Litcius/Paper detail

Comparative plasma proteomics in muscle atrophy during cancer‐cachexia and disuse: The search for atrokines

Seongkyun Lim, Kirsten R. Dunlap, Megan E. Rosa‐Caldwell, Wesley S. Haynie, Lisa T. Jansen, Tyrone A. Washington, Nicholas P. Greene

2020Physiological Reports22 citationsDOIOpen Access PDF

Abstract

FC greater in LLC than CON or HU, respectively, confirmed by immunoblot. Recent reports suggest SAA is sufficient to induce atrophy via TLR. Therefore, we assessed TLR2,4, and IL-6 mRNAs in hindlimb muscles. TLR mRNAs were not altered, suggesting SAA effects on atrophy during LLC are independent of TLR signaling. However, we noted > 6-fold induction of IL-6 in soleus of HU mice, despite minimal shift in the plasma proteome, indicating potential localized inflammation in atrophying muscle. Furthermore, paraoxonase 1 (PON1) was highly repressed in LLC mice and largely undetectable by immunoblot in this group. Our data suggest SAA and PON1 as potential novel atrokines for cancer cachexia and indicate localized inflammation in atrophying muscles independent of the plasma proteome.

Topics & Concepts

AtrophyMuscle atrophyCachexiaInflammationProteomeInternal medicineEndocrinologySkeletal muscleBiologyProteomicsMedicineCancerPathologyBioinformaticsBiochemistryGeneMuscle Physiology and DisordersNutrition and Health in AgingExercise and Physiological Responses