Your search keyword '"c-peptide"' showing total 780 results

1. Evidence for C-Peptide as a Validated Surrogate to Predict Clinical Benefits in Trials of Disease-Modifying Therapies for Type 1 Diabetes.

Author

Latres, Esther, Greenbaum, Carla J., Oyaski, Maria L., Dayan, Colin M., Colhoun, Helen M., Lachin, John M., Skyler, Jay S., Rickels, Michael R., Ahmed, Simi T., Dutta, Sanjoy, Herold, Kevan C., and Marinac, Marjana

Subjects

*TYPE 1 diabetes, *AUTOIMMUNE diseases, *BIOMARKERS, *C-peptide, *GLYCEMIC control, *CLINICAL trials, *INSULIN aspart

Abstract

Type 1 diabetes is a chronic autoimmune disease in which destruction of pancreatic β-cells causes life-threatening metabolic dysregulation. Numerous approaches are envisioned for new therapies, but limitations of current clinical outcome measures are significant disincentives to development efforts. C-peptide, a direct byproduct of proinsulin processing, is a quantitative biomarker of β-cell function that is not cleared by the liver and can be measured in the peripheral blood. Studies of quantitative measures of β-cell function have established a predictive relationship between stimulated C-peptide as a measure of β-cell function and clinical benefits. C-peptide levels at diagnosis are often high enough to afford glycemic control benefits associated with protection from end-organ complications of diabetes, and even lower levels offer protection from severe hypoglycemia in type 1 diabetes, as observed in large prospective cohort studies and interventional trials of islet transplantation. These observations support consideration of C-peptide not just as a biomarker of β-cell function but also as a specific, sensitive, feasible, and clinically meaningful outcome defining β-cell preservation or restoration for clinical trials of disease-modifying therapies. Regulatory acceptance of C-peptide as a validated surrogate for demonstration of efficacy would greatly facilitate development of disease-modifying therapies for type 1 diabetes. Article Highlights: Mixed-meal stimulated C-peptide level has been established as a biomarker of endogenous β-cell function and is used clinically to monitor disease progression in type 1 diabetes. Large prospective cohort studies and interventional trials of islet transplantation demonstrate the relationship between stimulated C-peptide levels and clinical benefits. A recent meta-analysis of interventional clinical trials aimed at preserving β-cell function in those recently diagnosed further supports stimulated C-peptide level as a validated surrogate end point for clinical trials of disease-modifying therapies in type 1 diabetes. [ABSTRACT FROM AUTHOR]

Published

2024

2. Low-Dose ATG/GCSF in Established Type 1 Diabetes: A Five-Year Follow-up Report.

Author

Lin, Andrea, Mack, Jasmine A, Bruggeman, Brittany, Jacobsen, Laura M, Posgai, Amanda L, Wasserfall, Clive H, Brusko, Todd M, Atkinson, Mark A, Gitelman, Stephen E, Gottlieb, Peter A, Gurka, Matthew J, Mathews, Clayton E, Schatz, Desmond A, and Haller, Michael J

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Diabetes, Clinical Research, Clinical Trials and Supportive Activities, Prevention, Metabolic and endocrine, Antilymphocyte Serum, Area Under Curve, C-Peptide, Diabetes Mellitus, Type 1, Granulocyte Colony-Stimulating Factor, Humans, Pilot Projects, Medical and Health Sciences, Endocrinology & Metabolism, Biomedical and clinical sciences

Abstract

Previously, we demonstrated low-dose antithymocyte globulin (ATG) and granulocyte colony-stimulating factor (GCSF) immunotherapy preserved C-peptide for 2 years in a pilot study of patients with established type 1 diabetes (n = 25). Here, we evaluated the long-term outcomes of ATG/GCSF in study participants with 5 years of available follow-up data (n = 15). The primary end point was area under the curve (AUC) C-peptide during a 2-h mixed-meal tolerance test. After 5 years, there were no statistically significant differences in AUC C-peptide when comparing those who received ATG/GCSF versus placebo (P = 0.41). A modeling framework based on mean trajectories in C-peptide AUC over 5 years, accounting for differing trends between groups, was applied to recategorize responders (n = 9) and nonresponders (n = 7). ATG/GCSF reponders demonstrated nearly unchanged HbA1c over 5 years (mean [95% CI] adjusted change 0.29% [-0.69%, 1.27%]), but the study was not powered for comparisons against nonresponders 1.75% (-0.57%, 4.06%) or placebo recipients 1.44% (0.21%, 2.66%). These data underscore the importance of long-term follow-up in previous and ongoing phase 2 trials of low-dose ATG in recent-onset type 1 diabetes.

Published

2021

3. Low-Dose Anti-Thymocyte Globulin Preserves C-Peptide, Reduces HbA1c, and Increases Regulatory to Conventional T-Cell Ratios in New-Onset Type 1 Diabetes: Two-Year Clinical Trial Data

Author

Haller, Michael J, Long, S Alice, Blanchfield, J Lori, Schatz, Desmond A, Skyler, Jay S, Krischer, Jeffrey P, Bundy, Brian N, Geyer, Susan M, Warnock, Megan V, Miller, Jessica L, Atkinson, Mark A, Becker, Dorothy J, Baidal, David A, DiMeglio, Linda A, Gitelman, Stephen E, Goland, Robin, Gottlieb, Peter A, Herold, Kevan C, Marks, Jennifer B, Moran, Antoinette, Rodriguez, Henry, Russell, William E, Wilson, Darrell M, Greenbaum, Carla J, Battaglia, Manuela, Becker, Dorothy, Bingley, Penelope, Bosi, Emanuele, Buckner, Jane, Clements, Mark, Colman, Peter G, DiMeglio, Linda, Evans-Molina, Carmella, Gottlieb, Peter, Herold, Kevan, Knip, Mikael, Lernmark, Ake, Moore, Wayne, Muir, Andrew, Palmer, Jerry, Peakman, Mark, Philipson, Louis, Raskin, Philip, Redondo, Maria, Russell, William, Sosenko, Jay M, Spain, Lisa, Wentworth, John, Wherrett, Diane, Winter, William, Ziegler, Anette, Anderson, Mark, Antinozzi, Peter, Insel, Richard, Kay, Thomas, Pugliese, Alberto, Roep, Bart, Toppari, Jorma, Leschek, Ellen, Bourcier, Katarzyna, Ridge, John, Rafkin, Lisa, Santiago, Irene, Bundy, Brian, Abbondondolo, Michael, Adams, Timothy, Asif, Ilma, Bjellquist, Jenna, Boonstra, Matthew, Burroughs, Cristina, Cleves, Mario, Cuthbertson, David, DeSalvatore, Meagan, Eberhard, Christopher, Fiske, Steve, Ford, Julie, Garmeson, Jennifer, Geyer, Susan, and Hays, Brian

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Immunology, Clinical Trials and Supportive Activities, Clinical Research, Diabetes, 6.1 Pharmaceuticals, Metabolic and endocrine, Adolescent, Adult, Antilymphocyte Serum, C-Peptide, CD4-CD8 Ratio, Child, Diabetes Mellitus, Type 1, Double-Blind Method, Female, Flow Cytometry, Glycated Hemoglobin, Granulocyte Colony-Stimulating Factor, Humans, Immunologic Factors, Male, T-Lymphocytes, Regulatory, Young Adult, Type 1 Diabetes TrialNet ATG-GCSF Study Group, Medical and Health Sciences, Endocrinology & Metabolism, Biomedical and clinical sciences

Abstract

A three-arm, randomized, double-masked, placebo-controlled phase 2b trial performed by the Type 1 Diabetes TrialNet Study Group previously demonstrated that low-dose anti-thymocyte globulin (ATG) (2.5 mg/kg) preserved β-cell function and reduced HbA1c for 1 year in new-onset type 1 diabetes. Subjects (N = 89) were randomized to 1) ATG and pegylated granulocyte colony-stimulating factor (GCSF), 2) ATG alone, or 3) placebo. Herein, we report 2-year area under the curve (AUC) C-peptide and HbA1c, prespecified secondary end points, and potential immunologic correlates. The 2-year mean mixed-meal tolerance test-stimulated AUC C-peptide, analyzed by ANCOVA adjusting for baseline C-peptide, age, and sex (n = 82) with significance defined as one-sided P < 0.025, was significantly higher in subjects treated with ATG versus placebo (P = 0.00005) but not ATG/GCSF versus placebo (P = 0.032). HbA1c was significantly reduced at 2 years in subjects treated with ATG (P = 0.011) and ATG/GCSF (P = 0.022) versus placebo. Flow cytometry analyses demonstrated reduced circulating CD4:CD8 ratio, increased regulatory T-cell:conventional CD4 T-cell ratios, and increased PD-1+CD4+ T cells following low-dose ATG and ATG/GCSF. Low-dose ATG partially preserved β-cell function and reduced HbA1c 2 years after therapy in new-onset type 1 diabetes. Future studies should determine whether low-dose ATG might prevent or delay the onset of type 1 diabetes.

Published

2019

4. The p66Shc Protein Mediates Insulin Resistance and Secretory Dysfunction in Pancreatic β-Cells Under Lipotoxic Conditions.

Author

Biondi, Giuseppina, Marrano, Nicola, Dipaola, Lucia, Borrelli, Anna, Rella, Martina, D'Oria, Rossella, Genchi, Valentina A., Caccioppoli, Cristina, Porreca, Immacolata, Cignarelli, Angelo, Perrini, Sebastio, Marchetti, Piero, Vincenti, Leonardo, Laviola, Luigi, Giorgino, Francesco, and Natalicchio, Annalisa

Subjects

*ANIMAL experimentation, *APOPTOSIS, *ISLANDS of Langerhans, *CELLULAR signal transduction, *INSULIN, *INSULIN resistance, *FATTY acids, *C-peptide, *MICE

Abstract

We evaluated the role of the p66Shc redox adaptor protein in pancreatic β-cell insulin resistance that develops under lipotoxic conditions and with excess body fat. Prolonged exposure to palmitate in vitro or the presence of overweight/obesity augmented p66Shc expression levels and caused an impaired ability of exogenous insulin to increase cellular insulin content and secreted C-peptide levels in INS-1E cells and human and murine islets. In INS-1E cells, p66Shc knockdown resulted in enhanced insulin-induced augmentation of insulin content and C-peptide secretion and prevented the ability of palmitate to impair these effects of insulin. Conversely, p66Shc overexpression impaired insulin-induced augmentation of insulin content and C-peptide secretion in both the absence and presence of palmitate. Under lipotoxic condition, the effects of p66Shc are mediated by a p53-induced increase in p66Shc protein levels and JNK-induced p66Shc phosphorylation at Ser36 and appear to involve the phosphorylation of the ribosomal protein S6 kinase at Thr389 and of insulin receptor substrate 1 at Ser307, resulting in the inhibition of insulin-stimulated protein kinase B phosphorylation at Ser473. Thus, the p66Shc protein mediates the impaired β-cell function and insulin resistance induced by saturated fatty acids and excess body fat. [ABSTRACT FROM AUTHOR]

Published

2022

5. Islet-Derived CD4 T Cells Targeting Proinsulin in Human Autoimmune Diabetes

Author

Michels, Aaron W, Landry, Laurie G, McDaniel, Kristen A, Yu, Liping, Campbell-Thompson, Martha, Kwok, William W, Jones, Kenneth L, Gottlieb, Peter A, Kappler, John W, Tang, Qizhi, Roep, Bart O, Atkinson, Mark A, Mathews, Clayton E, and Nakayama, Maki

Subjects

Diabetes, Autoimmune Disease, 2.1 Biological and endogenous factors, Aetiology, Metabolic and endocrine, Adolescent, Autoantigens, C-Peptide, CD4-Positive T-Lymphocytes, Child, Diabetes Mellitus, Type 1, Female, HLA-DQ Antigens, HLA-DR Antigens, Humans, Insulin, Insulin-Secreting Cells, Islets of Langerhans, Peptide Fragments, Proinsulin, Protein Precursors, Receptors, Antigen, T-Cell, Young Adult, Medical and Health Sciences, Endocrinology & Metabolism

Abstract

Type 1 diabetes results from chronic autoimmune destruction of insulin-producing β-cells within pancreatic islets. Although insulin is a critical self-antigen in animal models of autoimmune diabetes, due to extremely limited access to pancreas samples, little is known about human antigenic targets for islet-infiltrating T cells. Here we show that proinsulin peptides are targeted by islet-infiltrating T cells from patients with type 1 diabetes. We identified hundreds of T cells from inflamed pancreatic islets of three young organ donors with type 1 diabetes with a short disease duration with high-risk HLA genes using a direct T-cell receptor (TCR) sequencing approach without long-term cell culture. Among 85 selected CD4 TCRs tested for reactivity to preproinsulin peptides presented by diabetes-susceptible HLA-DQ and HLA-DR molecules, one T cell recognized C-peptide amino acids 19-35, and two clones from separate donors responded to insulin B-chain amino acids 9-23 (B:9-23), which are known to be a critical self-antigen-driving disease progress in animal models of autoimmune diabetes. These B:9-23-specific T cells from islets responded to whole proinsulin and islets, whereas previously identified B:9-23 responsive clones from peripheral blood did not, highlighting the importance of proinsulin-specific T cells in the islet microenvironment.

Published

2017

6. Circulating C-Peptide Levels in Living Children and Young People and Pancreatic β-Cell Loss in Pancreas Donors Across Type 1 Diabetes Disease Duration.

Author

Carr, Alice L.J., Inshaw, Jamie R.J., Flaxman, Christine S., Leete, Pia, Wyatt, Rebecca C., Russell, Lydia A., Palmer, Matthew, Prasolov, Dmytro, Worthington, Thomas, Hull, Bethany, Wicker, Linda S., Dunger, David B., Oram, Richard A., Morgan, Noel G., Todd, John A., Richardson, Sarah J., and Besser, Rachel E.J.

Subjects

*PANCREAS, *TYPE 1 diabetes, *ISLANDS of Langerhans, *RESEARCH funding, *C-peptide

Abstract

C-peptide declines in type 1 diabetes, although many long-duration patients retain low, but detectable levels. Histological analyses confirm that β-cells can remain following type 1 diabetes onset. We explored the trends observed in C-peptide decline in the UK Genetic Resource Investigating Diabetes (UK GRID) cohort (N = 4,079), with β-cell loss in pancreas donors from the network for Pancreatic Organ donors with Diabetes (nPOD) biobank and the Exeter Archival Diabetes Biobank (EADB) (combined N = 235), stratified by recently reported age at diagnosis endotypes (<7, 7-12, ≥13 years) across increasing diabetes durations. The proportion of individuals with detectable C-peptide declined beyond the first year after diagnosis, but this was most marked in the youngest age group (<1-year duration: age <7 years: 18 of 20 [90%], 7-12 years: 107 of 110 [97%], ≥13 years: 58 of 61 [95%] vs. 1-5 years postdiagnosis: <7 years: 172 of 522 [33%], 7-12 years: 604 of 995 [61%], ≥13 years: 225 of 289 [78%]). A similar profile was observed in β-cell loss, with those diagnosed at younger ages experiencing more rapid loss of islets containing insulin-positive (insulin+) β-cells <1 year postdiagnosis: age <7 years: 23 of 26 (88%), 7-12 years: 32 of 33 (97%), ≥13 years: 22 of 25 (88%) vs. 1-5 years postdiagnosis: <7 years: 1 of 12 (8.3%), 7-12 years: 7 of 13 (54%), ≥13 years: 7 of 8 (88%). These data should be considered in the planning and interpretation of intervention trials designed to promote β-cell retention and function. [ABSTRACT FROM AUTHOR]

Published

2022

7. Antithymocyte Globulin Plus G-CSF Combination Therapy Leads to Sustained Immunomodulatory and Metabolic Effects in a Subset of Responders With Established Type 1 Diabetes

Author

Haller, Michael J, Gitelman, Stephen E, Gottlieb, Peter A, Michels, Aaron W, Perry, Daniel J, Schultz, Andrew R, Hulme, Maigan A, Shuster, Jonathan J, Zou, Baiming, Wasserfall, Clive H, Posgai, Amanda L, Mathews, Clayton E, Brusko, Todd M, Atkinson, Mark A, and Schatz, Desmond A

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Immunology, Immunotherapy, Prevention, Diabetes, Clinical Research, Clinical Trials and Supportive Activities, 2.1 Biological and endogenous factors, Metabolic and endocrine, Good Health and Well Being, Adolescent, Adult, Antilymphocyte Serum, Area Under Curve, C-Peptide, CD4-Positive T-Lymphocytes, CD56 Antigen, CD8-Positive T-Lymphocytes, Child, Diabetes Mellitus, Type 1, Female, Forkhead Transcription Factors, Granulocyte Colony-Stimulating Factor, Humans, Immunologic Factors, Killer Cells, Natural, Male, Middle Aged, Monocytes, Polyethylene Glycols, Receptors, CXCR3, Receptors, IgG, Recombinant Proteins, T-Lymphocyte Subsets, T-Lymphocytes, Regulatory, Young Adult, Medical and Health Sciences, Endocrinology & Metabolism, Biomedical and clinical sciences

Abstract

Low-dose antithymocyte globulin (ATG) plus pegylated granulocyte colony-stimulating factor (G-CSF) preserves β-cell function for at least 12 months in type 1 diabetes. Herein, we describe metabolic and immunological parameters 24 months following treatment. Patients with established type 1 diabetes (duration 4-24 months) were randomized to ATG and pegylated G-CSF (ATG+G-CSF) (N = 17) or placebo (N = 8). Primary outcomes included C-peptide area under the curve (AUC) following a mixed-meal tolerance test (MMTT) and flow cytometry. "Responders" (12-month C-peptide ≥ baseline), "super responders" (24-month C-peptide ≥ baseline), and "nonresponders" (12-month C-peptide < baseline) were evaluated for biomarkers of outcome. At 24 months, MMTT-stimulated AUC C-peptide was not significantly different in ATG+G-CSF (0.49 nmol/L/min) versus placebo (0.29 nmol/L/min). Subjects treated with ATG+G-CSF demonstrated reduced CD4+ T cells and CD4+/CD8+ T-cell ratio and increased CD16+CD56hi natural killer cells (NK), CD4+ effector memory T cells (Tem), CD4+PD-1+ central memory T cells (Tcm), Tcm PD-1 expression, and neutrophils. FOXP3+Helios+ regulatory T cells (Treg) were elevated in ATG+G-CSF subjects at 6, 12, and 18 but not 24 months. Immunophenotyping identified differential HLA-DR expression on monocytes and NK and altered CXCR3 and PD-1 expression on T-cell subsets. As such, a group of metabolic and immunological responders was identified. A phase II study of ATG+G-CSF in patients with new-onset type 1 diabetes is ongoing and may support ATG+G-CSF as a prevention strategy in high-risk subjects.

Published

2016

8. Recommendations for the Definition of Clinical Responder in Insulin Preservation Studies

Author

Beam, Craig A, Gitelman, Stephen E, Palmer, Jerry P, and Group, the Type 1 Diabetes TrialNet Study

Subjects

Medical Biotechnology, Biomedical and Clinical Sciences, Diabetes, Clinical Trials and Supportive Activities, Clinical Research, Metabolic and endocrine, Adolescent, Bias, C-Peptide, Clinical Trials as Topic, Diabetes Mellitus, Type 1, Female, Humans, Hypoglycemic Agents, Insulin, Insulin-Secreting Cells, Male, Reproducibility of Results, Treatment Outcome, Type 1 Diabetes TrialNet Study Group, Medical and Health Sciences, Endocrinology & Metabolism, Biomedical and clinical sciences

Abstract

Clinical responder studies should contribute to the translation of effective treatments and interventions to the clinic. Since ultimately this translation will involve regulatory approval, we recommend that clinical trials prespecify a responder definition that can be assessed against the requirements and suggestions of regulatory agencies. In this article, we propose a clinical responder definition to specifically assist researchers and regulatory agencies in interpreting the clinical importance of statistically significant findings for studies of interventions intended to preserve β-cell function in newly diagnosed type 1 diabetes. We focus on studies of 6-month β-cell preservation in type 1 diabetes as measured by 2-h-stimulated C-peptide. We introduce criteria (bias, reliability, and external validity) for the assessment of responder definitions to ensure they meet U.S. Food and Drug Administration and European Medicines Agency guidelines. Using data from several published TrialNet studies, we evaluate our definition (no decrease in C-peptide) against published alternatives and determine that our definition has minimum bias with external validity. We observe that reliability could be improved by using changes in C-peptide later than 6 months beyond baseline. In sum, to support efficacy claims of β-cell preservation therapies in type 1 diabetes submitted to U.S. and European regulatory agencies, we recommend use of our definition.

Published

2014

9. Teplizumab (anti-CD3 mAb) treatment preserves C-peptide responses in patients with new-onset type 1 diabetes in a randomized controlled trial: metabolic and immunologic features at baseline identify a subgroup of responders.

Author

Herold, Kevan C, Gitelman, Stephen E, Ehlers, Mario R, Gottlieb, Peter A, Greenbaum, Carla J, Hagopian, William, Boyle, Karen D, Keyes-Elstein, Lynette, Aggarwal, Sudeepta, Phippard, Deborah, Sayre, Peter H, McNamara, James, Bluestone, Jeffrey A, and AbATE Study Team

Subjects

AbATE Study Team, Humans, Diabetes Mellitus, Type 1, C-Peptide, Adolescent, Adult, Child, Female, Male, Antibodies, Monoclonal, Humanized, Clinical Trials and Supportive Activities, Autoimmune Disease, Pediatric, Clinical Research, Diabetes, Metabolic and endocrine, Endocrinology & Metabolism, Medical and Health Sciences

Abstract

Trials of immune therapies in new-onset type 1 diabetes (T1D) have shown success, but not all subjects respond, and the duration of response is limited. Our aim was to determine whether two courses of teplizumab, an Fc receptor-nonbinding anti-CD3 monoclonal antibody, reduces the decline in C-peptide levels in patients with T1D 2 years after disease onset. We also set out to identify characteristics of responders. We treated 52 subjects with new-onset T1D with teplizumab for 2 weeks at diagnosis and after 1 year in an open-label, randomized, controlled trial. In the intent to treat analysis of the primary end point, patients treated with teplizumab had a reduced decline in C-peptide at 2 years (mean -0.28 nmol/L [95% CI -0.36 to -0.20]) versus control (mean -0.46 nmol/L [95% CI -0.57 to -0.35]; P = 0.002), a 75% improvement. The most common adverse events were rash, transient upper respiratory infections, headache, and nausea. In a post hoc analysis we characterized clinical responders and found that metabolic (HbA1c and insulin use) and immunologic features distinguished this group from those who did not respond to teplizumab. We conclude that teplizumab treatment preserves insulin production and reduces the use of exogenous insulin in some patients with new-onset T1D. Metabolic and immunologic features at baseline can identify a subgroup with robust responses to immune therapy.

Published

2013

10. Immune therapy and β-cell death in type 1 diabetes.

Author

Lebastchi, Jasmin, Deng, Songyan, Lebastchi, Amir, Beshar, Isabel, Willi, Steven, Gottlieb, Peter, Akirav, Eitan, Herold, Kevan, Gitelman, Stephen, and Bluestone, Jeffrey

Subjects

Adult, Antibodies, Monoclonal, Humanized, C-Peptide, CD3 Complex, Cytotoxicity Tests, Immunologic, Cytotoxicity, Immunologic, DNA Methylation, Diabetes Mellitus, Type 1, Female, Humans, Hypoglycemic Agents, Immunologic Factors, Immunotherapy, Insulin, Insulin Secretion, Insulin-Secreting Cells, Islets of Langerhans, Male, Postprandial Period, Young Adult

Abstract

Type 1 diabetes (T1D) results from immune-mediated destruction of insulin-producing β-cells. The killing of β-cells is not currently measurable; β-cell functional studies routinely used are affected by environmental factors such as glucose and cannot distinguish death from dysfunction. Moreover, it is not known whether immune therapies affect killing. We developed an assay to identify β-cell death by measuring relative levels of unmethylated INS DNA in serum and used it to measure β-cell death in a clinical trial of teplizumab. We studied 43 patients with recent-onset T1D, 13 nondiabetic subjects, and 37 patients with T1D treated with FcR nonbinding anti-CD3 monoclonal antibody (teplizumab) or placebo. Patients with recent-onset T1D had higher rates of β-cell death versus nondiabetic control subjects, but patients with long-standing T1D had lower levels. When patients with recent-onset T1D were treated with teplizumab, β-cell function was preserved (P < 0.05) and the rates of β-cell were reduced significantly (P < 0.05). We conclude that there are higher rates of β-cell death in patients with recent-onset T1D compared with nondiabetic subjects. Improvement in C-peptide responses with immune intervention is associated with decreased β-cell death.

Published

2013

11. Genetic Composition and Autoantibody Titers Model the Probability of Detecting C-Peptide Following Type 1 Diabetes Diagnosis.

Author

Williams, MacKenzie D., Bacher, Rhonda, Perry, Daniel J., Grace, C. Ramsey, McGrail, Kieran M., Posgai, Amanda L., Muir, Andrew, Chamala, Srikar, Haller, Michael J., Schatz, Desmond A., Brusko, Todd M., Atkinson, Mark A., and Wasserfall, Clive H.

Subjects

*TYPE 1 diabetes, *DIAGNOSIS of diabetes, *INSULINOMA, *C-peptide, *TITERS, *GENERALIZED estimating equations, *AUTOANTIBODIES, *RESEARCH, *CROSS-sectional method, *RESEARCH methodology, *PHOSPHATASES, *MEDICAL cooperation, *EVALUATION research, *COMPARATIVE studies, *RESEARCH funding

Abstract

We and others previously demonstrated that a type 1 diabetes genetic risk score (GRS) improves the ability to predict disease progression and onset in at-risk subjects with islet autoantibodies. Here, we hypothesized that GRS and islet autoantibodies, combined with age at onset and disease duration, could serve as markers of residual β-cell function following type 1 diabetes diagnosis. Generalized estimating equations were used to investigate whether GRS along with insulinoma-associated protein-2 autoantibody (IA-2A), zinc transporter 8 autoantibody (ZnT8A), and GAD autoantibody (GADA) titers were predictive of C-peptide detection in a largely cross-sectional cohort of 401 subjects with type 1 diabetes (median duration 4.5 years [range 0-60]). Indeed, a combined model with incorporation of disease duration, age at onset, GRS, and titers of IA-2A, ZnT8A, and GADA provided superior capacity to predict C-peptide detection (quasi-likelihood information criterion [QIC] = 334.6) compared with the capacity of disease duration, age at onset, and GRS as the sole parameters (QIC = 359.2). These findings support the need for longitudinal validation of our combinatorial model. The ability to project the rate and extent of decline in residual C-peptide production for individuals with type 1 diabetes could critically inform enrollment and benchmarking for clinical trials where investigators are seeking to preserve or restore endogenous β-cell function. [ABSTRACT FROM AUTHOR]

Published

2021

12. Baseline Assessment of Circulating MicroRNAs Near Diagnosis of Type 1 Diabetes Predicts Future Stimulated Insulin Secretion.

Author

Snowhite, Isaac, Pastori, Ricardo, Sosenko, Jay, Messinger Cayetano, Shari, and Pugliese, Alberto

Subjects

*TYPE 1 diabetes, *SECRETION, *INSULIN, *MICRORNA, *NUCLEOTIDE sequence, *RESEARCH, *RESEARCH methodology, *MEDICAL cooperation, *EVALUATION research, *COMPARATIVE studies, *C-peptide

Abstract

Type 1 diabetes is an autoimmune disease resulting in severely impaired insulin secretion. We investigated whether circulating microRNAs (miRNAs) are associated with residual insulin secretion at diagnosis and predict the severity of its future decline. We studied 53 newly diagnosed subjects enrolled in placebo groups of TrialNet clinical trials. We measured serum levels of 2,083 miRNAs, using RNA sequencing technology, in fasting samples from the baseline visit (<100 days from diagnosis), during which residual insulin secretion was measured with a mixed meal tolerance test (MMTT). Area under the curve (AUC) C-peptide and peak C-peptide were stratified by quartiles of expression of 31 miRNAs. After adjustment for baseline C-peptide, age, BMI, and sex, baseline levels of miR-3187-3p, miR-4302, and the miRNA combination of miR-3187-3p/miR-103a-3p predicted differences in MMTT C-peptide AUC/peak levels at the 12-month visit; the combination miR-3187-3p/miR-4723-5p predicted proportions of subjects above/below the 200 pmol/L clinical trial eligibility threshold at the 12-month visit. Thus, miRNA assessment at baseline identifies associations with C-peptide and stratifies subjects for future severity of C-peptide loss after 1 year. We suggest that miRNAs may be useful in predicting future C-peptide decline for improved subject stratification in clinical trials. [ABSTRACT FROM AUTHOR]

Published

2021

13. An Insulin-Chromogranin A Hybrid Peptide Activates DR11-Restricted T Cells in Human Type 1 Diabetes.

Author

Callebaut A, Guyer P, Baker RL, Gallegos JB, Hohenstein AC, Gottlieb PA, Mathieu C, Overbergh L, Haskins K, and James EA

Subjects

Humans, Animals, Mice, T-Lymphocytes, Proinsulin, C-Peptide, Chromogranin A, Peptides, Insulin, Regular, Human, Epitopes, Peptide Fragments, Insulin, Diabetes Mellitus, Type 1

Abstract

Hybrid insulin peptides (HIPs) formed through covalent cross-linking of proinsulin fragments to secretory granule peptides are detectable within murine and human islets. The 2.5HIP (C-peptide-chromogranin A [CgA] HIP), recognized by the diabetogenic BDC-2.5 clone, is a major autoantigen in the nonobese diabetic mouse. However, the relevance of this epitope in human disease is currently unclear. A recent study probed T-cell reactivity toward HIPs in patients with type 1 diabetes, documenting responses in one-third of the patients and isolating several HIP-reactive T-cell clones. In this study, we isolated a novel T-cell clone and showed that it responds vigorously to the human equivalent of the 2.5HIP (designated HIP9). Although the responding patient carried the risk-associated DRB1*04:01/DQ8 haplotype, the response was restricted by DRB1*11:03 (DR11). HLA class II tetramer staining revealed higher frequencies of HIP9-reactive T cells in individuals with diabetes than in control participants. Furthermore, in DR11+ participants carrying the DRB4 allele, HIP9-reactive T-cell frequencies were higher than observed frequencies for the immunodominant proinsulin 9-28 epitope. Finally, there was a negative correlation between HIP9-reactive T-cell frequency and age at diagnosis. These results provide direct evidence that this C-peptide-CgA HIP is relevant in human type 1 diabetes and suggest a mechanism by which nonrisk HLA haplotypes may contribute to the development of β-cell autoimmunity., (© 2024 by the American Diabetes Association.)

Published

2024

14. Ongoing β-Cell Turnover in Adult Nonhuman Primates Is Not Adaptively Increased in Streptozotocin-Induced Diabetes

Author

Saisho, Yoshifumi, Manesso, Erica, Butler, Alexandra E, Galasso, Ryan, Kavanagh, Kylie, Flynn, Mickey, Zhang, Li, Clark, Paige, Gurlo, Tatyana, Toffolo, Gianna M, Cobelli, Claudio, Wagner, Janice D, and Butler, Peter C

Subjects

Biomedical and Clinical Sciences, Autoimmune Disease, Stem Cell Research - Nonembryonic - Non-Human, Stem Cell Research, Regenerative Medicine, Diabetes, Metabolic and endocrine, Animals, Apoptosis, C-Peptide, Cell Division, Chlorocebus aethiops, Diabetes Mellitus, Experimental, Enzyme-Linked Immunosorbent Assay, Glucose Tolerance Test, Immunohistochemistry, Insulin, Insulin-Secreting Cells, Pancreas, Streptozocin, Medical and Health Sciences, Endocrinology & Metabolism, Biomedical and clinical sciences

Abstract

Objectiveβ-Cell turnover and its potential to permit β-cell regeneration in adult primates are unknown. Our aims were 1) to measure β-cell turnover in adult nonhuman primates; 2) to establish the relative contribution of β-cell replication and formation of new β-cells from other precursors (defined thus as β-cell neogenesis); and 3) to establish whether there is an adaptive increase in β-cell formation (attempted regeneration) in streptozotocin (STZ)-induced diabetes in adult nonhuman primates.Research design and methodsAdult (aged 7 years) vervet monkeys were administered STZ (45-55 mg/kg, n = 7) or saline (n = 9). Pancreas was obtained from each animal twice, first by open surgical biopsy and then by euthanasia. β-Cell turnover was evaluated by applying a mathematic model to measured replication and apoptosis rates.Resultsβ-Cell turnover is present in adult nonhuman primates (3.3 ± 0.9 mg/month), mostly (~80%) derived from β-cell neogenesis. β-Cell formation was minimal in STZ-induced diabetes. Despite marked hyperglycemia, β-cell apoptosis was not increased in monkeys administered STZ.ConclusionsThere is ongoing β-cell turnover in adult nonhuman primates that cannot be accounted for by β-cell replication. There is no evidence of β-cell regeneration in monkeys administered STZ. Hyperglycemia does not induce β-cell apoptosis in nonhuman primates in vivo.

Published

2011

15. Ongoing beta-cell turnover in adult nonhuman primates is not adaptively increased in streptozotocin-induced diabetes.

Author

Saisho, Yoshifumi, Manesso, Erica, Butler, Alexandra E, Galasso, Ryan, Kavanagh, Kylie, Flynn, Mickey, Zhang, Li, Clark, Paige, Gurlo, Tatyana, Toffolo, Gianna M, Cobelli, Claudio, Wagner, Janice D, and Butler, Peter C

Subjects

Pancreas, Animals, Diabetes Mellitus, Experimental, Streptozocin, Insulin, C-Peptide, Glucose Tolerance Test, Enzyme-Linked Immunosorbent Assay, Immunohistochemistry, Cell Division, Apoptosis, Insulin-Secreting Cells, Chlorocebus aethiops, Cercopithecus aethiops, Diabetes Mellitus, Experimental, Medical and Health Sciences, Endocrinology & Metabolism

Abstract

Objectiveβ-Cell turnover and its potential to permit β-cell regeneration in adult primates are unknown. Our aims were 1) to measure β-cell turnover in adult nonhuman primates; 2) to establish the relative contribution of β-cell replication and formation of new β-cells from other precursors (defined thus as β-cell neogenesis); and 3) to establish whether there is an adaptive increase in β-cell formation (attempted regeneration) in streptozotocin (STZ)-induced diabetes in adult nonhuman primates.Research design and methodsAdult (aged 7 years) vervet monkeys were administered STZ (45-55 mg/kg, n = 7) or saline (n = 9). Pancreas was obtained from each animal twice, first by open surgical biopsy and then by euthanasia. β-Cell turnover was evaluated by applying a mathematic model to measured replication and apoptosis rates.Resultsβ-Cell turnover is present in adult nonhuman primates (3.3 ± 0.9 mg/month), mostly (~80%) derived from β-cell neogenesis. β-Cell formation was minimal in STZ-induced diabetes. Despite marked hyperglycemia, β-cell apoptosis was not increased in monkeys administered STZ.ConclusionsThere is ongoing β-cell turnover in adult nonhuman primates that cannot be accounted for by β-cell replication. There is no evidence of β-cell regeneration in monkeys administered STZ. Hyperglycemia does not induce β-cell apoptosis in nonhuman primates in vivo.

Published

2011

16. Management of Latent Autoimmune Diabetes in Adults: A Consensus Statement From an International Expert Panel.

Author

Buzzetti, Raffaella, Tuomi, Tiinamaija, Mauricio, Didac, Pietropaolo, Massimo, Zhou, Zhiguang, Pozzilli, Paolo, and Leslie, Richard David

Subjects

*TYPE 1 diabetes, *DIABETES, *CLINICAL trials, *METABOLIC regulation, *TYPE 2 diabetes, *ADULTS, *ENZYME metabolism, *AUTOANTIBODIES, *RESEARCH, *RESEARCH methodology, *CONFERENCES & conventions, *HYPOGLYCEMIC agents, *SULFONYLUREAS, *EVALUATION research, *MEDICAL cooperation, *MEDICAL protocols, *COMPARATIVE studies, *DISEASE susceptibility, *C-peptide, *ALGORITHMS

Abstract

A substantial proportion of patients with adult-onset diabetes share features of both type 1 diabetes (T1D) and type 2 diabetes (T2D). These individuals, at diagnosis, clinically resemble T2D patients by not requiring insulin treatment, yet they have immunogenetic markers associated with T1D. Such a slowly evolving form of autoimmune diabetes, described as latent autoimmune diabetes of adults (LADA), accounts for 2-12% of all patients with adult-onset diabetes, though they show considerable variability according to their demographics and mode of ascertainment. While therapeutic strategies aim for metabolic control and preservation of residual insulin secretory capacity, endotype heterogeneity within LADA implies a personalized approach to treatment. Faced with a paucity of large-scale clinical trials in LADA, an expert panel reviewed data and delineated one therapeutic approach. Building on the 2020 American Diabetes Association (ADA)/European Association for the Study of Diabetes (EASD) consensus for T2D and heterogeneity within autoimmune diabetes, we propose "deviations" for LADA from those guidelines. Within LADA, C-peptide values, proxy for β-cell function, drive therapeutic decisions. Three broad categories of random C-peptide levels were introduced by the panel: 1) C-peptide levels <0.3 nmol/L: a multiple-insulin regimen recommended as for T1D; 2) C-peptide values ≥0.3 and ≤0.7 nmol/L: defined by the panel as a "gray area" in which a modified ADA/EASD algorithm for T2D is recommended; consider insulin in combination with other therapies to modulate β-cell failure and limit diabetic complications; 3) C-peptide values >0.7 nmol/L: suggests a modified ADA/EASD algorithm as for T2D but allowing for the potentially progressive nature of LADA by monitoring C-peptide to adjust treatment. The panel concluded by advising general screening for LADA in newly diagnosed non-insulin-requiring diabetes and, importantly, that large randomized clinical trials are warranted. [ABSTRACT FROM AUTHOR]

Published

2020

17. Subtypes of Type 2 Diabetes Determined From Clinical Parameters.

Author

Ahlqvist, Emma, Prasad, Rashmi B., and Groop, Leif

Subjects

*TYPE 2 diabetes, *ETIOLOGY of diseases, *DIABETIC nephropathies, *GLYCOSYLATED hemoglobin, *INSULIN resistance, *RESEARCH, *RESEARCH methodology, *TYPE 1 diabetes, *EVALUATION research, *MEDICAL cooperation, *COMPARATIVE studies, *C-peptide

Abstract

Type 2 diabetes (T2D) is defined by a single metabolite, glucose, but is increasingly recognized as a highly heterogeneous disease, including individuals with varying clinical characteristics, disease progression, drug response, and risk of complications. Identification of subtypes with differing risk profiles and disease etiologies at diagnosis could open up avenues for personalized medicine and allow clinical resources to be focused to the patients who would be most likely to develop diabetic complications, thereby both improving patient health and reducing costs for the health sector. More homogeneous populations also offer increased power in experimental, genetic, and clinical studies. Clinical parameters are easily available and reflect relevant disease pathways, including the effects of both genetic and environmental exposures. We used six clinical parameters (GAD autoantibodies, age at diabetes onset, HbA1c, BMI, and measures of insulin resistance and insulin secretion) to cluster adult-onset diabetes patients into five subtypes. These subtypes have been robustly reproduced in several populations and associated with different risks of complications, comorbidities, genetics, and response to treatment. Importantly, the group with severe insulin-deficient diabetes (SIDD) had increased risk of retinopathy and neuropathy, whereas the severe insulin-resistant diabetes (SIRD) group had the highest risk for diabetic kidney disease (DKD) and fatty liver, emphasizing the importance of insulin resistance for DKD and hepatosteatosis in T2D. In conclusion, we believe that subclassification using these highly relevant parameters could provide a framework for personalized medicine in diabetes. [ABSTRACT FROM AUTHOR]

Published

2020

18. Slowed Metabolic Decline After 1 Year of Oral Insulin Treatment Among Individuals at High Risk for Type 1 Diabetes in the Diabetes Prevention Trial-Type 1 (DPT-1) and TrialNet Oral Insulin Prevention Trials.

Author

Sosenko, Jay M., Skyler, Jay S., Herold, Kevan C., Schatz, Desmond A., Haller, Michael J., Pugliese, Alberto, Cleves, Mario, Geyer, Susan, Rafkin, Lisa E., Matheson, Della, Palmer, Jerry P., and Type 1 Diabetes TrialNet Study Group

Subjects

*TYPE 1 diabetes, *INSULIN, *GLUCOSE tolerance tests, *PLACEBOS, *DIABETES, *INSULIN therapy, *THERAPEUTIC use of monoclonal antibodies, *BLOOD sugar, *C-peptide, *COMPARATIVE studies, *RESEARCH methodology, *MEDICAL cooperation, *PHARMACOKINETICS, *RESEARCH, *EVALUATION research, *RANDOMIZED controlled trials

Abstract

We assessed whether oral insulin slowed metabolic decline after 1 year of treatment in individuals at high risk for type 1 diabetes. Two oral insulin trials that did not show efficacy overall and had type 1 diabetes as the primary end point were analyzed: the Diabetes Prevention Trial-Type 1 (DPT-1) and the TrialNet oral insulin trials. Oral glucose tolerance tests at baseline and after 1 year of treatment were analyzed. Among those at high risk (with a Diabetes Prevention Trial-Type 1 Risk Score [DPTRS] ≥6.75), the area under the curve (AUC) C-peptide increased significantly from baseline to 1 year in each oral insulin group, whereas the AUC glucose increased significantly in each placebo group. At 1 year, the AUC C-peptide/AUC glucose (AUC Ratio) was significantly higher in the oral insulin group than in the placebo group in each trial (P < 0.05; P = 0.057 when adjusted for age in the TrialNet trial) and in both trials combined (P < 0.01 with or without adjustment for age). For a DPTRS <6.75, oral insulin groups did not differ from placebo groups in the AUC Ratio. The findings suggest that 1 year of treatment with oral insulin slows metabolic deterioration in individuals at high risk for type 1 diabetes. Moreover, the findings further suggest that metabolic end points can be useful adjuncts to the diagnostic end point in assessments of preventive treatments for the disorder. [ABSTRACT FROM AUTHOR]

Published

2020

19. A Hybrid Insulin Epitope Maintains High 2D Affinity for Diabetogenic T Cells in the Periphery.

Author

Baoyu Liu, Hood, Jennifer D., Kolawole, Elizabeth M., Woodruff, Derek M., Vignali, Dario A., Bettini, Maria, Evavold, Brian D., and Liu, Baoyu

Subjects

*T cells, *TYPE 1 diabetes, *INSULIN, *ISLANDS of Langerhans, *IMMUNE recognition, *ANIMAL experimentation, *ANTIGEN-antibody reactions, *ANTIGENS, *C-peptide, *CELL receptors, *CELLS, *COMPARATIVE studies, *LYMPH nodes, *RESEARCH methodology, *MEDICAL cooperation, *MICE, *PEPTIDES, *PROTEIN precursors, *RESEARCH, *SPLEEN, *THYMUS, *EVALUATION research

Abstract

β-Cell antigen recognition by autoreactive T cells is essential in type 1 diabetes (T1D) pathogenesis. Recently, insulin hybrid peptides (HIPs) were identified as strong agonists for CD4 diabetogenic T cells. Here, using BDC2.5 transgenic and NOD mice, we investigated T-cell recognition of the HIP2.5 epitope, which is a fusion of insulin C-peptide and chromogranin A (ChgA) fragments, and compared it with the WE14 and ChgA29-42 epitopes. We measured in situ two-dimensional affinity on individual live T cells from thymus, spleen, pancreatic lymph nodes, and islets before and after diabetes. Although preselection BDC2.5 thymocytes possess higher affinity than splenic BDC2.5 T cells for all three epitopes, peripheral splenic T cells maintained high affinity only to the HIP2.5 epitope. In polyclonal NOD mice, a high frequency (∼40%) of HIP2.5-specific islet T cells were identified at both prediabetic and diabetic stages comprising two distinct high- and low-affinity populations that differed in affinity by 100-fold. This high frequency of high- and low-affinity HIP2.5 T cells in the islets potentially represents a major risk factor in diabetes pathogenesis. [ABSTRACT FROM AUTHOR]

Published

2020

20. The p66Shc Protein Mediates Insulin Resistance and Secretory Dysfunction in Pancreatic β-Cells Under Lipotoxic Conditions

Author

Giuseppina Biondi, Nicola Marrano, Lucia Dipaola, Anna Borrelli, Martina Rella, Rossella D’Oria, Valentina A. Genchi, Cristina Caccioppoli, Immacolata Porreca, Angelo Cignarelli, Sebastio Perrini, Piero Marchetti, Leonardo Vincenti, Luigi Laviola, Francesco Giorgino, and Annalisa Natalicchio

Subjects

Mice, Src Homology 2 Domain-Containing, Transforming Protein 1, C-Peptide, Insulin-Secreting Cells, Endocrinology, Diabetes and Metabolism, Palmitates, Internal Medicine, Animals, Humans, Insulin, Apoptosis, Insulin Resistance, Signal Transduction

Abstract

We evaluated the role of the p66Shc redox adaptor protein in pancreatic β-cell insulin resistance that develops under lipotoxic conditions and with excess body fat. Prolonged exposure to palmitate in vitro or the presence of overweight/obesity augmented p66Shc expression levels and caused an impaired ability of exogenous insulin to increase cellular insulin content and secreted C-peptide levels in INS-1E cells and human and murine islets. In INS-1E cells, p66Shc knockdown resulted in enhanced insulin-induced augmentation of insulin content and C-peptide secretion and prevented the ability of palmitate to impair these effects of insulin. Conversely, p66Shc overexpression impaired insulin-induced augmentation of insulin content and C-peptide secretion in both the absence and presence of palmitate. Under lipotoxic condition, the effects of p66Shc are mediated by a p53-induced increase in p66Shc protein levels and JNK-induced p66Shc phosphorylation at Ser36 and appear to involve the phosphorylation of the ribosomal protein S6 kinase at Thr389 and of insulin receptor substrate 1 at Ser307, resulting in the inhibition of insulin-stimulated protein kinase B phosphorylation at Ser473. Thus, the p66Shc protein mediates the impaired β-cell function and insulin resistance induced by saturated fatty acids and excess body fat.

Published

2022

21. Low-Dose Anti-Thymocyte Globulin Preserves C-Peptide, Reduces HbA1c, and Increases Regulatory to Conventional T-Cell Ratios in New-Onset Type 1 Diabetes: Two-Year Clinical Trial Data.

Author

Haller, Michael J., Long, S. Alice, Blanchfield, J. Lori, Schatz, Desmond A., Skyler, Jay S., Krischer, Jeffrey P., Bundy, Brian N., Geyer, Susan M., Warnock, Megan V., Miller, Jessica L., Atkinson, Mark A., Becker, Dorothy J., Baidal, David A., DiMeglio, Linda A., Gitelman, Stephen E., Goland, Robin, Gottlieb, Peter A., Herold, Kevan C., Marks, Jennifer B., and Moran, Antoinette

Subjects

*TYPE 1 diabetes, *C-peptide, *GLOBULINS, *CLINICAL trials, *T cells

Abstract

A three-arm, randomized, double-masked, placebo-controlled phase 2b trial performed by the Type 1 Diabetes TrialNet Study Group previously demonstrated that low-dose anti-thymocyte globulin (ATG) (2.5 mg/kg) preserved β-cell function and reduced HbA1c for 1 year in new-onset type 1 diabetes. Subjects (N = 89) were randomized to 1) ATG and pegylated granulocyte colony-stimulating factor (GCSF), 2) ATG alone, or 3) placebo. Herein, we report 2-year area under the curve (AUC) C-peptide and HbA1c, prespecified secondary end points, and potential immunologic correlates. The 2-year mean mixed-meal tolerance test-stimulated AUC C-peptide, analyzed by ANCOVA adjusting for baseline C-peptide, age, and sex (n = 82) with significance defined as one-sided P < 0.025, was significantly higher in subjects treated with ATG versus placebo (P = 0.00005) but not ATG/GCSF versus placebo (P = 0.032). HbA1c was significantly reduced at 2 years in subjects treated with ATG (P = 0.011) and ATG/GCSF (P = 0.022) versus placebo. Flow cytometry analyses demonstrated reduced circulating CD4:CD8 ratio, increased regulatory T-cell:conventional CD4 T-cell ratios, and increased PD-1+CD4+ T cells following low-dose ATG and ATG/GCSF. Low-dose ATG partially preserved β-cell function and reduced HbA1c 2 years after therapy in new-onset type 1 diabetes. Future studies should determine whether low-dose ATG might prevent or delay the onset of type 1 diabetes. [ABSTRACT FROM AUTHOR]

Published

2019

22. Circulating C-Peptide Levels in Living Children and Young People and Pancreatic β-Cell Loss in Pancreas Donors Across Type 1 Diabetes Disease Duration

Author

Alice L.J. Carr, Jamie R.J. Inshaw, Christine S. Flaxman, Pia Leete, Rebecca C. Wyatt, Lydia A. Russell, Matthew Palmer, Dmytro Prasolov, Thomas Worthington, Bethany Hull, Linda S. Wicker, David B. Dunger, Richard A. Oram, Noel G. Morgan, John A. Todd, Sarah J. Richardson, and Rachel E.J. Besser

Subjects

Diabetes Mellitus, Type 1, Adolescent, C-Peptide, Insulin-Secreting Cells, Endocrinology, Diabetes and Metabolism, Internal Medicine, Humans, Infant, Child, Pancreas, Tissue Donors

Abstract

C-peptide declines in type 1 diabetes, although many long-duration patients retain low, but detectable levels. Histological analyses confirm that β-cells can remain following type 1 diabetes onset. We explored the trends observed in C-peptide decline in the UK Genetic Resource Investigating Diabetes (UK GRID) cohort (N = 4,079), with β-cell loss in pancreas donors from the network for Pancreatic Organ donors with Diabetes (nPOD) biobank and the Exeter Archival Diabetes Biobank (EADB) (combined N = 235), stratified by recently reported age at diagnosis endotypes (

Published

2022

23. Increase Functional β-Cell Mass in Subcutaneous Alginate Capsules With Porcine Prenatal Islet Cells but Loss With Human Adult Islet Cells.

Author

De Mesmaeker, Ines, Robert, Thomas, Suenens, Krista G., Stangé, Geert M., Van Hulle, Freya, Ling, Zhidong, Tomme, Peter, Jacobs-Tulleneers-Thevissen, Daniel, Pipeleers, Bart Keymeulen and Daniel G., Keymeulen, Bart, and Pipeleers, Daniel G

Subjects

*ALGINIC acid, *ISLANDS of Langerhans, *METABOLIC regulation, *DNA replication, *PERITONEUM, *ISLANDS of Langerhans transplantation, *ALGINATES, *ANIMAL experimentation, *C-peptide, *PHARMACEUTICAL encapsulation, *COMPARATIVE studies, *INSULIN, *RESEARCH methodology, *MEDICAL cooperation, *MICE, *RESEARCH, *SWINE, *EVALUATION research

Abstract

Alginate (Alg)-encapsulated porcine islet cell grafts are developed to overcome limitations of human islet transplantation. They can generate functional implants in animals when prepared from fetal, perinatal, and adult pancreases. Implants have not yet been examined for efficacy to establish sustained, metabolically adequate functional β-cell mass (FBM) in comparison with human islet cells. This study in immune-compromised mice demonstrates that subcutaneous implants of Alg-encapsulated porcine prenatal islet cells with 4 × 105 β-cells form, over 10 weeks, a FBM that results in glucose-induced plasma C-peptide >2 ng/mL and metabolic control over the following 10 weeks, with higher efficiency than nonencapsulated, while failing in peritoneum. This intracapsular FBM formation involves β-cell replication, increasing number fourfold, and maturation toward human adult β-cells. Subcutaneous Alg-encapsulated human islet cells with similar β-cell number establish implants with plasma C-peptide >2 ng/mL for the first 10 weeks, with nonencapsulated cells failing; their β-cells do not replicate but progressively die (>70%), explaining C-peptide decline and insufficient metabolic control. An Alg matrix thus helps establish β-cell functions in subcutis. It allows formation of sustained metabolically adequate FBM by immature porcine β-cells with proliferative activity but not by human adult islet cells. These findings define conditions for evaluating its immune-protecting properties. [ABSTRACT FROM AUTHOR]

Published

2018

24. Genetic Determinants of Glycemic Traits and the Risk of Gestational Diabetes Mellitus.

Author

Powe, Camille E., Nodzenski, Michael, Talbot, Octavious, Allard, Catherine, Briggs, Catherine, Leya, Marysa V., Perron, Patrice, Bouchard, Luigi, Florez, Jose C., Scholtens, Denise M., Lowe Jr., William L., Hivert, Marie-France, and Lowe, William L Jr

Subjects

*GENETIC polymorphisms, *GESTATIONAL diabetes, *TYPE 2 diabetes, *HYPERGLYCEMIA, *GLUCOSE tolerance tests, *BLOOD sugar analysis, *BLOOD sugar, *C-peptide, *COMPARATIVE studies, *DISEASE susceptibility, *INSULIN resistance, *RESEARCH methodology, *MEDICAL cooperation, *RESEARCH, *RESEARCH funding, *EVALUATION research, *GENOTYPES

Abstract

Many common genetic polymorphisms are associated with glycemic traits and type 2 diabetes (T2D), but knowledge about genetic determinants of glycemic traits in pregnancy is limited. We tested genetic variants known to be associated with glycemic traits and T2D in the general population for associations with glycemic traits in pregnancy and gestational diabetes mellitus (GDM). Participants in two cohorts (Genetics of Glucose regulation in Gestation and Growth [Gen3G] and Hyperglycemia and Adverse Pregnancy Outcome [HAPO]) underwent oral glucose tolerance testing at 24-32 weeks' gestation. We built genetic risk scores (GRSs) for elevated fasting glucose and insulin, reduced insulin secretion and sensitivity, and T2D, using variants discovered in studies of nonpregnant individuals. We tested for associations between these GRSs, glycemic traits in pregnancy, and GDM. In both cohorts, the fasting glucose GRS was strongly associated with fasting glucose. The insulin secretion and sensitivity GRSs were also significantly associated with these traits in Gen3G, where insulin measurements were available. The fasting insulin GRS was weakly associated with fasting insulin (Gen3G) or C-peptide (HAPO). In HAPO (207 GDM case subjects), all five GRSs (T2D, fasting glucose, fasting insulin, insulin secretion, and insulin sensitivity) were significantly associated with GDM. In Gen3G (43 GDM case subjects), both the T2D and insulin secretion GRSs were associated with GDM; effect sizes for the other GRSs were similar to those in HAPO. Thus, despite the profound changes in glycemic physiology during pregnancy, genetic determinants of fasting glucose, fasting insulin, insulin secretion, and insulin sensitivity discovered outside of pregnancy influence GDM risk. [ABSTRACT FROM AUTHOR]

Published

2018

25. CD4 T Cells Reactive to Hybrid Insulin Peptides Are Indicators of Disease Activity in the NOD Mouse.

Author

Baker, Rocky L., Jamison, Braxton L., Wiles, Timothy A., Lindsay, Robin S., Barbour, Gene, Bradley, Brenda, Delong, Thomas, Friedman, Rachel S., Nakayama, Maki, and Haskins, Kathryn

Subjects

*CD4 antigen, *CD antigens, *VIRAL receptors, *T cells, *INSULIN, *PEPTIDES, *ANIMAL experimentation, *ANTIGENS, *AUTOIMMUNE diseases, *C-peptide, *CELL culture, *CELLS, *GENETICS, *GENETIC techniques, *IMMUNITY, *IMMUNOLOGY technique, *TYPE 1 diabetes, *MICE, *PROTEIN precursors, *RESEARCH funding, *DISEASE progression, *PANCREATIC hormones

Abstract

We recently established that hybrid insulin peptides (HIPs), formed in islet β-cells by fusion of insulin C-peptide fragments to peptides of chromogranin A or islet amyloid polypeptide, are ligands for diabetogenic CD4 T-cell clones. The goal of this study was to investigate whether HIP-reactive T cells were indicative of ongoing autoimmunity. MHC class II tetramers were used to investigate the presence, phenotype, and function of HIP-reactive and insulin-reactive T cells in NOD mice. Insulin-reactive T cells encounter their antigen early in disease, but they express FoxP3 and therefore may contribute to immune regulation. In contrast, HIP-reactive T cells are proinflammatory and highly diabetogenic in an adoptive transfer model. Because the frequency of antigen-experienced HIP-reactive T cells increases over progression of disease, they may serve as biomarkers of autoimmune diabetes. [ABSTRACT FROM AUTHOR]

Published

2018

26. Fetal Genotype and Maternal Glucose Have Independent and Additive Effects on Birth Weight.

Author

Hughes, Alice E., Nodzenski, Michael, Beaumont, Robin N., Talbot, Octavious, Shields, Beverley M., Scholtens, Denise M., Knight, Bridget A., Lowe Jr., William L., Hattersley, Andrew T., Freathy, Rachel M., and Lowe, William L Jr

Subjects

*FETAL development, *GENOTYPES, *BIRTH weight, *GLUCOSE, *MATERNAL health, *BLACK people, *BLOOD sugar, *C-peptide, *COMPARATIVE studies, *GESTATIONAL diabetes, *CORD blood, *HISPANIC Americans, *INSULIN, *RESEARCH methodology, *MEDICAL cooperation, *RESEARCH, *RESEARCH funding, *WHITE people, *EVALUATION research, *FETAL macrosomia, *SEQUENCE analysis

Abstract

Maternal glycemia is a key determinant of birth weight, but recent large-scale genome-wide association studies demonstrated an important contribution of fetal genetics. It is not known whether fetal genotype modifies the impact of maternal glycemia or whether it acts through insulin-mediated growth. We tested the effects of maternal fasting plasma glucose (FPG) and a fetal genetic score for birth weight on birth weight and fetal insulin in 2,051 European mother-child pairs from the Exeter Family Study of Childhood Health (EFSOCH) and the Hyperglycemia and Adverse Pregnancy Outcome (HAPO) study. The fetal genetic score influenced birth weight independently of maternal FPG and impacted growth at all levels of maternal glycemia. For mothers with FPG in the top tertile, the frequency of large for gestational age (birth weight ≥90th centile) was 31.1% for offspring with the highest tertile genetic score and only 14.0% for those with the lowest tertile genetic score. Unlike maternal glucose, the fetal genetic score was not associated with cord insulin or C-peptide. Similar results were seen for HAPO participants of non-European ancestry (n = 2,842 pairs). This work demonstrates that for any level of maternal FPG, fetal genetics has a major impact on fetal growth and acts predominantly through independent mechanisms. [ABSTRACT FROM AUTHOR]

Published

2018

27. Low-Dose ATG/GCSF in Established Type 1 Diabetes: A Five-Year Follow-up Report

Author

Stephen E. Gitelman, Desmond A. Schatz, Mark A. Atkinson, Jasmine A Mack, Laura M. Jacobsen, Brittany S. Bruggeman, Amanda L. Posgai, Peter A. Gottlieb, Michael J. Haller, Andrea Lin, Matthew J. Gurka, Todd M. Brusko, Clayton E. Mathews, and Clive Wasserfall

Subjects

0301 basic medicine, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, Clinical Trials and Supportive Activities, Pilot Projects, 030209 endocrinology & metabolism, Placebo, Medical and Health Sciences, Gastroenterology, Endocrinology & Metabolism, 03 medical and health sciences, 0302 clinical medicine, Clinical Research, Internal medicine, Granulocyte Colony-Stimulating Factor, Diabetes Mellitus, Internal Medicine, medicine, Clinical endpoint, Humans, Metabolic and endocrine, Antilymphocyte Serum, Type 1 diabetes, C-Peptide, business.industry, Diabetes, Low dose, Area under the curve, Five year follow up, medicine.disease, Diabetes Mellitus, Type 1, 030104 developmental biology, Area Under Curve, Immunology and Transplantation, business, Type 1

Abstract

Previously, we demonstrated low-dose anti-thymocyte globulin (ATG) and granulocyte colony stimulating factor (GCSF) immunotherapy preserved C-peptide for two years in a pilot study of subjects with established type 1 diabetes (n=25). Herein, we evaluated the long-term outcomes of ATG/GCSF in study participants with five years of available follow-up data (n=15). The primary endpoint was area under the curve (AUC) C-peptide during a two-hour mixed-meal tolerance test (MMTT). After five years, there were no statistically significant differences in AUC C-peptide when comparing subjects who received ATG/GCSF versus placebo (p = 0.41). A modeling framework based on mean trajectories in C-peptide AUC over five years, accounting for differing trends between groups, was applied to re-categorize responders (n=9) and non-responders (n=7). ATG/GCSF reponders demonstrated nearly unchanged HbA1c over five years [mean (95% CI) adjusted change = 0.29% (-0.69%, 1.27%)], but the study was not powered for comparisons against non-responders 1.75% (-0.57%, 4.06%) and placebo 1.44% (0.21%, 2.66%). These data underscore the importance of long-term follow up in previous and ongoing phase 2 trials of low-dose ATG in recent-onset type 1 diabetes.

Published

2021

28. Opioid Receptor Activation Impairs Hypoglycemic Counterregulation in Humans.

Author

Carey, Michelle, Gospin, Rebekah, Goyal, Akankasha, Tomuta, Nora, Sandu, Oana, Mbanya, Armand, Lontchi-Yimagou, Eric, Hulkower, Raphael, Shamoon, Harry, Gabriely, Ilan, and Hawkins, Meredith

Subjects

*OPIOID receptors, *GLYCEMIC control, *TYPE 1 diabetes, *HYPOGLYCEMIA, *BIOCHEMISTRY, *GLUCOSE metabolism, *ADRENALINE, *BLOOD sugar, *C-peptide, *CELL receptors, *COMPARATIVE studies, *CROSSOVER trials, *GLUCOSE, *HYDROCORTISONE, *INSULIN, *RESEARCH methodology, *MEDICAL cooperation, *MORPHINE, *NORADRENALINE, *RESEARCH, *EVALUATION research, *RANDOMIZED controlled trials, *GLUCOSE clamp technique, *PHARMACODYNAMICS

Abstract

Although intensive glycemic control improves outcomes in type 1 diabetes mellitus (T1DM), iatrogenic hypoglycemia limits its attainment. Recurrent and/or antecedent hypoglycemia causes blunting of protective counterregulatory responses, known as hypoglycemia-associated autonomic failure (HAAF). To determine whether and how opioid receptor activation induces HAAF in humans, 12 healthy subjects without diabetes (7 men, age 32.3 ± 2.2 years, BMI 25.1 ± 1.0 kg/m2) participated in two study protocols in random order over two consecutive days. On day 1, subjects received two 120-min infusions of either saline or morphine (0.1 μg/kg/min), separated by a 120-min break (all euglycemic). On day 2, subjects underwent stepped hypoglycemic clamps (nadir 60 mg/dL) with evaluation of counterregulatory hormonal responses, endogenous glucose production (EGP, using 6,6-D2-glucose), and hypoglycemic symptoms. Morphine induced an ∼30% reduction in plasma epinephrine response together with reduced EGP and hypoglycemia-associated symptoms on day 2. Therefore, we report the first studies in humans demonstrating that pharmacologic opioid receptor activation induces some of the clinical and biochemical features of HAAF, thus elucidating the individual roles of various receptors involved in HAAF's development and suggesting novel pharmacologic approaches for safer intensive glycemic control in T1DM. [ABSTRACT FROM AUTHOR]

Published

2017

29. Hepatic but Not Extrahepatic Insulin Clearance Is Lower in African American Than in European American Women.

Author

Piccinini, Francesca, Polidori, David C., Gower, Barbara A., and Bergman, Richard N.

Subjects

*INSULIN, *AFRICAN American women, *EUROPEAN Americans, *ETHNIC differences, *AFRICAN Americans, *C-peptide, *BLACK people, *BLOOD sugar, *GLUCOSE tolerance tests, *LIVER, *MATHEMATICAL models, *TYPE 2 diabetes, *RESEARCH funding, *WHITE people, *THEORY

Abstract

African Americans (AAs) tend to have higher plasma insulin concentrations than European Americans (EAs); the increased insulin concentrations have been attributed to increased secretion and/or decreased insulin clearance by liver or other tissues. This work characterizes the contributions of hepatic versus extrahepatic insulin degradation related to ethnic differences between AAs and EAs. By using a recently developed mathematical model that uses insulin and C-peptide measurements from the insulin-modified, frequently sampled intravenous glucose tolerance test (FSIGT), we estimated hepatic versus extrahepatic insulin clearance in 29 EA and 18 AA healthy women. During the first 20 min of the FSIGT, plasma insulin was approximately twice as high in AAs as in EAs. In contrast, insulin was similar in AAs and EAs after the 20-25 min intravenous insulin infusion. Hepatic insulin first-pass extraction was two-thirds lower in AAs versus EAs in the overnight-fasted state. In contrast, extrahepatic insulin clearance was not lower in AAs than in EAs. The difference in insulin degradation between AAs and EAs can be attributed totally to liver clearance. The mechanism underlying reduced insulin degradation in AAs remains to be clarified, as does the relative importance of reduced liver clearance to increased risk for type 2 diabetes. [ABSTRACT FROM AUTHOR]

Published

2017

30. The Effect of Ingested Glucose Dose on the Suppression of Endogenous Glucose Production in Humans.

Author

Kowalski, Greg M., Moore, Samantha M., Hamley, Steven, Selathurai, Ahrathy, and Bruce, Clinton R.

Subjects

*GLUCOSE analysis, *BLOOD sugar analysis, *GLUCOSE clamp technique, *BLOOD plasma, *PHYSIOLOGICAL effects of insulin, *GLUCOSE metabolism, *BLOOD sugar, *C-peptide, *DOSE-effect relationship in pharmacology, *FATTY acids, *GLUCAGON, *GLUCOSE, *HOMEOSTASIS, *INGESTION, *INSULIN

Abstract

Insulin clamp studies have shown that the suppressive actions of insulin on endogenous glucose production (EGP) are markedly more sensitive than for stimulating glucose disposal (Rd). However, clamp conditions do not adequately mimic postprandial physiological responses. Here, using the variable infusion dual-tracer approach, we used a threefold range of ingested glucose doses (25, 50, and 75 g) to investigate how physiological changes in plasma insulin influence EGP in healthy subjects. Remarkably, the glucose responses were similar for all doses tested, yet there was a dose-dependent increase in insulin secretion and plasma insulin levels. Nonetheless, EGP was suppressed with the same rapidity and magnitude (∼55%) across all doses. The progressive hyperinsulinemia, however, caused a dose-dependent increase in the estimated rates of Rd, which likely accounts for the lack of a dose effect on plasma glucose excursions. This suggests that after glucose ingestion, the body preferentially permits a transient and optimal degree of postprandial hyperglycemia to efficiently enhance insulin-induced changes in glucose fluxes, thereby minimizing the demand for insulin secretion. This may represent an evolutionarily conserved mechanism that not only reduces the secretory burden on β-cells but also avoids the potential negative consequences of excessive insulin release into the systemic arterial circulation. [ABSTRACT FROM AUTHOR]

Published

2017

31. A Genome-Wide Association Study of IVGTT-Based Measures of First-Phase Insulin Secretion Refines the Underlying Physiology of Type 2 Diabetes Variants.

Author

Wood, Andrew R., Jonsson, Anna, Jackson, Anne U., Nan Wang, van Leewen, Nienke, Palmer, Nicholette D., Sayuko Kobes, Deelen, Joris, Boquete-Vilarino, Lorena, Paananen, Jussi, Stanáčková, Alena, Boomsma, Dorret I., de Geus, Eco J. C., Eekhoff, Elisabeth M. W., Fritsche, Andreas, Kramer, Mark, Nijpels, Giel, Simonis-Bik, Annemarie, van Haeften, Timon W., and Mahajan, Anubha

Subjects

*TYPE 2 diabetes, *DISEASE susceptibility, *INSULIN, *GLUCOSE tolerance tests, *PEOPLE with diabetes, *ALLELES, *BLOOD sugar, *C-peptide, *COMPARATIVE studies, *GENETICS, *GENETIC techniques, *ISLANDS of Langerhans, *LIVER, *RESEARCH methodology, *MEDICAL cooperation, *PROTEINS, *REGRESSION analysis, *RESEARCH, *RESEARCH funding, *EVALUATION research, *SEQUENCE analysis, *GENOTYPES, *PHYSIOLOGY

Abstract

Understanding the physiological mechanisms by which common variants predispose to type 2 diabetes requires large studies with detailed measures of insulin secretion and sensitivity. Here we performed the largest genome-wide association study of first-phase insulin secretion, as measured by intravenous glucose tolerance tests, using up to 5,567 individuals without diabetes from 10 studies. We aimed to refine the mechanisms of 178 known associations between common variants and glycemic traits and identify new loci. Thirty type 2 diabetes or fasting glucose-raising alleles were associated with a measure of first-phase insulin secretion at P < 0.05 and provided new evidence, or the strongest evidence yet, that insulin secretion, intrinsic to the islet cells, is a key mechanism underlying the associations at the HNF1A, IGF2BP2, KCNQ1, HNF1B, VPS13C/C2CD4A, FAF1, PTPRD, AP3S2, KCNK16, MAEA, LPP, WFS1, and TMPRSS6 loci. The fasting glucose-raising allele near PDX1, a known key insulin transcription factor, was strongly associated with lower first-phase insulin secretion but has no evidence for an effect on type 2 diabetes risk. The diabetes risk allele at TCF7L2 was associated with a stronger effect on peak insulin response than on C-peptide-based insulin secretion rate, suggesting a possible additional role in hepatic insulin clearance or insulin processing. In summary, our study provides further insight into the mechanisms by which common genetic variation influences type 2 diabetes risk and glycemic traits. [ABSTRACT FROM AUTHOR]

Published

2017

32. [11C]5-hydroxy-tryptophan PET for Assessment of Islet Mass During Progression of Type 2 Diabetes.

Author

Carlbom, Lina, Espes, Daniel, Lubberink, Mark, Martinell, Mats, Johansson, Lars, Ahlström, Håkan, Carlsson, Per-Ola, Korsgren, Olle, and Eriksson, Olof

Subjects

*TRYPTOPHAN, *POSITRON emission tomography, *TYPE 2 diabetes, *DIABETES, *ISLANDS of Langerhans, *INSULIN therapy, *HYPOGLYCEMIC agents, *ANTHROPOMETRY, *ARGININE, *BLOOD sugar, *C-peptide, *CELL differentiation, *GLUCOSE, *MAGNETIC resonance imaging, *RADIOISOTOPES, *CROSS-sectional method, *CASE-control method, *DISEASE progression

Abstract

[11C]5-hydroxy-tryptophan ([11C]5-HTP) positron emission tomography of the pancreas has been shown to be a surrogate imaging biomarker of pancreatic islet mass. The change in islet mass in different stages of type 2 diabetes (T2D) as measured by noninvasive imaging is currently unknown. Here, we describe a cross-sectional study where subjects at different stages of T2D development with expected stratification of pancreatic islet mass were examined in relation to individuals without diabetes. The primary outcome was the [11C]5-HTP uptake and retention in pancreas, as a surrogate marker for the endogenous islet mass. We found that metabolic testing indicated a progressive loss of β-cell function, but this was not mirrored by a decrease in [11C]5-HTP tracer accumulation in the pancreas. This provides evidence of retained islet mass despite decreased β-cell function. The results herein indicate that β-cell dedifferentiation, and not necessarily endocrine cell loss, constitutes a major cause of β-cell failure in T2D. [ABSTRACT FROM AUTHOR]

Published

2017

33. Metabolite Profiling of LADA Challenges the View of a Metabolically Distinct Subtype.

Author

Al-Majdoub, Mahmoud, Ali, Arslan, Storm, Petter, Rosengren, Anders H., Groop, Leif, and Spégel, Peter

Subjects

*METABOLITES, *DIABETES, *AUTOANTIBODIES, *METABOLOMICS, *INSULIN therapy, *HYPOGLYCEMIC agents, *AGE factors in disease, *BLOOD sugar, *C-peptide, *ENZYMES, *FACTOR analysis, *GAS chromatography, *GLYCOSYLATED hemoglobin, *TYPE 1 diabetes, *MASS spectrometry, *METABOLISM, *TYPE 2 diabetes, *CASE-control method, *DISEASE progression

Abstract

Latent autoimmune diabetes in adults (LADA) usually refers to GAD65 autoantibodies (GADAb)-positive diabetes with onset after 35 years of age and no insulin treatment within the first 6 months after diagnosis. However, it is not always easy to distinguish LADA from type 1 or type 2 diabetes. In this study, we examined whether metabolite profiling could help to distinguish LADA (n = 50) from type 1 diabetes (n = 50) and type 2 diabetes (n = 50). Of 123 identified metabolites, 99 differed between the diabetes types. However, no unique metabolite profile could be identified for any of the types. Instead, the metabolome varied along a C-peptide-driven continuum from type 1 diabetes via LADA to type 2 diabetes. LADA was more similar to type 2 diabetes than to type 1 diabetes. In a principal component analysis, LADA patients overlapping with type 1 diabetes progressed faster to insulin therapy than those overlapping with type 2 diabetes. In conclusion, we could not find any unique metabolite profile distinguishing LADA from type 1 and type 2 diabetes. Rather, LADA was metabolically an intermediate of type 1 and type 2 diabetes, with those patients closer to the former showing a faster progression to insulin therapy than those closer to the latter. [ABSTRACT FROM AUTHOR]

Published

2017

34. Neu5Gc and α1-3 GAL Xenoantigen Knockout Does Not Affect Glycemia Homeostasis and Insulin Secretion in Pigs.

Author

Salama, Apolline, Mosser, Mathilde, Lévêque, Xavier, Perota, Andrea, Judor, Jean-Paul, Danna, Corentin, Pogu, Sylvie, Mouré, Anne, Jégou, Dominique, Gaide, Nicolas, Abadie, Jérôme, Gauthier, Olivier, Concordet, Jean-Paul, Bas-Bernardet, Stéphanie Le, Riochet, David, Berre, Ludmilla Le, Hervouet, Jérémy, Minault, David, Weiss, Pierre, and Guicheux, Jérôme

Subjects

*HOMEOSTASIS, *INSULIN, *LABORATORY swine, *IMMUNOGLOBULINS, *CYTIDINE phosphates, *BLOOD sugar, *C-peptide, *ISLANDS of Langerhans transplantation, *ANIMAL experimentation, *ANTIGENS, *DRUGS, *GENETIC techniques, *GLUCAGON, *GLUCOSE, *TYPE 1 diabetes, *ISLANDS of Langerhans, *NEUROTRANSMITTERS, *PANCREAS, *SWINE, *THEOPHYLLINE, *XENOGRAFTS, *HEXOSES, *PHARMACODYNAMICS

Abstract

Xenocell therapy from neonate or adult pig pancreatic islets is one of the most promising alternatives to allograft in type 1 diabetes for addressing organ shortage. In humans, however, natural and elicited antibodies specific for pig xenoantigens, α-(1,3)-galactose (GAL) and N-glycolylneuraminic acid (Neu5Gc), are likely to significantly contribute to xenoislet rejection. We obtained double-knockout (DKO) pigs lacking GAL and Neu5Gc. Because Neu5Gc-/- mice exhibit glycemic dysregulations and pancreatic β-cell dysfunctions, we evaluated islet function and glucose metabolism regulation in DKO pigs. Isolation of islets from neonate piglets yielded identical islet equivalent quantities to quantities obtained from control wild-type pigs. In contrast to wild-type islets, DKO islets did not induce anti-Neu5Gc antibody when grafted in cytidine monophosphate-N-acetylneuraminic acid hydroxylase KO mice and exhibited in vitro normal insulin secretion stimulated by glucose and theophylline. Adult DKO pancreata showed no histological abnormalities, and immunostaining of insulin and glucagon was similar to that from wild-type pancreata. Blood glucose, insulin, C-peptide, the insulin-to-glucagon ratio, and HOMA-insulin resistance in fasted adult DKO pigs and blood glucose and C-peptide changes after intravenous glucose or insulin administration were similar to wild-type pigs. This first evaluation of glucose homeostasis in DKO pigs for two major xenoantigens paves the way to their use in (pre)clinical studies. [ABSTRACT FROM AUTHOR]

Published

2017

35. Oxytocin Improves β-Cell Responsivity and Glucose Tolerance in Healthy Men.

Author

Klement, Johanna, Ott, Volker, Rapp, Kristina, Brede, Swantje, Piccinini, Francesca, Cobelli, Claudio, Lehnert, Hendrik, and Hallschmid, Manfred

Subjects

*PSYCHOSOCIAL factors, *OXYTOCIN, *NEUROPEPTIDES, *C-peptide, *INTRANASAL medication, *FREE fatty acids, *ADRENOCORTICOTROPIC hormone, *BLOOD sugar, *FATTY acids, *GLUCAGON, *GLUCOSE tolerance tests, *HYDROCORTISONE, *INSULIN, *ISLANDS of Langerhans, *HUMAN research subjects, *OXYTOCICS, *PHARMACODYNAMICS

Abstract

In addition to its pivotal role in psychosocial behavior, the hypothalamic neuropeptide oxytocin contributes to metabolic control by suppressing eating behavior. Its involvement in glucose homeostasis is less clear, although pilot experiments suggest that oxytocin improves glucose homeostasis. We assessed the effect of intranasal oxytocin (24 IU) administered to 29 healthy, fasted male subjects on glucose homeostasis measured by means of an oral glucose tolerance test. Parameters of glucose metabolism were analyzed according to the oral minimal model. Oxytocin attenuated the peak excursion of plasma glucose and augmented the early increases in insulin and C-peptide concentrations in response to the glucose challenge, while slightly blunting insulin and C-peptide peaks. Oral minimal model analyses revealed that oxytocin compared with placebo induced a pronounced increase in β-cell responsivity (PHItotal) that was largely due to an enhanced dynamic response (PHId), and a more than twofold improvement in glucose tolerance (disposition index). Adrenocorticotropic hormone (ACTH), cortisol, glucagon, and nonesterified fatty acid (NEFA) concentrations were not or were only marginally affected. These results indicate that oxytocin plays a significant role in the acute regulation of glucose metabolism in healthy humans and render the oxytocin system a potential target of antidiabetic treatment. [ABSTRACT FROM AUTHOR]

Published

2017

36. The Role of Glucagon in the Acute Therapeutic Effects of SGLT2 Inhibition

Author

Elisabeth Nielsen-Hannerup, Filip K. Knop, Tina Vilsbøll, Sofie Hædersdal, Henrik Maagensen, Gerrit van Hall, Asger Lund, and Jens J. Holst

Subjects

Blood Glucose, Glycerol, 0301 basic medicine, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, 030209 endocrinology & metabolism, Type 2 diabetes, Glucagon, Excretion, 03 medical and health sciences, 0302 clinical medicine, Glucosides, Internal medicine, Diabetes mellitus, Internal Medicine, medicine, Empagliflozin, Humans, Benzhydryl Compounds, Sodium-Glucose Transporter 2 Inhibitors, C-Peptide, business.industry, Biphenyl Compounds, Antagonist, medicine.disease, Metabolism, 030104 developmental biology, Postprandial, Endocrinology, Diabetes Mellitus, Type 2, Gastric Emptying, Drug Therapy, Combination, Energy Metabolism, business, Glucagon receptor, Half-Life

Abstract

Sodium–glucose cotransporter 2 inhibitors (SGLT2i) effectively lower plasma glucose (PG) concentration in patients with type 2 diabetes, but studies have suggested that circulating glucagon concentrations and endogenous glucose production (EGP) are increased by SGLT2i, possibly compromising their glucose-lowering ability. To tease out whether and how glucagon may influence the glucose-lowering effect of SGLT2 inhibition, we subjected 12 patients with type 2 diabetes to a randomized, placebo-controlled, double-blinded, crossover, double-dummy study comprising, on 4 separate days, a liquid mixed-meal test preceded by single-dose administration of either 1) placebo, 2) the SGLT2i empagliflozin (25 mg), 3) the glucagon receptor antagonist LY2409021 (300 mg), or 4) the combination empagliflozin + LY2409021. Empagliflozin and LY2409021 individually lowered fasting PG compared with placebo, and the combination further decreased fasting PG. Previous findings of increased glucagon concentrations and EGP during acute administration of SGLT2i were not replicated in this study. Empagliflozin reduced postprandial PG through increased urinary glucose excretion. LY2409021 reduced EGP significantly but gave rise to a paradoxical increase in postprandial PG excursion, which was annulled by empagliflozin during their combination (empagliflozin + LY2409021). In conclusion, our findings do not support that an SGLT2i-induced glucagonotropic effect is of importance for the glucose-lowering property of SGLT2 inhibition.

Published

2020

37. Subtypes of Type 2 Diabetes Determined From Clinical Parameters

Author

Rashmi B. Prasad, Emma Ahlqvist, Leif Groop, Centre of Excellence in Complex Disease Genetics, HUS Abdominal Center, Institute for Molecular Medicine Finland, and University of Helsinki

Subjects

Male, 0301 basic medicine, Endocrinology, Diabetes and Metabolism, VARIANT, 030209 endocrinology & metabolism, Type 2 diabetes, Disease, Bioinformatics, DISEASE, GLUCOSE, 03 medical and health sciences, 0302 clinical medicine, Insulin resistance, Diabetes mellitus, Internal Medicine, medicine, Humans, SUBGROUPS, Diabetic Nephropathies, INSULIN-RESISTANCE, C-Peptide, business.industry, Fatty liver, medicine.disease, GENE, 3. Good health, TCF7L2, Diabetes Mellitus, Type 1, 030104 developmental biology, Diabetes Mellitus, Type 2, 3121 General medicine, internal medicine and other clinical medicine, Female, Personalized medicine, Insulin Resistance, business, Retinopathy

Abstract

Type 2 diabetes (T2D) is defined by a single metabolite, glucose, but is increasingly recognized as a highly heterogeneous disease, including individuals with varying clinical characteristics, disease progression, drug response, and risk of complications. Identification of subtypes with differing risk profiles and disease etiologies at diagnosis could open up avenues for personalized medicine and allow clinical resources to be focused to the patients who would be most likely to develop diabetic complications, thereby both improving patient health and reducing costs for the health sector. More homogeneous populations also offer increased power in experimental, genetic, and clinical studies. Clinical parameters are easily available and reflect relevant disease pathways, including the effects of both genetic and environmental exposures. We used six clinical parameters (GAD autoantibodies, age at diabetes onset, HbA1c, BMI, and measures of insulin resistance and insulin secretion) to cluster adult-onset diabetes patients into five subtypes. These subtypes have been robustly reproduced in several populations and associated with different risks of complications, comorbidities, genetics, and response to treatment. Importantly, the group with severe insulin-deficient diabetes (SIDD) had increased risk of retinopathy and neuropathy, whereas the severe insulin-resistant diabetes (SIRD) group had the highest risk for diabetic kidney disease (DKD) and fatty liver, emphasizing the importance of insulin resistance for DKD and hepatosteatosis in T2D. In conclusion, we believe that subclassification using these highly relevant parameters could provide a framework for personalized medicine in diabetes.

Published

2020

38. Slowed Metabolic Decline After 1 Year of Oral Insulin Treatment Among Individuals at High Risk for Type 1 Diabetes in the Diabetes Prevention Trial–Type 1 (DPT-1) and TrialNet Oral Insulin Prevention Trials

Author

Jerry P. Palmer, Lisa E. Rafkin, Susan Geyer, Desmond A. Schatz, Alberto Pugliese, Della Matheson, Jay S. Skyler, Michael J. Haller, Jay M. Sosenko, Mario A Cleves, and Kevan C. Herold

Subjects

0301 basic medicine, Blood Glucose, Male, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, 030209 endocrinology & metabolism, Placebo, Antibodies, Monoclonal, Humanized, 03 medical and health sciences, 0302 clinical medicine, Diabetes mellitus, Internal medicine, Internal Medicine, Clinical endpoint, Medicine, Humans, Insulin, Type 1 diabetes, Framingham Risk Score, C-Peptide, business.industry, Trial Type, Area under the curve, Glucose Tolerance Test, medicine.disease, Pharmacology and Therapeutics, 030104 developmental biology, Diabetes Mellitus, Type 1, Area Under Curve, Female, business

Abstract

We assessed whether oral insulin slowed metabolic decline after 1 year of treatment in individuals at high risk for type 1 diabetes. Two oral insulin trials that did not show efficacy overall and had type 1 diabetes as the primary end point were analyzed: the Diabetes Prevention Trial–Type 1 (DPT-1) and the TrialNet oral insulin trials. Oral glucose tolerance tests at baseline and after 1 year of treatment were analyzed. Among those at high risk (with a Diabetes Prevention Trial–Type 1 Risk Score [DPTRS] ≥6.75), the area under the curve (AUC) C-peptide increased significantly from baseline to 1 year in each oral insulin group, whereas the AUC glucose increased significantly in each placebo group. At 1 year, the AUC C-peptide/AUC glucose (AUC Ratio) was significantly higher in the oral insulin group than in the placebo group in each trial (P < 0.05; P = 0.057 when adjusted for age in the TrialNet trial) and in both trials combined (P < 0.01 with or without adjustment for age). For a DPTRS

Published

2020

39. A Hybrid Insulin Epitope Maintains High 2D Affinity for Diabetogenic T Cells in the Periphery

Author

Derek M Woodruff, Elizabeth Motunrayo Kolawole, Baoyu Liu, Brian D. Evavold, Jennifer D. Hood, Dario A. A. Vignali, and Maria Bettini

Subjects

CD4-Positive T-Lymphocytes, 0301 basic medicine, T-Lymphocytes, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Antibody Affinity, Receptors, Antigen, T-Cell, Epitopes, T-Lymphocyte, Mice, Transgenic, 030209 endocrinology & metabolism, Spleen, Thymus Gland, Epitope, Islets of Langerhans, Mice, 03 medical and health sciences, 0302 clinical medicine, Antigen, Mice, Inbred NOD, Internal Medicine, medicine, Animals, NOD mice, Type 1 diabetes, Thymocytes, C-Peptide, biology, Chemistry, Insulin, Chromogranin A, medicine.disease, Molecular biology, Peptide Fragments, Diabetes Mellitus, Type 1, 030104 developmental biology, medicine.anatomical_structure, Polyclonal antibodies, biology.protein, Lymph Nodes, Immunology and Transplantation

Abstract

β-Cell antigen recognition by autoreactive T cells is essential in type 1 diabetes (T1D) pathogenesis. Recently, insulin hybrid peptides (HIPs) were identified as strong agonists for CD4 diabetogenic T cells. Here, using BDC2.5 transgenic and NOD mice, we investigated T-cell recognition of the HIP2.5 epitope, which is a fusion of insulin C-peptide and chromogranin A (ChgA) fragments, and compared it with the WE14 and ChgA29–42 epitopes. We measured in situ two-dimensional affinity on individual live T cells from thymus, spleen, pancreatic lymph nodes, and islets before and after diabetes. Although preselection BDC2.5 thymocytes possess higher affinity than splenic BDC2.5 T cells for all three epitopes, peripheral splenic T cells maintained high affinity only to the HIP2.5 epitope. In polyclonal NOD mice, a high frequency (∼40%) of HIP2.5-specific islet T cells were identified at both prediabetic and diabetic stages comprising two distinct high- and low-affinity populations that differed in affinity by 100-fold. This high frequency of high- and low-affinity HIP2.5 T cells in the islets potentially represents a major risk factor in diabetes pathogenesis.

Published

2020

40. The Impact of Different Implantation Sites and Sex on the Differentiation of Human Pancreatic Endoderm Cells Into Insulin-Secreting Cells In Vivo.

Author

Saber N, Ellis CE, Iworima DG, Baker RK, Rezania A, and Kieffer TJ

Subjects

Humans, Male, Female, Mice, Animals, C-Peptide, Endoderm transplantation, Cell Differentiation, Glucose, Insulin-Secreting Cells

Abstract

Few studies have examined the differentiation of human embryonic stem cell (hESC)-derived pancreatic endoderm cells (PECs) in different implantation sites. Here, we investigate the influence of implantation site and recipient sex on the differentiation of hESC-derived PECs in vivo. Male and female mice were implanted with 5 × 106 hESC-derived PECs under the kidney capsule, in the gonadal fat pad, or subcutaneously within macroencapsulation (TheraCyte) devices. PECs implanted within TheraCyte devices developed glucose-stimulated human C-peptide secretion faster than cells implanted under the kidney capsule or in the gonadal fat pad. Interestingly, hESC-derived PECs implanted under the kidney capsule in females developed glucose-stimulated human C-peptide faster than in males and secreted higher levels of arginine-stimulated glucagon and glucagon-like peptide 1 than other implantation sites. Furthermore, hESC-derived grafts collected from the kidney capsule and gonadal fat pad sites displayed a mix of endocrine and ductal cells as well as contained cysts, whereas TheraCyte device grafts displayed mostly endocrine cells and cysts were not observed. Here we demonstrate that the macroencapsulated subcutaneous site and the female recipient can promote faster differentiation of hESC-derived PECs to endocrine cells in mice., Article Highlights: Few studies have directly compared the differentiation of human embryonic stem cell-derived progenitors in different implantation sites in male and female recipients. We investigated whether the site of implantation and/or the sex of the recipient influenced the differentiation of pancreatic progenitors in vivo in mice. Mice implanted with cells in macroencapsulation devices contained fewer off-target structures and developed stimulated insulin release faster than other implant sites, while females implanted with cells under the kidney capsule developed stimulated insulin release before males. Macroencapsulation devices reduced the formation of off-target cells from human embryonic stem cell-derived progenitors, a useful characteristic for clinical applications., (© 2023 by the American Diabetes Association.)

Published

2023

41. Essential Role of Transglutaminase 2 in Vascular Endothelial Growth Factor-Induced Vascular Leakage in the Retina of Diabetic Mice.

Author

Yeon-Ju Lee, Se-Hui Jung, Su-Hyeon Kim, Min-Soo Kim, Sungeun Lee, JongYun Hwang, Soo-Youl Kim, Young-Myeong Kim, Kwon-Soo Ha, Lee, Yeon-Ju, Jung, Se-Hui, Kim, Su-Hyeon, Kim, Min-Soo, Lee, Sungeun, Hwang, JongYun, Kim, Soo-Youl, Kim, Young-Myeong, and Ha, Kwon-Soo

Subjects

*DIABETIC retinopathy, *VASCULAR endothelial growth factors, *TRANSGLUTAMINASES, *HYPERGLYCEMIA, *CYSTAMINE, *ANIMAL models in research, *CALCIUM metabolism, *MUSCLE protein metabolism, *REACTIVE oxygen species, *ANIMAL experimentation, *BIOLOGICAL models, *C-peptide, *CARRIER proteins, *CYTOSKELETAL proteins, *DIABETES, *GLYCOPROTEINS, *MICE, *MUSCLE proteins, *RETINA, *RNA, *TRANSFERASES, *WESTERN immunoblotting

Abstract

Diabetic retinopathy is predominantly caused by vascular endothelial growth factor (VEGF)-induced vascular leakage; however, the underlying mechanism is unclear. Here we designed an in vivo transglutaminase (TGase) activity assay in mouse retina and demonstrated that hyperglycemia induced vascular leakage by activating TGase2 in diabetic retina. VEGF elevated TGase2 activity through sequential elevation of intracellular Ca(2+) and reactive oxygen species (ROS) concentrations in endothelial cells. The TGase inhibitors cystamine and monodansylcadaverin or TGase2 small interfering RNA (siRNA) prevented VEGF-induced stress fiber formation and vascular endothelial (VE)-cadherin disruption, which play a critical role in modulating endothelial permeability. Intravitreal injection of two TGase inhibitors or TGase2 siRNA successfully inhibited hyperglycemia-induced TGase activation and microvascular leakage in the retinas of diabetic mice. C-peptide or ROS scavengers also inhibited TGase activation in diabetic mouse retinas. The role of TGase2 in VEGF-induced vascular leakage was further supported using diabetic TGase2(-/-) mice. Thus, our findings suggest that ROS-mediated activation of TGase2 plays a key role in VEGF-induced vascular leakage by stimulating stress fiber formation and VE-cadherin disruption. [ABSTRACT FROM AUTHOR]

Published

2016

42. Connections Between the Gut Microbiome and Metabolic Hormones in Early Pregnancy in Overweight and Obese Women.

Author

Gomez-Arango, Luisa F., Barrett, Helen L., McIntyre, H. David, Callaway, Leonie K., Morrison, Mark, Dekker Nitert, Marloes, and SPRING Trial Group

Subjects

*OBESITY in women, *GESTATIONAL diabetes, *INSULIN resistance, *METABOLISM, *RIBOSOMAL RNA, *GRAM-positive bacteria, *BLOOD sugar, *C-peptide, *ENERGY metabolism, *ENZYME-linked immunosorbent assay, *GESTATIONAL age, *INSULIN, *OBESITY, *PEPTIDE hormones, *RNA, *PHYSIOLOGY

Abstract

Overweight and obese women are at a higher risk for gestational diabetes mellitus. The gut microbiome could modulate metabolic health and may affect insulin resistance and lipid metabolism. The aim of this study was to reveal relationships between gut microbiome composition and circulating metabolic hormones in overweight and obese pregnant women at 16 weeks' gestation. Fecal microbiota profiles from overweight (n = 29) and obese (n = 41) pregnant women were assessed by 16S rRNA sequencing. Fasting metabolic hormone (insulin, C-peptide, glucagon, incretin, and adipokine) concentrations were measured using multiplex ELISA. Metabolic hormone levels as well as microbiome profiles differed between overweight and obese women. Furthermore, changes in some metabolic hormone levels were correlated with alterations in the relative abundance of specific microbes. Adipokine levels were strongly correlated with Ruminococcaceae and Lachnospiraceae, which are dominant families in energy metabolism. Insulin was positively correlated with the genus Collinsella. Gastrointestinal polypeptide was positively correlated with the genus Coprococcus but negatively with family Ruminococcaceae This study shows novel relationships between gut microbiome composition and the metabolic hormonal environment in overweight and obese pregnant women at 16 weeks' gestation. These results suggest that manipulation of the gut microbiome composition may influence pregnancy metabolism. [ABSTRACT FROM AUTHOR]

Published

2016

43. Renal Denervation for Resistant Hypertension Fails to Improve Insulin Resistance as Assessed by Hyperinsulinemic-Euglycemic Step Clamp.

Author

Miroslawska, Atena K., Gjessing, Petter F., Solbu, Marit D., Fuskevåg, Ole M., Jenssen, Trond G., and Steigen, Terje K.

Subjects

*INSULIN resistance, *GLUCOSE, *METABOLIC syndrome, *BLOOD pressure, *PERIPHERAL nervous system, *KIDNEY innervation, *GLUCOSE metabolism, *BLOOD sugar, *C-peptide, *DENERVATION, *FASTING, *GLUCOSE tolerance tests, *HYPERTENSION, *INSULIN, *GLUCOSE clamp technique

Abstract

We assessed whether insulin sensitivity improved after renal denervation (RDN) for resistant hypertension. Twenty-three patients underwent a two-step hyperinsulinemic-euglycemic clamp (HEC) with glucose tracer and labeled glucose infusion and oral glucose tolerance test (OGTT) before and 6 months after RDN. Eighteen patients had metabolic syndrome at baseline. Blood pressure declined significantly after RDN, whereas mean (SD) fasting plasma glucose concentration (5.9 ± 0.7 mmol/L), median (minimum-maximum) insulin concentration (254 pmol/L [88-797 pmol/L]), and median C-peptide concentration (2.4 nmol/L [0.9-5.7 nmol/L]) remained unchanged. Endogenous glucose release during HEC was less suppressed after RDN, suggesting a slight decrease in hepatic insulin sensitivity. During high-dose insulin infusion, whole-body glucose disposal was low and remained unchanged after RDN, indicating persistent peripheral insulin resistance (IR). Area under the curve for 0-120 min for glucose and insulin during OGTT, Quantitative Insulin Sensitivity Check Index, Simple Index Assessing Insulin Sensitivity Oral Glucose Tolerance, and HOMA-IR were high, and did not improve after RDN. Despite a significant decrease in blood pressure, neither peripheral nor hepatic insulin sensitivity improved 6 months after RDN treatment in this group of insulin-resistant patients without diabetes and with resistant hypertension, as measured with gold standard methods. [ABSTRACT FROM AUTHOR]

Published

2016

44. Hepatic and Extrahepatic Insulin Clearance Are Differentially Regulated: Results From a Novel Model-Based Analysis of Intravenous Glucose Tolerance Data.

Author

Polidori, David C., Bergman, Richard N., Chung, Stephanie T., and Sumner, Anne E.

Subjects

*INSULIN, *GLUCOSE, *TREATMENT of diabetes, *INSULIN resistance, *C-peptide, *BIOLOGICAL models, *BLACK people, *BLOOD sugar, *FASTING, *GLUCOSE tolerance tests, *INTRAVENOUS injections, *LIVER, *RESEARCH funding

Abstract

Insulin clearance is a highly variable and important factor that affects circulating insulin concentrations. We developed a novel model-based method to estimate both hepatic and extrahepatic insulin clearance using plasma insulin and C-peptide profiles obtained from the insulin-modified frequently sampled intravenous glucose tolerance test. Data from 100 African immigrants without diabetes (mean age 38 years, body weight 81.7 kg, fasting plasma glucose concentration 83 mg/dL, and fasting insulin concentration 37 pmol/L) were used. Endogenous insulin secretion (calculated by C-peptide deconvolution) and insulin infusion rates were used as inputs to a new two-compartment model of insulin kinetics and hepatic and extrahepatic clearance parameters were estimated. Good agreement between modeled and measured plasma insulin profiles was observed (mean normalized root mean square error 6.8%), and considerable intersubject variability in parameters of insulin clearance among individuals was identified (the mean [interquartile range] for hepatic extraction was 25.8% [32.7%], and for extrahepatic insulin clearance was 20.7 mL/kg/min [11.7 mL/kg/min]). Parameters of insulin clearance were correlated with measures of insulin sensitivity and acute insulin response to glucose. The method described appears promising for future research aimed at characterizing variability in insulin clearance and the mechanisms involved in the regulation of insulin clearance. [ABSTRACT FROM AUTHOR]

Published

2016

45. Monitoring C-Peptide Storage and Secretion in Islet β-Cells In Vitro and In Vivo.

Author

Shuaishuai Zhu, Larkin, Dennis, Shusheng Lu, Inouye, Candice, Haataja, Leena, Anjum, Arfah, Kennedy, Robert, Castle, David, Arvan, Peter, Zhu, Shuaishuai, and Lu, Shusheng

Subjects

*PROINSULIN, *PEPTIDES, *GREEN fluorescent protein, *TRANSGENIC animals, *INSULIN, *ANIMAL experimentation, *BLOOD sugar, *C-peptide, *DIABETES, *ELECTRON microscopy, *GLUCOSE, *ISLANDS of Langerhans, *MICE, *PROTEINS, *RESEARCH funding, *DISEASE progression, *IN vitro studies, *IMPACT of Event Scale

Abstract

Human proinsulin with C-peptide-bearing Superfolder Green Fluorescent Protein (CpepSfGFP) has been expressed in transgenic mice, driven by the Ins1 promoter. The protein, expressed exclusively in β-cells, is processed and stored as CpepSfGFP and human insulin comprising only ∼0.04% of total islet proinsulin plus insulin, exerting no metabolic impact. The kinetics of the release of insulin and CpepSfGFP from isolated islets appear identical. Upon a single acute stimulatory challenge in vitro, fractional release of insulin does not detectably deplete islet fluorescence. In vivo, fluorescence imaging of the pancreatic surface allows, for the first time, visual assessment of pancreatic islet insulin content, and we demonstrate that CpepSfGFP visibly declines upon diabetes progression in live lepR(db/db) mice. In anesthetized mice, after intragastric or intravenous saline delivery, pancreatic CpepSfGFP (insulin) content remains undiminished. Remarkably, however, within 20 min after acute intragastric or intravenous glucose delivery (with blood glucose concentrations reaching >15 mmol/L), a small subset of islets shows rapid dispossession of a major fraction of their stored CpepSfGFP (insulin) content, whereas most islets exhibit no demonstrable loss of CpepSfGFP (insulin). These studies strongly suggest that there are "first responder" islets to an in vivo glycemic challenge, which cannot be replicated by islets in vitro. [ABSTRACT FROM AUTHOR]

Published

2016

46. Low-Dose Anti-Thymocyte Globulin Preserves C-Peptide, Reduces HbA1c, and Increases Regulatory to Conventional T-Cell Ratios in New-Onset Type 1 Diabetes: Two-Year Clinical Trial Data

Author

Antoinette Moran, S. Alice Long, Susan Geyer, Megan V. Warnock, Linda A. DiMeglio, Henry Rodriguez, Jennifer B. Marks, Dorothy J. Becker, David A. Baidal, J Lori Blanchfield, Darrell M. Wilson, Peter A. Gottlieb, Stephen E. Gitelman, Desmond A. Schatz, Brian N. Bundy, Jessica L. Miller, Mark A. Atkinson, Michael J. Haller, Jay S. Skyler, Carla J. Greenbaum, Robin Goland, Jeffrey P. Krischer, Kevan C. Herold, and William E. Russell

Subjects

0301 basic medicine, Adult, Male, medicine.medical_specialty, Adolescent, Endocrinology, Diabetes and Metabolism, T cell, CD4-CD8 Ratio, 030209 endocrinology & metabolism, Placebo, T-Lymphocytes, Regulatory, 03 medical and health sciences, chemistry.chemical_compound, Young Adult, 0302 clinical medicine, Double-Blind Method, Internal medicine, Diabetes mellitus, Granulocyte Colony-Stimulating Factor, Internal Medicine, medicine, Humans, Immunologic Factors, Child, Antilymphocyte Serum, Glycated Hemoglobin, Type 1 diabetes, C-Peptide, C-peptide, business.industry, Area under the curve, medicine.disease, Flow Cytometry, Anti-thymocyte globulin, 030104 developmental biology, Endocrinology, medicine.anatomical_structure, Diabetes Mellitus, Type 1, chemistry, Female, Immunology and Transplantation, business, CD8

Abstract

A three-arm, randomized, double-masked, placebo-controlled phase 2b trial performed by the Type 1 Diabetes TrialNet Study Group previously demonstrated that low-dose anti-thymocyte globulin (ATG) (2.5 mg/kg) preserved β-cell function and reduced HbA1c for 1 year in new-onset type 1 diabetes. Subjects (N = 89) were randomized to 1) ATG and pegylated granulocyte colony-stimulating factor (GCSF), 2) ATG alone, or 3) placebo. Herein, we report 2-year area under the curve (AUC) C-peptide and HbA1c, prespecified secondary end points, and potential immunologic correlates. The 2-year mean mixed-meal tolerance test–stimulated AUC C-peptide, analyzed by ANCOVA adjusting for baseline C-peptide, age, and sex (n = 82) with significance defined as one-sided P < 0.025, was significantly higher in subjects treated with ATG versus placebo (P = 0.00005) but not ATG/GCSF versus placebo (P = 0.032). HbA1c was significantly reduced at 2 years in subjects treated with ATG (P = 0.011) and ATG/GCSF (P = 0.022) versus placebo. Flow cytometry analyses demonstrated reduced circulating CD4:CD8 ratio, increased regulatory T-cell:conventional CD4 T-cell ratios, and increased PD-1+CD4+ T cells following low-dose ATG and ATG/GCSF. Low-dose ATG partially preserved β-cell function and reduced HbA1c 2 years after therapy in new-onset type 1 diabetes. Future studies should determine whether low-dose ATG might prevent or delay the onset of type 1 diabetes.

Published

2019

47. 122-OR: Insulin and C-Peptide in Human Choroid Plexus of Type 1 Diabetes Mellitus

Author

Qing-Rong Liu, Josephine M. Egan, Stefano Marenco, Min Zhu, and Caio Henrique Mazucanti

Subjects

endocrine system, medicine.medical_specialty, Type 1 diabetes, endocrine system diseases, C-peptide, business.industry, Endocrinology, Diabetes and Metabolism, Insulin, medicine.medical_treatment, medicine.disease, chemistry.chemical_compound, Endocrinology, chemistry, Internal medicine, Internal Medicine, medicine, Choroid plexus, business

Abstract

The choroid plexus (CP) produces cerebrospinal fluid (CSF) and forms a blood-CSF barrier. We already reported that mouse CP epithelial (CPE) cells synthesize and secrete insulin in response to serotonin but not glucose. We now report that insulin expression is present in human postmortem CP samples of humans - nondiabetic, T2DM, and T1DM - by RT-qPCR, in situ hybridization and LC-MS/MS based Selected Reaction Monitoring assay. Human CPE contains all the INS splicing machinery and the major INS splicing variants that are present in islets. Known β-cell specific transcription factors are also expressed in CPE, except for PDX1 and PAX4, which are absent. The SRM assay detected INS A-chain, B-chain, and C-peptide at similar levels in nondiabetic, T2DM, and T1DM islets and CP postmortem samples. Islet amyloid polypeptide (IAPP) expression was not detected in CPE in contrast to human islets where INS and IAPP mRNA, as expected, colocalize in β-cells. Furthermore, INS colocalizes with transthyretin (TTR) mRNA in CPE cells but in islets, TTR is expressed in α-cells and not β-cells. We found less or no expression of T1DM autoantigens in CPE compared to β-cells, with the exception of ICA1 (islet cell autoantigen1), which has similar expression in both tissues. In conclusion, human CPE expresses and synthesizes insulin, it is protected from autoimmune destruction and from IAPP amyloidogenic fibril formation. Disclosure Q. Liu: None. M. Zhu: None. C. Mazucanti: None. S. Marenco: None. J. M. Egan: None. Funding National Institute on Aging

Published

2021

48. 94-OR: Reappearance of C-Peptide during the Third Trimester in Type 1 Diabetes Pregnancy: Pancreatic Regeneration or Fetal Hyperinsulinism?

Author

Denice S. Feig, Helen R. Murphy, Claire L Meek, Timothy J. McDonald, Richard A. Oram, and Andrew T. Hattersley

Subjects

medicine.medical_specialty, Pregnancy, Type 1 diabetes, Fetus, business.industry, C-peptide, Endocrinology, Diabetes and Metabolism, Regeneration (biology), medicine.disease, Third trimester, chemistry.chemical_compound, Endocrinology, chemistry, Internal medicine, Internal Medicine, Medicine, business, Hyperinsulinism

Published

2021

49. 153-OR: Measurement of C-Peptide at Diagnosis Informs Glycemic Control but Not Hypoglycemic Risk in Type 1 Diabetes

Author

Parth Narendran, Robert Andrews, Richard A. Oram, and Alice L. J. Carr

Subjects

Type 1 diabetes, medicine.medical_specialty, Continuous glucose monitoring, business.industry, C-peptide, Endocrinology, Diabetes and Metabolism, Newly diagnosed, Hypoglycemia, medicine.disease, Mixed meal, Gastroenterology, Insulin dose, chemistry.chemical_compound, chemistry, Internal medicine, Internal Medicine, medicine, business, Glycemic

Abstract

Background and Aims: High residual C-peptide in longer duration type 1 diabetes associates with fewer hypoglycemic events and reduced glycemic variability. However, little is known about the impact of C-peptide close to diagnosis. Using continuous glucose monitoring (CGM) data from a study of newly diagnosed adults with type 1 diabetes, we aimed to explore if variation in C-peptide close to diagnosis influenced glycemic variability and risk of hypoglycaemia. Materials and Methods: We studied newly diagnosed adults with type 1 diabetes who wore a Dexcom G4 CGM as part the EXTOD study. We examined the relationship between peak stimulated C-peptide in a mixed meal tolerance test and glycemic metrics of variability and hypoglycemia for 36 CGM traces from 23 participants. Results: Higher levels of C-peptide associated with lower glycemic variability, more time in range and less hyperglycemia. For every 100 pmol/L increase in peak C-peptide, percentage time spent in the range 3.9-10 mmol/L was increased by 2.39% [95% CI: 0.51,4.26], p=0.012) with a reduction in time spent in level 1 hyperglycaemia (> 10 mmol/L) and level 2 hyperglycemia (> 13.9 mmol/L) glucose levels by 2.64% [95% CI: -4.87, -0.41, p=0.018) and 1.33% [95% CI: -2.66, -0.0057], p= 0.041) respectively. Glucose levels were on average lower by 0.19 mmol/L ([95 % CI: -0.39,0.015], p=0.06) and standard deviation reduced by 0.14 [95% CI: -0.25, -0.023], p=0.017) for every 100 pmol/L increase in peak C-peptide. Hypoglycemia was not common in this group and no association was observed between time spent in hypoglycemia (p=0.967) or hypoglycemic risk (p=0.721). There was no association between peak C-peptide and insulin dose (p=0.707), HbA1C (p=0.364) or insulin dose adjusted HbA1c (IDAA1c, p=0.452). Conclusion: C-peptide associates with time spent in normal glucose range and with less hyperglycemia, but not risk of hypoglycemia in newly diagnosed people with type 1 diabetes. Disclosure A. Carr: None. R. A. Oram: Consultant; Self; Janssen Research & Development, LLC. P. Narendran: Speaker’s Bureau; Self; Novo Nordisk Inc., Sanofi. R. C. Andrews: None.

Published

2021

50. 1160-P: Does Yoga Reduce the Risk of Conversion from Prediabetes to Diabetes by Improving Acute Phase Insulin Release? An Observation from an RCT

Author

Venugopal Vijayakumar, Hongasandra R. Nagendra, Jintu Kurian, Ramesh N. Mavathur, and Raghuram Nagarathna

Subjects

medicine.medical_specialty, C-peptide, business.industry, Endocrinology, Diabetes and Metabolism, Insulin, medicine.medical_treatment, Serum insulin, medicine.disease, law.invention, chemistry.chemical_compound, chemistry, Randomized controlled trial, law, Internal medicine, Diabetes mellitus, Internal Medicine, medicine, Heart rate variability, Prediabetes, business, Balance (ability)

Abstract

Background: Acute phase insulin secretion is disturbed in individuals with prediabetes. We have previously shown a significant risk reduction in 4,417 prediabetes individuals through Yoga. The present study explores yoga’s mechanism of action. Method: This randomized control trial included 42 (20 yoga;22 walkings;5 days/ week, 3Months) prediabetes (fasting glucose of 100 to 125 mg/dl) adults between 23 to 50 years. Serum Insulin and C peptide were assessed at 0, 3, 5, 7, 10, 15, 30,60and 90th minutes after 75grams of oral glucose. Pre-post assessments included fasting Glucose, HOMA%B(derived), GLP-1, free Triiodothyronine, perceived stress, and Heart rate variability. Results: There was a significant increase in the 10th minute (acute phase) Insulin and c-peptide levels in the yoga as compared to the control group. Improvement in GLP-1 and HOMA%B was significantly better in yoga than walking group. Yoga group also showed positive change in perceived stress and HRV. Simple linear regression of post data using acute phase Insulin as the dependent variable indicated a significant association between all measures(R2 = 0.806; p = Conclusion: The shift to normoglycemia, due to an increase in acute phase insulin release, was associated with improved autonomic balance and reduced stress after yoga. More studies may confirm this unique first time observation. Disclosure R. Nagarathna: None. J. Kurian: None. V. Vijayakumar: None. H. R. Nagendra: None. R. N. Mavathur: None. Funding Ministry of AYUSH, Government of India (Z.28015-HPC (EMR)-AYUSH-B)

Published

2021