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

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

Skeletal muscle atrophy is common across a variety of pathologies. Underlying mechanisms of atrophy differ between pathologies, and in many conditions, circulating factors are tied to muscle atrophy. Therefore, we sought to identify alterations to the plasma proteome across divergent forms of muscle...

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Veröffentlicht in:Physiological reports 2020-10, Vol.8 (19), p.e14608-n/a
Hauptverfasser: Lim, Seongkyun, Dunlap, Kirsten R., Rosa‐Caldwell, Megan E., Haynie, Wesley S., Jansen, Lisa T., Washington, Tyrone A., Greene, Nicholas P.
Format: Artikel
Sprache:eng
Schlagworte:
Age
Amyloid
Animals
Atrophy
Cachexia
Cachexia - metabolism
Cachexia - pathology
Cancer
Female
hindlimb suspension
Hindlimb Suspension - physiology
Inflammation
Laboratories
Lewis lung carcinoma
Lung cancer
Lung carcinoma
Male
Mice, Inbred C57BL
Mice, Transgenic
Mortality
muscle wasting
Muscle, Skeletal - metabolism
Muscular Atrophy - metabolism
Musculoskeletal system
Neoplasms - drug therapy
Neoplasms - metabolism
Neoplasms - pathology
Original Research
Paraoxonase
Paraoxonase 1
Physiology
Plasma
PON1
Protein synthesis
Proteins
Proteomes
Proteomics
serum amyloid A
Skeletal muscle
TLR2 protein
Toll-like receptors
Unloading
Vagina
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Zusammenfassung:Skeletal muscle atrophy is common across a variety of pathologies. Underlying mechanisms of atrophy differ between pathologies, and in many conditions, circulating factors are tied to muscle atrophy. Therefore, we sought to identify alterations to the plasma proteome across divergent forms of muscle atrophy, disuse and cancer cachexia, as potential mediators of atrophy. C57BL6/J mice were assigned to Lewis Lung Carcinoma (LLC)‐induced cachexia, disuse by hindlimb unloading (HU), or control (CON). Plasma samples were submitted for discovery proteomics and targets of interest confirmed by immunoblot. Considerably more peptides were altered in plasma from LLC (91) than HU (9) as compared to CON. Five total proteins were similarly modulated in HU and LLC compared to CON, none reached criteria for differential expression. Serum Amyloid A1 (SAA) was 4 and 6 Log2FC 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. Skeletal muscle atrophy is a debilitating condition associated with increased morbidity and mortality. In this study, bloodborne factors were assessed via plasma proteomics to identify candidates which may contribute to the development of this condition in disuse and cancer cachexia. We identify Serum Amyloid A as a factor heavily induced in cancer cachexia which may contribute to muscle atrophy in the tumor‐bearing state.
ISSN:2051-817X
DOI:10.14814/phy2.14608