Literature DB >> 30226473

A carnosine analog mitigates metabolic disorders of obesity by reducing carbonyl stress.

Ethan J Anderson1,2, Giulio Vistoli3, Lalage A Katunga2, Katsuhiko Funai4, Luca Regazzoni3, T Blake Monroe1,2, Ettore Gilardoni3, Luca Cannizzaro3, Mara Colzani3, Danilo De Maddis3, Giuseppe Rossoni5, Renato Canevotti6, Stefania Gagliardi6, Marina Carini3, Giancarlo Aldini3.   

Abstract

Sugar- and lipid-derived aldehydes are reactive carbonyl species (RCS) frequently used as surrogate markers of oxidative stress in obesity. A pathogenic role for RCS in metabolic diseases of obesity remains controversial, however, partly because of their highly diffuse and broad reactivity and the lack of specific RCS-scavenging therapies. Naturally occurring histidine dipeptides (e.g., anserine and carnosine) show RCS reactivity, but their therapeutic potential in humans is limited by serum carnosinases. Here, we present the rational design, characterization, and pharmacological evaluation of carnosinol, i.e., (2S)-2-(3-amino propanoylamino)-3-(1H-imidazol-5-yl)propanol, a derivative of carnosine with high oral bioavailability that is resistant to carnosinases. Carnosinol displayed a suitable ADMET (absorption, distribution, metabolism, excretion, and toxicity) profile and was determined to have the greatest potency and selectivity toward α,β-unsaturated aldehydes (e.g., 4-hydroxynonenal, HNE, ACR) among all others reported thus far. In rodent models of diet-induced obesity and metabolic syndrome, carnosinol dose-dependently attenuated HNE adduct formation in liver and skeletal muscle, while simultaneously mitigating inflammation, dyslipidemia, insulin resistance, and steatohepatitis. These improvements in metabolic parameters with carnosinol were not due to changes in energy expenditure, physical activity, adiposity, or body weight. Collectively, our findings illustrate a pathogenic role for RCS in obesity-related metabolic disorders and provide validation for a promising new class of carbonyl-scavenging therapeutic compounds rationally derived from carnosine.

Entities:  

Keywords:  Diabetes; Drug therapy; Endocrinology; Metabolism; Obesity

Mesh:

Substances:

Year:  2018        PMID: 30226473      PMCID: PMC6264636          DOI: 10.1172/JCI94307

Source DB:  PubMed          Journal:  J Clin Invest        ISSN: 0021-9738            Impact factor:   14.808


  76 in total

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Review 7.  Physiology and pathophysiology of carnosine.

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Review 8.  Nonalcoholic Fatty Liver Disease: Pathogenesis and Disease Spectrum.

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  31 in total

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Authors:  Amy K Hauck; Yimao Huang; Ann V Hertzel; David A Bernlohr
Journal:  J Biol Chem       Date:  2018-12-18       Impact factor: 5.157

2.  Therapeutic potential of carbonyl-scavenging carnosine derivative in metabolic disorders.

Authors:  Jacob M Haus; John P Thyfault
Journal:  J Clin Invest       Date:  2018-10-22       Impact factor: 14.808

3.  A Highly Sensitive, Reproducible Assay for Determining 4-hydroxynonenal Protein Adducts in Biological Material.

Authors:  T Blake Monroe; Ethan J Anderson
Journal:  Bio Protoc       Date:  2019-10-05

4.  Carnosine Activates Cellular Stress Response in Podocytes and Reduces Glycative and Lipoperoxidative Stress.

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5.  Comparative Cerebroprotective Potential of d- and l-Carnosine Following Ischemic Stroke in Mice.

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7.  A carnosine analog with therapeutic potentials in the treatment of disorders related to oxidative stress.

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9.  Oral anserine supplementation does not attenuate type-2 diabetes or diabetic nephropathy in BTBR ob/ob mice.

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10.  GADL1 is a multifunctional decarboxylase with tissue-specific roles in β-alanine and carnosine production.

Authors:  Elaheh Mahootchi; Selina Cannon Homaei; Rune Kleppe; Ingeborg Winge; Tor-Arne Hegvik; Roberto Megias-Perez; Christian Totland; Floriana Mogavero; Anne Baumann; Jeffrey Colm Glennon; Hrvoje Miletic; Petri Kursula; Jan Haavik
Journal:  Sci Adv       Date:  2020-07-17       Impact factor: 14.136

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