The Regulation of Fuel Metabolism and Substrate Availability During the Prolonged Fast of the Northern Elephant Seal

Food deprivation in mammals results in profound changes in fuel metabolism and substrate regulation. Among these changes are decreased reliance on the counter-regulatory dynamics by insulin-glucagon due to reduced glucose utilization, and increased concentrations of lipid substrates in plasma to mee...

Full description

Bibliographic Details
Main Author: Viscarra, Jose Abraham
Other Authors: Ortiz, Rudy M
Format: Other/Unknown Material
Language:English
Published: eScholarship, University of California 2013
Subjects:
Physiology
Endocrinology
Biochemistry
Adipose Tissue
Elephant Seal
Fasting
Insulin Resistance
Lipid Metabolism
Elephant Seals
Online Access:https://escholarship.org/uc/item/8qz1j1t8
id ftcdlib:oai:escholarship.org/ark:/13030/qt8qz1j1t8
record_format openpolar
institution Open Polar
collection University of California: eScholarship
op_collection_id ftcdlib
language English
topic Physiology
Endocrinology
Biochemistry
Adipose Tissue
Elephant Seal
Fasting
Insulin Resistance
Lipid Metabolism
spellingShingle Physiology
Endocrinology
Biochemistry
Adipose Tissue
Elephant Seal
Fasting
Insulin Resistance
Lipid Metabolism
Viscarra, Jose Abraham
The Regulation of Fuel Metabolism and Substrate Availability During the Prolonged Fast of the Northern Elephant Seal
topic_facet Physiology
Endocrinology
Biochemistry
Adipose Tissue
Elephant Seal
Fasting
Insulin Resistance
Lipid Metabolism
description Food deprivation in mammals results in profound changes in fuel metabolism and substrate regulation. Among these changes are decreased reliance on the counter-regulatory dynamics by insulin-glucagon due to reduced glucose utilization, and increased concentrations of lipid substrates in plasma to meet the energetic demands of peripheral tissues. Prolonged food deprivation also increases lipid oxidation and utilization, which may contribute to the onset of the insulin resistance associated with fasting. Because insulin resistance promotes the preservation of glucose and oxidation of fat, it has been suggested to be an adaptive response to food deprivation. As the primary storage site of lipid substrates, adipose serves as a primary contributor to the regulation of metabolism in food deprived states. Through its regulation of lipolysis, adipose influences the availability of carbohydrate, lipid, and protein, and so, may potentially be a key regulator of fasting metabolism.The northern elephant seal pup (Mirounga angustirostris) naturally undergoes a 2-3 month post-weaning fast during which it depends primarily on the oxidation of fatty acids to meet its energetic demands. The concentration of non-esterified fatty acids (NEFA) increases and is associated with the development of insulin resistance-like symptoms in late-fasted pups. Additionally, plasma NEFA concentrations respond differentially to an intravenous glucose tolerance test (ivGTT) depending on fasting duration suggesting that impaired insulin action may play a key role in the regulation of metabolic substrates in prolong-fasted animals. However, because fasting mammals also exhibit hypoinsulinemia, the insulin resistance-like conditions they experience may actually result from reduced pancreatic sensitivity/capacity, necessitating further assessment to better understand these dynamic responses.We have previously reported that adipose Glut4 expression and AMP kinase (AMPK) activity increase and plasma glucose decreases in fasting seals suggesting that AMPK activity contributes to the regulation of metabolism via Glut4 during insulin resistance-like conditions in late fasted pups. Therefore the goals of this study were: (1) to assess the impact of fasting on the regulation of metabolic substrates and thereby identify the mechanisms that allow fasting-adapted mammals to tolerate prolonged food deprivation, and (2) to assess the insulin sensitivity status of fasting elephant seals pups to determine whether fasting results in insulin resistance or pancreatic dysfunction.To accomplish this we infused early- and late-fasted seals with either glucose (0.05 g/kg) or insulin (0.065 U/kg), and a separate group of late-fasted seals with low (10 pM/kg) or high (100 pM/kg) dosages of glucagon-like peptide-1 (GLP-1) immediately following a glucose bolus (0.5g/kg), and measured the systemic and cellular responses. Because GLP-1 facilitates the glucose-stimulated insulin secretion, these infusions provide a method to assess pancreatic capacity and responsiveness. Adipose tissue and plasma samples collected prior to the infusions were used to determine the effects of fasting duration. Samples collected during the infusions were used to assess insulin sensitivity and pancreatic function.Fasting was associated with an increased NEFA:glycerol ratio in plasma and an increased DAG:TAG ratio in adipose. Furthermore, fasting decreased the expressions of fatty acid transporters and hormone sensitive lipase, and increased the expression of adipose triglyceride lipase. This suggests that increased plasma NEFA results from: (1) decreased tissue NEFA uptake, and (2) the transition to partial hydrolysis. Insulin infusions increased the phosphorylation of insulin receptor and Akt in adipose and muscle; however the timing of the signaling response was blunted in adipose. Despite the dose-dependent increases in insulin and increased glucose clearance (high dose), both GLP-1 dosages produced increases in plasma cortisol and glucagon, and may have contributed to the glucogenic role of GLP-1.Results suggest that long-term fasting induces shifts in the regulation of lipolysis and lipid metabolism that contribute to the onset of insulin resistance in adipose, all-the-while maintaining insulin sensitivity in muscle. Furthermore, fasting does not impair pancreatic capacity, but does lead to decreased glucose tolerance. Impaired glucose tolerance may facilitate the onset of a whole-body insulin resistance-like condition despite the maintenance of skeletal muscle insulin sensitivity that serves to promote the preservation of metabolic substrates, especially glucose, while allowing for the continued development of fasting elephant seal pups.
author2 Ortiz, Rudy M
format Other/Unknown Material
author Viscarra, Jose Abraham
author_facet Viscarra, Jose Abraham
author_sort Viscarra, Jose Abraham
title The Regulation of Fuel Metabolism and Substrate Availability During the Prolonged Fast of the Northern Elephant Seal
title_short The Regulation of Fuel Metabolism and Substrate Availability During the Prolonged Fast of the Northern Elephant Seal
title_full The Regulation of Fuel Metabolism and Substrate Availability During the Prolonged Fast of the Northern Elephant Seal
title_fullStr The Regulation of Fuel Metabolism and Substrate Availability During the Prolonged Fast of the Northern Elephant Seal
title_full_unstemmed The Regulation of Fuel Metabolism and Substrate Availability During the Prolonged Fast of the Northern Elephant Seal
title_sort regulation of fuel metabolism and substrate availability during the prolonged fast of the northern elephant seal
publisher eScholarship, University of California
publishDate 2013
url https://escholarship.org/uc/item/8qz1j1t8
genre Elephant Seal
Elephant Seals
genre_facet Elephant Seal
Elephant Seals
op_relation qt8qz1j1t8
https://escholarship.org/uc/item/8qz1j1t8
op_rights public
_version_ 1766401169341546496
spelling ftcdlib:oai:escholarship.org/ark:/13030/qt8qz1j1t8 2023-05-15T16:05:16+02:00 The Regulation of Fuel Metabolism and Substrate Availability During the Prolonged Fast of the Northern Elephant Seal Viscarra, Jose Abraham Ortiz, Rudy M 2013-01-01 application/pdf https://escholarship.org/uc/item/8qz1j1t8 en eng eScholarship, University of California qt8qz1j1t8 https://escholarship.org/uc/item/8qz1j1t8 public Physiology Endocrinology Biochemistry Adipose Tissue Elephant Seal Fasting Insulin Resistance Lipid Metabolism etd 2013 ftcdlib 2019-12-06T23:53:03Z Food deprivation in mammals results in profound changes in fuel metabolism and substrate regulation. Among these changes are decreased reliance on the counter-regulatory dynamics by insulin-glucagon due to reduced glucose utilization, and increased concentrations of lipid substrates in plasma to meet the energetic demands of peripheral tissues. Prolonged food deprivation also increases lipid oxidation and utilization, which may contribute to the onset of the insulin resistance associated with fasting. Because insulin resistance promotes the preservation of glucose and oxidation of fat, it has been suggested to be an adaptive response to food deprivation. As the primary storage site of lipid substrates, adipose serves as a primary contributor to the regulation of metabolism in food deprived states. Through its regulation of lipolysis, adipose influences the availability of carbohydrate, lipid, and protein, and so, may potentially be a key regulator of fasting metabolism.The northern elephant seal pup (Mirounga angustirostris) naturally undergoes a 2-3 month post-weaning fast during which it depends primarily on the oxidation of fatty acids to meet its energetic demands. The concentration of non-esterified fatty acids (NEFA) increases and is associated with the development of insulin resistance-like symptoms in late-fasted pups. Additionally, plasma NEFA concentrations respond differentially to an intravenous glucose tolerance test (ivGTT) depending on fasting duration suggesting that impaired insulin action may play a key role in the regulation of metabolic substrates in prolong-fasted animals. However, because fasting mammals also exhibit hypoinsulinemia, the insulin resistance-like conditions they experience may actually result from reduced pancreatic sensitivity/capacity, necessitating further assessment to better understand these dynamic responses.We have previously reported that adipose Glut4 expression and AMP kinase (AMPK) activity increase and plasma glucose decreases in fasting seals suggesting that AMPK activity contributes to the regulation of metabolism via Glut4 during insulin resistance-like conditions in late fasted pups. Therefore the goals of this study were: (1) to assess the impact of fasting on the regulation of metabolic substrates and thereby identify the mechanisms that allow fasting-adapted mammals to tolerate prolonged food deprivation, and (2) to assess the insulin sensitivity status of fasting elephant seals pups to determine whether fasting results in insulin resistance or pancreatic dysfunction.To accomplish this we infused early- and late-fasted seals with either glucose (0.05 g/kg) or insulin (0.065 U/kg), and a separate group of late-fasted seals with low (10 pM/kg) or high (100 pM/kg) dosages of glucagon-like peptide-1 (GLP-1) immediately following a glucose bolus (0.5g/kg), and measured the systemic and cellular responses. Because GLP-1 facilitates the glucose-stimulated insulin secretion, these infusions provide a method to assess pancreatic capacity and responsiveness. Adipose tissue and plasma samples collected prior to the infusions were used to determine the effects of fasting duration. Samples collected during the infusions were used to assess insulin sensitivity and pancreatic function.Fasting was associated with an increased NEFA:glycerol ratio in plasma and an increased DAG:TAG ratio in adipose. Furthermore, fasting decreased the expressions of fatty acid transporters and hormone sensitive lipase, and increased the expression of adipose triglyceride lipase. This suggests that increased plasma NEFA results from: (1) decreased tissue NEFA uptake, and (2) the transition to partial hydrolysis. Insulin infusions increased the phosphorylation of insulin receptor and Akt in adipose and muscle; however the timing of the signaling response was blunted in adipose. Despite the dose-dependent increases in insulin and increased glucose clearance (high dose), both GLP-1 dosages produced increases in plasma cortisol and glucagon, and may have contributed to the glucogenic role of GLP-1.Results suggest that long-term fasting induces shifts in the regulation of lipolysis and lipid metabolism that contribute to the onset of insulin resistance in adipose, all-the-while maintaining insulin sensitivity in muscle. Furthermore, fasting does not impair pancreatic capacity, but does lead to decreased glucose tolerance. Impaired glucose tolerance may facilitate the onset of a whole-body insulin resistance-like condition despite the maintenance of skeletal muscle insulin sensitivity that serves to promote the preservation of metabolic substrates, especially glucose, while allowing for the continued development of fasting elephant seal pups. Other/Unknown Material Elephant Seal Elephant Seals University of California: eScholarship

Similar Items