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

Author

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

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

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

Published
2011

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

Author

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

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

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

Published
2011

16. Contributors

Author

Barnwell, John W., primary, Bielitzki, Joseph, additional, Brady, Alan G., additional, Brammer, David W., additional, Brignolo, Laurie, additional, Cann, Jennifer A., additional, Carville, Angela A.L., additional, Clarkson, Thomas B., additional, Cline, J. Mark, additional, Eberhard, Mark l., additional, Else, James G., additional, Fahey, M.A., additional, Flynn, JoAnne L., additional, Ford, Elizabeth W., additional, Galinski, Mary R., additional, Gelovani, Juri G., additional, Gibson, Susan, additional, Harwood, H. James, additional, Hotchkiss, Charlotte E., additional, Kaplan, Jay R., additional, Kessler, Matthew J., additional, Kramer, Joshua A., additional, Krause, Stephen M., additional, Lemon, Roger, additional, Levesque, Paul C., additional, Lin, Philana Ling, additional, Lowenstine, Linda J., additional, Mankowski, Joseph L., additional, Mansfield, Keith, additional, McCracken, Paul J., additional, Miller, Andrew D., additional, Osborn, Kent G., additional, Platt, Donna M., additional, Pritzker, Kenneth P.H., additional, Rowlett, James K., additional, Sasseville, Vito G., additional, Shelton, Kathryn A., additional, Simmons, Joe, additional, Strait, Karen, additional, Wachtman, Lynn, additional, Wagner, Janice D., additional, Westmoreland, S.V., additional, Winkelmann, Christopher T., additional, and Zhang, Li, additional

Published
2012
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17. Caloric restriction and cardiovascular aging in cynomolgus monkeys (Macaca fascicularis): metabolic, physiologic, and atherosclerotic measures from a 4-year intervention trial

Author

Cefalu, William T., Wang, Zhong Q., Bell-Farrow, Audrey D., Collins, Joel, Morgan, Timothy, and Wagner, Janice D.

Subjects
Aging -- Research, Health, Seniors
Abstract

Caloric restriction (CR) retards aging processes, extends maximal life span, and consistently improves insulin resistance in lower species. Insulin resistance is associated with cardiovascular disease, but data is lacking demonstrating that increased insulin sensitivity reduces atherosclerosis progression. We initiated a study in 32 adult cynomolgus monkeys to evaluate increased insulin sensitivity secondary to CR on atherosclerosis extent. Following pretrial determinations, animals were randomized to a moderately atherogenic (0.25 mg cholesterol/Cal containing 30% of calories from fat)-fed control group or CR group (30% reduction) with equivalent dietary cholesterol intake. CR significantly improved insulin sensitivity and reduced intraabdominal fat over the 4-year intervention, while no significant differences were seen for the lipid profile between groups. Despite improved insulin sensitivity with CR, atherosclerosis extent did not differ between the ad libitum-fed or CR groups. These studies demonstrate that CR significantly improves insulin sensitivity, but when elevated plasma cholesterol concentrations were held similar, there was no effect on atherosclerosis extent. However, the composition of these lesions and changes in endothelial function may have been improved but were not evaluated in this study. Thus, further studies are needed to determine if improved insulin sensitivity might decrease arterial inflammation and improve endothelial function, despite no changes in atherosclerosis extent.

Published
2004

19. Intact dietary soy protein, but not adding an isoflavone-rich soy extract to casein, improves plasma lipids in ovariectomized cynomolgus monkeys

Author

Greaves, Kathryn A., Parks, John S., Williams, J. Koudy, and Wagner, Janice D.

Subjects
Soymilk -- Health aspects, Proteins in animal nutrition -- Research, Casein -- Health aspects, Blood lipids -- Research, Kra -- Food and nutrition, Food/cooking/nutrition
Abstract

The dietary consumption of soy protein has been linked to a reduction in coronary heart disease and improvements in a number of related risk factors. Recent investigations have focused on isoflavone components of soy protein. The purpose of this study was to examine plasma lipids and lipoproteins, particularly LDL, with the intake of intact soy protein or casein-lactalbumin diets with and without a semipurified extract of soy, rich in isoflavones. Sixty ovariectomized cynomolgus monkeys were assigned to one of three groups fed diets containing the following: 1) casein-lactalbumin as the protein source (CAS; n = 20); 2) CAS plus a semipurified extract of soy, rich in isoflavones (ISO; n = 20); or 3) intact soy protein (SOY; n = 20) for 12 wk. Lipoproteins were fractionated by combined ultracentrifugation and HPLC. Isolated LDL particles were further subfractionated by dividing the LDL peak into three fractions for compositional analyses. The SOY group had significantly lower plasma total cholesterol, VLDL plus IDL cholesterol and LDL cholesterol, and significantly less HDL cholesterol than the CAS group. LDL particles from the SOY group had a significantly less cholesteryl ester than the CAS group. The semipurified extract of soy, rich in isoflavones, added to casein-lactalbumin protein did not have the same effects as intact soy protein on plasma lipids and lipoproteins. Other components of soy protein, either alone or in combination with isoflavones, may be involved in the effects seen in this study. KEY WORDS: cynomolgus monkeys; isoflavones; lipoproteins; menopause; soy protein

Published
1999

24. A study of caloric restriction and cardiovascular aging in cynomolgus monkeys (Macaca fascicularis): a potential model for aging research

Author

Cefalu, William T., Wagner, Janice D., Wang, Zhong Q., Bell-Farrow, Audrey D., Collins, Joel, Haskell, Darren, Bechtold, Robert, and Morgan, Timothy

Subjects
Kra -- Physiological aspects, Cardiovascular system -- Aging, Aging -- Physiological aspects, Health, Seniors
Abstract

Caloric restriction has been demonstrated to retard aging processes and extend maximal life span in rodents, and is currently being evaluated in several nonhuman primate trials. We initiated a study in 32 adult cynomolgus monkeys to evaluate the effect of caloric restriction on parameters contributing to atherosclerosis extent. Following pretrial determinations, at which time a baseline measure of ad libitum (ad lib) dietary intake was assessed, animals were randomized to an ad lib fed group (control) or a caloric restriction group (30% reduction from baseline intake). The animals are being evaluated for glycated proteins, insulin, glucose, insulin sensitivity measures, and specific measures of body fat composition by CT scans (e.g., intra-abdominal fat) over specified intervals. The results from the first year of observation demonstrate a significant diet effect on body weight, and specifically intra-abdominal fat. Further, insulin sensitivity has been significantly increased after 1 year of caloric restriction compared to the ad lib fed group. These studies indicate that caloric restriction has a marked effect on a pathologic fat depot, and this change is associated significantly with an improvement in peripheral tissue insulin sensitivity.

Published
1997

34. Effects of 17 alpha-dihydroequilenin sulfate on atherosclerotic male and female rhesus monkeys

Author

Washburn, Scott A., Honore, Erika K., Cline, J. Mark, Helman, Melissa, Wagner, Janice D., Adelman, Steven J., and Clarkson, Thomas B.

Subjects
Progesterone -- Physiological aspects, Hormone therapy -- Evaluation, Atherosclerosis -- Prevention, Estradiol -- Physiological aspects, Health
Abstract

Treatment with the hormone 17a-dihydroequilenin (DHEN) may be effective in reducing obstructive heart disease in men and women past menopause. Researchers evaluated the effects of five weeks of DHEN treatment, estradiol treatment, or no treatment in 33 adult male and 50 adult female rhesus monkeys fed a lifetime high-fat diet. DHEN treatment prevented vessel constriction during vessel scans in intact males and in females with their ovaries removed. Uterus and breast tissue were equally deteriorated in all treatment groups. Treatments did not affect the amount of vessel blockage in any group.

Published
1996

36. Arterial heparan sulfate is negatively associated with hyperglycemia and atherosclerosis in diabetic monkeys

Author

Litwak Kenneth N, Vogl-Willis Catherine A, Wagner Janice D, Edwards Iris J, and Cefalu William T

Subjects
glycosaminoglycans, proteoglycans, arteries, atherosclerosis, diabetes, hyperglycemia., Diseases of the circulatory (Cardiovascular) system, RC666-701
Abstract

Abstract Background Arterial proteoglycans are implicated in the pathogenesis of atherosclerosis by their ability to trap plasma lipoproteins in the arterial wall and by their influence on cellular migration, adhesion and proliferation. In addition, data have suggested an anti-atherogenic role for heparan sulfate proteoglycans and a pro-atherogenic role for dermatan sulfate proteoglycans. Using a non-human primate model for human diabetes, studies examined diabetes-induced changes in arterial proteoglycans that may increase susceptibility to atherosclerosis. Methods Control (n = 7) and streptozotocin-induced diabetic (n = 8) cynomolgous monkeys were assessed for hyperglycemia by measurement of plasma glycated hemoglobin (GHb). Thoracic aortas obtained at necropsy, were extracted with 4 M guanidine HCL and proteoglycans were measured as hexuronic acid. Atherosclerosis was measured by enzymatic analysis of extracted tissue cholesterol. Glycosaminoglycan chains of arterial proteoglycans were released with papain, separated by agarose electrophoresis and analysed by scanning densitometry. Results Tissue cholesterol was positively associated with hexuronic acid content in diabetic arteries (r = .82, p < .025) but not in control arteries. Glycosaminoglycan chain analysis demonstrated that dermatan sulfate was associated with increased tissue cholesterol in both control (r = .8, p < 0.05) and diabetic (r = .8, p < .025) arteries, whereas a negative relationship was observed between heparan sulfate and tissue cholesterol in diabetic arteries only (r = -.7, p < .05). GHb, which was significantly higher in diabetic animals (8.2 ± 0.9 vs 3.8 ± 0.2%, p < .0005) was negatively associated with heparan sulfate in diabetic arteries (r = -.7, p < .05). Conclusions These data implicate hyperglycemia induced modifications in arterial proteoglycans that may promote atherosclerosis.

Published
2004
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39. Effects of soy vs. casein protein on body weight and glycemic control in female monkeys and their offspring

Author

Shively, Carol A., Clarkson, Thomas B., Wagner, Janice D., Jorgensen, Matthew J., Cline, J. Mark, Lees, Cynthia J., Franke, Adrian A., Li Zhang, Ayers, Melissa R., Schultz, Carrie, and Kaplan, Jay R.

Subjects
Soy protein -- Nutritional aspects, Soybean products -- Nutritional aspects, Casein -- Health aspects, Obesity -- Diet therapy, Monkeys -- Physiological aspects, Glycemic index -- Evaluation, Isoflavones -- Health aspects, Isoflavones -- Research, Anthropology/archeology/folklore, Biological sciences, Health, Psychology and mental health
Published
2009

42. High Dietary Cholesterol Diets May Attenuate Hypocholesterolemic Effects of Soy Consumption

Author

Greaves, Kathryn A., Wilson, Martha D., Rudel, Lawrence L., and Wagner, Janice D.

Subjects
Soyfoods -- Health aspects, Dietary fat -- Physiological aspects, Hypocholesteremia -- Physiological aspects, Food/cooking/nutrition
Abstract

We previously reported that one mechanism for the hypocholesterolemic effects of soy may be a reduction in cholesterol absorption. In this abstract, we report that reductions in cholesterol absorption may be attenuated by high amounts of cholesterol in the diet. Results from two studies examining 20 wk of soy protein consumption in ovariectomized cynomolgus monkeys are reported. All monkeys were fed either caseinlactalbumin (CAS) or isolated soy protein (SOY) as a protein source. In the first study, monkeys were fed diets containing 0.28 mg cholesterol/kcal. In the second study, monkeys were fed diets containing 0.36 mg cholesterol/kcal. Cholesterol absorption was determined by using the fecal isotope ratio method. Data are presented as means [+ or -] SEM. A significant reduction in cholesterol absorption was found in monkeys consuming isolated soy protein with 0.28 mg cholesterol/kcal compared with monkeys consuming casein-lactalbumin protein (SOY 66 [+ or -] 3% vs. CAS 74 [+ or -] 2%). However, there was no significant difference between the SOY and CAS groups consuming 0.36 mg cholesterol/kcal (SOY 63 [+ or -] 2% vs. CAS 66 [+ or -] 3%). Additionally, non-HDL cholesterol concentrations were significantly lowered in the SOY group compared with CAS group consuming 0.28 mg cholesterol/kcal (SOY 118 [+ or -] 14% vs. CAS 326 [+ or -] 37%). This was not the case in the monkeys consuming 0.36 mg cholesterol/kcal (SOY 324 [+ or -] 51% vs. CAS 403 [+ or -] 51%). Although many studies in humans suggest that soy protein is more beneficial in hypercholesterolemic individuals, most of these studies have included a low cholesterol diet in their design. The results from this study suggest that a threshold of dietary cholesterol consumption may exist above which soy protein may not be effective in lowering plasma cholesterol.

Published
2000

43. Soy Protein Reduces Arterial LDL Concentration and LDL Delivery in Both Diabetic and Nondiabetic Cynomolgus Monkeys

Author

Wagner, Janice D., Zhang, Li, Greaves, Kathryn A., and Schwenke, Dawn C.

Subjects
Cholesterol, LDL -- Measurement, Kra -- Testing, Soybean meal -- Health aspects, Food/cooking/nutrition
Abstract

We previously showed that soy protein consumption improves lipoprotein concentrations and reduces progression of atherosclerosis in cynomolgus monkeys. The mechanism for these beneficial effects is unclear. The purpose of this study was to determine potential mechanisms for the atheroprotective effects and to determine whether these effects extend to diabetic monkeys. As such, we designed an experiment with a 2 x 2 factorial design in which adult male monkeys (n = 23) were fed an atherogenic diet; the protein source was soy isolate (n = 11) or casein lactalbumin (n = 12), and monkeys were either control (n = 12) or streptozotocin-induced diabetic (n = 11). Diabetics had significantly increased fasting glucose and glycated hemoglobin levels; this relationship was not affected by protein consumption. Soy consumption significantly reduced total cholesterol and increased HDL cholesterol concentrations in both control and diabetic monkeys. To determine plasma and arterial LDL metabolism, radiolabeled LDL was injected before necropsy, 125I-LDL was injected 48 h and 131I-tyramine cellobiose-LDL was injected 1 h before necropsy to determine arterial LDL concentration and permeability, respectively. An increase in whole-body plasma LDL fractional catabolic rate was found with soy consumption. Soy reduced arterial LDL concentration across all arterial sites and LDL permeability in the carotid bifurcation and internal carotid arteries. Arterial delivery of LDL was calculated as LDL permeability X plasma LDL concentration and was also reduced across all arterial sites. There was no additional effect of diabetes. In conclusion, these beneficial effects of soy on both plasma and arterial LDL metabolism would be expected to reduce atherosclerosis progression and were found in both control and diabetic monkeys.

Published
2000

44. Brain-Wide Insulin Resistance, Tau Phosphorylation Changes, and Hippocampal Neprilysin and Amyloid-β Alterations in a Monkey Model of Type 1 Diabetes

Author

Morales-Corraliza, Jose, primary, Wong, Harrison, additional, Mazzella, Matthew J., additional, Che, Shaoli, additional, Lee, Sang Han, additional, Petkova, Eva, additional, Wagner, Janice D., additional, Hemby, Scott E., additional, Ginsberg, Stephen D., additional, and Mathews, Paul M., additional

Published
2016
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47. Hydrogen and Oxygen Isotope Ratios in Body Water and Hair: Modeling Isotope Dynamics in Nonhuman Primates

Author

O’Grady, Shannon P., Valenzuela, Luciano O., Remien, Christopher H., Enright, Lindsey E., Jorgensen, Matthew J., Kaplan, Jay R., Wagner, Janice D., Cerling, Thure E., and Ehleringer, James R.

Subjects
Male, Macaca fascicularis, Body Water, Drinking Water, Models, Animal, Animals, Female, Oxygen Isotopes, Deuterium, Article, Food Analysis, Diet, Hair
Abstract

The stable isotopic composition of drinking water, diet, and atmospheric oxygen influence the isotopic composition of body water ((2)H/(1)H, (18)O/(16)O expressed as δ(2) H and δ(18)O). In turn, body water influences the isotopic composition of organic matter in tissues, such as hair and teeth, which are often used to reconstruct historical dietary and movement patterns of animals and humans. Here, we used a nonhuman primate system (Macaca fascicularis) to test the robustness of two different mechanistic stable isotope models: a model to predict the δ(2)H and δ(18)O values of body water and a second model to predict the δ(2)H and δ(18)O values of hair. In contrast to previous human-based studies, use of nonhuman primates fed controlled diets allowed us to further constrain model parameter values and evaluate model predictions. Both models reliably predicted the δ(2)H and δ(18)O values of body water and of hair. Moreover, the isotope data allowed us to better quantify values for two critical variables in the models: the δ(2)H and δ(18)O values of gut water and the (18)O isotope fractionation associated with a carbonyl oxygen-water interaction in the gut (α(ow)). Our modeling efforts indicated that better predictions for body water and hair isotope values were achieved by making the isotopic composition of gut water approached that of body water. Additionally, the value of α(ow) was 1.0164, in close agreement with the only other previously measured observation (microbial spore cell walls), suggesting robustness of this fractionation factor across different biological systems.

Published
2012

48. The Progestin, Medroxyprogesterone Acetate, Impairs Insulin Sensitivity in Isolated Adipocytes, Independent of Body Composition

Author

SHADOAN, MELANIE K., ZHANG, LI, and WAGNER, JANICE D.

Subjects
Hormone therapy -- Physiological aspects, Diabetes -- Care and treatment, Glucose metabolism, Health
Abstract

Previous studies in our lab have shown that estrogen therapy compared to combined estrogen and progestin hormone replacement therapy improves whole body insulin metabolism and decreases abdominal fat mass in [...]

Published
2000

50. Comparative Analyses of Single-Nucleotide Polymorphisms in the TNF Promoter Region Provide Further Validation for the Vervet Monkey Model of Obesity

Author

Gray, Stanton B, Howard, Timothy D, Langefeld, Carl D, Hawkins, Gregory A, Diallo, Abdoulaye F, and Wagner, Janice D

Subjects
Male, Disease Models, Animal, Base Sequence, Tumor Necrosis Factor-alpha, Nonhuman Primate Models, Chlorocebus aethiops, Animals, Female, Obesity, Promoter Regions, Genetic, Polymorphism, Single Nucleotide, Linkage Disequilibrium, DNA Primers
Abstract

Tumor necrosis factor is a cytokine that plays critical roles in inflammation, the innate immune response, and a variety of other physiologic and pathophysiologic processes. In addition, TNF has recently been shown to mediate an intersection of chronic, low-grade inflammation and concurrent metabolic dysregulation associated with obesity and its comorbidities. As part of an ongoing initiative to further characterize vervet monkeys originating from St Kitts as an animal model of obesity and inflammation, we sequenced and genotyped the human ortholog vervet TNF gene and approximately 1 kb of the flanking 3' and 5' regions from 265 monkeys in a closed, pedigreed colony. This process revealed a total of 11 single-nucleotide polymorphisms (SNPs) and a single 4-bp insertion-deletion, with minor allele frequencies of 0.08 to 0.39. Many of these polymorphisms were in strong or complete linkage disequilibrium with each other, and all but 1 were contained within a single haplotype block, comprising 5 haplotypes with frequencies of 0.075 to 0.298. Using sequences from humans, chimpanzees, vervets, baboons, and rhesus macaques, phylogenetic shadowing of the TNF promoter region revealed that vervet SNPs, like the SNPs in related species, were clustered nonrandomly and nonuniformly around conserved transcription factor binding sites. These data, combined with previously defined heritable phenotypes, permit future association analyses in this nonhuman primate model and have great potential to help dissect the genetic and nongenetic contributions to complex diseases like obesity. More broadly, the sequence data and comparative analyses reported herein facilitates study of the evolution of regulatory sequences of inflammatory and immune-related genes.

Published
2009

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