Developmental programming of the cell stress response and metabolic inflammation in liver and adipose tissue in an ovine model

Developmental programming of the cell stress response and metabolic inflammation in liver and adipose tissue in an ovine model

A state of chronic metabolic inflammation and activation of the cell stress response in organs such as liver and adipose tissue are important pathogenic adaptations with the onset of obesity and the metabolic syndrome. The extent to which these processes are modulated by the early life nutritional e...

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Main Author: Saroha, Vivek
Format: Thesis (University of Nottingham only)
Language:English
Published: 2017
Subjects:
Developmenta programming
Perinatal nutrition
Cell stress
ER stress
UPR
Autophagy
Cell death
Crown like strictures
Adipose
Liver
Omentum
Ovine
Sheep
Hepatic
DOHAD
Metabolic inflammation
Inflammation
IUGR
SGA
Formula feeding
Postnatal growth
Gestational nutrition
Obesity
Metabolic syndrome
Insulin resistance
Online Access:https://eprints.nottingham.ac.uk/47527/
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author Saroha, Vivek
author_facet Saroha, Vivek
author_sort Saroha, Vivek
building Nottingham Research Data Repository
collection Online Access
description A state of chronic metabolic inflammation and activation of the cell stress response in organs such as liver and adipose tissue are important pathogenic adaptations with the onset of obesity and the metabolic syndrome. The extent to which these processes are modulated by the early life nutritional experience is not well established, especially in large animal models. The overall aim of this thesis was to identify whether nutritional programming during prenatal and postnatal development enhances metabolic inflammation and cell stress response of obesity. A nutritional model of fetal growth restriction achieved by maternal nutrient restriction (NR) to 60% of requirements during late gestation (110 days to term at 147 days) in twin bearing sheep was used. Combination of prenatal and postnatal nutritional interventions were studied with the following three study protocols: 1. Offspring of twin bearing sheep born to mothers nutrient restricted or fed to appetite were separated after weaning at 3 months of age and then exposed to either restricted physical activity leading to obesity or to unrestricted activity and remained lean. 2. Following maternal NR, both twins or only one twin were reared on their mother’s milk during suckling period in order to achieve a relatively faster growth rate in the latter. 3. Twin offspring of sheep randomised to NR or feeding to requirement during late gestation were separated after birth and randomised to either formula feeding or being fed by the mother until weaning followed by obesogenic rearing. Total body weight of sheep in the obese group was raised by ~30% and was unaffected by any intervention. Obesity led to an increased insulin response to the glucose tolerance test, together with hepatic triglyceride deposition, and adipocyte hypertrophy with macrophage infiltration in omental adipose tissue. NR exacerbated obesity associated hepatic triglyceride deposition and upregulated gene expression of hepatic autophagy and omental unfolded protein response. Formula feeding of sheep offspring following NR was associated with slower weight gain and decreased gene expression for MTOR. Sheep offspring fed by mother as singleton gained weight at faster rate during suckling period as compared to offspring fed by their mothers as twins. Neither postnatal interventions exacerbated the state of obesity associated metabolic inflammation and cell stress response. It is possible that the increased hepatic autophagic gene expression is a reflection of defective autophagy and future work should include study of markers of autophagic function. Possible mechanisms of upregulated omental adipose UPR in offspring of sheep undergoing NR could include a programmed decrease in adipocyte number or selective survival of preadipocytes with effective ER stress response. Such adaptations followed by obesity would predispose the adipocytes to initiate inflammation and cell death pathways.
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spelling nottingham-475272025-02-28T11:59:41Z https://eprints.nottingham.ac.uk/47527/ Developmental programming of the cell stress response and metabolic inflammation in liver and adipose tissue in an ovine model Saroha, Vivek A state of chronic metabolic inflammation and activation of the cell stress response in organs such as liver and adipose tissue are important pathogenic adaptations with the onset of obesity and the metabolic syndrome. The extent to which these processes are modulated by the early life nutritional experience is not well established, especially in large animal models. The overall aim of this thesis was to identify whether nutritional programming during prenatal and postnatal development enhances metabolic inflammation and cell stress response of obesity. A nutritional model of fetal growth restriction achieved by maternal nutrient restriction (NR) to 60% of requirements during late gestation (110 days to term at 147 days) in twin bearing sheep was used. Combination of prenatal and postnatal nutritional interventions were studied with the following three study protocols: 1. Offspring of twin bearing sheep born to mothers nutrient restricted or fed to appetite were separated after weaning at 3 months of age and then exposed to either restricted physical activity leading to obesity or to unrestricted activity and remained lean. 2. Following maternal NR, both twins or only one twin were reared on their mother’s milk during suckling period in order to achieve a relatively faster growth rate in the latter. 3. Twin offspring of sheep randomised to NR or feeding to requirement during late gestation were separated after birth and randomised to either formula feeding or being fed by the mother until weaning followed by obesogenic rearing. Total body weight of sheep in the obese group was raised by ~30% and was unaffected by any intervention. Obesity led to an increased insulin response to the glucose tolerance test, together with hepatic triglyceride deposition, and adipocyte hypertrophy with macrophage infiltration in omental adipose tissue. NR exacerbated obesity associated hepatic triglyceride deposition and upregulated gene expression of hepatic autophagy and omental unfolded protein response. Formula feeding of sheep offspring following NR was associated with slower weight gain and decreased gene expression for MTOR. Sheep offspring fed by mother as singleton gained weight at faster rate during suckling period as compared to offspring fed by their mothers as twins. Neither postnatal interventions exacerbated the state of obesity associated metabolic inflammation and cell stress response. It is possible that the increased hepatic autophagic gene expression is a reflection of defective autophagy and future work should include study of markers of autophagic function. Possible mechanisms of upregulated omental adipose UPR in offspring of sheep undergoing NR could include a programmed decrease in adipocyte number or selective survival of preadipocytes with effective ER stress response. Such adaptations followed by obesity would predispose the adipocytes to initiate inflammation and cell death pathways. 2017-12-15 Thesis (University of Nottingham only) NonPeerReviewed application/pdf en arr https://eprints.nottingham.ac.uk/47527/1/Vivek_Saroha_PhD_Thesis.pdf Saroha, Vivek (2017) Developmental programming of the cell stress response and metabolic inflammation in liver and adipose tissue in an ovine model. PhD thesis, University of Nottingham. Developmenta programming Perinatal nutrition Cell stress ER stress UPR Autophagy Cell death Crown like strictures Adipose Liver Omentum Ovine Sheep Hepatic DOHAD Metabolic inflammation Inflammation IUGR SGA Formula feeding Postnatal growth Gestational nutrition Obesity Metabolic syndrome Insulin resistance
spellingShingle Developmenta programming
Perinatal nutrition
Cell stress
ER stress
UPR
Autophagy
Cell death
Crown like strictures
Adipose
Liver
Omentum
Ovine
Sheep
Hepatic
DOHAD
Metabolic inflammation
Inflammation
IUGR
SGA
Formula feeding
Postnatal growth
Gestational nutrition
Obesity
Metabolic syndrome
Insulin resistance
Saroha, Vivek
Developmental programming of the cell stress response and metabolic inflammation in liver and adipose tissue in an ovine model
title Developmental programming of the cell stress response and metabolic inflammation in liver and adipose tissue in an ovine model
title_full Developmental programming of the cell stress response and metabolic inflammation in liver and adipose tissue in an ovine model
title_fullStr Developmental programming of the cell stress response and metabolic inflammation in liver and adipose tissue in an ovine model
title_full_unstemmed Developmental programming of the cell stress response and metabolic inflammation in liver and adipose tissue in an ovine model
title_short Developmental programming of the cell stress response and metabolic inflammation in liver and adipose tissue in an ovine model
title_sort developmental programming of the cell stress response and metabolic inflammation in liver and adipose tissue in an ovine model
topic Developmenta programming
Perinatal nutrition
Cell stress
ER stress
UPR
Autophagy
Cell death
Crown like strictures
Adipose
Liver
Omentum
Ovine
Sheep
Hepatic
DOHAD
Metabolic inflammation
Inflammation
IUGR
SGA
Formula feeding
Postnatal growth
Gestational nutrition
Obesity
Metabolic syndrome
Insulin resistance
url https://eprints.nottingham.ac.uk/47527/

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