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Defining the Mechanisms of Uncoupling Protein 3-induced Thermogenesis and Metabolism in Brown Adipose Tissue

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Release : 2014
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Book Synopsis Defining the Mechanisms of Uncoupling Protein 3-induced Thermogenesis and Metabolism in Brown Adipose Tissue by : Sonya Maria Veron

Download or read book Defining the Mechanisms of Uncoupling Protein 3-induced Thermogenesis and Metabolism in Brown Adipose Tissue written by Sonya Maria Veron. This book was released on 2014. Available in PDF, EPUB and Kindle. Book excerpt: Uncoupling proteins (UCPs) constitute a highly conserved subset of mitochondrial solute carriers. Discovered in small rodents in the early 1970's, UCPs and their homologs have since been found in nematodes, plants, birds, and, most recently, in significant depots within humans (Krauss et al. 2005, Van marken Lichtenbelt 2009). Following activation by long chain fatty acids (LCFA, e.g. oleic acid) and reactive oxygen species (ROS, e.g. 4-hydroxynonenal (4HNE)), UCPs form a proton channel within the inner mitochondrial membrane and permit the influx of hydrogen ions from the inter membrane space into the mitochondrial matrix. UCPs effectively uncouple oxidative phosphorylation (OX-PHOS) from ATP generation, resulting in increasing oxygen consumption and dissipating the chemical energy in the form of heat. Found primarily in brown adipose tissue (BAT) of small hibernating mammals, the canonical role of uncoupling protein 1 (UCP1) in mammalian adaptive thermogenesis has been thoroughly studied. However, UCP1 is not the only member of the uncoupling family found within BAT. Also playing a key role in this tissue is uncoupling protein 3 (UCP3), which is a close homolog to UCP1. However, in spite of the fact that UCP3 shares more than 50% amino acid homology and tissue localization with UCP1, the true function UCP3 is very poorly elucidated. Part of the difficulty in determining this function lies in the expression levels of the UCP3 protein, which are hundreds of folds less than UCP1 in this tissue. In addition, their homologous structure makes teasing apart UCP3-specific phenomena from UCP1-mediated mechanisms very difficult using conventional techniques in cell and molecular biology. While UCP1 is almost exclusively found in BAT, UCP3 is expressed primarily in skeletal muscle (SKM), which lacks UCP1 completely (Krauss et al. 2005). Because UCP3 is so enriched in SKM, many studies have focused on its role in that tissue and have then tried to transpose these functions into BAT. As a result, UCP3 has been implicated in facilitating numerous biological processes, including non-adaptive facultative thermogenesis, affecting SKM oxidative capacity by modulating LCFA export, and ameliorating elevated levels of ROS-mediated stress within the tissue via glutathionine (GSH) interacting moieties. Ultimately, however, little consensus exists on the function of UCP3 within SKM, and subsequently, even less is known about its purpose in BAT. Previous data has shown that murine UCP1 has the capacity to bind to itself and form homo-tetramers when expressed in vitro in recombinant E. coli (Hoang T. et al. 2013). Here we show that UCP1 interacts with UCP3 in BAT in vivo, supporting Hoang's research above by showing that UCP1 has the capacity to not only homodimerize but potentially oligomerize with other UCP homologs. While many groups using UCP3-null mice have reported no gross changes in physiologic responses, data previously published in the lab showed that mice lacking UCP3 were protected from potentially fatal hyperthermic effects when administered sympathomimetic agents such as 3,4-Methylenedioxymethamphetamine (MDMA), methamphetamine (METH), lipopolysaccharide (LPS), or norepinephrine (NE) (Mills et al. 2003, Kenaston et al. 2010). This implies that UCP3 plays an intimate role in sympathetic nervous system (SNS) mediated thermogenesis. Based upon the foregoing, the primary goal of the research discussed in this thesis was to elucidate the functions of UCP3 within BAT. In this study, we recapitulated results seen by other students in this lab: that global UCP3-null mice do indeed exhibit a blunted thermogenic response when treated with sympathomimetic agonists. In addition, despite the near-ubiquitous expression of UCP2 throughout the mammalian organism, this UCP is not involved in SNS-mediated thermogenesis (Arsenijevic et al. 2000). Our data shows that UCP3 is vital to the catecholamine-mediated thermogenic responses following sympathomimetic drug administration. When challenged by METH, UCP3-null mice were able to respond, albeit with a blunted increase in body temperature. Furthermore, when challenged by NE, a key neurotransmitter involved in mediating the responses initiated by the SNS following METH exposure, UCP3-null mice were able to mount half the hyperthermic response seen in WT littermates. However, UCP1/UCP3 double-null animals exhibited an almost four-fold hypothermic effect compared to WT littermates when challenged with NE. In addition, UCP1/UCP3 double-null mice were unable to restore body temperatures back to baseline values, an effect seen in all the other genotypes. This implies that UCP3 plays an important role in restoring body temperatures to physiological norms. Therefore, while the mechanism underlying the decreased responsiveness to NE remains unclear, it is clear that whether localized to SKM or BAT, UCP3 is a major player in the mammalian response to SNS-mediated thermogenesis and global thermoregulation.

The Adipose Organ

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Release : 1999
Genre : Medical
Kind : eBook
Book Rating : 329/5 ( reviews)

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Book Synopsis The Adipose Organ by : Saverio Cinti

Download or read book The Adipose Organ written by Saverio Cinti. This book was released on 1999. Available in PDF, EPUB and Kindle. Book excerpt:

Mammalian Thermogenesis

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Release : 2012-12-06
Genre : Science
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Book Rating : 325/5 ( reviews)

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Book Synopsis Mammalian Thermogenesis by : Lucien Girardier

Download or read book Mammalian Thermogenesis written by Lucien Girardier. This book was released on 2012-12-06. Available in PDF, EPUB and Kindle. Book excerpt: an attempt to rationalize these terminological and conceptual difficulties we have considered the origins of mammalian heat production from two different points of view. The scheme depicted in Fig. 1. 1 illustrates the fate of energy in the body as seen by the nutritionist. After allowing for losses of energy in faeces and urine, the metabolizable energy obtained from food is utilized for main taining and increasing body energy content (maintenance, external work, growth and production). The transformation of metabolizable energy into these forms of net energy also involves inevitable energy losses in the form of heat - thermic energy. Similarly, maintaining homeothermy in cold en vironments involves shivering and non-shivering thermogenesis (NST) and the energy costs of assimilating nutrients and retaining net energy results in obligatory heat losses due to diet-induced thermogenesis (DIT). This obligatory DIT is mainly due to the energy cost of protein and fat synthesis but, in addition to this, there is an adaptive component of DIT that helps maintain body energy content (i. e. body weight) by dissipating the metabolizable energy consumed in excess of the requirements for maintenance, growth and production. In Fig. 1. 2, we have converted this nutritionist's scheme (A) into one that A B r-------. . . , I I Production, Growth I I External work I I I I Essential energy expenditure NET BASAL Obligatory 1 I ENERGY Maintenance HEAT heat I FASTING at (BMR) productlpn for t ROC thermoneutrallty homeothermia r.

Thermogenic Molecules

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Release : 2023-11-07
Genre :
Kind : eBook
Book Rating : 233/5 ( reviews)

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Book Synopsis Thermogenic Molecules by : Anusha Jahagirdar

Download or read book Thermogenic Molecules written by Anusha Jahagirdar. This book was released on 2023-11-07. Available in PDF, EPUB and Kindle. Book excerpt: "Thermogenic Molecules: Dietary Conversion of Adipose Tissue" by Anusha Jahagirdar is a comprehensive guide that delves into the molecular mechanisms underlying energy expenditure and obesity. The book covers topics related to the biology of adipose tissue, including brown adipose tissue (BAT) and white adipose tissue (WAT), and their respective roles in regulating energy expenditure and metabolism. The book provides a thorough understanding of the molecular and cellular mechanisms of thermogenesis and how it contributes to energy expenditure. It discusses the role of mitochondria and uncoupling protein 1 (UCP1) in thermogenesis, as well as the activation of thermogenesis by sympathetic nervous system and catecholamines. The book also explores the regulation of nutrient sensing pathways, such as AMPK, mTOR, and PPARs, and their impact on thermogenesis and adipose tissue function. Furthermore, the book delves into the impact of various dietary components on thermogenesis, including carbohydrates, proteins, and fats, and the role of ketosis in regulating energy expenditure. It also discusses the impact of exercise, cold exposure, and diet-induced thermogenesis on adipose tissue function and energy expenditure. The book also covers the link between obesity and various diseases, such as diabetes, cardiovascular diseases, non-alcoholic fatty liver disease, and cancer, and how pharmacological interventions and natural compounds can modulate adipose tissue function and metabolism to prevent and treat these conditions. Overall, "Thermogenic Molecules: Dietary Conversion of Adipose Tissue" is a valuable resource for researchers, students, and professionals in the field of metabolism, nutrition, and obesity, providing a comprehensive overview of the molecular mechanisms regulating energy expenditure and their role in preventing and treating obesity-related diseases.

Progress in Obesity Research: 8

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Release : 1999
Genre : Cytology
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Book Synopsis Progress in Obesity Research: 8 by : Bernard Guy-Grand

Download or read book Progress in Obesity Research: 8 written by Bernard Guy-Grand. This book was released on 1999. Available in PDF, EPUB and Kindle. Book excerpt:

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