Cardiac and skeletal muscles show molecularly distinct responses to cancer cachexia

Physiol Genomics. 2015 Dec;47(12):588-99. doi: 10.1152/physiolgenomics.00128.2014. Epub 2015 Sep 22.

Abstract

Cancer cachexia is a systemic, paraneoplastic syndrome seen in patients with advanced cancer. There is growing interest in the altered muscle pathophysiology experienced by cachectic patients. This study reports the microarray analysis of gene expression in cardiac and skeletal muscle in the colon 26 (C26) carcinoma mouse model of cancer cachexia. A total of 268 genes were found to be differentially expressed in cardiac muscle tissue, compared with nontumor-bearing controls. This was fewer than the 1,533 genes that changed in cachectic skeletal muscle. In addition to different numbers of genes changing, different cellular functions were seen to change in each tissue. The cachectic heart showed signs of inflammation, similar to cachectic skeletal muscle, but did not show the upregulation of ubiquitin-dependent protein catabolic processes or downregulation of genes involved in cellular energetics and muscle regeneration that characterizes skeletal muscle cachexia. Quantitative PCR was used to investigate a subset of inflammatory genes in the cardiac and skeletal muscle of independent cachectic samples; this revealed that B4galt1, C1s, Serpina3n, and Vsig4 were significantly upregulated in cardiac tissue, whereas C1s and Serpina3n were significantly upregulated in skeletal tissue. Our skeletal muscle microarray results were also compared with those from three published microarray studies and found to be consistent in terms of the genes differentially expressed and the functional processes affected. Our study highlights that skeletal and cardiac muscles are affected differently in the C26 mouse model of cachexia and that therapeutic strategies cannot assume that both muscle types will show a similar response.

Keywords: cancer cachexia; cardiac muscle; colon (C26) carcinoma; differentially expressed genes; skeletal muscle.

Publication types

  • Research Support, Non-U.S. Gov't

MeSH terms

  • Acute-Phase Proteins / genetics
  • Acute-Phase Proteins / metabolism
  • Animals
  • Cachexia / complications*
  • Colonic Neoplasms / complications*
  • Colonic Neoplasms / metabolism*
  • Disease Models, Animal
  • Muscle, Skeletal / metabolism*
  • Muscle, Skeletal / physiopathology
  • Myocardium / metabolism*
  • Myocardium / pathology
  • Polymerase Chain Reaction
  • Receptors, Complement / genetics
  • Receptors, Complement / metabolism

Substances

  • Acute-Phase Proteins
  • Receptors, Complement