Literature DB >> 23344889

Metabolic derangements in the gastrocnemius and the effect of Compound A therapy in a murine model of cancer cachexia.

Hirak Der-Torossian1, Ashley Wysong, Scott Shadfar, Monte S Willis, Jonathan McDunn, Marion E Couch.   

Abstract

BACKGROUND: Cancer cachexia is a severe wasting syndrome characterized by the progressive loss of lean body mass and systemic inflammation. Inhibiting the signaling of the transcription factor nuclear factor kappa B (NF-κB) largely prevents cancer-induced muscle wasting in murine models. We have previously shown the utility of Compound A, a highly selective novel NF-κB inhibitor that targets the IκB kinase complex, to provide clinical benefit in cancer-induced skeletal muscle and cardiac atrophy.
METHODS: Using a metabolomics approach, we describe the changes found between cachectic and noncachectic gastrocnemius muscles before and after Compound A treatment at various doses.
RESULTS: Of the 234 metabolites in the gastrocnemius, cachexia-induced changes in gastrocnemius metabolism reset the steady-state abundances of 42 metabolites (p < 0.05). These changes, not evenly distributed across biochemical categories, are concentrated in amino acids, peptides, carbohydrates and energetics intermediates, and lipids. The gastrocnemius glycolytic pathway is markedly altered-changes consistent with tumor Warburg physiology. This is the first account of a Warburg effect that is not exclusively restricted to cancer cells or rapidly proliferating nonmalignant cells. Cachectic gastrocnemius also displays tricarboxylic acid cycle disruptions, signs of oxidative stress, and impaired redox homeostasis. Compound A only partially rescues the phenotype of the cachectic gastrocnemius, failing to restore the gastrocnemius' baseline metabolic profile.
CONCLUSIONS: The findings in the present manuscript enumerate the metabolic consequences of cachexia in the gastrocnemius and demonstrate that NF-kB targeted treatment only partly rescues the cachectic metabolic phenotype. These data strengthen the previous findings from metabolomic characterization of serum in cachectic animals, suggesting that many of the metabolic alterations observed in the blood originate in the diseased muscle. These findings provide significant insight into the complex pathophysiology of cancer cachexia and provide objective criteria for evaluating future therapeutics.

Entities:  

Year:  2013        PMID: 23344889      PMCID: PMC3684703          DOI: 10.1007/s13539-012-0101-7

Source DB:  PubMed          Journal:  J Cachexia Sarcopenia Muscle        ISSN: 2190-5991            Impact factor:   12.910


  45 in total

Review 1.  Cytokines and oxidative signalling in skeletal muscle.

Authors:  M B Reid; Y P Li
Journal:  Acta Physiol Scand       Date:  2001-03

2.  Oral resveratrol therapy inhibits cancer-induced skeletal muscle and cardiac atrophy in vivo.

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3.  Resistance to the skeletal muscle injury expressed by repeated treatment with compound A that has HMG-CoA reductase inhibitory activity.

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4.  Both oxidative and nitrosative stress are associated with muscle wasting in tumour-bearing rats.

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Journal:  FEBS Lett       Date:  2005-03-14       Impact factor: 4.124

5.  Molecular, cellular and physiological characterization of the cancer cachexia-inducing C26 colon carcinoma in mouse.

Authors:  Paola Aulino; Emanuele Berardi; Veronica M Cardillo; Emanuele Rizzuto; Barbara Perniconi; Carla Ramina; Fabrizio Padula; Enrico P Spugnini; Alfonso Baldi; Fabio Faiola; Sergio Adamo; Dario Coletti
Journal:  BMC Cancer       Date:  2010-07-08       Impact factor: 4.430

6.  Organization of GC/MS and LC/MS metabolomics data into chemical libraries.

Authors:  Corey D Dehaven; Anne M Evans; Hongping Dai; Kay A Lawton
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7.  Discovery of metabolomics biomarkers for early detection of nephrotoxicity.

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8.  Expression of NF-kappaB and IkappaB proteins in skeletal muscle of gastric cancer patients.

Authors:  Mary G Rhoads; Susan C Kandarian; Fabio Pacelli; Giovan Battista Doglietto; Maurizio Bossola
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Review 9.  The warburg effect: why and how do cancer cells activate glycolysis in the presence of oxygen?

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Journal:  Anticancer Agents Med Chem       Date:  2008-04       Impact factor: 2.505

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1.  Hepatic alterations during the development and progression of cancer cachexia.

Authors:  Megan E Rosa-Caldwell; Jacob L Brown; David E Lee; Michael P Wiggs; Richard A Perry; Wesley S Haynie; Aaron R Caldwell; Tyrone A Washington; Wen-Juo Lo; Nicholas P Greene
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Review 2.  Phenotypes of Obesity: How it Impacts Management.

Authors:  Meera Shah; Ryan T Hurt; Manpreet S Mundi
Journal:  Curr Gastroenterol Rep       Date:  2017-09-25

3.  Preclinical Investigation of the Novel Histone Deacetylase Inhibitor AR-42 in the Treatment of Cancer-Induced Cachexia.

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Journal:  J Natl Cancer Inst       Date:  2015-10-12       Impact factor: 13.506

4.  The wasting-associated metabolite succinate disrupts myogenesis and impairs skeletal muscle regeneration.

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5.  Post-translationally modified muscle-specific ubiquitin ligases as circulating biomarkers in experimental cancer cachexia.

Authors:  Roberto Mota; Jessica E Rodríguez; Andrea Bonetto; Thomas M O'Connell; Scott A Asher; Traci L Parry; Pamela Lockyer; Christopher R McCudden; Marion E Couch; Monte S Willis
Journal:  Am J Cancer Res       Date:  2017-09-01       Impact factor: 6.166

Review 6.  Sarcopenic obesity: how do we treat it?

Authors:  Matthew F Bouchonville; Dennis T Villareal
Journal:  Curr Opin Endocrinol Diabetes Obes       Date:  2013-10       Impact factor: 3.243

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8.  Pharmacological or genetic inhibition of iNOS prevents cachexia-mediated muscle wasting and its associated metabolism defects.

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9.  Moving on up: the Journal of Cachexia, Sarcopenia and Muscle.

Authors:  Stephan von Haehling; Stefan D Anker
Journal:  J Cachexia Sarcopenia Muscle       Date:  2015-09       Impact factor: 12.910

10.  Muscle wasting: an overview of recent developments in basic research.

Authors:  Sandra Palus; Stephan von Haehling; Jochen Springer
Journal:  J Cachexia Sarcopenia Muscle       Date:  2014-08-28       Impact factor: 12.910

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