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Isolation and characterization of muscle fatigue substance with anti-tumor activities. | LitMetric

AI Article Synopsis

  • Research from the 1950s to 1978 suggested that exercise could help reduce tumor growth, particularly in tumor-bearing rats that were exercised until fatigue.
  • An extract called F-Substance was isolated from fatigued muscle tissues, which showed significant inhibition of tumor growth in experiments.
  • Recent advancements in technology allowed for the identification of specific cytokines, like LIX, TIMP-1, and sICAM, that appear to have a strong correlation with the antitumor effects observed in the extracts from electrically stimulated muscles compared to unstimulated ones.

Article Abstract

Research during the 1950's indicated that exercise played a role in the reduction of tumor growth. In the 1960's our studies confirmed that tumor-bearing rats, exercised to fatigue, demonstrated tumor inhibition. Our further studies isolated an extract (Fatigue Substance, or F-Substance) from rectus femoris muscles of rats which had been electrically stimulated to fatigue. This extract significantly inhibited growth of transplanted rat tumors. Research continued until 1978 when it became apparent the methodology at that time was not able to further identify the substance's active components. Using current technology, we now report on the further isolation and characterization of F-Substance. In cell proliferation assays, extracts from electrically stimulated rat rectus femoris muscles had more significant inhibitory effect on the breast cancer cell line MCF-7 than those isolated from unstimulated muscles. To identify the molecule(s) responsible for the antitumor activity, a rat cytokine antibody array was used to profile the cytokines in the substances. Among the 29 different cytokines contained on the array, 3 showed greater than 3-fold difference between the substances isolated from the stimulated and unstimulated muscles. LIX (also known as CXCL5) is 6-fold higher in the substances isolated from stimulated muscles than those from the unstimulated muscles. TIMP-1 is 4.6 fold higher and sICAM is 3.6 fold higher in the substances from the stimulated muscles. Our results indicated that cytokines released from contracting muscles might be responsible for the antitumor effect of F-Substance.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3654491PMC
http://dx.doi.org/10.7150/jca.5418DOI Listing

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