Read Books Online and Download eBooks, EPub, PDF, Mobi, Kindle, Text Full Free.
The Roles Of Cellular Retinol Binding Protein In The Pathway Of Retinoic Acid Biosynthesis Characterization And Purification Of A Microsomal Nadp Dependent Retinol Dehydrogenase
Download The Roles Of Cellular Retinol Binding Protein In The Pathway Of Retinoic Acid Biosynthesis Characterization And Purification Of A Microsomal Nadp Dependent Retinol Dehydrogenase full books in PDF, epub, and Kindle. Read online The Roles Of Cellular Retinol Binding Protein In The Pathway Of Retinoic Acid Biosynthesis Characterization And Purification Of A Microsomal Nadp Dependent Retinol Dehydrogenase ebook anywhere anytime directly on your device. Fast Download speed and no annoying ads. We cannot guarantee that every ebooks is available!
Book Synopsis The Roles of Cellular Retinol-binding Protein in the Pathway of Retinoic Acid Biosynthesis. Characterization and Purification of a Microsomal NADP-dependent Retinol Dehydrogenase by : Manja Hermina Elisabeth Maria Boerman
Download or read book The Roles of Cellular Retinol-binding Protein in the Pathway of Retinoic Acid Biosynthesis. Characterization and Purification of a Microsomal NADP-dependent Retinol Dehydrogenase written by Manja Hermina Elisabeth Maria Boerman and published by . This book was released on 1994 with total page 418 pages. Available in PDF, EPUB and Kindle. Book excerpt:
Book Synopsis The Biochemistry of Retinoid Signaling II by : Mary Ann Asson-Batres
Download or read book The Biochemistry of Retinoid Signaling II written by Mary Ann Asson-Batres and published by Springer. This book was released on 2016-11-09 with total page 267 pages. Available in PDF, EPUB and Kindle. Book excerpt: The role of vitamin A in living organisms has been known throughout human history. In the last 100 years, the biochemical nature of vitamin A and its active derivative, retinoic acid, its physiological impact on growth processes, and the essential details of its mechanism of action have been revealed by investigations carried out by researchers using vertebrate and more recently invertebrate models to study a multiplicity of processes and conditions, encompassing embryogenesis, postnatal development to old age. A wealth of intercellular interactions, intracellular signaling systems, and molecular mechanisms have been described and the overall conclusion is that retinoic acid is essential for life. This book series, with chapters authored by experts in every aspect of this complex field, unifies the knowledge base and mechanisms currently known in detailed, engaging, well-illustrated, focused chapters that synthesize information for each specific area. In view of the recent information explosion in this field, it is timely to publish a contemporary, comprehensive, book series recapitulating the most exciting developments in the field and covering fundamental research in molecular mechanisms of vitamin A action, its role in physiology, development, and continued well-being, and the potential of vitamin A derivatives and synthetic mimetics to serve as therapeutic treatments for cancers and other debilitating human diseases. Volume II is divided into nine chapters contributed by prominent experts in their respective fields. Each chapter starts with the history of the area of research. Then, the key findings that contributed to development of the field are described, followed by a detailed look at key findings and progress that are being made in current, ongoing research. Each chapter is concluded with a discussion of the relevance of the research and a perspective on missing pieces and lingering gaps that the author recommends will be important in defining future directions in vitamin A research.
Download or read book Retinoid Signaling Pathways written by and published by Academic Press. This book was released on 2020-04-29 with total page 612 pages. Available in PDF, EPUB and Kindle. Book excerpt: Retinoid Signaling Pathways, Volume 637, the latest release in the Methods in Enzymology series, continues the legacy of this premier serial with quality chapters authored by leaders in the field. Sections in this release include The chemistry and biochemistry of Vitamin A and its natural derivative, Biosynthesis of retinoic acids, Biodegration of retinoic acids mediated by retinoid binding proteins, Retinoic acid homeostasis, Cryo Electron Microscopy to study retinol update via the STRA6 receptor, Immuno-detection of retinoic acid synthesis enzymes in the brain, classical pathway of gene regulation by retinoids, Protein-protein interactions in the regulation of retinoid acid receptors activity, and much more. Provides the authority and expertise of leading contributors from an international board of authors Presents the latest release in the Methods in Enzymology series Includes the latest information on retinoid signaling pathways
Book Synopsis Expression, Purification and Characterization of Cellular Retinoic Acid Binding Protein Types I and II. A Role in Vitamin A Metabolism by : Paul Douglas Fiorella
Download or read book Expression, Purification and Characterization of Cellular Retinoic Acid Binding Protein Types I and II. A Role in Vitamin A Metabolism written by Paul Douglas Fiorella and published by . This book was released on 1995 with total page 472 pages. Available in PDF, EPUB and Kindle. Book excerpt:
Book Synopsis Functional Studies of Intracellular Retinoid Binding Proteins by : Ulf Eriksson
Download or read book Functional Studies of Intracellular Retinoid Binding Proteins written by Ulf Eriksson and published by . This book was released on 1984 with total page 48 pages. Available in PDF, EPUB and Kindle. Book excerpt:
Download or read book The Retinoids written by Pascal Dollé and published by John Wiley & Sons. This book was released on 2015-04-13 with total page 634 pages. Available in PDF, EPUB and Kindle. Book excerpt: The Retinoids: Biology, Biochemistry, and Disease provides an overview and synthesis of the retinoid molecules, from basic biology to mechanisms of diseases and therapy. Divided into five sections, the book covers retinoic acid signaling from biochemical, genetic, developmental, and clinical perspectives. The text is divided into five sections, the first of which examines vitamin A metabolic and enzymatic pathways. Focus then shifts to the role of retinoic acid signaling in development, and then to retinoids and physiological function. The book concludes with chapters on retinoids, disease and therapy. Comprehensive in scope and written by leading researchers in the field, The Retinoids: Biology, Biochemistry, and Disease will be an essential reference for biologists, biochemists, geneticists and developmental biologists, as well as for clinicians and pharmacists engaged in clinical research involving retinoids.
Book Synopsis Retinoid Protocols by : Christopher Redfern
Download or read book Retinoid Protocols written by Christopher Redfern and published by Humana Press. This book was released on 1998-01-16 with total page 434 pages. Available in PDF, EPUB and Kindle. Book excerpt: Interest in retinoic acid, the main biologically active derivative of vi- min A or retinol, increased dramatically between 1989 and 1993, following the cloning of nuclear receptors or RARs reported in 1987 (Fig. 1). Important discoveries since then have shown how RARs work as all-trans retinoic ac- dependent heterodimers with related nuclear receptors for 9-cis retinoic acid called RXRs. This has stimulated the development of synthetic analogs s- cific for each type of receptor, and opens the way to develop new methods for regulating pharmacologically the activity ofretinoic acid-dependent pathways of gene activation. The potential for the development of new drugs by the pharmaceutical industry is now a maj or factor driving forward our understa- ing of vitamin A-regulated pathways in animal development and homeostasis. However, apart from the real potential ofretinoid analogs as novel pharma- logical agents, there remains the considerable intellectual challenge of und- standing the way in which vitamin A and its derivatives function in cell development and differentiation. Retinoid Protocols is an attempt to bring together various methodologies that will be vital for rising to this challenge in the future. Retinoid molecular biology has few methods of its own, but is reliant on standard molecular biology methods applied to this particular research area.
Book Synopsis Retinoid Receptors and Cellular Retinoic Acid Binding Proteins by : Ding Dong
Download or read book Retinoid Receptors and Cellular Retinoic Acid Binding Proteins written by Ding Dong and published by . This book was released on 2000 with total page 222 pages. Available in PDF, EPUB and Kindle. Book excerpt:
Book Synopsis Impact of Cellular Retinol Binding Protein, Type I on Retinoic Acid Biosynthesis and Homeostasis by : Keely A. Pierzchalski
Download or read book Impact of Cellular Retinol Binding Protein, Type I on Retinoic Acid Biosynthesis and Homeostasis written by Keely A. Pierzchalski and published by . This book was released on 2015 with total page 0 pages. Available in PDF, EPUB and Kindle. Book excerpt:
Book Synopsis Physiological Characterization of the Interaction Between Retinoid Homeostasis and Energy Metabolism by : Alexandra Efthymios Folias
Download or read book Physiological Characterization of the Interaction Between Retinoid Homeostasis and Energy Metabolism written by Alexandra Efthymios Folias and published by . This book was released on 2008 with total page 310 pages. Available in PDF, EPUB and Kindle. Book excerpt:
Book Synopsis Dissertation Abstracts International by :
Download or read book Dissertation Abstracts International written by and published by . This book was released on 1994 with total page 556 pages. Available in PDF, EPUB and Kindle. Book excerpt:
Book Synopsis The Function of Retinol Dehydrogenase 1 in Retinoic Acid Synthesis and Metabolic Regulation by : Charles Robert Krois
Download or read book The Function of Retinol Dehydrogenase 1 in Retinoic Acid Synthesis and Metabolic Regulation written by Charles Robert Krois and published by . This book was released on 2011 with total page 169 pages. Available in PDF, EPUB and Kindle. Book excerpt: Retinol dehydrogenases (RDH) convert retinol into retinal, the intermediate in the biosynthesis of retinoic acid. All-trans-retinoic acid (atRA) regulates gene transcription and/or translation through retinoic acid receptors (RARs) and PPAR[delta] (1). To test function of Rdh1, an efficient (Vmax/Km) and widely distributed RDH (2), our lab created Rdh1 knockout (KO) mice (3). Initial study of Rdh1-KO mice determined that when fed a low or vitamin A-deficient (VAD) diet, Rdh1-KO mice gain 33% more weight than wild-type (WT). However, when fed a chow diet (22+ IU vitamin A/g diet--i.e. copious), KO mice appeared identical to WT. Our continued work on the Rdh1-KO mouse reveals additional insight into the role of Rdh1 in both retinoic acid synthesis and energy regulation. Both a 10% increase in length and 33% increase in adiposity contribute to weight gain in VAD-fed KO animals. Based on measurements of adipocyte size, increased adiposity results from hyperplasia of white adipose tissue. Rdh1-KO mice, fed a diet with the recommended amount of vitamin A (4 IU/g), also increase in weight and adiposity, but not length. Interestingly, high fat diet feeding fails to exacerbate weight or adiposity. Increased weight contributes to a decline in Rdh1-KO mouse health. Whereas young animals respond normally to tests of glucose and insulin tolerance, older Rdh1-KO mice become insulin resistant and glucose intolerant, with 2.5-fold higher insulin levels. These changes in Rdh1-KO glucose metabolism cannot be attributed to changes in pancreatic 9-cis-retinoic acid (9cRA) (4). As expected in heavier animals, leptin levels also increase 1.8-fold in Rdh1-KO mice. In addition, loss of Rdh1 reduces circulating thyroid hormones T4 and T3 by 12% and 17%, respectively, though TSH levels remain unchanged. These data demonstrate that atRA, generated by Rdh1, contributes to control of body weight, and does so to a physiologically relevant extent. Increased weight results from either increased caloric intake or decreased energy expenditure. Overall, Rdh1-KO mice move just as much as WT, and their food intake increases only in proportion to body weight. Normalized to body weight, we observe no change to energy expenditure by indirect calorimetry. Thermogenesis, the generation of heat for body temperature maintenance, also contributes to energy expenditure. Rdh1-KO mice respond normally to cold challenge and [beta]3-adrenergic stimulation, but appear reduced in body temperature, especially when stressed by fasting. Consistent with these observations, the brown adipose tissue (BAT) of Rdh1-KO mice expresses normal levels of the [beta]2- and [beta]3-adrenergic receptors and lower levels of Gbpar1, a bile acid receptor also involved in thermogenesis (5). Ucp1 expression increases when KO mice are fasted and returns to WT levels upon refeeding, suggesting UCP1 compensates for, rather than causes, reduced thermogenesis. We used stable isotopes to measure de novo lipogenesis and triglyceride turnover in Rdh1-KO animals. Long term studies reveal reduced de novo lipogenesis, with less newly synthesized palmitate accumulating in white adipose tissue. In short term studies, brown adipose accumulated less new palmitate during 5 hours of refeeding. Comparable levels of total palmitate per gram tissue suggest increased storage of dietary lipid. Reduced rates of de novo lipogenesis, however, cannot explain increased adiposity in Rdh1-KO mice. In samples of liver, white and brown adipose, we measured the relative levels of the most common fatty acids. In animals refed after fasting, the relative contribution of stearate is less in the brown adipose and liver of Rdh1-KO mice. In ad lib fed animals, white and brown adipose have reduced relative stearate levels. These changes to lipid composition are likely due to reduced expression of elongase Elovl6 in Rdh1-KO livers. Loss of Rdh1 does not affect atRA, retinal, retinol or retinyl ester levels in ad lib fed mice in any tissue studied. However, studies of atRA during fasting and refeeding proved insightful to atRA function in WT and KO animals. In WT animals, atRA levels increase 1.3-1.5-fold in brown adipose tissue when refed 2-4 hours after a fast. In liver, atRA levels decline 30% after 5 hours of refeeding. Furthermore, reductions in hepatic retinol and retinyl ester during refeeding coincide with transient increases to serum levels, suggesting export of retinoid in the transition from fasting. Cold exposure had a similar impact on liver retinoids, but did not affect levels in brown adipose tissue. During refeeding, Rdh1-KO animals fail to maintain normal atRA levels in BAT and appear delayed in the export of retinol and esters from liver to serum. Gene expression of retinoid synthesis genes also suggests coordination or retinoid metabolism with fasting and refeeding. In brown adipose tissue, Rdh1, Aldh1a1, Rbp1, Rbp4 and Rbp7 expression decrease between fasting and 6.5 hours of refeeding. Increased atRA, despite decreased gene expression, suggests additional regulatory mechanisms of atRA synthesis in BAT. In liver, multiple Rdh (Rdh1, Dhrs9, Rdh10), retinal dehydrogenases (Aldh1a1, Aldh1a2, Aldh1a3), retinol binding proteins (Rbp1, Rbp4) and Cyp2c39 decrease expression during refeeding. Alternately, Cyp26a1 expression increases with refeeding. Hepatic gene expression changes during refeeding are generally consistent with decreased atRA. Additional work on retinoid gene expression suggests some of these expression changes occur within 2.5 hours of refeeding and that high retinol diet disrupts the regulation of some retinoid metabolism genes. To better understand the molecular mechanisms underlying the Rdh1-KO phenotype, we performed global gene expression analysis in liver, epididymal white adipose tissue (EWAT), testes and brown adipose tissue. Despite little to no Rdh1 expression in EWAT, we found nearly 3,000 gene changes in Rdh1-KO. We suspect many of these changes are secondary to weight gain. Microarray of liver, EWAT and BAT identified the gene Gbp1 upregulated in Rdh1-KO mice. Using qPCR, we found increases of 3-fold, 40-fold, and over 500-fold, respectively. Many inflammatory cytokines regulate the expression of Gbp1, yet serum levels of TNF[alpha] and IL-6 appear normal in KO mice. Based on our microarray study, we identified increased expression of Cap1, Klf2, Rbp4 and Gmpr and decreased expression of Adh1, Car5b and Orm2. Interestingly, increased Rbp4 expression does not lead to increased BAT expression of Pparg or Socs3, gene expression targets of RBP-STRA6 signaling (6). We have yet to determine which gene changes in BAT are direct retinoic acid targets or which lead to the weight and adiposity increases in Rdh1-KO mice.
Book Synopsis Energy Metabolism Regulates Retinoic Acid Synthesis and Homeostasis in Physiological Contexts by : Kristin Marie Obrochta
Download or read book Energy Metabolism Regulates Retinoic Acid Synthesis and Homeostasis in Physiological Contexts written by Kristin Marie Obrochta and published by . This book was released on 2014 with total page 119 pages. Available in PDF, EPUB and Kindle. Book excerpt: Mounting evidence supports a regulated and reciprocal relationship between retinoid homeostasis and energy metabolism, with a physiologically relevant consequence of disrupted energy balance. This research was motivated by an observation that all-trans-retinoic acid (atRA), and biosynthetic precursors, were responsive to acute shifts in energy status, in wild type animals with normal body weight and glucose tolerance, i.e. not consequent to metabolic syndrome. My dissertation was designed to characterize associations of retinoid changes under different metabolic conditions by targeting synthesis of retinoic acid, identifying underlying mechanism(s), and describing consequent function(s) in four contexts. A model that compared fasted versus re-fed ad-libitum animals was used to evaluate the impact of an acute shift in whole body metabolism on retinoid status. In liver, atRA was elevated in fasted mice, and reduced by 50% in re-fed counterparts. Consistent with synthesis driving the atRA concentration in liver, expression of retinol dehydrogenase (Rdh) genes, Rdh10 and Rdh1, were elevated by fasting, and reduced 50% in re-fed as well as glucose and insulin treated mice, which preceded the reduction in atRA. Subsequent characterization of Rdh10 and Rdh16 (human orthologue of mouse Rdh1) regulation in a human hepatoma (HepG2) cell line identified transcriptional repression by insulin that required PI3K, Akt (PKB) and suppression of the transcription factor FoxO1, which was required for optimal expression of Rdhs. Conversely, expressions of Rdhs were elevated and stabilized in serum free medium conditions. This study illustrated that liver atRA, and specifically its synthesis, is regulated by acute changes in feeding status. This controlled fluctuation in atRA concentration enables transcriptional regulation by atRA in a physiological context, and reinforces an established link between atRA and liver glucose metabolism via phosphoenolpyruvate carboxy kinase. In pancreas tissue, the 9-cis-retinoic acid (9cRA) concentration was reduced in animals that were fed ad-libitum, versus a fasted state, and also decreased rapidly and transiently in response to a glucose bolus versus a fasted state. 9cRA functions in pancreas to attenuate insulin secretion and synthesis, with the physiological impact of preventing hypoglycemia. In a fed, or glucose treated state, reduced 9cRA sensitizes pancreas for optimum insulin secretion. To understand metabolic regulation of 9cRA, synthesis was characterized with focus on Rdh5 expression in a beta cell model (832/13 rat insulinoma cells). Rdh5 expression and activity were reduced by glucose and cAMP, and overexpression of Rdh5 was sufficient to increase 9c-retinal and 9cRA synthesis. This work identified Rdh5 as a physiologically relevant regulator of 9cRA synthesis in beta cells. A third project aimed to characterize a regulatory function of atRA in central nervous system (CNS) mediated energy balance. The hypothalamus brain region is an integrative center for peripheral signals, and regulates a range of functions including reproduction, autonomic nervous system, immune response, sleep, thermoregulation, fluid homeostasis, food intake and energy expenditure. Research established active atRA metabolism by regionally distinct concentrations of atRA, expression of genes for synthesis and response to atRA, and in situ synthesis of atRA in hypothalamus tissue explants. However, the atRA concentration did not change during dietary interventions of acute fasting and feeding, high fat diet feeding, or to cold exposure. Nuclear receptor PPAR[delta] localized to nuclei and axon structures of neurons in hypothalamus and other brain regions, as demonstrated by immuno-histochemistry and confocal microscopy. This work set a foundation for study of atRA activity, and non-genomic function of PPAR[delta] in hypothalamus, but was unsuccessful in establishing a regulatory function of atRA on CNS mediated energy balance. The impact of dietary vitamin A on retinoid levels was evaluated in multiple tissues of five mouse strains, over three generations. The model transitioned mice from chow diet, containing copious vitamin A, to a semi-purified, vitamin A sufficient (VAS) diet. Three generations of VAS feeding decreased atRA in most tissues of most strains, in some cases more than 50%, and maintained an order of liver = testis> kidney> white adipose tissue = serum. Neither serum retinol nor atRA reflected tissue atRA concentrations. Strain and tissue-specific differences in retinol and atRA that reflect different amounts of dietary vitamin A could have profound effects on retinoid action, and are predictive of strain dependent differences in enzymes regulating atRA synthesis and catabolism. Consequently, the lab has continued to provide semi-purified VAS diet in mouse studies that evaluate retinoid homeostasis. In total, this collection of work provides original and novel insights into metabolic regulation of atRA biosynthesis. The controlled fluctuation in atRA concentrations, as demonstrated in multiple contexts of physiologically relevant shifts in energy status, enables dynamic regulation of downstream transcriptional targets of atRA.
Download or read book Cumulated Index Medicus written by and published by . This book was released on 1989 with total page 1400 pages. Available in PDF, EPUB and Kindle. Book excerpt:
Book Synopsis American Doctoral Dissertations by :
Download or read book American Doctoral Dissertations written by and published by . This book was released on 1993 with total page 704 pages. Available in PDF, EPUB and Kindle. Book excerpt:
Download or read book The Retinoids written by Michael B. Sporn and published by Academic Press. This book was released on 2012-12-02 with total page 441 pages. Available in PDF, EPUB and Kindle. Book excerpt: The Retinoids, Volume 1 covers the chemistry and biology of retinoids, with an emphasis on the role of retinoids in nutrition and in vision. After briefly discussing the discovery and nomenclature of retinoids, this six-chapter volume describes the chemical and physical properties of natural and synthetic retinoids, as well as the retinoidal benzoic acid derivatives. The book goes on describing various reactions with radioisotopes for the synthesis of retinoids and related compounds. Considerable chapters explain the chemical, physical, and biological methodologies for separating and measuring retinoids. A discussion on the relationships between structure and activity of retinoids is included. The last chapter addresses the role of vitamin A in animal and human nutrition. This volume also discusses the metabolism of vitamin A in normal and disease states, as well as its interaction with hormones, micronutrients, drugs, and alcohol. This volume is an ideal source for nutritionists, clinicians, and researchers who are interested in the progressing field of retinoid research.
Download or read book Index Medicus written by and published by . This book was released on 2004 with total page 2068 pages. Available in PDF, EPUB and Kindle. Book excerpt: Vols. for 1963- include as pt. 2 of the Jan. issue: Medical subject headings.
