Your search keyword '"Pancreas drug effects"' showing total 433 results

1. Renalase peptides reduce pancreatitis severity in mice.

Author

Kolodecik TR, Guo X, Shugrue CA, Guo X, Desir GV, Wen L, and Gorelick F

Subjects

Animals, Male, Mice, Female, Disease Models, Animal, Severity of Illness Index, Peptides pharmacology, Pancreas pathology, Pancreas drug effects, Pancreas metabolism, Anti-Inflammatory Agents pharmacology, Chymases metabolism, Monoamine Oxidase, Pancreatitis prevention & control, Pancreatitis pathology, Ceruletide, Mice, Inbred C57BL

Abstract

Acute pancreatitis, an acute inflammatory injury of the pancreas, lacks a specific treatment. The circulatory protein renalase is produced by the kidney and other tissues and has potent anti-inflammatory and prosurvival properties. Recombinant renalase can reduce the severity of mild cerulein pancreatitis; the activity is contained in a conserved 20 aa renalase site (RP220). Here, we investigated the therapeutic effects of renalase on pancreatitis using two clinically relevant models of acute pancreatitis. The ability of peptides containing the RP220 site to reduce injury in a 1-day post-endoscopic retrograde cholangiopancreatography (ERCP) and a 2-day severe cerulein induced in mice was examined. The initial dose of renalase peptides was given either prophylactically (before) or therapeutically (after) the initiation of the disease. Samples were collected to determine early pancreatitis responses (tissue edema, plasma amylase, active zymogens) and later histologic tissue injury and inflammatory changes. In both preclinical models, renalase peptides significantly reduced histologic damage associated with pancreatitis, especially inflammation, necrosis, and overall injury. Quantifying inflammation using specific immunohistochemical markers demonstrated that renalase peptides significantly reduced overall bone marrow-derived inflammation and neutrophils and macrophage populations in both models. In the severe cerulein model, administering a renalase peptide with or without pretreatment significantly reduced injury. Pancreatitis and renalase peptide effects appeared to be the same in female and male mice. These studies suggest renalase peptides that retain the anti-inflammatory and prosurvival properties of recombinant renalase can reduce the severity of acute pancreatitis and might be attractive candidates for therapeutic development. NEW & NOTEWORTHY Renalase is a secretory protein. The prosurvival and anti-inflammatory effects of the whole molecule are contained in a 20 aa renalase site (RP220). Systemic treatment with peptides containing this renalase site reduced the severity of post-endoscopic retrograde cholangiopancreatography (ERCP) and severe cerulein pancreatitis in mouse models.

Published

2024

2. Buprenorphine affects the initiation and severity of interleukin-induced acute pancreatitis in mice.

Author

Jahangir S, Khatua B, Smichi N, Rajalingamgari P, Narayana Pillai A, Summers MJ, McFayden B, Kostenko S, Gades NM, and Singh VP

Subjects

Animals, Mice, Analgesics, Opioid pharmacology, Disease Models, Animal, Male, Interleukin-12 metabolism, Interleukin-18 metabolism, Interleukin-18 blood, Mice, Obese, Acute Disease, Pancreas pathology, Pancreas drug effects, Mice, Inbred C57BL, Buprenorphine pharmacology, Pancreatitis chemically induced, Pancreatitis pathology

Abstract

Acute pancreatitis (AP) is a common disease with no targeted therapy and has varied outcomes ranging from spontaneous resolution to being lethal. Although typically painful, AP can also be painless. Various agents, including opioids, are used for pain control in AP; the risks and benefits of which are often debated. As experimental AP in mice is used to study the efficacy of potential therapies, we studied the effect of a commonly used opioid, buprenorphine, on the initiation and progression of AP. For this, we administered extended-release buprenorphine subcutaneously before inducing the previously established severe AP model that uses interleukins 12 and 18 (IL12,18) in genetically obese (ob/ob) mice and compared this to mice with AP but without the drug. Mice were monitored over 3 days, and parameters of AP induction and progression were compared. Buprenorphine significantly reduced serum amylase, lipase, pancreatic necrosis, and AP-associated fat necrosis, which is ubiquitous in obese mice and humans. Buprenorphine delayed the AP-associated reduction of carotid artery pulse distention and the development of hypothermia, hastened renal injury, and muted the early increase in respiratory rate versus IL12,18 alone. The site of buprenorphine injection appeared erythematous, inflamed, and microscopically showed thinning, loss of epidermal layers that had increased apoptosis. In summary, subcutaneous extended-release buprenorphine interfered with the induction of AP by reducing serum amylase, lipase, pancreatic and fat necrosis, the worsening of AP by delaying hypotension, hypothermia, while hastening renal injury, respiratory depression, and causing cutaneous injury at the site of injection. NEW & NOTEWORTHY Extended-release buprenorphine interferes with the initiation and progression of acute pancreatitis at multiple levels.

Published

2024

3. Single-cell analyses of human pancreas: characteristics of two populations of acinar cells in chronic pancreatitis.

Author

Blobner BM, Saloman JL, Shelton Ohlsen CA, Brand R, Lafyatis R, Bottino R, Wijkstrom M, Zureikat AH, Lee KK, Singhi AD, Ross MA, Stolz D, and Whitcomb DC

Subjects

Acinar Cells drug effects, Acinar Cells pathology, Cell Dedifferentiation, Cluster Analysis, Feasibility Studies, Humans, Muscarinic Agonists pharmacology, Pancreas drug effects, Pancreas pathology, Pancreas surgery, Pancreatectomy, Pancreaticoduodenectomy, Pancreatitis, Chronic metabolism, Pancreatitis, Chronic pathology, Pancreatitis, Chronic surgery, Protease Inhibitors pharmacology, Acinar Cells metabolism, Gene Expression Profiling, Pancreas metabolism, Pancreatitis, Chronic genetics, RNA-Seq, Single-Cell Analysis, Transcriptome

Abstract

Chronic pancreatitis (CP) is a complex inflammatory disorder with numerous associated genetic and environmental risk factors. The most distressing characteristic of CP is recalcitrant pain, often requiring surgical resection including total pancreatectomy with islet autotransplantation (TPIAT). We studied five consented subjects undergoing pancreatic resection and processed isolated cells for single-cell RNA sequencing (scRNA-Seq). Using high-dimensional transcriptomic cluster analysis, we identified 11 unique cell clusters in the pancreas tissue. These cell clusters include a cluster of undifferentiated/dedifferentiated cells and two unique clusters of acinar cells, one of which appears to be in a transitional stage. To determine the cellular response to protease inhibitor and stimulation, we treated aliquots of cells from one subject with a protease inhibitor cocktail with and without bethanechol (a muscarinic receptor agonist) at 100 and 400 µM and compared gene expression profiles. The protease inhibitors appeared to reduce cell stress. Pancreatic digestive enzymes and islet hormones were upregulated in both doses of bethanechol-treated cells compared with naïve cells. High-dose bethanechol appeared to be toxic and consistent with hyperstimulation. These studies demonstrate the feasibility of investigating human acinar cell physiology at the single-cell level and initial evidence that these cells retain responsiveness to agonist stimulation with predicted second messenger and transcriptomic responses. NEW & NOTEWORTHY We conducted single cell RNA sequencing on pancreas tissue from five individuals. We identified eleven unique cell clusters including a large population of dedifferentiated cells as well as two unique clusters of acinar cells, one of which appears to exist in a transitional state. We also examined the cellular response of pancreas tissue to stimulation and identified affected genes and pathways, including pancreatic digestive enzymes.

Published

2021

4. Ketamine and xylazine effects in murine model of acute pancreatitis.

Author

Wang M and Gorelick FS

Subjects

Analgesics pharmacology, Animals, Atropine pharmacology, Autophagy drug effects, Cell Proliferation drug effects, Disease Models, Animal, Drug Therapy, Combination, Female, Ketamine pharmacology, Male, Mice, Treatment Outcome, Xylazine pharmacology, Analgesics therapeutic use, Ketamine therapeutic use, Pancreas drug effects, Pancreatitis drug therapy, Xylazine therapeutic use

Abstract

Ketamine and xylazine (Ket/Xyl) are anesthetic agents that target neural pathways and are commonly used in combination in mouse studies. Since neural pathways can modulate acute pancreatitis severity, we asked if Ket/Xyl affect disease severity. C57BL/6 mice were treated with six hourly injections of cerulein to induce mild acute pancreatitis. Mice were also treated with and without ketamine, xylazine, and Ket/Xyl before pancreatitis induction in vivo and in vitro. Ket/Xyl pretreatment in vivo increased selected parameters of pancreatitis severity such as trypsin activity and edema; these effects were predominantly mediated by xylazine. Ket/Xyl also changed markers of autophagy. These in vivo effects of Ket/Xyl were not attenuated by atropine. The drugs had no little to no effect on pancreatitis responses in isolated pancreatic cells or lobules. These findings suggest that Ket/Xyl administration can have substantial effect on acute pancreatitis outcomes through nonmuscarinic neural pathways. Given widespread use of this anesthetic combination in experimental animal models, future studies of inflammation and injury using Ket/Xyl should be interpreted with caution. NEW & NOTEWORTHY Ketamine and xylazine anesthetic agent administration before acute pancreatitis induction in mice lead to changes in pancreatitis responses independent of acute pancreatitis induction. Future studies should consider the potential effects of anesthesia administration when studying disease processes associated with inflammation and injury.

Published

2021

5. Proinflammatory cytokines inhibit thiamin uptake by human and mouse pancreatic acinar cells: involvement of transcriptional mechanism(s).

Author

Anandam KY, Srinivasan P, Yasujima T, Al-Juburi S, and Said HM

Subjects

Acinar Cells metabolism, Animals, Cytokines metabolism, Epithelial Cells metabolism, Humans, Membrane Transport Proteins drug effects, Membrane Transport Proteins genetics, Mice, Pancreas drug effects, Pancreas metabolism, Pancreas, Exocrine drug effects, Pancreas, Exocrine metabolism, Promoter Regions, Genetic drug effects, RNA, Messenger metabolism, Acinar Cells drug effects, Biological Transport drug effects, Cytokines pharmacology, Epithelial Cells drug effects

Abstract

Thiamin (vitamin B1) plays critical roles in normal metabolism and function of all mammalian cells. Pancreatic acinar cells (PACs) import thiamin from circulation via specific carrier-mediated uptake that involves thiamin transporter-1 and -2 (THTR-1 and -2; products of SLC19A2 and SLC19A3 , respectively). Our aim in this study was to investigate the effect(s) of proinflammatory cytokines on thiamin uptake by PACs. We used human primary (h)PACs, PAC 266-6 cells, and mice in vivo as models in the investigations. First, we examined the level of expression of THTR-1 and -2 mRNA in pancreatic tissues of patients with chronic pancreatitis and observed severe reduction in their expression compared with normal control subjects. Exposing hPACs and PAC 266-6 to proinflammatory cytokines (hyper IL-6, TNF-α, and IL-1β) was found to lead to a significant inhibition in thiamin uptake. Focusing on hyper-IL-6 (which also inhibited thiamin uptake by primary mouse PACs), the inhibition in thiamin uptake was found to be associated with significant reduction in THTR-1 and -2 proteins and mRNA expression as well as in activity of the SLC19A2 and SLC19A3 promoters; it was also associated with reduction in level of expression of the transcription factor Sp1 (which is required for activity of these promoters). Finally, blocking the intracellular Stat3 signaling pathway was found to lead to a significant reversal in the inhibitory effect of hyper IL-6 on thiamin uptake by PAC 266-6. These results show that exposure of PACs to proinflammatory cytokines negatively impacts thiamin uptake via (at least in part) transcriptional mechanism(s). NEW & NOTEWORTHY Findings of the current study demonstrate, for the first time, that exposure of pancreatic acinar cells to proinflammatory cytokines (including hyper IL-6) cause significant inhibition in vitamin B1 (thiamin; a micronutrient that is essential for normal cellular energy metabolism) and that this effect is mediated at the level of transcription of the thiamin transporter genes SLC19A2 and SLC19A3 .

Published

2021

6. Ethanol feeding accelerates pancreatitis progression in CPA1 N256K mutant mice.

Author

Orekhova A, Geisz A, and Sahin-Tóth M

Subjects

Animals, Body Weight, Carboxypeptidases A genetics, Eating, Endoplasmic Reticulum Chaperone BiP, Endoplasmic Reticulum Stress drug effects, Ethanol administration & dosage, Genetic Predisposition to Disease, Mice, Mice, Inbred C57BL, Mice, Transgenic, Pancreatitis, Alcoholic pathology, Carboxypeptidases A metabolism, Ethanol toxicity, Pancreas drug effects, Pancreatitis, Alcoholic genetics

Abstract

Alcoholic pancreatitis is a multifactorial, progressive, inflammatory disorder of the pancreas. Alcohol initiates pancreatitis and promotes its progression in the context of genetic susceptibility and/or other environmental risk factors such as smoking. Genetic mutations can cause digestive enzyme misfolding, which induces endoplasmic reticulum (ER) stress and elicits pancreatitis. Here, we tested the hypothesis that alcohol synergizes with misfolding in promoting ER stress and thereby accelerates chronic pancreatitis progression. To this end, we fed an ethanol-containing diet to CPA1 N256K mice, which carry the human p.N256K CPA1 mutation and develop spontaneous chronic pancreatitis. Inexplicably, CPA1 N256K mice suffered generalized seizures after 2-3 wk of ethanol feeding, which resulted in high mortality and the early termination of the study. Analysis of CPA1 N256K mice euthanized after 3-3.5 wk of ethanol feeding revealed more severe chronic pancreatitis associated with significantly increased Hspa5 [ER chaperone immunoglobulin heavy chain-binding protein (BiP)] mRNA levels when compared with CPA1 N256K mice on a control liquid diet. In contrast, ethanol feeding of C57BL/6N mice for 4 wk increased Hspa5 levels to a lesser degree and caused no pancreatitis. We conclude that ethanol feeding synergizes with the misfolding CPA1 mutant in promoting ER stress and thereby accelerates progression of chronic pancreatitis in CPA1 N256K mice. NEW & NOTEWORTHY Alcoholic pancreatitis is a multifactorial, progressive, inflammatory disorder of the pancreas. This study demonstrates that alcohol synergizes with digestive enzyme misfolding in promoting endoplasmic reticulum stress and thereby accelerates progression of chronic pancreatitis.

Published

2020

7. Protective effects of maresin 1 against inflammation in experimentally induced acute pancreatitis and related lung injury.

Author

Munir F, Jamshed MB, Shahid N, Muhammad SA, Bhandari A, and Zhang Q

Subjects

Acute Disease, Animals, Inflammation pathology, Lipopolysaccharides pharmacology, Lung Injury pathology, Male, Mice, Inbred C57BL, Pancreas drug effects, Pancreas pathology, Anti-Inflammatory Agents pharmacology, Docosahexaenoic Acids pharmacology, Inflammation drug therapy, Lung Injury drug therapy

Abstract

Severe acute pancreatitis (SAP) is an inflammatory disorder that progresses with local and systemic difficulties accompanied by a relatively high mortality rate. In recent years, maresin 1 (MaR1) has been shown to be a macrophage mediator with effective proresolving and anti-inflammatory properties that prevents the occurrence of various inflammatory conditions. The purpose of this study was to investigate the role of MaR1 in SAP and related lung injury. Experimental SAP was induced in mice with a combination of cerulean and lipopolysaccharide. MaR1 was administered 30 min before the primary injection of cerulean. Biochemical markers and histological injury scores were used to evaluate the severity of acute pancreatitis. To determine the degree of inflammation, serum cytokines and myeloperoxidase activity in pancreas and lung tissues were measured. Western blot analysis detected the activation of NF-κB. After MaR1 pretreatment, the activities of amylase, lipase, TNF-α, IL-1β, and IL-6 were decreased in serum, and the myeloperoxidase activity both in pancreas and in lung tissues significantly decreased, whereas the activity of anti-inflammatory cytokine IL-10 in serum was increased. MaR1-pretreated mice reduced the activation of pancreatic NF-κB and decreased the severity of pancreatic and lung-related injuries. These results confirm that MaR1 alleviated inflammation of the pancreas and lung by inhibiting the activity of NF-κB in experimentally induced acute pancreatitis and exerted anti-inflammatory effects. These findings suggest that MaR1 could be a new and useful drug in the treatment of SAP. NEW & NOTEWORTHY These results provided us evidence to confirm that maresin 1 (MaR1) can alleviate inflammation of the pancreas and lung by inhibiting the activity of NF-κB in experimental induced acute pancreatitis and exerts certain anti-inflammatory effects. These findings suggest that MaR1 could be a new and useful drug in the treatment of severe acute pancreatitis.

Published

2019

8. Ghrelin in rat pancreatic islets decreases islet blood flow.

Author

Drott CJ, Franzén P, and Carlsson PO

Subjects

Animals, Blood Glucose drug effects, Blood Glucose metabolism, Blood Pressure drug effects, Cells, Cultured, Ghrelin blood, Ghrelin pharmacology, Insulin Secretion drug effects, Male, Oligopeptides pharmacology, Pancreas blood supply, Pancreas drug effects, Pancreas metabolism, Rats, Rats, Sprague-Dawley, Regional Blood Flow drug effects, Splanchnic Circulation drug effects, Splanchnic Circulation physiology, Ghrelin metabolism, Islets of Langerhans blood supply, Islets of Langerhans metabolism

Abstract

The peptide ghrelin is mainly produced in some of the epithelial cells in the stomach, but also, during starvation, by the ε-cells in the endocrine pancreas. Ghrelin, as an endogenous ligand for the growth hormone secretagogue receptor (GHS-R1α), exerts a variety of metabolic functions including stimulation of appetite and weight gain. Its complete role is not yet fully understood, including whether it has any vascular functions. The present study evaluated if ghrelin affects pancreatic and islet blood flow. Ghrelin and the GHS-R1α receptor antagonist GHRP-6 were injected intravenously in rats followed by blood flow measurements using a microsphere technique. Ghrelin decreased, while GHRP-6 in fasted, but not fed, rats selectively increased islet blood flow fourfold. GHS-R1α was identified not only on glucagon-producing cells but also seemed to be present in the islet arterioles. GHRP-6 in fasted rats, only, also improved the peak insulin response to glucose in vivo, thereby substantially blunting the hyperglycemia. GHRP-6 doubled glucose-stimulated insulin release in vitro of both islets obtained from fed and fasted rats. Our results indicate a novel role for endogenous ghrelin acting directly or indirectly as a local vasoconstrictor in the islets during fasting, thereby restricting the insulin response to hyperglycemia. This is to the best of our knowledge the first report that shows this physiological mechanism to restrict insulin delivery from the islets by acting on the vasculature; a mode of action that can be envisaged to complement the previously well-described mechanisms of ghrelin acting directly on the islet endocrine cells.

Published

2019

9. Cyclic AMP-dependent protein kinase A and EPAC mediate VIP and secretin stimulation of PAK4 and activation of Na + ,K + -ATPase in pancreatic acinar cells.

Author

Ramos-Alvarez I, Lee L, and Jensen RT

Subjects

Acinar Cells metabolism, Animals, Cyclic AMP Response Element-Binding Protein drug effects, Cyclic AMP Response Element-Binding Protein metabolism, Cyclic AMP-Dependent Protein Kinases metabolism, Guanine Nucleotide Exchange Factors metabolism, Male, Pancreas drug effects, Pancreas metabolism, Pyrazoles pharmacology, Pyrroles pharmacology, Quinazolines pharmacology, Rats, Sprague-Dawley, Secretin drug effects, Acinar Cells drug effects, Antineoplastic Agents pharmacology, Cyclic AMP metabolism, Guanine Nucleotide Exchange Factors drug effects

Abstract

Rat pancreatic acinar cells possess only the p21-activated kinase (PAKs), PAK4 of the group II PAK, and it is activated by gastrointestinal hormones/neurotransmitters stimulating PLC and by a number of growth factors. However, little is known generally of cAMP agents causing PAK4 activation, and there are no studies with gastrointestinal hormones/neurotransmitters activating cAMP cascades. In the present study, we examined the ability of VIP and secretin, which stimulate cAMP generation in pancreatic acini, to stimulate PAK4 activation, the signaling cascades involved, and their possible role in activating sodium-potassium adenosine triphosphatase (Na + ,K + -ATPase). PAK4 activation was compared with activation of the well-established cAMP target, cyclic AMP response element binding protein (CREB). Secretin-stimulated PAK4 activation was inhibited by KT-5720 and PKA Type II inhibitor (PKI), protein kinase A (PKA) inhibitors, whereas VIP activation was inhibited by ESI-09 and HJC0197, exchange protein directly activated by cAMP (EPAC) inhibitors. In contrast, both VIP/secretin-stimulated phosphorylation of CREB (pCREB) via EPAC activation; however, it was inhibited by the p44/42 inhibitor PD98059 and the p38 inhibitor SB202190. The specific EPAC agonist 8-CPT-2- O-Me-cAMP as well 8-Br-cAMP and forskolin stimulated PAK4 activation. Secretin/VIP activation of Na + ,K + -ATPase, was inhibited by PAK4 inhibitors (PF-3758309, LCH-7749944). These results demonstrate PAK4 is activated in pancreatic acini by stimulation of both VIP-/secretin-preferring receptors, as is CREB. However, they differ in their signaling cascades. Furthermore, PAK4 activation is needed for Na + ,K + ATPase activation, which mediates pancreatic fluid secretion. These results, coupled with recent studies reporting PAKs are involved in both pancreatitis/pancreatic cancer growth/enzyme secretion, show that PAK4, similar to PAK2, likely plays an important role in both pancreatic physiological/pathological responses. NEW & NOTEWORTHY Pancreatic acini possess only the group II p21-activated kinase, PAK4, which is activated by PLC-stimulating agents/growth factors and is important in enzyme-secretion/growth/pancreatitis. Little information exists on cAMP-activating agents stimulating group II PAKs. We studied ability/effect of cyclic AMP-stimulating agents [vasoactive intestinal polypeptide (VIP), secretin] on PAK4 activity in rat pancreatic-acini. Both VIP/secretin activated PAK4/CREB, but the cAMP signaling cascades differed for EPAC, MAPK, and PKA pathways. Both hormones require PAK4 activation to stimulate sodium-potassium adenosine triphosphatase activity. This study shows PAK4 plays an important role in VIP-/secretin-stimulated pancreatic fluid secretion and suggests it plays important roles in pancreatic acinar physiological/pathophysiological responses mediated by cAMP-activating agents.

Published

2019

10. Maternal methyl donor and cofactor supplementation in late pregnancy increases β-cell numbers at 16 days of life in growth-restricted twin lambs.

Author

Sulaiman SA, De Blasio MJ, Harland ML, Gatford KL, and Owens JA

Subjects

Animals, Animals, Newborn, Blood Glucose drug effects, Blood Glucose metabolism, Body Composition drug effects, Case-Control Studies, Cell Count, Diabetes Mellitus, Type 2 metabolism, Dietary Supplements, Female, Humans, Pancreas drug effects, Pregnancy, Prenatal Exposure Delayed Effects metabolism, Sheep, Cobalt pharmacology, Fetal Growth Retardation, Folic Acid pharmacology, Insulin metabolism, Insulin Resistance, Insulin-Secreting Cells drug effects, Methionine pharmacology, Pregnancy, Twin, Sulfur pharmacology

Abstract

Restricted growth before birth (IUGR) increases adult risk of Type 2 diabetes by impairing insulin sensitivity and secretion. Altered fetal one-carbon metabolism is implicated in developmental programming of adult health and disease by IUGR. Therefore, we evaluated effects of maternal dietary supplementation with methyl donors and cofactors (MMDS), designed to increase fetal supply, on insulin action in the spontaneously IUGR twin lamb. In vivo glucose-stimulated insulin secretion and insulin sensitivity were measured at days 12-14 in singleton controls (CON, n = 7 lambs from 7 ewes), twins (IUGR, n = 8 lambs from 8 ewes), and twins from ewes that received MMDS (2 g rumen-protected methionine, 300 mg folic acid, 1.2 g sulfur, 0.7 mg cobalt) daily from 120 days after mating (~0.8 of term) until delivery (IUGR+MMDS, n = 8 lambs from 4 ewes). Body composition and pancreas morphometry were assessed in lambs at day 16 IUGR reduced size at birth and increased neonatal fractional growth rate. MMDS normalized long bone lengths but not other body dimensions of IUGR lambs at birth. IUGR did not impair glucose control or insulin action at days 12-14 , compared with controls. MMDS increased metabolic clearance rate of insulin and increased β-cell numerical density and tended to improve insulin sensitivity, compared with untreated IUGR lambs. This demonstrates that effects of late-pregnancy methyl donor supplementation persist until at least the third week of life. Whether these effects of MMDS persist beyond early postnatal life and improve metabolic outcomes after IUGR in adults and the underlying mechanisms remain to be determined., (Copyright © 2017 the American Physiological Society.)

Published

2017

11. The New Biology and Pharmacology of Glucagon.

Author

Müller TD, Finan B, Clemmensen C, DiMarchi RD, and Tschöp MH

Subjects

Animals, Brain drug effects, Gastrointestinal Tract drug effects, Glucagon pharmacology, Homeostasis physiology, Humans, Liver drug effects, Pancreas drug effects, Brain metabolism, Gastrointestinal Tract metabolism, Glucagon metabolism, Liver metabolism, Metabolic Diseases metabolism, Pancreas metabolism

Abstract

In the last two decades we have witnessed sizable progress in defining the role of gastrointestinal signals in the control of glucose and energy homeostasis. Specifically, the molecular basis of the huge metabolic benefits in bariatric surgery is emerging while novel incretin-based medicines based on endogenous hormones such as glucagon-like peptide 1 and pancreas-derived amylin are improving diabetes management. These and related developments have fostered the discovery of novel insights into endocrine control of systemic metabolism, and in particular a deeper understanding of the importance of communication across vital organs, and specifically the gut-brain-pancreas-liver network. Paradoxically, the pancreatic peptide glucagon has reemerged in this period among a plethora of newly identified metabolic macromolecules, and new data complement and challenge its historical position as a gut hormone involved in metabolic control. The synthesis of glucagon analogs that are biophysically stable and soluble in aqueous solutions has promoted biological study that has enriched our understanding of glucagon biology and ironically recruited glucagon agonism as a central element to lower body weight in the treatment of metabolic disease. This review summarizes the extensive historical record and the more recent provocative direction that integrates the prominent role of glucagon in glucose elevation with its under-acknowledged effects on lipids, body weight, and vascular health that have implications for the pathophysiology of metabolic diseases, and the emergence of precision medicines to treat metabolic diseases., (Copyright © 2017 the American Physiological Society.)

Published

2017

12. Inhibition of pancreatic acinar mitochondrial thiamin pyrophosphate uptake by the cigarette smoke component 4-(methylnitrosamino)-1-(3-pyridyl)-1-butanone.

Author

Srinivasan P, Thrower EC, Gorelick FS, and Said HM

Subjects

Acinar Cells drug effects, Animals, Anion Transport Proteins genetics, Anion Transport Proteins metabolism, Biological Transport, Cell Line, Histones metabolism, Mice, Mice, Inbred C57BL, Mitochondrial Membrane Transport Proteins, Mitochondrial Proteins genetics, Mitochondrial Proteins metabolism, Pancreas cytology, Pancreas drug effects, Promoter Regions, Genetic, Protein Processing, Post-Translational, RNA, Messenger genetics, RNA, Messenger metabolism, Acinar Cells metabolism, Carcinogens toxicity, Nitrosamines toxicity, Pancreas metabolism, Thiamine Pyrophosphate metabolism, Tobacco Smoke Pollution adverse effects

Abstract

Thiamin is essential for normal metabolism in pancreatic acinar cells (PAC) and is obtained from their microenvironment through specific plasma-membrane transporters, converted to thiamin pyrophosphate (TPP) in the cytoplasm, followed by uptake of TPP by mitochondria through the mitochondrial TPP (MTPP) transporter (MTPPT; product of SLC25A19 gene). TPP is essential for normal mitochondrial function. We examined the effect of long-term/chronic exposure of PAC in vitro (pancreatic acinar 266-6 cells) and in vivo (wild-type or transgenic mice carrying the SLC25A19 promoter) of the cigarette smoke toxin, 4-(methylnitrosamino)-1-(3-pyridyl)-1-butanone (NNK), on the MTPP uptake process. Our in vitro and in vivo findings demonstrate that NNK negatively affects MTPP uptake and reduced expression of MTPPT protein, MTPPT mRNA, and heterogenous nuclear RNA, as well as SLC25A19 promoter activity. The effect of NNK on Slc25a19 transcription was neither mediated by changes in expression of transcriptional factor NFY-1 (known to drive SLC25A19 transcription), nor due to changes in methylation profile of the Slc25a19 promoter. Rather, it appears to be due to changes in histone modifications that involve significant decreases in histone H3K4-trimethylation and H3K9-acetylation (activation markers). The effect of NNK on MTPPT function is mediated through the nonneuronal α7-nicotinic acetylcholine receptor (α7-nAChR), as indicated by both in vitro (using the nAChR antagonist mecamylamine) and in vivo (using an α7-nAchR(-/-) mouse model) studies. These findings demonstrate that chronic exposure of PAC to NNK negatively impacts PAC MTPP uptake. This effect appears to be exerted at the level of Slc25a19 transcription, involve epigenetic mechanism(s), and is mediated through the α7-nAchR.

Published

2016

13. Involvement of myristoylated alanine-rich C kinase substrate phosphorylation and translocation in cholecystokinin-induced amylase release in rat pancreatic acini.

Author

Satoh K, Narita T, Katsumata-Kato O, Sugiya H, and Seo Y

Subjects

Acetophenones pharmacology, Animals, Benzopyrans pharmacology, Cell Membrane drug effects, Cell Membrane metabolism, Cholecystokinin antagonists & inhibitors, Cytosol drug effects, Cytosol metabolism, Intracellular Signaling Peptides and Proteins genetics, Male, Membrane Microdomains metabolism, Membrane Proteins genetics, Myristoylated Alanine-Rich C Kinase Substrate, Pancreas drug effects, Pancreas enzymology, Phosphorylation, Protein Kinase C-delta drug effects, Protein Kinase C-delta metabolism, Qa-SNARE Proteins metabolism, Rats, Rats, Sprague-Dawley, Translocation, Genetic, Amylases metabolism, Cholecystokinin pharmacology, Intracellular Signaling Peptides and Proteins biosynthesis, Membrane Proteins biosynthesis, Pancreas metabolism, Protein Kinase C metabolism

Abstract

Cholecystokinin (CCK) is a gastrointestinal hormone that induces exocytotic amylase release in pancreatic acinar cells. The activation of protein kinase C (PKC) is involved in the CCK-induced pancreatic amylase release. Myristoylated alanine-rich C kinase substrate (MARCKS) is a ubiquitously expressed substrate of PKC. MARCKS has been implicated in membrane trafficking in several cell types. The phosphorylation of MARCKS by PKC results in the translocation of MARCKS from the membrane to the cytosol. Here, we studied the involvement of MARCKS in the CCK-induced amylase release in rat pancreatic acini. Employing Western blotting, we detected MARCKS protein in the rat pancreatic acini. CCK induced MARCKS phosphorylation. A PKC-δ inhibitor, rottlerin, inhibited the CCK-induced MARCKS phosphorylation and amylase release. In the translocation assay, we also observed CCK-induced PKC-δ activation. An immunohistochemistry study showed that CCK induced MARCKS translocation from the membrane to the cytosol. When acini were lysed by a detergent, Triton X-100, CCK partially induced displacement of the MARCKS from the GM1a-rich detergent-resistant membrane fractions (DRMs) in which Syntaxin2 is distributed. A MARCKS-related peptide inhibited the CCK-induced amylase release. These findings suggest that MARCKS phosphorylation by PKC-δ and then MARCKS translocation from the GM1a-rich DRMs to the cytosol are involved in the CCK-induced amylase release in pancreatic acinar cells., (Copyright © 2016 the American Physiological Society.)

Published

2016

14. Direct effect of incretin hormones on glucose and glycerol metabolism and hemodynamics.

Author

Karstoft K, Mortensen SP, Knudsen SH, and Solomon TP

Subjects

Adolescent, Adult, Blood Glucose drug effects, Blood Glucose metabolism, Blood Pressure drug effects, Carotid Artery, Common drug effects, Carotid Artery, Common physiology, Glucose Clamp Technique, Heart Rate drug effects, Humans, Hyperglycemia metabolism, Male, Pancreas drug effects, Pancreas metabolism, Regional Blood Flow drug effects, Young Adult, Glucose metabolism, Glycerol metabolism, Hemodynamics drug effects, Incretins pharmacology

Abstract

The objective of this study was to assess the insulin-independent effects of incretin hormones on glucose and glycerol metabolism and hemodynamics under euglycemic and hyperglycemic conditions. Young, healthy men (n=10) underwent three trials in a randomized, controlled, crossover study. Each trial consisted of a two-stage (euglycemia and hyperglycemia) pancreatic clamp (using somatostatin to prevent endogenous insulin secretion). Glucose and lipid metabolism was measured via infusion of stable glucose and glycerol isotopic tracers. Hemodynamic variables (femoral, brachial, and common carotid artery blood flow and flow-mediated dilation of the brachial artery) were also measured. The three trials differed as follows: 1) saline [control (CON)], 2) glucagon-like peptide (GLP-1, 0.5 pmol·kg(-1)·min(-1)), and 3) glucose-dependent insulinotropic polypeptide (GIP, 1.5 pmol·kg(-1)·min(-1)). No between-trial differences in glucose infusion rates (GIR) or glucose or glycerol kinetics were seen during euglycemia, whereas hyperglycemia resulted in increased GIR and glucose rate of disappearance during GLP-1 compared with CON and GIP (P<0.01 for all). However, when normalized to insulin levels, no differences between trials were seen for GIR or glucose rate of disappearance. Besides a higher femoral blood flow during hyperglycemia with GIP (vs. CON and GLP-1, P<0.001), no between-trial differences were seen for the hemodynamic variables. In conclusion, GLP-1 and GIP have no direct effect on whole body glucose metabolism or hemodynamics during euglycemia. On the contrary, during hyperglycemia, GIP increases femoral artery blood flow with no effect on glucose metabolism, whereas GLP-1 increases glucose disposal, potentially due to increased insulin levels., (Copyright © 2015 the American Physiological Society.)

Published

2015

15. Chronic alcohol exposure inhibits biotin uptake by pancreatic acinar cells: possible involvement of epigenetic mechanisms.

Author

Srinivasan P, Kapadia R, Biswas A, and Said HM

Subjects

Acinar Cells drug effects, Animals, Biological Transport, Active, Cells, Cultured, CpG Islands, DNA Methylation, Ethanol toxicity, Humans, Kruppel-Like Factor 4, Kruppel-Like Transcription Factors genetics, Kruppel-Like Transcription Factors metabolism, Mice, Pancreas cytology, Pancreas metabolism, Promoter Regions, Genetic, RNA, Messenger genetics, RNA, Messenger metabolism, Sodium pharmacology, Symporters genetics, Acinar Cells metabolism, Alcoholism metabolism, Biotin metabolism, Epigenesis, Genetic, Pancreas drug effects, Symporters metabolism

Abstract

Chronic exposure to alcohol affects different physiological aspects of pancreatic acinar cells (PAC), but its effect on the uptake process of biotin is not known. We addressed this issue using mouse-derived pancreatic acinar 266-6 cells chronically exposed to alcohol and wild-type and transgenic mice (carrying the human SLC5A6 5'-promoter) fed alcohol chronically. First we established that biotin uptake by PAC is Na(+) dependent and carrier mediated and involves sodium-dependent multivitamin transporter (SMVT). Chronic exposure of 266-6 cells to alcohol led to a significant inhibition in biotin uptake, expression of SMVT protein, and mRNA as well as in the activity of the SLC5A6 promoter. Similarly, chronic alcohol feeding of wild-type and transgenic mice carrying the SLC5A6 promoter led to a significant inhibition in biotin uptake by PAC, as well as in the expression of SMVT protein and mRNA and the activity of the SLC5A6 promoters expressed in the transgenic mice. We also found that chronic alcohol feeding of mice is associated with a significant increase in the methylation status of CpG islands predicted to be in the mouse Slc5a6 promoters and a decrease in the level of expression of transcription factor KLF-4, which plays an important role in regulating SLC5A6 promoter activity. These results demonstrate, for the first time, that chronic alcohol exposure negatively impacts biotin uptake in PAC and that this effect is exerted (at least in part) at the level of transcription of the SLC5A6 gene and may involve epigenetic/molecular mechanisms., (Copyright © 2014 the American Physiological Society.)

Published

2014

16. Leptin restores the insulinotropic effect of exenatide in a mouse model of type 2 diabetes with increased adiposity induced by streptozotocin and high-fat diet.

Author

Sakai T, Kusakabe T, Ebihara K, Aotani D, Yamamoto-Kataoka S, Zhao M, Gumbilai VM, Ebihara C, Aizawa-Abe M, Yamamoto Y, Noguchi M, Fujikura J, Hosoda K, Inagaki N, and Nakao K

Subjects

Adiposity drug effects, Animals, Anti-Obesity Agents administration & dosage, Anti-Obesity Agents therapeutic use, Diabetes Mellitus, Type 2 complications, Diabetes Mellitus, Type 2 metabolism, Diet, High-Fat adverse effects, Drug Implants, Drug Synergism, Drug Therapy, Combination, Exenatide, Glucagon-Like Peptide 1 agonists, Glucagon-Like Peptide 1 metabolism, Hyperglycemia prevention & control, Hypoglycemic Agents administration & dosage, Insulin metabolism, Insulin Secretion, Leptin administration & dosage, Leptin genetics, Male, Mice, Inbred C57BL, Overweight drug therapy, Overweight etiology, Overweight metabolism, Pancreas metabolism, Peptides administration & dosage, Recombinant Proteins administration & dosage, Recombinant Proteins genetics, Recombinant Proteins therapeutic use, Streptozocin, Triglycerides metabolism, Venoms administration & dosage, Diabetes Mellitus, Type 2 drug therapy, Disease Models, Animal, Hypoglycemic Agents therapeutic use, Leptin therapeutic use, Overweight complications, Pancreas drug effects, Peptides therapeutic use, Venoms therapeutic use

Abstract

Leptin may reduce pancreatic lipid deposition, which increases with progression of obesity and can impair β-cell function. The insulinotropic effect of glucagon-like peptide-1 (GLP-1) and the efficacy of GLP-1 receptor agonist are reduced associated with impaired β-cell function. In this study, we examined whether leptin could restore the efficacy of exenatide, a GLP-1 receptor agonist, in type 2 diabetes with increased adiposity. We chronically administered leptin (500 μg·kg⁻¹·day⁻¹) and/or exenatide (20 μg·kg⁻¹·day⁻¹) for 2 wk in a mouse model of type 2 diabetes with increased adiposity induced by streptozotocin and high-fat diet (STZ/HFD mice). The STZ/HFD mice exhibited hyperglycemia, overweight, increased pancreatic triglyceride level, and reduced glucose-stimulated insulin secretion (GSIS); moreover, the insulinotropic effect of exenatide was reduced. However, leptin significantly reduced pancreatic triglyceride level, and adding leptin to exenatide (LEP/EX) remarkably enhanced GSIS. These results suggested that the leptin treatment restored the insulinotropic effect of exenatide in the mice. In addition, LEP/EX reduced food intake, body weight, and triglyceride levels in the skeletal muscle and liver, and corrected hyperglycemia to a greater extent than either monotherapy. The pair-feeding experiment indicated that the marked reduction of pancreatic triglyceride level and enhancement of GSIS by LEP/EX occurred via mechanisms other than calorie restriction. These results suggest that leptin treatment may restore the insulinotropic effect of exenatide associated with the reduction of pancreatic lipid deposition in type 2 diabetes with increased adiposity. Combination therapy with leptin and exenatide could be an effective treatment for patients with type 2 diabetes with increased adiposity., (Copyright © 2014 the American Physiological Society.)

Published

2014

17. Blood lipids affect rat islet blood flow regulation through β₃-adrenoceptors.

Author

Lai E, Pettersson U, Verdugo AD, Carlsson PO, Bodin B, Källskog Ö, Persson AE, Sandberg M, and Jansson L

Subjects

Adrenergic beta-3 Receptor Antagonists pharmacology, Animals, Emulsions adverse effects, Fatty Acids, Nonesterified blood, Fatty Acids, Nonesterified metabolism, Hyperlipidemias blood, Hyperlipidemias etiology, Hyperlipidemias metabolism, Insulin blood, Insulin Secretion, Islets of Langerhans drug effects, Islets of Langerhans innervation, Islets of Langerhans metabolism, Male, Mice, Inbred C57BL, Pancreas blood supply, Pancreas drug effects, Pancreas innervation, Pancreas metabolism, Perfusion, Phospholipids adverse effects, Propanolamines pharmacology, Rats, Inbred WF, Receptors, Adrenergic, beta-3 chemistry, Soybean Oil adverse effects, Triglycerides blood, Triglycerides metabolism, Vagotomy, Truncal, Vagus Nerve drug effects, Vagus Nerve surgery, Hyperlipidemias physiopathology, Insulin metabolism, Islets of Langerhans blood supply, Receptors, Adrenergic, beta-3 metabolism, Regional Blood Flow drug effects, Up-Regulation drug effects, Vagus Nerve physiopathology

Abstract

Pancreatic islet blood perfusion varies according to the needs for insulin secretion. We examined the effects of blood lipids on pancreatic islet blood flow in anesthetized rats. Acute administration of Intralipid to anesthetized rats increased both triglycerides and free fatty acids, associated with a simultaneous increase in total pancreatic and islet blood flow. A preceding abdominal vagotomy markedly potentiated this and led acutely to a 10-fold increase in islet blood flow associated with a similar increase in serum insulin concentrations. The islet blood flow and serum insulin response could be largely prevented by pretreatment with propranolol and the selective β₃-adrenergic inhibitor SR-59230A. The nitric oxide synthase inhibitor N(G)-nitro-l-arginine methyl ester prevented the blood flow increase but was less effective in reducing serum insulin. Increased islet blood flow after Intralipid administration was also seen in islet and whole pancreas transplanted rats, i.e., models with different degrees of chronic islet denervation, but the effect was not as pronounced. In isolated vascularly perfused single islets Intralipid dilated islet arterioles, but this was not affected by SR-59230A. Both the sympathetic and parasympathetic nervous system are important for the coordination of islet blood flow and insulin release during hyperlipidemia, with a previously unknown role for β₃-adrenoceptors., (Copyright © 2014 the American Physiological Society.)

Published

2014

18. ERK activation is required for CCK-mediated pancreatic adaptive growth in mice.

Author

Holtz BJ, Lodewyk KB, Sebolt-Leopold JS, Ernst SA, and Williams JA

Subjects

Animals, Cell Cycle Proteins metabolism, DNA Replication, Early Growth Response Transcription Factors metabolism, Enzyme Activation, Extracellular Signal-Regulated MAP Kinases antagonists & inhibitors, Male, Mice, Inbred ICR, Mitogen-Activated Protein Kinase Kinases antagonists & inhibitors, Mitogen-Activated Protein Kinase Kinases metabolism, Pancreas drug effects, Pancreas growth & development, Protein Kinase Inhibitors pharmacology, RNA biosynthesis, Time Factors, Trypsin Inhibitors pharmacology, Cell Proliferation drug effects, Cholecystokinin metabolism, Extracellular Signal-Regulated MAP Kinases metabolism, MAP Kinase Signaling System drug effects, Pancreas enzymology

Abstract

High levels of cholecystokinin (CCK) can stimulate pancreatic adaptive growth in which mature acinar cells divide, leading to enhanced pancreatic mass with parallel increases in protein, DNA, RNA, and digestive enzyme content. Prolonged release of CCK can be induced by feeding trypsin inhibitor (TI) to disrupt normal feedback control. This leads to exocrine growth in a CCK-dependent manner. The extracellular signal-related kinase (ERK) pathway regulates many proliferative processes in various tissues and disease models. The aim of this study was to evaluate the role of ERK signaling in pancreatic adaptive growth using the MEK inhibitors PD-0325901 and trametinib (GSK-1120212). It was determined that PD-0325901 given two times daily by gavage or mixed into powdered chow was an effective and specific inhibitor of ERK signaling in vivo. TI-containing chow led to a robust increase in pancreatic mass, protein, DNA, and RNA content. This pancreatic adaptive growth was blocked in mice fed chow containing the MEK inhibitors. PD-0325901 blocked TI-induced ERK-regulated early response genes, cell-cycle proteins, and mitogenesis by acinar cells. It was determined that ERK signaling is necessary for the initiation of pancreatic adaptive growth but not necessary to maintain it. PD-0325901 blocked adaptive growth when given before cell-cycle initiation but not after mitogenesis had been established. Furthermore, GSK-1120212, a chemically distinct inhibitor of the ERK pathway that is now approved for clinical use, inhibited growth similar to PD-0325901. These data demonstrate that the ERK pathway is required for CCK-stimulated pancreatic adaptive growth., (Copyright © 2014 the American Physiological Society.)

Published

2014

19. Genetic inhibition of protein kinase Cε attenuates necrosis in experimental pancreatitis.

Author

Liu Y, Yuan J, Tan T, Jia W, Lugea A, Mareninova O, Waldron RT, and Pandol SJ

Subjects

Acinar Cells drug effects, Acinar Cells metabolism, Animals, CASP8 and FADD-Like Apoptosis Regulating Protein genetics, CASP8 and FADD-Like Apoptosis Regulating Protein metabolism, Ceruletide toxicity, Cytochromes c metabolism, Ethanol pharmacology, Inhibitor of Apoptosis Proteins genetics, Inhibitor of Apoptosis Proteins metabolism, Mice, Mice, Inbred C57BL, Necrosis, Pancreas drug effects, Pancreas pathology, Pancreatitis genetics, Pancreatitis pathology, Protein Kinase C-epsilon genetics, Proto-Oncogene Proteins c-bcl-2 genetics, Proto-Oncogene Proteins c-bcl-2 metabolism, Receptor-Interacting Protein Serine-Threonine Kinases metabolism, Sincalide pharmacology, bcl-2 Homologous Antagonist-Killer Protein genetics, bcl-2 Homologous Antagonist-Killer Protein metabolism, Apoptosis, Gene Deletion, Pancreas metabolism, Pancreatitis metabolism, Protein Kinase C-epsilon metabolism

Abstract

Understanding the regulation of death pathways, necrosis and apoptosis, in pancreatitis is important for developing therapies directed to the molecular pathogenesis of the disease. Protein kinase Cε (PKCε) has been previously shown to regulate inflammatory responses and zymogen activation in pancreatitis. Furthermore, we demonstrated that ethanol specifically activated PKCε in pancreatic acinar cells and that PKCε mediated the sensitizing effects of ethanol on inflammatory response in pancreatitis. Here we investigated the role of PKCε in the regulation of death pathways in pancreatitis. We found that genetic deletion of PKCε resulted in decreased necrosis and severity in the in vivo cerulein-induced pancreatitis and that inhibition of PKCε protected the acinar cells from CCK-8 hyperstimulation-induced necrosis and ATP reduction. These findings were associated with upregulation of mitochondrial Bak and Bcl-2/Bcl-xL, proapoptotic and prosurvival members in the Bcl-2 family, respectively, as well as increased mitochondrial cytochrome c release, caspase activation, and apoptosis in pancreatitis in PKCε knockout mice. We further confirmed that cerulein pancreatitis induced a dramatic mitochondrial translocation of PKCε, suggesting that PKCε regulated necrosis in pancreatitis via mechanisms involving mitochondria. Finally, we showed that PKCε deletion downregulated inhibitors of apoptosis proteins, c-IAP2, survivin, and c-FLIPs while promoting cleavage/inactivation of receptor-interacting protein kinase (RIP). Taken together, our findings provide evidence that PKCε activation during pancreatitis promotes necrosis through mechanisms involving mitochondrial proapoptotic and prosurvival Bcl-2 family proteins and upregulation of nonmitochondrial pathways that inhibit caspase activation and RIP cleavage/inactivation. Thus PKCε is a potential target for prevention and/or treatment of acute pancreatitis., (Copyright © 2014 the American Physiological Society.)

Published

2014

20. Chronic rapamycin treatment causes diabetes in male mice.

Author

Schindler CE, Partap U, Patchen BK, and Swoap SJ

Subjects

Administration, Oral, Animals, Blood Glucose drug effects, Blood Glucose metabolism, Diabetes Mellitus blood, Diabetes Mellitus pathology, Diabetes Mellitus prevention & control, Diabetes Mellitus urine, Estradiol administration & dosage, Estrogen Replacement Therapy, Female, Glucose Intolerance blood, Glucose Intolerance chemically induced, Glycosuria chemically induced, Glycosuria urine, Male, Mice, Orchiectomy, Ovariectomy, Pancreas drug effects, Pancreas metabolism, Pancreas pathology, Protein Kinase Inhibitors administration & dosage, Pyruvic Acid metabolism, Sex Factors, Sirolimus administration & dosage, TOR Serine-Threonine Kinases antagonists & inhibitors, TOR Serine-Threonine Kinases metabolism, Testosterone metabolism, Time Factors, Diabetes Mellitus chemically induced, Protein Kinase Inhibitors toxicity, Sirolimus toxicity

Abstract

Current evidence indicates that the mammalian target of rapamycin inhibitor rapamycin both increases longevity and, seemingly contradictorily, impairs glucose homeostasis. Most studies exploring the dimensions of this paradox have been based on rapamycin treatment in mice for up to 20 wk. We sought to better understand the metabolic effects of oral rapamycin over a substantially longer period of time in HET3 mice. We observed that treatment with rapamycin for 52 wk induced diabetes in male mice, characterized by hyperglycemia, significant urine glucose levels, and severe glucose and pyruvate intolerance. Glucose intolerance occurred in male mice by 4 wk on rapamycin and could be only partially reversed with cessation of rapamycin treatment. Female mice developed moderate glucose intolerance over 1 yr of rapamycin treatment, but not diabetes. The role of sex hormones in the differential development of diabetic symptoms in male and female mice was further explored. HET3 mice treated with rapamycin for 52 wk were gonadectomized and monitored over 10 wk. Castrated male mice remained glucose intolerant, while ovariectomized females developed significant glucose intolerance over the same time period. Subsequent replacement of 17β-estradiol (E2) in ovariectomized females promoted a recovery of glucose tolerance over a 4-wk period, suggesting the protective role of E2 against rapamycin-induced diabetes. These results indicate that 1) oral rapamycin treatment causes diabetes in male mice, 2) the diabetes is partially reversible with cessation of treatment, and 3) E2 plays a protective role against the development of rapamycin-induced diabetes., (Copyright © 2014 the American Physiological Society.)

Published

2014

21. Minimal modeling of insulin secretion in the perfused rat pancreas: a drug effect case study.

Author

Riz M, Pedersen MG, Toffolo GM, Haschke G, Schneider HC, Klabunde T, Margerie D, and Cobelli C

Subjects

Algorithms, Animals, Glucagon-Like Peptide 1 agonists, Glucagon-Like Peptide 1 pharmacology, Glucagon-Like Peptide-1 Receptor, Hypoglycemic Agents agonists, Hypoglycemic Agents metabolism, Hypoglycemic Agents pharmacology, In Vitro Techniques, Insulin Secretion, Insulin-Secreting Cells drug effects, Kinetics, Male, Monomeric GTP-Binding Proteins metabolism, Monomeric GTP-Binding Proteins pharmacology, Pancreas drug effects, Pancreas metabolism, Peptides pharmacology, Perfusion, Rats, Rats, Sprague-Dawley, Receptors, G-Protein-Coupled agonists, Receptors, G-Protein-Coupled metabolism, Receptors, Glucagon agonists, Reproducibility of Results, Glucagon-Like Peptide 1 metabolism, Glucose metabolism, Insulin metabolism, Insulin-Secreting Cells metabolism, Models, Biological, Receptors, Glucagon metabolism, Signal Transduction drug effects

Abstract

The experimental protocol of the perfused rat pancreas is commonly used to evaluate β-cell function. In this context, mathematical models become useful tools through the determination of indexes that allow the assessment of β-cell function in different experimental groups and the quantification of the effects of antidiabetic drugs, secretagogues, or treatments. However, a minimal model applicable to the isolated perfused rat pancreas has so far been unavailable. In this work, we adapt the C-peptide minimal model applied previously to the intravenous glucose tolerance test to obtain a specific model for the experimental settings of the perfused pancreas. Using the model, it is possible to estimate indexes describing β-cell responsivity for first (ΦD) and second phase (ΦS, T) of insulin secretion. The model was initially applied to untreated pancreata and afterward used for the assessment of pharmacologically relevant agents (the gut hormone GLP-1, the potent GLP-1 receptor agonist lixisenatide, and a GPR40/FFAR1 agonist, SAR1) to quantify and differentiate their effect on insulin secretion. Model fit was satisfactory, and parameters were estimated with good precision for both untreated and treated pancreata. Model application showed that lixisenatide reaches improvement of β-cell function similarly to GLP-1 (11.7- vs. 13.1-fold increase in ΦD and 2.3- vs. 2.8-fold increase in ΦS) and demonstrated that SAR1 leads to an additional improvement of β-cell function in the presence of postprandial GLP-1 levels.

Published

2014

22. Defective prolactin signaling impairs pancreatic β-cell development during the perinatal period.

Author

Auffret J, Freemark M, Carré N, Mathieu Y, Tourrel-Cuzin C, Lombès M, Movassat J, and Binart N

Subjects

Animals, Animals, Newborn, Cell Differentiation, Cells, Cultured, Embryo, Mammalian, Female, Insulin-Secreting Cells cytology, Insulin-Secreting Cells drug effects, Mice, Mice, Knockout, Pancreas drug effects, Pancreas growth & development, Pregnancy, Prolactin pharmacology, Rats, Rats, Wistar, Receptors, Prolactin genetics, Signal Transduction drug effects, Signal Transduction physiology, Insulin-Secreting Cells physiology, Pancreas embryology, Prolactin metabolism, Receptors, Prolactin metabolism

Abstract

Prolactin (PRL) and placental lactogens stimulate β-cell replication and insulin production in pancreatic islets and insulinoma cells through binding to the PRL receptor (PRLR). However, the contribution of PRLR signaling to β-cell ontogeny and function in perinatal life and the effects of the lactogens on adaptive islet growth are poorly understood. We provide evidence that expansion of β-cell mass during both embryogenesis and the postnatal period is impaired in the PRLR(-/-) mouse model. PRLR(-/-) newborns display a 30% reduction of β-cell mass, consistent with reduced proliferation index at E18.5. PRL stimulates leucine incorporation and S6 kinase phosphorylation in INS-1 cells, supporting a role for β-cell mTOR signaling in PRL action. Interestingly, a defect in the development of acini is also observed in absence of PRLR signaling, with a sharp decline in cellular size in both endocrine and exocrine compartments. Of note, a decrease in levels of IGF-II, a PRL target, in the Goto-Kakizaki (GK) rat, a spontaneous model of type 2 diabetes, is associated with a lack of PRL-mediated β-cell proliferation in embryonic pancreatic buds. Reduced pancreatic IGF-II expression in both rat and mouse models suggests that this factor may constitute a molecular link between PRL signaling and cell ontogenesis. Together, these results provide evidence that PRL signaling is essential for pancreas ontogenesis during the critical perinatal window responsible for establishing functional β-cell reserve.

Published

2013

23. One year of sitagliptin treatment protects against islet amyloid-associated β-cell loss and does not induce pancreatitis or pancreatic neoplasia in mice.

Author

Aston-Mourney K, Subramanian SL, Zraika S, Samarasekera T, Meier DT, Goldstein LC, and Hull RL

Subjects

Animals, Diabetes Mellitus, Type 2 metabolism, Diabetes Mellitus, Type 2 pathology, Dipeptidyl-Peptidase IV Inhibitors adverse effects, Drug Therapy, Combination adverse effects, Hemizygote, Humans, Hypoglycemic Agents adverse effects, Hypoglycemic Agents therapeutic use, Insulin-Secreting Cells metabolism, Insulin-Secreting Cells pathology, Islet Amyloid Polypeptide genetics, Islet Amyloid Polypeptide metabolism, Male, Metformin adverse effects, Metformin therapeutic use, Mice, Mice, Transgenic, Pancreas drug effects, Pancreas metabolism, Pancreas pathology, Pancreatic Neoplasms chemically induced, Pancreatitis chemically induced, Pyrazines adverse effects, Random Allocation, Recombinant Proteins biosynthesis, Recombinant Proteins genetics, Recombinant Proteins metabolism, Sitagliptin Phosphate, Time Factors, Triazoles adverse effects, Diabetes Mellitus, Type 2 drug therapy, Dipeptidyl-Peptidase IV Inhibitors therapeutic use, Insulin-Secreting Cells drug effects, Islet Amyloid Polypeptide biosynthesis, Plaque, Amyloid prevention & control, Pyrazines therapeutic use, Triazoles therapeutic use

Abstract

The dipeptidyl peptidase-4 (DPP-4) inhibitor sitagliptin is an attractive therapy for diabetes, as it increases insulin release and may preserve β-cell mass. However, sitagliptin also increases β-cell release of human islet amyloid polypeptide (hIAPP), the peptide component of islet amyloid, which is cosecreted with insulin. Thus, sitagliptin treatment may promote islet amyloid formation and its associated β-cell toxicity. Conversely, metformin treatment decreases islet amyloid formation by decreasing β-cell secretory demand and could therefore offset sitagliptin's potential proamyloidogenic effects. Sitagliptin treatment has also been reported to be detrimental to the exocrine pancreas. We investigated whether long-term sitagliptin treatment, alone or with metformin, increased islet amyloid deposition and β-cell toxicity and induced pancreatic ductal proliferation, pancreatitis, and/or pancreatic metaplasia/neoplasia. hIAPP transgenic and nontransgenic littermates were followed for 1 yr on no treatment, sitagliptin, metformin, or the combination. Islet amyloid deposition, β-cell mass, insulin release, and measures of exocrine pancreas pathology were determined. Relative to untreated mice, sitagliptin treatment did not increase amyloid deposition, despite increasing hIAPP release, and prevented amyloid-induced β-cell loss. Metformin treatment alone or with sitagliptin decreased islet amyloid deposition to a similar extent vs untreated mice. Ductal proliferation was not altered among treatment groups, and no evidence of pancreatitis, ductal metaplasia, or neoplasia were observed. Therefore, long-term sitagliptin treatment stimulates β-cell secretion without increasing amyloid formation and protects against amyloid-induced β-cell loss. This suggests a novel effect of sitagliptin to protect the β-cell in type 2 diabetes that appears to occur without adverse effects on the exocrine pancreas.

Published

2013

24. Intraportal GLP-1 stimulates insulin secretion predominantly through the hepatoportal-pancreatic vagal reflex pathways.

Author

Nishizawa M, Nakabayashi H, Uehara K, Nakagawa A, Uchida K, and Koya D

Subjects

Animals, Area Under Curve, Blood Glucose metabolism, Electrophysiological Phenomena physiology, Glucagon-Like Peptide 1 administration & dosage, Glucose administration & dosage, Glucose pharmacology, Incretins physiology, Infusions, Intravenous, Insulin blood, Insulin Secretion, Liver drug effects, Liver innervation, Male, Pancreas drug effects, Postprandial Period physiology, Rats, Reflex drug effects, Signal Transduction drug effects, Vagotomy, Vagus Nerve drug effects, Glucagon-Like Peptide 1 pharmacology, Insulin metabolism, Liver metabolism, Pancreas metabolism, Portal Vein physiology, Vagus Nerve physiology

Abstract

We previously reported that glucagon-like peptide-1 (GLP-1) appearance in the portal vein facilitates hepatic vagal afferent activity, and this further augments reflexively the pancreatic vagal efferents in anesthetized rats, suggesting a neuroincretin effect of GLP-1. To determine whether the GLP-1-induced vagal pathways lead to a neuronal-mediated component (NMC) of insulin secretion, we infused GLP-1 at a physiological or pharmacological dose (1 or 3 pmol·kg(-1)·min(-1), respectively) into the portal vein in conscious rats with selective hepatic vagotomy (Vagox) or sham operation (Sham). The experiments consisted of two sequential 10-min intraportal infusions (P1 and P2): glucose at a physiological rate (56 μmol·kg(-1)·min(-1)) in P1 and the glucose plus GLP-1 or vehicle in P2. Under arterial isoglycemia across the groups, the physiological GLP-1 infusion in Sham augmented promptly and markedly arterial insulin levels, approximately twofold the levels in glucose alone infusion (P < 0.005), and insulin levels in Vagox diminished apparently (P < 0.05). Almost 60% of the GLP-1-induced insulin secretion (AUC) in Sham met the NMC, i.e., difference between insulin secretion in Sham and Vagox, (AUC 976 ± 65 vs. 393 ± 94 pmol·min/l, respectively, P < 0.005). Intraportal pharmacological GLP-1 infusion further augmented insulin secretion in both groups, but the NMC remained in 46% (NS; Sham vs. Vagox). In contrast, "isoglycemic" intravenous GLP-1 infusion (3 pmol·kg(-1)·min(-1)) evoked an equal insulin secretion in both groups. Thus, the present results indicate that GLP-1 appearing in the portal vein evokes a powerful neuronal-mediated insulinotropic effect, suggesting the neuroincretin effect.

Published

2013

25. Large molecule protein feeding during the suckling period is required for the development of pancreatic digestive functions in rats.

Author

Kinouchi T, Koyama S, Harada E, and Yajima T

Subjects

Animals, Cholecystokinin blood, Dietary Proteins pharmacology, Female, Insulin blood, Male, Models, Animal, Pancreas drug effects, Pancreatic Juice metabolism, Protein Hydrolysates pharmacology, Rats, Rats, Sprague-Dawley, Animals, Suckling metabolism, Dietary Proteins metabolism, Pancreas enzymology, Proteolysis

Abstract

We examined if large molecule protein feeding during the suckling period is prerequisite for the proper development of pancreatic digestive functions. Most amino acids in breast milk exist as the constituent of large proteins and not as oligopeptides or free amino acids. Accumulating evidence indicates the nutritional importance of large protein feeding for suckling infants; however, evidence on the physiological significance remains small. We thus artificially reared rat pups on a standard rat formula with milk protein or a formula with milk protein hydrolysate from 7 to 21 days of age, and thereafter, fed a standard solid diet until 42 days of age. Pancreas weight and the stock of pancreatic digestive enzymes in the hydrolysate-fed rats were significantly lower than those in the protein-fed rats during and also after the suckling period. Plasma insulin, a stimulator of amylase synthesis, was also significantly low in the hydrolysate-fed rats compared with the protein-fed rats. At 28 days of age, we evaluated the pancreatic secretory ability in response to dietary protein and cholecystokinin (CCK) by means of pancreatic duct cannulation. Pancreatic secretion stimulated by dietary protein in the hydrolysate-fed rats was significantly weaker than that in the protein-fed rats. No significant difference was observed in the increasing rate of pancreatic enzyme secretion in response to CCK between the two groups. These results suggest that the presence of large proteins in breast milk is significant for the development of pancreatic digestive functions and the outcomes could remain even later on in life.

Published

2012

26. Cerulein hyperstimulation decreases AMP-activated protein kinase levels at the site of maximal zymogen activation.

Author

Shugrue CA, Alexandre M, Diaz de Villalvilla A, Kolodecik TR, Young LH, Gorelick FS, and Thrower EC

Subjects

AMP-Activated Protein Kinases genetics, Amino Acid Sequence, Aminoimidazole Carboxamide analogs & derivatives, Aminoimidazole Carboxamide pharmacology, Animals, Cells, Cultured, Cyclic AMP-Dependent Protein Kinases genetics, Cyclic AMP-Dependent Protein Kinases metabolism, Gene Expression Regulation drug effects, Gene Expression Regulation physiology, Male, Metformin pharmacology, Octoxynol, Phosphorylation, Pyrazoles pharmacology, Pyrimidines pharmacology, Rats, Rats, Sprague-Dawley, Ribonucleotides pharmacology, Sodium Dodecyl Sulfate, AMP-Activated Protein Kinases metabolism, Ceruletide pharmacology, Enzyme Precursors metabolism, Pancreas cytology, Pancreas drug effects

Abstract

The premature activation of digestive enzyme zymogens in the pancreatic acinar cell is an important initiating event in acute pancreatitis. We have previously demonstrated that vacuolar ATPase (vATPase) activity is required for zymogen activation. Adenosine monophosphate-activated protein kinase (AMPK) regulates vATPase function in kidney and epididymal clear cells. To determine whether AMPK could affect pancreatitis responses, its effects were first examined in a cellular model of pancreatitis, cerulein-hyperstimulated (100 nM) pancreatic acini. This treatment caused a prominent increase in trypsin and chymotrypsin activities. Pretreatment with AICAR or metformin (AMPK activators) or compound C (an AMPK inhibitor) reduced or increased cerulein-induced zymogen activation, respectively. The association of the vATPase E subunit with membranes, a marker of its activation, tended to be inversely related to AMPK activity (assessed by AICAR and compound C treatments). Cerulein treatment did not change AMPK (α and β) levels but did lead to an increase in its activation (phosphorylation of Thr172) and induced the time-dependent translocation of the enzyme to a Triton-insoluble compartment. Basal in vivo studies showed that AMPK was widely distributed between membrane and soluble fractions generated by differential centrifugation. After cerulein hyperstimulation, AMPK levels selectively decreased in fractions containing the highest levels of active zymogens. These studies suggest that AMPK activity has a protective role in the pancreatic acinar cell that inhibits zymogen activation in the basal state, and this AMPK effect is reduced during pancreatitis. Therapies that prevent the selective reduction of AMPK in compartments that support zymogen activation could reduce injury during pancreatitis.

Published

2012

27. Tobacco carcinogen 4-(methylnitrosamino)-1-(3-pyridyl)-1-butanone initiates and enhances pancreatitis responses.

Author

Alexandre M, Uduman AK, Minervini S, Raoof A, Shugrue CA, Akinbiyi EO, Patel V, Shitia M, Kolodecik TR, Patton R, Gorelick FS, and Thrower EC

Subjects

Animals, Atropine pharmacology, Carcinogens administration & dosage, Cells, Cultured, Ceruletide administration & dosage, Ceruletide toxicity, Edema chemically induced, Enzyme Precursors genetics, Enzyme Precursors metabolism, L-Lactate Dehydrogenase metabolism, Male, Mecamylamine pharmacology, Nitrosamines administration & dosage, Rats, Rats, Sprague-Dawley, Receptors, Adrenergic, beta genetics, Receptors, Adrenergic, beta metabolism, Receptors, Nicotinic metabolism, Sincalide analogs & derivatives, Sincalide pharmacology, alpha7 Nicotinic Acetylcholine Receptor, Tobacco Products, Carcinogens toxicity, Nitrosamines toxicity, Pancreas drug effects, Pancreatitis chemically induced

Abstract

Clinical studies indicate that cigarette smoking increases the risk for developing acute pancreatitis. The nicotine metabolite 4-(methylnitrosamino)-1-(3-pyridyl)-1-butanone (NNK) is a major cigarette smoke toxin. We hypothesized that NNK could sensitize to pancreatitis and examined its effects in isolated rat pancreatic acini and in vivo. In acini, 100 nM NNK caused three- and fivefold activation of trypsinogen and chymotrypsinogen, respectively, above control. Furthermore, NNK pretreatment in acini enhanced zymogen activation in a cerulein pancreatitis model. The long-term effects of NNK were examined in vivo after intraperitoneal injection of NNK (100 mg/kg body wt) three times weekly for 2 wk. NNK alone caused zymogen activation (6-fold for trypsinogen and 2-fold for chymotrypsinogen vs. control), vacuolization, pyknotic nuclei, and edema. This NNK pretreatment followed by treatment with cerulein (40 μg/kg) for 1 h to induce early pancreatitis responses enhanced trypsinogen and chymotrypsinogen activation, as well as other parameters of pancreatitis, compared with cerulein alone. Potential targets of NNK include nicotinic acetylcholine receptors and β-adrenergic receptors; mRNA for both receptor types was detected in acinar cell preparations. Studies with pharmacological inhibitors of these receptors indicate that NNK can mediate acinar cell responses through an nonneuronal α(7)-nicotinic acetylcholine receptor (α(7)-nAChR). These studies suggest that prolonged exposure to this tobacco toxin can cause pancreatitis and sensitize to disease. Therapies targeting NNK-mediated pathways may prove useful in treatment of smoking-related pancreatitis.

Published

2012

28. The effects of 13 wk of liraglutide treatment on endocrine and exocrine pancreas in male and female ZDF rats: a quantitative and qualitative analysis revealing no evidence of drug-induced pancreatitis.

Author

Vrang N, Jelsing J, Simonsen L, Jensen AE, Thorup I, Søeborg H, and Knudsen LB

Subjects

Animals, Blood Glucose drug effects, Cell Proliferation drug effects, Exenatide, Female, Glucagon-Like Peptide 1 administration & dosage, Glucagon-Like Peptide 1 adverse effects, Glycated Hemoglobin analysis, Hypoglycemic Agents administration & dosage, Lipase blood, Liraglutide, Male, Pancreas pathology, Pancreatic alpha-Amylases blood, Pancreatitis pathology, Peptides administration & dosage, Peptides adverse effects, Rats, Rats, Zucker, Venoms administration & dosage, Venoms adverse effects, Glucagon-Like Peptide 1 analogs & derivatives, Hypoglycemic Agents adverse effects, Pancreas drug effects, Pancreatitis chemically induced

Abstract

A possible association between glucagon-like peptide-1 (GLP-1) analogs and incidences of pancreatitis has been suggested based on clinical studies. In male and female diabetic Zucker diabetic fatty (ZDF) rats, we investigated the effects of continuous administration of liraglutide and exenatide on biochemical [lipase, pancreatic amylase (P-amylase)] and histopathological markers of pancreatitis. Male and female ZDF rats were dosed for 13 wk with liraglutide (0.4 or 1.0 mg·kg(-1)·day(-1) sc once daily) or exenatide (0.25 mg·kg(-1)·day(-1) sc, Alzet osmotic minipumps). P-amylase and lipase plasma activity were measured, and an extended histopathological and stereological (specific cell mass and proliferation rate) evaluation of the exocrine and the endocrine pancreas was performed. Expectedly, liraglutide and exenatide lowered blood glucose and Hb A(1c) in male and female ZDF rats, whereas β-cell mass and proliferation rate were increased with greatly improved blood glucose control. Whereas neither analog affected lipase activity, small increases in P-amylase activity were observed in animals treated with liraglutide and exenatide. However, concurrent or permanent increases in lipase and P-amylase activity were never observed. Triglycerides were lowered by both GLP-1 analogs. The qualitative histopathological findings did not reveal adverse effects of liraglutide. The findings were mainly minimal in severity and focal in distribution. Similarly, the quantitative stereological analyses revealed no effects of liraglutide or exenatide on overall pancreas weight or exocrine and duct cell mass or proliferation. The present study demonstrates that, in overtly diabetic male and female ZDF rats, prolonged exposure to GLP-1 receptor agonists does not affect biochemical or histopathological markers of pancreatitis, and whereas both exenatide and liraglutide increase β-cell mass, they have no effect on the exocrine pancreas. However, clinical outcome studies and studies using primate tissues and/or studies in nonhuman primates are needed to further assess human risk.

Published

2012

29. c-Jun/AP-1 is required for CCK-induced pancreatic acinar cell dedifferentiation and DNA synthesis in vitro.

Author

Guo L, Sans MD, Hou Y, Ernst SA, and Williams JA

Subjects

Acinar Cells drug effects, Amylases metabolism, Animals, Cadherins metabolism, Cell Dedifferentiation drug effects, Cell Proliferation drug effects, Cells, Cultured, Cyclin D1 metabolism, DNA Replication drug effects, Mice, Pancreas drug effects, Pancreas metabolism, Signal Transduction drug effects, Signal Transduction physiology, beta Catenin metabolism, Acinar Cells metabolism, Cell Dedifferentiation physiology, Cholecystokinin pharmacology, DNA Replication physiology, Proto-Oncogene Proteins c-jun metabolism, Transcription Factor AP-1 metabolism

Abstract

Endogenous CCK plays an important role in pancreatic regeneration after pancreatitis. We used primary culture of mouse pancreatic acinar cells to evaluate the effect of CCK on acinar cell morphology and gene expression and to determine signaling pathways required for proliferation of acinar cells in vitro. Over 4 days in culture, cells grew out from acini and formed patches of monolayer, which displayed a reduced expression of acinar cell markers including digestive enzymes and Mist1 and an increased expression of ductal and embryonic markers, including cytokeratin 7, β-catenin, E-cadherin, pdx-1, and nestin. There was no appearance of stellate cell markers. CCK enhanced cellular spreading, DNA synthesis, and cyclin D1 expression. When signaling pathways were evaluated, CCK stimulation increased c-Jun expression, JNK and ERK activity, and AP-1 activation. Chemical inhibitors of JNK and ERK pathways, dominant-negative JNK and c-Jun, and c-Jun shRNA significantly inhibited CCK-induced DNA synthesis, CCK-induced AP-1 activation, and cyclin D1 expression. Furthermore, dominant-negative c-Jun reduced the increased expression of β-catenin and the decreased expression of amylase during culture. These results show that MAPK/c-Jun/AP-1 pathway plays an important role in pancreatic acinar cell dedifferentiation and proliferation in culture. Monolayer culture can serve as a model to study acinar cell proliferation similar to regeneration after pancreatitis in vivo.

Published

2012

30. Developmental programming of neonatal pancreatic β-cells by a maternal low-protein diet in rats involves a switch from proliferation to differentiation.

Author

Rodríguez-Trejo A, Ortiz-López MG, Zambrano E, Granados-Silvestre Mde L, Méndez C, Blondeau B, Bréant B, Nathanielsz PW, and Menjivar M

Subjects

Animals, Animals, Newborn, Blood Glucose metabolism, Body Weight drug effects, Cell Separation, Diet, Eating drug effects, Female, Fluorescent Antibody Technique, Gene Expression Regulation drug effects, Immunohistochemistry, Insulin blood, Male, Organ Size drug effects, Pancreas cytology, Pancreas drug effects, Pancreas growth & development, Pregnancy, Rats, Rats, Wistar, Transcription Factors biosynthesis, Transcription Factors genetics, Cell Differentiation drug effects, Cell Proliferation drug effects, Diet, Protein-Restricted, Insulin-Secreting Cells drug effects

Abstract

Maternal low-protein diets (LP) impair pancreatic β-cell development, resulting in later-life failure and susceptibility to type 2 diabetes (T2D). We hypothesized that intrauterine and/or postnatal developmental programming seen in this situation involve altered β-cell structure and relative time course of expression of genes critical to β-cell differentiation and growth. Pregnant Wistar rats were fed either control (C) 20% or restricted (R) 6% protein diets during pregnancy (1st letter) and/or lactation (2nd letter) in four groups: CC, RR, RC, and CR. At postnatal days 7 and 21, we measured male offspring β-cell fraction, mass, proliferation, aggregate number, and size as well as mRNA level for 13 key genes regulating β-cell development and function in isolated islets. Compared with CC, pre- and postnatal LP (RR) decreased β-cell fraction, mass, proliferation, aggregate size, and number and increased Hnf1a, Hnf4a, Pdx1, Isl1, Rfx6, and Slc2a2 mRNA levels. LP only in pregnancy (RC) also decreased β-cell fraction, mass, proliferation, aggregate size, and number and increased Hnf1a, Hnf4a, Pdx1, Rfx6, and Ins mRNA levels. Postnatal LP offspring (CR) showed decreased β-cell mass but increased β-cell fraction, aggregate number, and Hnf1a, Hnf4a, Rfx6, and Slc2a2 mRNA levels. We conclude that LP in pregnancy sets the trajectory of postnatal β-cell growth and differentiation, whereas LP in lactation has smaller effects. We propose that LP promotes differentiation through upregulation of transcription factors that stimulate differentiation at the expense of proliferation. This results in a decreased β-cell reserve, which can contribute to later-life predisposition to T2D.

Published

2012

31. Pharmacological and genetic inhibition of calcineurin protects against carbachol-induced pathological zymogen activation and acinar cell injury.

Author

Muili KA, Ahmad M, Orabi AI, Mahmood SM, Shah AU, Molkentin JD, and Husain SZ

Subjects

Acinar Cells enzymology, Amylases metabolism, Animals, Calcineurin physiology, Cholecystokinin pharmacology, Chymotrypsin metabolism, DNA genetics, Dose-Response Relationship, Drug, Enzyme Activation drug effects, Enzyme Activation genetics, Female, Genotype, L-Lactate Dehydrogenase metabolism, Male, Mice, Mice, Knockout, Pancreas cytology, Pancreas drug effects, Pancreas enzymology, Phosphoric Monoester Hydrolases metabolism, Real-Time Polymerase Chain Reaction, Trypsin metabolism, Acinar Cells drug effects, Calcineurin genetics, Calcineurin Inhibitors, Carbachol antagonists & inhibitors, Carbachol toxicity, Enzyme Precursors metabolism, Nicotinic Agonists toxicity

Abstract

Acute pancreatitis is a major health burden for which there are currently no targeted therapies. Premature activation of digestive proenzymes, or zymogens, within the pancreatic acinar cell is an early and critical event in this disease. A high-amplitude, sustained rise in acinar cell Ca(2+) is required for zymogen activation. We previously showed in a cholecystokinin-induced pancreatitis model that a potential target of this aberrant Ca(2+) signaling is the Ca(2+)-activated phosphatase calcineurin (Cn). However, in this study, we examined the role of Cn on both zymogen activation and injury, in the clinically relevant condition of neurogenic stimulation (by giving the acetylcholine analog carbachol) using three different Cn inhibitors or Cn-deficient acinar cells. In freshly isolated mouse acinar cells, pretreatment with FK506, calcineurin inhibitory peptide (CiP), or cyclosporine (CsA) blocked intra-acinar zymogen activation (n = 3; P < 0.05). The Cn inhibitors also reduced leakage of lactate dehydrogenase (LDH) by 79%, 62%, and 63%, respectively (n = 3; P < 0.05). Of the various Cn isoforms, the β-isoform of the catalytic A subunit (CnAβ) was strongly expressed in mouse acinar cells. For this reason, we obtained acinar cells from CnAβ-deficient mice (CnAβ-/-) and observed an 84% and 50% reduction in trypsin and chymotrypsin activation, respectively, compared with wild-type controls (n = 3; P < 0.05). LDH release in the CnAβ-deficient cells was reduced by 50% (n = 2; P < 0.05). The CnAβ-deficient cells were also protected against zymogen activation and cell injury induced by the cholecystokinin analog caerulein. Importantly, amylase secretion was generally not affected by either the Cn inhibitors or Cn deficiency. These data provide both pharmacological and genetic evidence that implicates Cn in intra-acinar zymogen activation and cell injury during pancreatitis.

Published

2012

32. Acute activation of central GLP-1 receptors enhances hepatic insulin action and insulin secretion in high-fat-fed, insulin resistant mice.

Author

Burmeister MA, Ferre T, Ayala JE, King EM, Holt RM, and Ayala JE

Subjects

AMP-Activated Protein Kinases metabolism, Animals, Diet, High-Fat adverse effects, Glucagon-Like Peptide 1 administration & dosage, Glucagon-Like Peptide-1 Receptor, Glucose Clamp Technique, Glycogenolysis drug effects, Hypothalamus drug effects, Hypothalamus enzymology, Infusions, Intraventricular, Insulin blood, Insulin Secretion, Lipid Metabolism drug effects, Liver drug effects, Liver enzymology, Male, Mice, Mice, Inbred C57BL, Nerve Tissue Proteins agonists, Nerve Tissue Proteins antagonists & inhibitors, Nerve Tissue Proteins metabolism, Neurons drug effects, Neurons enzymology, Neurons metabolism, Organ Specificity, Pancreas drug effects, Proto-Oncogene Proteins c-akt metabolism, Receptors, Glucagon agonists, Receptors, Glucagon antagonists & inhibitors, Signal Transduction drug effects, Glucagon-Like Peptide 1 metabolism, Hypothalamus metabolism, Insulin metabolism, Insulin Resistance, Liver metabolism, Pancreas metabolism, Receptors, Glucagon metabolism

Abstract

Glucagon-like peptide-1 (GLP-1) receptor knockout (Glp1r(-/-)) mice exhibit impaired hepatic insulin action. High fat (HF)-fed Glp1r(-/-) mice exhibit improved, rather than the expected impaired, hepatic insulin action. This is due to decreased lipogenic gene expression and triglyceride accumulation. The present studies overcome these secondary adaptations by acutely modulating GLP-1R action in HF-fed wild-type mice. The central GLP-1R was targeted given its role as a regulator of hepatic insulin action. We hypothesized that acute inhibition of the central GLP-1R impairs hepatic insulin action beyond the effects of HF feeding. We further hypothesized that activation of the central GLP-1R improves hepatic insulin action in HF-fed mice. Insulin action was assessed in conscious, unrestrained mice using the hyperinsulinemic euglycemic clamp. Mice received intracerebroventricular (icv) infusions of artificial cerebrospinal fluid, GLP-1, or the GLP-1R antagonist exendin-9 (Ex-9) during the clamp. Intracerebroventricular Ex-9 impaired the suppression of hepatic glucose production by insulin, whereas icv GLP-1 improved it. Neither treatment affected tissue glucose uptake. Intracerebroventricular GLP-1 enhanced activation of hepatic Akt and suppressed hypothalamic AMP-activated protein kinase. Central GLP-1R activation resulted in lower hepatic triglyceride levels but did not affect muscle, white adipose tissue, or plasma triglyceride levels during hyperinsulinemia. In response to oral but not intravenous glucose challenges, activation of the central GLP-1R improved glucose tolerance. This was associated with higher insulin levels. Inhibition of the central GLP-1R had no effect on oral or intravenous glucose tolerance. These results show that inhibition of the central GLP-1R deteriorates hepatic insulin action in HF-fed mice but does not affect whole body glucose homeostasis. Contrasting this, activation of the central GLP-1R improves glucose homeostasis in HF-fed mice by increasing insulin levels and enhancing hepatic insulin action.

Published

2012

33. Profiling CCK-mediated pancreatic growth: the dynamic genetic program and the role of STATs as potential regulators.

Author

Gurda GT, Wang JY, Guo L, Ernst SA, and Williams JA

Subjects

Animals, Cholecystokinin metabolism, Cluster Analysis, Fasting metabolism, Fasting physiology, Gene Expression Profiling, Gene Regulatory Networks, Male, Mice, Mice, Inbred ICR, Microarray Analysis, Pancreas metabolism, STAT Transcription Factors metabolism, Signal Transduction drug effects, Signal Transduction genetics, Time Factors, Cholecystokinin pharmacology, Gene Expression Regulation drug effects, Gene Expression Regulation genetics, Pancreas drug effects, Pancreas growth & development, STAT Transcription Factors physiology

Abstract

Feeding mice with protease inhibitor (PI) leads to increased endogenous cholecystokinin (CCK) release and results in pancreatic growth. This adaptive response requires calcineurin (CN)-NFAT and AKT-mTOR pathways, but the genes involved, the dynamics of their expression, and other regulatory pathways remain unknown. Here, we examined the early (1-8 h) transcriptional program that underlies pancreatic growth. We found 314 upregulated and 219 downregulated genes with diverse temporal and functional profiles. Several new identifications include the following: stress response genes Gdf15 and Txnip, metabolic mediators Pitpnc1 and Hmges2, as well as components of growth factor response Fgf21, Atf3, and Egr1. The genes fell into seven self-organizing clusters, each with a distinct pattern of expression; a representative gene within each of the upregulated clusters (Egr1, Gadd45b, Rgs2, and Serpinb1a) was validated by qRT-PCR. Genes up at any point throughout the time course and CN-dependent genes were subjected to further bioinformatics-based networking and promoter analysis, yielding STATs as potential transcriptional regulators. As shown by PCR, qPCR, and Western blots, the active phospho-form of STAT3 and the Jak-STAT feedback inhibitor Socs2 were both increased throughout early pancreatic growth. Moreover, immunohistochemistry showed a CCK-dependent and acinar cell-specific increase in nuclear localization of p-STAT3, with >75% nuclear occupancy in PI-fed mice vs. <0.1% in controls. Thus, the study identified novel genes likely to be important for CCK-driven pancreatic growth, characterized and biologically validated the dynamic pattern of their expression and investigated STAT-Socs signaling as a new player in this trophic response.

Published

2012

34. Sympathetic and cardiovascular responses to venous distension in an occluded limb.

Author

Cui J, Leuenberger UA, Gao Z, and Sinoway LI

Subjects

Adult, Arm blood supply, Dose-Response Relationship, Drug, Drug Administration Schedule, Female, Humans, Liver drug effects, Liver pathology, Male, Muscle, Skeletal physiology, Pancreas drug effects, Pancreas pathology, Respiration, Sodium Chloride administration & dosage, Sodium Chloride pharmacology, Vasoconstriction, Blood Pressure physiology, Heart Rate physiology, Muscle, Skeletal innervation, Sympathetic Nervous System physiology, Vasodilation physiology

Abstract

We recently showed that a fixed volume (i.e., 40 ml) of saline infused into the venous circulation of an arterially occluded vascular bed increases muscle sympathetic nerve activity (MSNA) and blood pressure. In the present report, we hypothesized that the volume and rate of infusion would influence the magnitude of the sympathetic response. Blood pressure, heart rate, and MSNA were assessed in 13 young healthy subjects during forearm saline infusions (arrested circulation). The effects of different volumes of saline (i.e., 2%, 3%, 4%, or 5% forearm volume at 30 ml/min) and different rates of infusion (i.e., 5% forearm volume at 10, 20, or 30 ml/min) were evaluated. MSNA and blood pressure responses were linked with the infusion volume. Infusion of 5% of forearm volume evoked greater MSNA responses than did infusion of 2% of forearm volume (Δ11.6 ± 1.9 vs. Δ3.1 ± 1.8 bursts/min and Δ332 ± 105 vs. Δ38 ± 32 units/min, all P < 0.05). Moreover, greater MSNA responses were evoked by saline infusion at 30 ml/min than 10 ml/min (P < 0.05). Sonographic measurements confirmed that the saline infusions induced forearm venous distension. The results suggest that volume and rate of saline infusion are important factors in evoking sympathetic activation. We postulate that venous distension contributes to cardiovascular autonomic adjustment in humans.

Published

2011

35. Assessment of the protective effects of oral tocotrienols in arginine chronic-like pancreatitis.

Author

González AM, Garcia T, Samper E, Rickmann M, Vaquero EC, and Molero X

Subjects

Administration, Oral, Animals, Arginine, Disease Models, Animal, Disease Progression, Male, Pancreas drug effects, Pancreatitis, Chronic chemically induced, Pancreatitis, Chronic pathology, Rats, Rats, Wistar, Tocotrienols administration & dosage, Treatment Outcome, Pancreas pathology, Pancreatitis, Chronic drug therapy, Tocotrienols therapeutic use

Abstract

Tocotrienols exhibit anti-inflammatory properties over macrophages and promote cytotoxicity in activated pancreatic stellate cells, suggesting that they may limit chronic pancreatitis progression. We aimed to quantitate the effect of oral tocotrienols on a rat model of chronic pancreatic injury. Chronic-like pancreatitis was induced by repeated arginine pancreatitis. Palm oil tocotrienol-rich fraction (TRF) was given by gavage before and after pancreatitis inductions. Amylase and hydroxyproline were determined in pancreatic homogenates; collagen, fibronectin, α-smooth muscle actin (SMA), glial fibrillary acidic protein (GFAP), and phosphorylated Smad3 were assessed by Western blotting. Transforming growth factor (TGF)-β1 was measured in plasma. Morphological assessment included light microscopy, fibrosis area fraction, and collagen network fractal analysis. Arginine pancreatitis induced pancreatic atrophy and increased hydroxyproline that ameliorated after TRF. Arginine increased TGF-β1 (185 ± 40 vs. 15 ± 2 ng/ml; P <0.01) that was blunted by TRF (53 ± 19; P < 0.01). TRF reduced protease and Smad3 activation, collagen, and fibronectin. α-SMA increased and GFAP diminished in arginine pancreatitis, consistent with long-term stellate cell activation, and TRF reverted these changes to basal. Arginine pancreatitis increased fibrosis area fraction (4.5 ± 0.3% vs. 0.2 ± 0.2%), collagen network complexity (fractal dimension 1.52 ± 0.03 vs. 1.42 ± 0.01; P < 0.001), and inhomogeneity (lacunarity 0.63 ± 0.03 vs. 0.40 ± 0.02; P < 0.001), which were all reduced by TRF (1.3 ± 0.4%, 1.43 ± 0.02%, and 0.51 ± 0.03%, respectively; P < 0.01). Best correlation coefficients were obtained when comparing fibrosis area fraction with lacunarity (r = 0.88) and both parameters with pancreatic weight (r = -0.91 and -0.79, respectively). TRF administered only before pancreatitis best, but not fully, recapitulated the beneficial effects of TRF. Tocotrienols improve quantitative measures of chronic pancreatic damage. They may be of benefit in human chronic pancreatitis.

Published

2011

36. Tauroursodeoxycholic acid reduces endoplasmic reticulum stress, acinar cell damage, and systemic inflammation in acute pancreatitis.

Author

Seyhun E, Malo A, Schäfer C, Moskaluk CA, Hoffmann RT, Göke B, and Kubisch CH

Subjects

Acinar Cells metabolism, Acinar Cells pathology, Animals, Ceruletide, Endoplasmic Reticulum drug effects, Endoplasmic Reticulum metabolism, Endoplasmic Reticulum physiology, Inflammation metabolism, Inflammation pathology, Male, Pancreas drug effects, Pancreas metabolism, Pancreas pathology, Pancreatitis chemically induced, Pancreatitis metabolism, Pancreatitis pathology, Rats, Rats, Wistar, Taurochenodeoxycholic Acid pharmacology, Acinar Cells drug effects, Endoplasmic Reticulum Stress drug effects, Inflammation drug therapy, Pancreatitis drug therapy, Taurochenodeoxycholic Acid therapeutic use, Unfolded Protein Response drug effects

Abstract

In acute pancreatitis, endoplasmic reticulum (ER) stress prompts an accumulation of malfolded proteins inside the ER, initiating the unfolded protein response (UPR). Because the ER chaperone tauroursodeoxycholic acid (TUDCA) is known to inhibit the UPR in vitro, this study examined the in vivo effects of TUDCA in an acute experimental pancreatitis model. Acute pancreatitis was induced in Wistar rats using caerulein, with or without prior TUDCA treatment. UPR components were analyzed, including chaperone binding protein (BiP), phosphorylated protein kinase-like ER kinase (pPERK), X-box binding protein (XBP)-1, phosphorylated c-Jun NH(2)-terminal kinase (pJNK), CCAAT/enhancer binding protein homologues protein, and caspase 12 and 3 activation. In addition, pancreatitis biomarkers were measured, such as serum amylase, trypsin activation, edema formation, histology, and the inflammatory reaction in pancreatic and lung tissue. TUDCA treatment reduced intracellular trypsin activation, edema formation, and cell damage, while leaving amylase levels unaltered. The activation of myeloperoxidase was clearly reduced in pancreas and lung. Furthermore, TUDCA prevented caerulein-induced BiP upregulation, reduced XBP-1 splicing, and caspase 12 and 3 activation. It accelerated the downregulation of pJNK. In controls without pancreatitis, TUDCA showed cytoprotective effects including pPERK signaling and activation of downstream targets. We concluded that ER stress responses activated in acute pancreatitis are grossly attenuated by TUDCA. The chaperone reduced the UPR and inhibited ER stress-associated proapoptotic pathways. TUDCA has a cytoprotective potential in the exocrine pancreas. These data hint at new perspectives for an employment of chemical chaperones, such as TUDCA, in prevention of acute pancreatitis.

Published

2011

37. COX-2 is not required for the development of murine chronic pancreatitis.

Author

Silva A, Weber A, Bain M, Reding T, Heikenwalder M, Sonda S, and Graf R

Subjects

Actins genetics, Actins metabolism, Age Factors, Animals, Ceruletide, Collagen genetics, Collagen metabolism, Cyclooxygenase 2 deficiency, Cyclooxygenase 2 genetics, Cyclooxygenase 2 Inhibitors pharmacology, Disease Models, Animal, Gene Expression Regulation, Lactones pharmacology, Mice, Mice, Knockout, Pancreas drug effects, Pancreas pathology, Pancreatitis, Chronic chemically induced, Pancreatitis, Chronic genetics, Pancreatitis, Chronic pathology, Pancreatitis, Chronic prevention & control, Species Specificity, Sulfones pharmacology, Time Factors, Transforming Growth Factor beta genetics, Transforming Growth Factor beta metabolism, Cyclooxygenase 2 metabolism, Pancreas enzymology, Pancreatitis, Chronic enzymology

Abstract

Chronic pancreatitis is a severe inflammation of the pancreas associated with destruction of the parenchyma, fibrosis, and persistent abdominal pain. Cyclooxygenase-2 (COX-2) and COX-2-derived prostaglandins, key mediators of the inflammatory response, are elevated in patients with chronic pancreatitis. Previous studies investigated COX-2 as a therapeutic target. These reports showed a reduced pathology in COX-2-deficient mice with a better outcome. Here we compared the role of COX-2 in acute and chronic pancreatic inflammation using the same COX-2(-/-) mouse model of cerulein-induced pancreatitis. In a setting of acute pancreatitis, juvenile COX-2(-/-) mice exhibited a reduced histopathological score compared with wild-type littermates; on the contrary, adult mice did not show any difference in the development of the disease. Similarly, in a setting of chronic pancreatitis induced over a period of 4 wk, adult mice of the two strains showed comparable histological score and collagen deposition. However, the abundance of mRNAs coding for profibrotic genes, such as collagen, α-smooth muscle actin, and transforming growth factor-β was consistently lower in COX-2(-/-) mice. In addition, comparable histological scores and collagen deposition were observed in wild-type mice treated with a COX-2 inhibitor. We conclude that, in contrast to what was observed in the rat pancreatitis models, COX-2 has a limited and age-dependent effect on inflammatory processes in the mouse pancreas. These results suggest that COX-2 modulates the inflammatory process during the development of pancreatitis in a species-specific manner. Thus the pathophysiological roles of COX-2 and its therapeutic implications in patients with pancreatitis should be reexamined.

Published

2011

38. Serine proteases mediate inflammatory pain in acute pancreatitis.

Author

Ceppa EP, Lyo V, Grady EF, Knecht W, Grahn S, Peterson A, Bunnett NW, Kirkwood KS, and Cattaruzza F

Subjects

Abdominal Pain enzymology, Abdominal Pain pathology, Abdominal Pain prevention & control, Acute Disease, Amylases blood, Analgesics therapeutic use, Animals, Azetidines pharmacology, Benzylamines pharmacology, Ceruletide, Disease Models, Animal, Enteropeptidase metabolism, Enzyme Activation, Humans, Kinetics, Male, Pain Measurement, Pancreas drug effects, Pancreas pathology, Pancreatitis chemically induced, Pancreatitis drug therapy, Pancreatitis enzymology, Pancreatitis pathology, Peroxidase blood, Proto-Oncogene Proteins c-fos metabolism, Rats, Rats, Sprague-Dawley, Receptor, PAR-2 metabolism, Recombinant Proteins metabolism, Soybean Proteins pharmacology, Spinal Cord enzymology, Trypsin Inhibitors pharmacology, Abdominal Pain etiology, Pancreas enzymology, Pancreatitis complications, Signal Transduction drug effects, Trypsin metabolism

Abstract

Acute pancreatitis is a life-threatening inflammatory disease characterized by abdominal pain of unknown etiology. Trypsin, a key mediator of pancreatitis, causes inflammation and pain by activating protease-activated receptor 2 (PAR(2)), but the isoforms of trypsin that cause pancreatitis and pancreatic pain are unknown. We hypothesized that human trypsin IV and rat P23, which activate PAR(2) and are resistant to pancreatic trypsin inhibitors, contribute to pancreatic inflammation and pain. Injections of a subinflammatory dose of exogenous trypsin increased c-Fos immunoreactivity, indicative of spinal nociceptive activation, but did not cause inflammation, as assessed by measuring serum amylase and myeloperoxidase activity and by histology. The same dose of trypsin IV and P23 increased some inflammatory end points and caused a more robust effect on nociception, which was blocked by melagatran, a trypsin inhibitor that also inhibits polypeptide-resistant trypsin isoforms. To determine the contribution of endogenous activation of trypsin and its minor isoforms, recombinant enterokinase (ENK), which activates trypsins in the duodenum, was administered into the pancreas. Intraductal ENK caused nociception and inflammation that were diminished by polypeptide inhibitors, including soybean trypsin inhibitor and a specific trypsin inhibitor (type I-P), and by melagatran. Finally, the secretagogue cerulein induced pancreatic nociceptive activation and nocifensive behavior that were reversed by melagatran. Thus trypsin and its minor isoforms mediate pancreatic pain and inflammation. In particular, the inhibitor-resistant isoforms trypsin IV and P23 may be important in mediating prolonged pancreatic inflammatory pain in pancreatitis. Our results suggest that inhibitors of these isoforms could be novel therapies for pancreatitis pain.

Published

2011

39. Characterization of glucose-insulin responsiveness and impact of fetal number and sex difference on insulin response in the sheep fetus.

Author

Green AS, Macko AR, Rozance PJ, Yates DT, Chen X, Hay WW Jr, and Limesand SW

Subjects

Animals, Body Weight drug effects, Dose-Response Relationship, Drug, Female, Glucose pharmacology, Glucose Clamp Technique, Insulin-Secreting Cells drug effects, Insulin-Secreting Cells metabolism, Pancreas anatomy & histology, Pancreas drug effects, Pregnancy, Sex Characteristics, Sheep, Domestic, Stimulation, Chemical, Blood Glucose metabolism, Fetus physiology, Hypoglycemic Agents pharmacology, Insulin blood, Insulin pharmacology

Abstract

GSIS is often measured in the sheep fetus by a square-wave hyperglycemic clamp, but maximal β-cell responsiveness and effects of fetal number and sex difference have not been fully evaluated. We determined the dose-response curve for GSIS in fetal sheep (0.9 of gestation) by increasing plasma glucose from euglycemia in a stepwise fashion. The glucose-insulin response was best fit by curvilinear third-order polynomial equations for singletons (y = 0.018x(3) - 0.26x(2) + 1.2x - 0.64) and twins (y = -0.012x(3) + 0.043x(2) + 0.40x - 0.16). In singles, maximal insulin secretion was achieved at 3.4 ± 0.2 mmol/l glucose but began to plateau after 2.4 ± 0.2 mmol/l glucose (90% of maximum), whereas the maximum for twins was reached at 4.8 ± 0.4 mmol/l glucose. In twin (n = 18) and singleton (n = 49) fetuses, GSIS was determined with a square-wave hyperglycemic clamp >2.4 mmol/l glucose. Twins had a lower basal glucose concentration, and plasma insulin concentrations were 59 (P < 0.01) and 43% (P < 0.05) lower in twins than singletons during the euglycemic and hyperglycemic periods, respectively. The basal glucose/insulin ratio was approximately doubled in twins vs. singles (P < 0.001), indicating greater insulin sensitivity. In a separate cohort of fetuses, twins (n = 8) had lower body weight (P < 0.05) and β-cell mass (P < 0.01) than singleton fetuses (n = 7) as a result of smaller pancreata (P < 0.01) and a positive correlation (P < 0.05) between insulin immunopositive area and fetal weight (P < 0.05). No effects of sex difference on GSIS or β-cell mass were observed. These findings indicate that insulin secretion is less responsive to physiological glucose concentrations in twins, due in part to less β-cell mass.

Published

2011

40. Exenatide does not evoke pancreatitis and attenuates chemically induced pancreatitis in normal and diabetic rodents.

Author

Tatarkiewicz K, Smith PA, Sablan EJ, Polizzi CJ, Aumann DE, Villescaz C, Hargrove DM, Gedulin BR, Lu MG, Adams L, Whisenant T, Roy D, and Parkes DG

Subjects

Analysis of Variance, Animals, Area Under Curve, Cytokines metabolism, Diabetes Mellitus, Experimental metabolism, Diabetes Mellitus, Experimental pathology, Exenatide, Hypoglycemic Agents pharmacology, Hypoglycemic Agents therapeutic use, Mice, Pancreas metabolism, Pancreas pathology, Pancreatitis chemically induced, Pancreatitis complications, Pancreatitis pathology, Peptides therapeutic use, Rats, Rats, Sprague-Dawley, Venoms therapeutic use, Diabetes Mellitus, Experimental complications, Pancreas drug effects, Pancreatitis drug therapy, Peptides pharmacology, Venoms pharmacology

Abstract

The risk of developing pancreatitis is elevated in type 2 diabetes and obesity. Cases of pancreatitis have been reported in type 2 diabetes patients treated with GLP-1 (GLP-1R) receptor agonists. To examine whether the GLP-1R agonist exenatide potentially induces or modulates pancreatitis, the effect of exenatide was evaluated in normal or diabetic rodents. Normal and diabetic rats received a single exenatide dose (0.072, 0.24, and 0.72 nmol/kg) or vehicle. Diabetic ob/ob or HF-STZ mice were infused with exenatide (1.2 and 7.2 nmol·kg(-1)·day(-1)) or vehicle for 4 wk. Post-exenatide treatment, pancreatitis was induced with caerulein (CRN) or sodium taurocholate (ST), and changes in plasma amylase and lipase were measured. In ob/ob mice, plasma cytokines (IL-1β, IL-2, IL-6, MCP-1, IFNγ, and TNFα) and pancreatitis-associated genes were assessed. Pancreata were weighed and examined histologically. Exenatide treatment alone did not modify plasma amylase or lipase in any models tested. Exenatide attenuated CRN-induced release of amylase and lipase in normal rats and ob/ob mice but did not modify the response to ST infusion. Plasma cytokines and pancreatic weight were unaffected by exenatide. Exenatide upregulated Reg3b but not Il6, Ccl2, Nfkb1, or Vamp8 expression. Histological analysis revealed that the highest doses of exenatide decreased CRN- or ST-induced acute inflammation, vacuolation, and acinar single cell necrosis in mice and rats, respectively. Ductal cell proliferation rates were low and similar across all groups of ob/ob mice. In conclusion, exenatide did not modify plasma amylase and lipase concentrations in rodents without pancreatitis and improved chemically induced pancreatitis in normal and diabetic rodents.

Published

2010

41. Tauroursodeoxycholic acid reduces endoplasmic reticulum stress, trypsin activation, and acinar cell apoptosis while increasing secretion in rat pancreatic acini.

Author

Malo A, Krüger B, Seyhun E, Schäfer C, Hoffmann RT, Göke B, and Kubisch CH

Subjects

Amylases metabolism, Animals, Apoptosis drug effects, Calcium Signaling drug effects, Cathepsin B metabolism, Cholagogues and Choleretics pharmacology, Dose-Response Relationship, Drug, Endoplasmic Reticulum physiology, Enzyme Activation, Pancreas metabolism, Rats, Stress, Physiological, Endoplasmic Reticulum drug effects, Pancreas cytology, Pancreas drug effects, Taurochenodeoxycholic Acid pharmacology, Trypsin metabolism

Abstract

Endoplasmic reticulum (ER) stress leads to accumulation of un- or misfolded proteins inside the ER and initiates the unfolded protein response (UPR). Several UPR components are physiologically involved in pancreatic development and are pathophysiologically activated during acute pancreatitis. However, the exact role of ER stress in exocrine pancreatic acini is mainly unclear. The present study examined the effects of tauroursodeoxycholic acid (TUDCA), a known ER chaperone, on acinar function and UPR components. Isolated rat pancreatic acini were stimulated by increasing concentrations of cholecystokinin (CCK-8) with or without preincubation of TUDCA. UPR components were analyzed, including chaperone binding protein (BiP), protein kinase-like ER kinase (PERK), X-box binding protein (XBP)-1, c-Jun NH(2)-terminal kinase (JNK), CCAAT/enhancer binding protein homologues protein (CHOP), caspase 3 activation, and apoptosis. In addition, TUDCA effects were measured on amylase secretion, calcium signaling, trypsin, and cathepsin B activation. TUDCA preincubation led to a significant increase in amylase secretion after CCK-8 stimulation, a 50% reduction of intracellular trypsin activation, and reduced cathepsin B activity, although the effects for cathepsin B were not statistical significant. Furthermore, TUDCA prevented the CCK-8-induced BiP upregulation, diminished PERK and JNK phosphorylation, and prohibited the expression of CHOP, caspase 3 activation and apoptosis. XBP-1 splicing was not altered. ER stress response mechanisms are activated in pancreatic inflammation. Chemical chaperones enhance enzyme secretion of pancreatic acini, reduce ER stress responses, and attenuate ER stress-associated apoptosis. These data hint new perspectives for an employment of chemical chaperones in the therapy of acute pancreatitis.

Published

2010

42. Transient receptor potential ion channels V4 and A1 contribute to pancreatitis pain in mice.

Author

Ceppa E, Cattaruzza F, Lyo V, Amadesi S, Pelayo JC, Poole DP, Vaksman N, Liedtke W, Cohen DM, Grady EF, Bunnett NW, and Kirkwood KS

Subjects

Aldehydes toxicity, Animals, Cysteine Proteinase Inhibitors toxicity, Female, Ganglia, Spinal physiology, Gene Expression Regulation drug effects, Gene Expression Regulation physiology, Irritants toxicity, Male, Mice, Mice, Knockout, Mustard Plant toxicity, Nociceptors physiology, Pain etiology, Pancreas drug effects, Pancreas innervation, Pancreas pathology, Pancreatitis chemically induced, Pancreatitis metabolism, Plant Oils toxicity, Spinal Cord metabolism, TRPA1 Cation Channel, TRPV Cation Channels agonists, TRPV Cation Channels genetics, Transient Receptor Potential Channels agonists, Transient Receptor Potential Channels genetics, Pain metabolism, Pancreatitis complications, TRPV Cation Channels metabolism, Transient Receptor Potential Channels metabolism

Abstract

The mechanisms of pancreatic pain, a cardinal symptom of pancreatitis, are unknown. Proinflammatory agents that activate transient receptor potential (TRP) channels in nociceptive neurons can cause neurogenic inflammation and pain. We report a major role for TRPV4, which detects osmotic pressure and arachidonic acid metabolites, and TRPA1, which responds to 4-hydroxynonenal and cyclopentenone prostaglandins, in pancreatic inflammation and pain in mice. Immunoreactive TRPV4 and TRPA1 were detected in pancreatic nerve fibers and in dorsal root ganglia neurons innervating the pancreas, which were identified by retrograde tracing. Agonists of TRPV4 and TRPA1 increased intracellular Ca(2+) concentration ([Ca(2+)](i)) in these neurons in culture, and neurons also responded to the TRPV1 agonist capsaicin and are thus nociceptors. Intraductal injection of TRPV4 and TRPA1 agonists increased c-Fos expression in spinal neurons, indicative of nociceptor activation, and intraductal TRPA1 agonists also caused pancreatic inflammation. The effects of TRPV4 and TRPA1 agonists on [Ca(2+)](i), pain and inflammation were markedly diminished or abolished in trpv4 and trpa1 knockout mice. The secretagogue cerulein induced pancreatitis, c-Fos expression in spinal neurons, and pain behavior in wild-type mice. Deletion of trpv4 or trpa1 suppressed c-Fos expression and pain behavior, and deletion of trpa1 attenuated pancreatitis. Thus TRPV4 and TRPA1 contribute to pancreatic pain, and TRPA1 also mediates pancreatic inflammation. Our results provide new information about the contributions of TRPV4 and TRPA1 to inflammatory pain and suggest that channel antagonists are an effective therapy for pancreatitis, when multiple proinflammatory agents are generated that can activate and sensitize these channels.

Published

2010

43. Intravenous or luminal amino acids are insufficient to maintain pancreatic growth and digestive enzyme expression in the absence of intact dietary protein.

Author

Baumler MD, Koopmann MC, Thomas DD, Ney DM, and Groblewski GE

Subjects

Adaptation, Physiological drug effects, Administration, Oral, Amylases metabolism, Animals, Atrophy, Chymotrypsinogen metabolism, Diet, Protein-Restricted, Growth, Injections, Intravenous, Intestinal Mucosa drug effects, Intestine, Small drug effects, Lipase metabolism, Male, Pancreas drug effects, Pancreas pathology, Parenteral Nutrition, Total, Rats, Rats, Sprague-Dawley, Trypsinogen metabolism, Amino Acids administration & dosage, Dietary Proteins metabolism, Pancreas physiopathology, Protein Deficiency physiopathology

Abstract

We previously reported that rats receiving total parenteral nutrition (TPN) undergo significant pancreatic atrophy characterized by reduced total protein and digestive enzyme expression due to a lack of intestinal stimulation by nutrients (Baumler MD, Nelson DW, Ney DM, Groblewski GE. Am J Physiol Gastrointest Liver Physiol 292: G857-G866, 2007). Essentially identical results were recently reported in mice fed protein-free diets (Crozier SJ, D'Alecy LG, Ernst SA, Ginsburg LE, Williams JA. Gastroenterology 137: 1093-1101, 2009), provoking the question of whether reductions in pancreatic protein and digestive enzyme expression could be prevented by providing amino acids orally or by intravenous (IV) infusion while maintaining intestinal stimulation with fat and carbohydrate. Controlled studies were conducted in rats with IV catheters including orally fed/saline infusion or TPN-fed control rats compared with rats fed a protein-free diet, oral amino acid, or IV amino acid feeding, all with oral carbohydrate and fat. Interestingly, neither oral nor IV amino acids were sufficient to prevent the pancreatic atrophy seen for TPN controls or protein-free diets. Oral and IV amino acids partially attenuated the 75-90% reductions in pancreatic amylase and trypsinogen expression; however, values remained 50% lower than orally fed control rats. Lipase expression was more modestly reduced by a lack of dietary protein but did respond to IV amino acids. In comparison, chymotrypsinogen expression was induced nearly twofold in TPN animals but was not altered in other experimental groups compared with oral control animals. In contrast to pancreas, protein-free diets had no detectable effects on jejunal mucosal villus height, total mass, protein, DNA, or sucrase activity. These data underscore that, in the rat, intact dietary protein is essential in maintaining pancreatic growth and digestive enzyme adaptation but has surprisingly little effect on small intestinal mucosa.

Published

2010

44. Angiotensin II signaling through the AT1a and AT1b receptors does not have a role in the development of cerulein-induced chronic pancreatitis in the mouse.

Author

Ulmasov B, Xu Z, Talkad V, Oshima K, and Neuschwander-Tetri BA

Subjects

Actins metabolism, Angiotensin II Type 1 Receptor Blockers pharmacology, Animals, Atrophy, Ceruletide, Collagen metabolism, Disease Models, Animal, Fibrosis, Losartan pharmacology, Mice, Mice, Inbred C57BL, Mice, Knockout, Pancreas drug effects, Pancreas pathology, Pancreatitis, Chronic chemically induced, Pancreatitis, Chronic genetics, Pancreatitis, Chronic pathology, Pancreatitis, Chronic prevention & control, RNA, Messenger metabolism, Receptor, Angiotensin, Type 1 deficiency, Receptor, Angiotensin, Type 1 drug effects, Receptor, Angiotensin, Type 1 genetics, Severity of Illness Index, Angiotensin II metabolism, Pancreas metabolism, Pancreatitis, Chronic metabolism, Receptor, Angiotensin, Type 1 metabolism, Renin-Angiotensin System drug effects, Renin-Angiotensin System genetics, Signal Transduction drug effects

Abstract

The intraorgan renin-angiotensin system (RAS) plays an important role in the pathophysiology of a variety of diseases and has been implicated in fibrogenesis. The role of RAS in the development of chronic pancreatitis is not well established. The blockade of RAS in rat models with angiotensin-converting enzyme inhibitors (ACEi) or angiotensin receptor 1 (AT1) blockers (ARBs) mostly have reduced pancreatic inflammation and fibrosis with a few exceptions. At the same time, the use of ACEi and ARBs in humans is associated with a modest risk of acute pancreatitis. The aim of this study was to elucidate the effect of the AT1 signaling pathway in the development of pancreatitis using AT1a- and AT1b-deficient mice as well as the ARB losartan. Chronic pancreatitis was induced by repetitive cerulein administration in C57BL/6J wild-type (WT) and AT1a- and AT1b-deficient mice (AT1a-/- and AT1b-/-), and pancreatic injury was assessed at day 10. Pancreatic weight of cerulein treated groups was significantly reduced. There was severe parenchymal atrophy and fibrosis assessed by histological examination. Fibrosis was accompanied by activation of pancreatic stellate cells (PSC) evaluated by Western blot analysis for alpha-smooth muscle actin. No differences were seen between cerulein-treated WT, AT1a-/- , AT1b-/- mice, or losartan treated-WT mice with regards to morphological or molecular alterations induced by cerulein. Our results demonstrate that AT1a and AT1b receptor pathways do not seem to be essential for the development of pancreatitis in the mouse model of pancreatitis induced by repetitive cerulein injury.

Published

2010

45. Dantrolene mitigates caerulein-induced pancreatitis in vivo in mice.

Author

Orabi AI, Shah AU, Ahmad MU, Choo-Wing R, Parness J, Jain D, Bhandari V, and Husain SZ

Subjects

Amylases blood, Animals, Apoptosis drug effects, Ceruletide, Cytoprotection, Disease Models, Animal, Enzyme Activation, Fluorescent Antibody Technique, In Situ Nick-End Labeling, Male, Mice, Mice, Inbred C57BL, Microscopy, Electron, Pancreas metabolism, Pancreas ultrastructure, Pancreatitis chemically induced, Pancreatitis metabolism, Pancreatitis pathology, Ryanodine Receptor Calcium Release Channel genetics, Ryanodine Receptor Calcium Release Channel metabolism, Severity of Illness Index, Time Factors, Trypsin metabolism, Calcium Channel Blockers pharmacology, Calcium Signaling drug effects, Dantrolene pharmacology, Pancreas drug effects, Pancreatitis prevention & control, Ryanodine Receptor Calcium Release Channel drug effects

Abstract

Acute pancreatitis is a painful, inflammatory disorder for which adequate treatments are lacking. An early, critical step in its development is the aberrant signaling of Ca(2+) within the pancreatic acinar cell. This Ca(2+) release is modulated by the intracellular Ca(2+) channel the ryanodine receptor (RYR). We have previously shown that RYR inhibition reduces pathological intra-acinar protease activation, an early marker of pancreatitis. In this study, we examined whether pretreatment with the RYR inhibitor dantrolene attenuates the severity of caerulein-induced pancreatitis in mice. Immunofluorescent labeling for RYR from mouse pancreatic sections showed localization to the basolateral region of the acinar cell. After 1 h of caerulein hyperstimulation in vivo, dantrolene 1) reduced pancreatic trypsin activity by 59% (P < 0.05) and 2) mitigated early ultrastructural derangements within the acinar cell. Eight hours after pancreatitis induction, dantrolene reduced pancreatic trypsin activity and serum amylase by 61 and 32%, respectively (P < 0.05). At this later time point, overall histological severity of pancreatitis was reduced by 63% with dantrolene pretreatment (P < 0.05). TUNEL-positive cells were reduced by 58% (P < 0.05). These data suggest that the RYR plays an important role in mediating early acinar cell events during in vivo pancreatitis and contributes to disease severity. Blockade of Ca(2+) signals and particularly RYR-Ca(2+) may be useful as prophylactic treatment for this disease in high-risk settings for pancreatitis.

Published

2010

46. Mechanism and regulation of folate uptake by pancreatic acinar cells: effect of chronic alcohol consumption.

Author

Said HM, Mee L, Sekar VT, Ashokkumar B, and Pandol SJ

Subjects

Animals, Cell Line, Drug Administration Schedule, Ethanol administration & dosage, Humans, Hydrogen-Ion Concentration, Male, Rats, Rats, Sprague-Dawley, Temperature, Ethanol metabolism, Ethanol toxicity, Folic Acid metabolism, Pancreas cytology, Pancreas drug effects

Abstract

Folate plays an essential role in one-carbon metabolism, and a relationship exists between methyl group metabolism and pancreatic exocrine function. Little, however, is known about the mechanism(s) and regulation of folate uptake by pancreatic acinar cells and the effect of chronic alcohol use on the process. We addressed these issues using the rat-derived pancreatic acinar cell line AR42J and freshly isolated primary rat pancreatic acinar cells as models. We found [(3)H]folic acid uptake to be 1) temperature and pH dependent with a higher uptake at acidic than at neutral/alkaline pH; 2) saturable as a function of substrate concentration at both buffer pH 7.4 and 6.0; 3) inhibited by folate structural analogs and by anion transport inhibitors at both buffer pH 7.4 and 6.0; 4) trans-stimulated by unlabeled folate; 5) adaptively regulated by the prevailing extracellular folate level, and 6) inhibited by modulators of the cAMP/PKA-mediated pathway. Both the reduced folate carrier (RFC) and the proton-coupled folate transporter (PCFT) were found to be expressed in AR42J and in primary pancreatic acinar cells, as well as in native human pancreas with expression of RFC being higher than PCFT. Chronic alcohol feeding of rats (4 wk; 36% of calories from ethanol) led to a significant decrease in folate uptake by freshly isolated primary pancreatic acinar cells compared with cells from pair-fed controls; this effect was associated with a parallel decrease in the level of expression of RFC and PCFT. These studies reveal that folate uptake by pancreatic acinar cells is via a regulated carrier-mediated process which may involve RFC and PCFT. In addition, chronic alcohol feeding leads to a marked inhibition in folate uptake by pancreatic acinar cells, an effect that is associated with reduction in level of expression of RFC and PCFT.

Published

2010

47. Transgenic expression of pancreatic secretory trypsin inhibitor-1 rescues SPINK3-deficient mice and restores a normal pancreatic phenotype.

Author

Romac JM, Ohmuraya M, Bittner C, Majeed MF, Vigna SR, Que J, Fee BE, Wartmann T, Yamamura K, and Liddle RA

Subjects

Amino Acid Sequence, Amylases blood, Animals, Body Size genetics, Ceruletide pharmacology, Female, Glycoproteins metabolism, Heterozygote, Intercellular Signaling Peptides and Proteins metabolism, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Mice, Transgenic, Molecular Sequence Data, Organ Size genetics, Pancreas drug effects, Pancreas metabolism, Pancreas, Exocrine pathology, Pancreas, Exocrine ultrastructure, Pancreatitis chemically induced, Pancreatitis pathology, Prostatic Secretory Proteins metabolism, Rats, Sequence Homology, Amino Acid, Survival Rate, Trypsin metabolism, Trypsin Inhibitor, Kazal Pancreatic, Glycoproteins genetics, Intercellular Signaling Peptides and Proteins genetics, Pancreas pathology, Pancreatitis genetics, Prostatic Secretory Proteins genetics, Transgenes genetics

Abstract

Endogenous trypsin inhibitors are synthesized, stored, and secreted by pancreatic acinar cells. It is believed that they play a protective role in the pancreas by inhibiting trypsin within the cell should trypsinogen become prematurely activated. Rodent trypsin inhibitors are highly homologous to human serine protease inhibitor Kazal-type 1 (SPINK1). The mouse has one pancreatic trypsin inhibitor known as SPINK3, and the rat has two trypsin inhibitors commonly known as pancreatic secretory trypsin inhibitors I and II (PSTI-I and -II). Rat PSTI-I is a 61-amino acid protein that shares 65% sequence identity with mouse SPINK3. It was recently demonstrated that mice with genetic deletion of the Spink3 gene (Spink3(-/-)) do not survive beyond 15 days and lack normal pancreata because of pancreatic autophagy. We have shown that targeted transgenic expression of the rat Psti1 gene to acinar cells in mice [TgN(Psti1)] protects mice against caerulein-induced pancreatitis. To determine whether the autophagic phenotype and lethality in Spink3(-/-) mice were due to lack of pancreatic trypsin inhibitor, we conducted breeding studies with Spink3(+/-) heterozygous mice and TgN(Psti1) mice. We observed that, whereas Spink3(+/+), Spink3(+/-), and Spink3(-/-)/TgN(Psti1) mice had similar survival rates, no Spink3(-/-) mice survived longer than 1 wk. The level of expression of SPINK3 protein in acini was reduced in heterozygote mice compared with wild-type mice. Furthermore, endogenous trypsin inhibitor capacity was reduced in the pancreas of heterozygote mice compared with wild-type or knockout mice rescued with the rat Psti1 gene. Surprisingly, the lesser amount of SPINK3 present in the pancreata of heterozygote mice did not predispose animals to increased susceptibility to caerulein-induced acute pancreatitis. We propose that a threshold level of expression is sufficient to protect against pancreatitis.

Published

2010

48. Molecular mechanism by which pioglitazone preserves pancreatic beta-cells in obese diabetic mice: evidence for acute and chronic actions as a PPARgamma agonist.

Author

Kanda Y, Shimoda M, Hamamoto S, Tawaramoto K, Kawasaki F, Hashiramoto M, Nakashima K, Matsuki M, and Kaku K

Subjects

Animals, Apoptosis physiology, Cell Differentiation drug effects, Diabetes Mellitus, Type 2 complications, Diabetes Mellitus, Type 2 metabolism, Diabetes Mellitus, Type 2 pathology, Disease Models, Animal, Gene Expression Profiling, Insulin-Secreting Cells metabolism, Insulin-Secreting Cells pathology, Male, Mice, Mice, Inbred C57BL, Mice, Mutant Strains, Mice, Obese, Obesity complications, Obesity metabolism, Organ Size drug effects, Oxidative Stress drug effects, Oxidative Stress physiology, PPAR gamma drug effects, PPAR gamma metabolism, Pancreas cytology, Pancreas drug effects, Pancreas metabolism, Pioglitazone, Apoptosis drug effects, Cell Proliferation drug effects, Diabetes Mellitus, Type 2 drug therapy, Hypoglycemic Agents pharmacology, Insulin-Secreting Cells drug effects, Thiazolidinediones pharmacology

Abstract

Pioglitazone preserves pancreatic beta-cell morphology and function in diabetic animal models. In this study, we investigated the molecular mechanisms by which pioglitazone protects beta-cells in diabetic db/db mice. In addition to the morphological analysis of the islets, gene expression profiles of the pancreatic islet were analyzed using laser capture microdissection and were compared with real-time RT-PCR of db/db and nondiabetic m/m mice treated with or without pioglitazone for 2 wk or 2 days. Pioglitazone treatment (2 wk) ameliorated dysmetabolism, increased islet insulin content, restored glucose-stimulated insulin secretion, and preserved beta-cell mass in db/db mice but had no significant effects in m/m mice. Pioglitazone upregulated genes that promote cell differentiation/proliferation in diabetic and nondiabetic mice. In db/db mice, pioglitazone downregulated the apoptosis-promoting caspase-activated DNase gene and upregulated anti-apoptosis-related genes. The above-mentioned effects of pioglitazone treatment were also observed after 2 days of treatment. By contrast, the oxidative stress-promoting NADPH oxidase gene was downregulated, and antioxidative stress-related genes were upregulated, in db/db mice treated with pioglitazone for 2 wk, rather than 2 days. Morphometric results for proliferative cell number antigen and 4-hydroxy-2-noneal modified protein were consistent with the results of gene expression analysis. The present results strongly suggest that pioglitazone preserves beta-cell mass in diabetic mice mostly by two ways; directly, by acceleration of cell differentiation/proliferation and suppression of apoptosis (acute effect); and indirectly, by deceleration of oxidative stress because of amelioration of the underlying metabolic disorder (chronic effect).

Published

2010

49. Galanin potentiates supramaximal caerulein-stimulated pancreatic amylase secretion via its action on somatostatin secretion.

Author

Barreto SG, Carati CJ, Schloithe AC, Toouli J, and Saccone GT

Subjects

Animals, Atropine pharmacology, Diazoxide pharmacology, Dose-Response Relationship, Drug, Galanin analogs & derivatives, Insulin metabolism, Mice, Muscarinic Antagonists pharmacology, Octreotide pharmacology, Pancreas enzymology, Pancreas metabolism, Receptors, Galanin drug effects, Receptors, Galanin metabolism, Receptors, Somatostatin drug effects, Receptors, Somatostatin metabolism, Somatostatin analogs & derivatives, Somatostatin pharmacology, Substance P analogs & derivatives, Substance P pharmacology, Tetrodotoxin pharmacology, Amylases metabolism, Ceruletide pharmacology, Galanin pharmacology, Pancreas drug effects, Somatostatin metabolism

Abstract

Galanin inhibits pancreatic amylase secretion from mouse lobules induced by physiological concentrations of caerulein via an insulin-dependent mechanism. We aimed to determine the effect and elucidate the mechanism of action of exogenous galanin on pancreatic amylase secretion induced by supramaximal concentrations of caerulein. Amylase secretion from isolated murine pancreatic lobules was measured. Lobules were coincubated with galanin (10(-12)-10(-7) M) and caerulein (10(-7) M). Lobules were preincubated with atropine (10(-5) M), tetrodotoxin (10(-5) M), diazoxide (10(-7) M), or the galanin antagonist galantide (10(-12)-10(-7) M) for 30 min followed by incubation with caerulein alone, or combined with galanin (10(-12) M). Lobules were also coincubated with combinations of galanin (10(-12) M), caerulein, octreotide (10(-12)-10(-7) M) or cyclo-(7-aminoheptanoyl-Phe-D-Trp-Lys-Thr[BZL]), a somatostatin receptor antagonist (10(-9) M). Amylase secretion was expressed as percent of total lobular amylase. Caerulein stimulated amylase secretion to 124% of control. Diazoxide pretreatment abolished the caerulein-stimulated amylase secretion, whereas atropine or tetrodotoxin caused a partial inhibition. Galanin (10(-12)-10(-7) M) potentiated caerulein-stimulated amylase secretion to 160% of control. Preincubation with a combination of atropine and diazoxide abolished the potentiating effect of galanin, indicating muscarinic receptor and insulin mediation. Preincubation with galantide abolished the galanin effect, implying galanin receptor involvement. Coincubation with caerulein, galanin, and octreotide significantly reduced the potentiating effect galanin. However, coincubation with the somatostatin receptor antagonist, alone or in combination with galanin, significantly increased caerulein-stimulated amylase secretion to a level comparable to the galanin potentiation. Taken together, these data suggest that, at supramaximal caerulein concentrations, galanin acts via its receptors to further increase caerulein-stimulated amylase secretion by inhibiting the caerulein-induced release of somatostatin.

Published

2009

50. Protease activation during in vivo pancreatitis is dependent on calcineurin activation.

Author

Shah AU, Sarwar A, Orabi AI, Gautam S, Grant WM, Park AJ, Shah AU, Liu J, Mistry PK, Jain D, and Husain SZ

Subjects

Animals, Calcineurin Inhibitors, Ceruletide pharmacology, Enzyme Activation, HSP70 Heat-Shock Proteins metabolism, Interleukin-6 blood, Lung drug effects, Lung enzymology, Male, Mice, Mice, Inbred Strains, Pancreas drug effects, Pancreas metabolism, Pancreas pathology, Pancreatic alpha-Amylases blood, Pancreatitis chemically induced, Pancreatitis pathology, Pancreatitis prevention & control, Peroxidase metabolism, Tacrolimus administration & dosage, Tacrolimus pharmacology, Tacrolimus therapeutic use, Trypsin metabolism, Calcineurin metabolism, Pancreatitis enzymology, Peptide Hydrolases metabolism

Abstract

The premature activation of digestive proenzymes, specifically proteases, within the pancreatic acinar cell is an early and critical event during acute pancreatitis. Our previous studies demonstrate that this activation requires a distinct pathological rise in cytosolic Ca(2+). Furthermore, we have shown that a target of aberrant Ca(2+) in acinar cells is the Ca(2+)/calmodulin-dependent phosphatase calcineurin (PP2B). In this study, we hypothesized that PP2B mediates in vivo protease activation and pancreatitis severity. To test this, pancreatitis was induced in mice over 8 h by administering hourly intraperitoneal injections of the cholecystokinin analog caerulein (50 microg/kg). Treatment with the PP2B inhibitor FK506 at 1 and 8 h after pancreatitis induction reduced trypsin activities by greater than 50% (P < 0.005). Serum amylase and IL-6 was reduced by 86 and 84% relative to baseline (P < 0.0005) at 8 h, respectively. Histological severity of pancreatitis, graded on the basis of pancreatic edema, acinar cell vacuolization, inflammation, and apoptosis, was reduced early in the course of pancreatitis. Myeloperoxidase activity from both pancreas and lung was reduced by 93 and 83% relative to baseline, respectively (P < 0.05). These data suggest that PP2B is an important target of the aberrant acinar cell Ca(2+) rise associated with pathological protease activation and pancreatitis.

Published

2009