatory cytokine, Group VI Phospholipases A2, chemistry.chemical_compound, Interferon-gamma, Islets of Langerhans, Mice, Endocrinology, Immune system, Internal medicine, medicine, Animals, Humans, Mice, Knockout, geography, geography.geographical_feature_category, Diabetes-Insulin-Glucagon-Gastrointestinal, Islet, Endoplasmic Reticulum Stress, Lysophosphatidylcholine, Cytokine, Diabetes Mellitus, Type 1, chemistry, Unfolded protein response, Cytokines, Female, Sterol Regulatory Element Binding Protein 1

Abstract

Type 1 diabetes (T1D) results from autoimmune destruction of islet β-cells, but the underlying mechanisms that contribute to this process are incompletely understood, especially the role of lipid signals generated by β-cells. Proinflammatory cytokines induce ER stress in β-cells and we previously found that the Ca2+-independent phospholipase A2β (iPLA2β) participates in ER stress-induced β-cell apoptosis. In view of reports of elevated iPLA2β in T1D, we examined if iPLA2β participates in cytokine-mediated islet β-cell apoptosis. We find that the proinflammatory cytokine combination IL-1β+IFNγ, induces: a) ER stress, mSREBP-1, and iPLA2β, b) lysophosphatidylcholine (LPC) generation, c) neutral sphingomyelinase-2 (NSMase2), d) ceramide accumulation, e) mitochondrial membrane decompensation, f) caspase-3 activation, and g) β-cell apoptosis. The presence of a sterol regulatory element in the iPLA2β gene raises the possibility that activation of SREBP-1 after proinflammatory cytokine exposure contributes to iPLA2β induction. The IL-1β+IFNγ-induced outcomes (b–g) are all inhibited by iPLA2β inactivation, suggesting that iPLA2β-derived lipid signals contribute to consequential islet β-cell death. Consistent with this possibility, ER stress and β-cell apoptosis induced by proinflammatory cytokines are exacerbated in islets from RIP-iPLA2β-Tg mice and blunted in islets from iPLA2β-KO mice. These observations suggest that iPLA2β-mediated events participate in amplifying β-cell apoptosis due to proinflammatory cytokines and also that iPLA2β activation may have a reciprocal impact on ER stress development. They raise the possibility that iPLA2β inhibition, leading to ameliorations in ER stress, apoptosis, and immune responses resulting from LPC-stimulated immune cell chemotaxis, may be beneficial in preserving β-cell mass and delaying/preventing T1D evolution.

Published

2014

29. Genetic modulation of islet β-cell iPLA₂β expression provides evidence for its impact on β-cell apoptosis and autophagy

Author

Xiaoyong, Lei, Robert N, Bone, Tomader, Ali, Mary, Wohltmann, Ying, Gai, Karen J, Goodwin, Alan E, Bohrer, John, Turk, and Sasanka, Ramanadham

Subjects

autophagy, caspase-3, Apoptosis, Mice, Transgenic, iPLA2β, Ceramides, Gene Expression Regulation, Enzymologic, Sarcoplasmic Reticulum Calcium-Transporting ATPases, Tissue Culture Techniques, Islets of Langerhans, Mice, mitochondrial membrane potential, Insulin-Secreting Cells, Diabetes Mellitus, Animals, Enzyme Inhibitors, Membrane Potential, Mitochondrial, Mice, Knockout, Caspase 3, Group IV Phospholipases A2, RIP-iPLA2β-Tg, Endoplasmic Reticulum Stress, β-cell, Enzyme Activation, Sphingomyelin Phosphodiesterase, Unfolded Protein Response, iPLA2β-KO, Research Paper

Abstract

β-cell apoptosis is a significant contributor to β-cell dysfunction in diabetes and ER stress is among the factors that contributes to β-cell death. We previously identified that the Ca2+-independent phospholipase A2β (iPLA2β), which in islets is localized in β-cells, participates in ER stress-induced β-cell apoptosis. Here, direct assessment of iPLA2β role was made using β-cell-specific iPLA2β overexpressing (RIP-iPLA2β-Tg) and globally iPLA2β-deficient (iPLA2β-KO) mice. Islets from Tg, but not KO, express higher islet iPLA2β and neutral sphingomyelinase, decrease in sphingomyelins, and increase in ceramides, relative to WT group. ER stress induces iPLA2β, ER stress factors, loss of mitochondrial membrane potential (∆Ψ), caspase-3 activation, and β-cell apoptosis in the WT and these are all amplified in the Tg group. Surprisingly, β-cells apoptosis while reduced in the KO is higher than in the WT group. This, however, was not accompanied by greater caspase-3 activation but with larger loss of ∆Ψ, suggesting that iPLA2β deficiency impacts mitochondrial membrane integrity and causes apoptosis by a caspase-independent manner. Further, autophagy, as reflected by LC3-II accumulation, is increased in Tg and decreased in KO, relative to WT. Our findings suggest that (1) iPLA2β impacts upstream (UPR) and downstream (ceramide generation and mitochondrial) pathways in β-cells and (2) both over- or under-expression of iPLA2β is deleterious to the β-cells. Further, we present for the first time evidence for potential regulation of autophagy by iPLA2β in islet β-cells. These findings support the hypothesis that iPLA2β induction under stress, as in diabetes, is a key component to amplifying β-cell death processes.

Published

2013

30. Gene transfer of active Akt1 by an infectivity-enhanced adenovirus impacts β-cell survival and proliferation differentially in vitro and in vivo

Author

Ji-Bin Peng, Mert Icyuz, Yanqing Zhang, Yuan Zhang, Wanxing Cui, Robert N. Bone, Qiana L. Matthews, Hongjun Wang, Hongju Wu, and Gene P. Siegal

Subjects

medicine.medical_specialty, Cell Survival, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Genetic Vectors, AKT1, Cell Growth Processes, Mice, SCID, Gene delivery, Biology, Viral vector, Adenoviridae, Diabetes Mellitus, Experimental, Rats, Sprague-Dawley, Mice, Endocrinology, In vivo, Mice, Inbred NOD, Internal medicine, Insulin-Secreting Cells, β-cell proliferation, medicine, Animals, Humans, Protein kinase B, islets, Akt1, diabetes, Pancreatic islets, Insulin, Gene Transfer Techniques, adenovirus, Streptozotocin, Immunohistochemistry, 3. Good health, Rats, Mice, Inbred C57BL, medicine.anatomical_structure, Diabetes Mellitus, Type 1, Cancer research, Proto-Oncogene Proteins c-akt, medicine.drug, Research Paper

Abstract

Type 1 Diabetes is characterized by an absolute insulin deficiency due to the autoimmune destruction of insulin producing β-cells in the pancreatic islets. Akt1/Protein Kinase B is the direct downstream target of PI3 Kinase activation, and has shown potent anti-apoptotic and proliferation-inducing activities. This study was designed to explore whether gene transfer of constitutively active Akt1 (CA-Akt1) would promote β-cell survival and proliferation, thus be protective against experimental diabetes. In the study, a fiber-modified infectivity-enhanced adenoviral vector, Ad5RGDpK7, was used to deliver rat insulin promoter (RIP)-driven CA-Akt1 into β-cells. Our data showed this vector efficiently delivered CA-Akt1 into freshly isolated pancreatic islets, and promoted islet cell survival and β-cell proliferation in vitro. The therapeutic effect of the vector in vivo was assessed using streptozotocin (STZ)-induced diabetes mice. Two means of vector administration were explored: intravenous and intra-bile ductal injections. While direct vector administration into pancreas via bile-ductal injection resulted in local adverse effect, intravenous injection of the vectors offered therapeutic benefits. Further analysis suggests systemic vector administration caused endogenous Akt expression and activation in islets, which may be responsible, at least in part, for the protective effect of the infectivity-enhanced CA-Akt1 gene delivery vector. Taken together, our data suggest CA-Akt1 is effective in promoting β-cell survival and proliferation in vitro, but direct in vivo use is compromised by the efficacy of transgene delivery into β-cells. Nonetheless, the vector evoked the expression and activation of endogenous Akt in the islets, thus offering beneficial bystander effect against STZ-induced diabetes.

Published

2012

31. Characterization of FKGK18 as Inhibitor of Group VIA Ca2+-Independent Phospholipase A2 (iPLA2β): Candidate Drug for Preventing Beta-Cell Apoptosis and Diabetes

Author

William D. Hancock, James A. Mobley, Sasanka Ramanadham, Victoria Magrioti, Robert N. Bone, George Kokotos, and Tomader Ali

Subjects

Time Factors, Enzyme Metabolism, Drug Evaluation, Preclinical, lcsh:Medicine, Apoptosis, Sphingomyelin phosphodiesterase, Pharmacology, Biochemistry, Mice, chemistry.chemical_compound, Cytosol, Endocrinology, 0302 clinical medicine, Insulin-Secreting Cells, Insulin Secretion, Drug Discovery, Molecular Cell Biology, Chymotrypsin, Insulin, Enzyme Inhibitors, lcsh:Science, chemistry.chemical_classification, 0303 health sciences, Multidisciplinary, Cell Death, biology, Ketones, Endoplasmic Reticulum Stress, Lipids, Enzymes, Sphingomyelin Phosphodiesterase, Medicine, Arachidonic acid, Research Article, Drugs and Devices, Proteases, Drug Research and Development, Naphthalenes, Dinoprostone, Group VI Phospholipases A2, Lipid Mediators, 03 medical and health sciences, Phospholipase A2, In vivo, Diabetes Mellitus, Animals, Humans, Biology, 030304 developmental biology, Diabetic Endocrinology, Endocrine Physiology, Myocardium, lcsh:R, Cell Membrane, Diabetes Mellitus Type 1, Lipid Metabolism, Glucose, Metabolism, Enzyme, chemistry, Pyrones, biology.protein, lcsh:Q, Calcium, 030217 neurology & neurosurgery, Ex vivo

Abstract

Ongoing studies suggest an important role for iPLA2β in a multitude of biological processes and it has been implicated in neurodegenerative, skeletal and vascular smooth muscle disorders, bone formation, and cardiac arrhythmias. Thus, identifying an iPLA2βinhibitor that can be reliably and safely used in vivo is warranted. Currently, the mechanism-based inhibitor bromoenol lactone (BEL) is the most widely used to discern the role of iPLA2β in biological processes. While BEL is recognized as a more potent inhibitor of iPLA2 than of cPLA2 or sPLA2, leading to its designation as a "specific" inhibitor of iPLA2, it has been shown to also inhibit non-PLA2 enzymes. A potential complication of its use is that while the S and R enantiomers of BEL exhibit preference for cytosol-associated iPLA2β and membrane-associated iPLA2γ, respectively, the selectivity is only 10-fold for both. In addition, BEL is unstable in solution, promotes irreversible inhibition, and may be cytotoxic, making BEL not amenable for in vivo use. Recently, a fluoroketone (FK)-based compound (FKGK18) was described as a potent inhibitor of iPLA2β. Here we characterized its inhibitory profile in beta-cells and find that FKGK18: (a) inhibits iPLA2β with a greater potency (100-fold) than iPLA2γ, (b) inhibition of iPLA2β is reversible, (c) is an ineffective inhibitor of α-chymotrypsin, and (d) inhibits previously described outcomes of iPLA2β activation including (i) glucose-stimulated insulin secretion, (ii) arachidonic acid hydrolysis; as reflected by PGE2 release from human islets, (iii) ER stress-induced neutral sphingomyelinase 2 expression, and (iv) ER stress-induced beta-cell apoptosis. These findings suggest that FKGK18 is similar to BEL in its ability to inhibit iPLA2β. Because, in contrast to BEL, it is reversible and not a non-specific inhibitor of proteases, it is suggested that FKGK18 is more ideal for ex vivo and in vivo assessments of iPLA2β role in biological functions.

Published

2013

32. Regeneration of Pancreatic Non-β Endocrine Cells in Adult Mice following a Single Diabetes-Inducing Dose of Streptozotocin

Author

Hongjun Wang, Ji-Bin Peng, Yanqing Zhang, Yuan Zhang, Gene P. Siegal, Robert N. Bone, Wanxing Cui, and Hongju Wu

Subjects

Anatomy and Physiology, endocrine system diseases, lcsh:Medicine, Cell Count, Enteroendocrine cell, Mice, Endocrinology, 0302 clinical medicine, Insulin-Secreting Cells, Insulin, lcsh:Science, 0303 health sciences, Multidisciplinary, medicine.anatomical_structure, Medicine, PDX1, Stem cell, Somatostatin, Research Article, medicine.drug, Somatostatin-Secreting Cells, endocrine system, medicine.medical_specialty, Endocrine System, 030209 endocrinology & metabolism, Gastroenterology and Hepatology, Biology, Streptozocin, Diabetes Mellitus, Experimental, Islets of Langerhans, 03 medical and health sciences, Internal medicine, medicine, Animals, Regeneration, Progenitor cell, Pancreas, Cell Proliferation, 030304 developmental biology, Diabetic Endocrinology, Homeodomain Proteins, Delta cell, Endocrine Physiology, Dose-Response Relationship, Drug, Pancreatic islets, Regeneration (biology), lcsh:R, Diabetes Mellitus Type 1, Glucagon, Streptozotocin, Mice, Inbred C57BL, Disease Models, Animal, Glucagon-Secreting Cells, Trans-Activators, lcsh:Q, Endocrine Cells

Abstract

The non-β endocrine cells in pancreatic islets play an essential counterpart and regulatory role to the insulin-producing β-cells in the regulation of blood-glucose homeostasis. While significant progress has been made towards the understanding of β-cell regeneration in adults, very little is known about the regeneration of the non-β endocrine cells such as glucagon-producing α-cells and somatostatin producing δ-cells. Previous studies have noted the increase of α-cell composition in diabetes patients and in animal models. It is thus our hypothesis that non-β-cells such as α-cells and δ-cells in adults can regenerate, and that the regeneration accelerates in diabetic conditions. To test this hypothesis, we examined islet cell composition in a streptozotocin (STZ)-induced diabetes mouse model in detail. Our data showed the number of α-cells in each islet increased following STZ-mediated β-cell destruction, peaked at Day 6, which was about 3 times that of normal islets. In addition, we found δ-cell numbers doubled by Day 6 following STZ treatment. These data suggest α- and δ-cell regeneration occurred rapidly following a single diabetes-inducing dose of STZ in mice. Using in vivo BrdU labeling techniques, we demonstrated α- and δ-cell regeneration involved cell proliferation. Co-staining of the islets with the proliferating cell marker Ki67 showed α- and δ-cells could replicate, suggesting self-duplication played a role in their regeneration. Furthermore, Pdx1(+)/Insulin(-) cells were detected following STZ treatment, indicating the involvement of endocrine progenitor cells in the regeneration of these non-β cells. This is further confirmed by the detection of Pdx1(+)/glucagon(+) cells and Pdx1(+)/somatostatin(+) cells following STZ treatment. Taken together, our study demonstrated adult α- and δ-cells could regenerate, and both self-duplication and regeneration from endocrine precursor cells were involved in their regeneration.

Published

2012

33. Characterization of FKGK18 as inhibitor of group VIA Ca2+-independent phospholipase A2 (iPLA2β): candidate drug for preventing beta-cell apoptosis and diabetes.

Author

Tomader Ali, George Kokotos, Victoria Magrioti, Robert N Bone, James A Mobley, William Hancock, and Sasanka Ramanadham

Subjects

Medicine, Science

Abstract

Ongoing studies suggest an important role for iPLA2β in a multitude of biological processes and it has been implicated in neurodegenerative, skeletal and vascular smooth muscle disorders, bone formation, and cardiac arrhythmias. Thus, identifying an iPLA2βinhibitor that can be reliably and safely used in vivo is warranted. Currently, the mechanism-based inhibitor bromoenol lactone (BEL) is the most widely used to discern the role of iPLA2β in biological processes. While BEL is recognized as a more potent inhibitor of iPLA2 than of cPLA2 or sPLA2, leading to its designation as a "specific" inhibitor of iPLA2, it has been shown to also inhibit non-PLA2 enzymes. A potential complication of its use is that while the S and R enantiomers of BEL exhibit preference for cytosol-associated iPLA2β and membrane-associated iPLA2γ, respectively, the selectivity is only 10-fold for both. In addition, BEL is unstable in solution, promotes irreversible inhibition, and may be cytotoxic, making BEL not amenable for in vivo use. Recently, a fluoroketone (FK)-based compound (FKGK18) was described as a potent inhibitor of iPLA2β. Here we characterized its inhibitory profile in beta-cells and find that FKGK18: (a) inhibits iPLA2β with a greater potency (100-fold) than iPLA2γ, (b) inhibition of iPLA2β is reversible, (c) is an ineffective inhibitor of α-chymotrypsin, and (d) inhibits previously described outcomes of iPLA2β activation including (i) glucose-stimulated insulin secretion, (ii) arachidonic acid hydrolysis; as reflected by PGE2 release from human islets, (iii) ER stress-induced neutral sphingomyelinase 2 expression, and (iv) ER stress-induced beta-cell apoptosis. These findings suggest that FKGK18 is similar to BEL in its ability to inhibit iPLA2β. Because, in contrast to BEL, it is reversible and not a non-specific inhibitor of proteases, it is suggested that FKGK18 is more ideal for ex vivo and in vivo assessments of iPLA2β role in biological functions.

Published

2013

34. Regeneration of pancreatic non-β endocrine cells in adult mice following a single diabetes-inducing dose of streptozotocin.

Author

Yanqing Zhang, Yuan Zhang, Robert N Bone, Wanxing Cui, Ji-Bin Peng, Gene P Siegal, Hongjun Wang, and Hongju Wu

Subjects

Medicine, Science

Abstract

The non-β endocrine cells in pancreatic islets play an essential counterpart and regulatory role to the insulin-producing β-cells in the regulation of blood-glucose homeostasis. While significant progress has been made towards the understanding of β-cell regeneration in adults, very little is known about the regeneration of the non-β endocrine cells such as glucagon-producing α-cells and somatostatin producing δ-cells. Previous studies have noted the increase of α-cell composition in diabetes patients and in animal models. It is thus our hypothesis that non-β-cells such as α-cells and δ-cells in adults can regenerate, and that the regeneration accelerates in diabetic conditions. To test this hypothesis, we examined islet cell composition in a streptozotocin (STZ)-induced diabetes mouse model in detail. Our data showed the number of α-cells in each islet increased following STZ-mediated β-cell destruction, peaked at Day 6, which was about 3 times that of normal islets. In addition, we found δ-cell numbers doubled by Day 6 following STZ treatment. These data suggest α- and δ-cell regeneration occurred rapidly following a single diabetes-inducing dose of STZ in mice. Using in vivo BrdU labeling techniques, we demonstrated α- and δ-cell regeneration involved cell proliferation. Co-staining of the islets with the proliferating cell marker Ki67 showed α- and δ-cells could replicate, suggesting self-duplication played a role in their regeneration. Furthermore, Pdx1(+)/Insulin(-) cells were detected following STZ treatment, indicating the involvement of endocrine progenitor cells in the regeneration of these non-β cells. This is further confirmed by the detection of Pdx1(+)/glucagon(+) cells and Pdx1(+)/somatostatin(+) cells following STZ treatment. Taken together, our study demonstrated adult α- and δ-cells could regenerate, and both self-duplication and regeneration from endocrine precursor cells were involved in their regeneration.

Published

2012