Thermogenesis, aging and obesity in the LA Ntul/-cp (corpulent) rat

Tulp, Orien L.; Einstein, George P.

doi:10.15406/aowmc.2021.11.00333

Cited by 17 publications

(26 citation statements)

References 30 publications

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“…The characteristics of non-shivering thermogenesis have been reported to be impaired in both obese and obese-T2DM rats bearing the -cp trait, despite having a greater mass of BAT than occurs in their lean littermates. 20,32 While measures of metabolic rate or the thermogenic impact of exogenously adminis-tered norepinephrine were not included in the current study, norepinephrine is the neurohormone that normally innervates BAT, and the greater IBAT mass exhibited hyperplasia and hypertrophy of brown adipocytes and would be expected to demonstrate an increased capacity for NST independent of the stigmata of obesity and T2DM. [1][2][3]5 In the presence of the obese-2DM stigmata and its associated insulin resistance however the endogenous capacity for NST would likely become impaired, thereby enabling a greater efficiency of caloric utilization.…”

Section: Discussionmentioning

confidence: 99%

“…19 Urine glucose was det1ermined qualitatively, and urinary vanilmandelic acid as a reflection of sympathetic activity measured as outlined previously. 20,21 Tissue depots were dissected in their entirety and weighed on an Ohaus electronic balance to the nearest 0.1gram within one minute, and before significant dehydration could occur. Values beyond 9 months of age were not obtained in this other studies with this strain as the lifespan of the obese-T2DM rats began to decline beyond 10 months of age and seldom exceeded 12 months of age, while the lean phenotype was often observed to survive to 12-15 months of age.…”

Section: Methodsmentioning

confidence: 99%

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A Review of Brown Adipose Tissue Development in T2DM-SHR/N-cp (Corpulent) Rats

Tulp¹

2022

SOJCEM

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Brown adipose tissue (BAT) plays a significant role in the expression of non-shivering thermogenesis in response to perturbations in diet and environment in man and animals. The SHR/N-cp rat is an animal model of obesity and T2DM and has been reported to exhibit an impaired thermogenic response to parameters of diet and environment. Groups of lean and obese male SHR/N-cp rats were maintained in hanging wire-bottomed steel cages and fed a nutritionally complete diet containing 54% CHO, 22% protein,16.5% mixed fats, and 4.5% essential fiber, plus vitamins, minerals, and essential micronutrients from 1 to 9 months of age. Measures of body weight were monitored and 24-hour urinary vanil mandelic acid (VMA) were determined at the end of the study. Animals were sacrificed by decapitation and the Interscapular BAT depots excised in their entirety for measures of adipocyte size, number, and lipid content. Bode weights, net weight gain and relative adiposity of Obese was significantly greater than their lean littermates throughout the study. Urinary VMA of lean > obese rats. The IBAT weight and IBAT weight: Body weight of obese >> lean. IBAT cell number, cell lipid content and % lipid of IBAT tissues of obese >> lean rats. The results of this study indicate that while the development of IBAT mass and cellularity becomes exaggerated in the obese-diabetic animals, the superimposition of the T2DM stigmata including likely insulin resistance may further compromise the capacity of the obese diabetic animals to fully express BAT-mediated contributions to nonshivering thermogenesis .

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Section: Discussionmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

A Review of Brown Adipose Tissue Development in T2DM-SHR/N-cp (Corpulent) Rats

Tulp¹

2022

SOJCEM

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“…All animals used in this study were females due to the less severe magnitude of insulin resistance and disordered magnitude of glucose intolerance that develops in female than in male obese animals of this strain. 21 Animals were housed in plastic showbox cages, lined with one inch of pine shavings, and received Purina Chow (#5012) and house water ad libitum, at 22 ±1°C. and 50% RH on a conventional light cycle.…”

Section: Methodsmentioning

confidence: 99%

“…Measures of resting oxygen consumption were obtained in animals after an 8 hour fast in a small animal respiratory apparatus as described previously. 21,22 After obtaining a satisfactory RMR in quietly resting animals, lean and obese rats were administered caffeine (20 mg/rat, s.c., EPH 200 µg/KG BW, s.c) or both agents together, and measures of VO2 continued for up to 45 minutes post injection. An additional group was administered a submaximal dose of the β-agonist norepinephrine, 100 µg/kg BW for comparison.…”

Section: Methodsmentioning

confidence: 99%

“…Over time the rate of weight loss for an individual is likely to occur only gradually as the energy content of the stored fat is considerable greater than is observed during the oxidation of carbohydrate or protein in concert with hyperinsulinemia and the insulin-linked antilipolytic effects in adipose tissue in addition to the protein sparing effects of hyperinsulinemia on protein turnover. 21 As a potential added attribute, the mood stabilizing effects of the caffeine and ephedrine likely compliment and improve the psychological impact that may occur during dieting and attempted processes associated with weight loss.…”

Section: Synergistic Effects Of Caffeine and Ephedrinementioning

confidence: 99%

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2023

AOWMC

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2021

AOWMC

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Obesity develops in the obese phenotype of the congenic LA/Ntul//-cp (corpulent) rat strain by 6 weeks of age. 1 To gain insight into the contributors to the expression of obesity in the obese phenotype of this strain, groups [n=12-20 rats/phenotype] of congenic male lean and obese LA/Ntul//-cp (corpulent) rats were fed an ad libitum standardized Purina chow diet (CHOW) from 6 to 12 weeks or age, and subgroups (n=6 rats / subgroup) were overfed with a highly palatable cafeteria diet (CAFÉ) from 9 to 12 weeks of age (WOA). A subgroup of obese rats (n=6) were subjected to bilateral adrenalectomy (ADX) at 6 WOA and followed the same dietary regimen and treatment schedule. BW of lean and obese animals were similar at 6 WOA and increased by 88% in lean phenotype and 281% in obese phenotype during the 6 weeks study, while in ADX obese rats, BW were similar at 6 and 9 WOA but BW increased to 2.5-fold above starting weights and 1.8-fold above 9-week weights between 9 and 12 WOA. The CAFE supplement was without significant effect on final body weights in the lean phenotypes, but was associated with significantly greater body weights at ages 9 and 12 WOA in the obese phenotype (p=<0.05) and in the obese-ADX at 12 WOA. CE (kcal/gram gain of BW per day) remained relatively constant in lean and obese-ADX rats throughout the study, but CE was more efficient in the obese phenotype at all ages studied and was more efficient with the CAFE supplement feeding regimen.Fasting I:G ratios at 12 weeks of age were 4.2-fold greater in obese than lean and were partially normalized in obese-ADX to 1.7-fold increase at 12 WOA. Relative adiposity of obese rats was 3.8-fold greater in obese than lean phenotype, with the greatest increase in the SQ depot. Resting VO2 (RMR) was lower in obese than lean rats at each age studied and was increased by ADX. Thermogenic interscapular brown adipose tissue (IBAT) mass was greater in obese and obese-ADX than lean rats. The results of this study indicate that CE is associated with the predisposition for the expression and development of adiposity in the obese phenotype of this strain and is associated with an increased I:G ratio and IBAT mass that is consistent with insulin resistance and an impaired capacity for energy expenditure and became normalized on the Chow but not the CAFE diet following ADX. These observations implicate likely multiple metabolic factors that contribute to a greater efficiency of energy storage, utilization and or energy conservation in the obese than in the lean phenotype of this strain and which is partially corrected in the obese phenotype by ADX. The metabolic impact of added caloric intake was associated with an additive impact on the CE of weight gain and adiposity in the obese phenotype of this congenic rodent strain and was partially corrected via ADX.

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Thermogenesis, aging and obesity in the LA Ntul/-cp (corpulent) rat

Cited by 17 publications

References 30 publications

A Review of Brown Adipose Tissue Development in T2DM-SHR/N-cp (Corpulent) Rats

A Review of Brown Adipose Tissue Development in T2DM-SHR/N-cp (Corpulent) Rats

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