Volume 31, Issue 200 (9-2021)
J Mazandaran Univ Med Sci 2021, 31(200): 38-48 |
Back to browse issues page
Download citation:
BibTeX | RIS | EndNote | Medlars | ProCite | Reference Manager | RefWorks
Send citation to:
BibTeX | RIS | EndNote | Medlars | ProCite | Reference Manager | RefWorks
Send citation to:
Behjati S, Nikooie R, Aminaie M. Suppression of Autophagy-Related Gene Expression Following Chronic Endurance Training in Tumors of Breast Cancer-Bearing BALB/c Mice. J Mazandaran Univ Med Sci 2021; 31 (200) :38-48
URL: http://jmums.mazums.ac.ir/article-1-16302-en.html
URL: http://jmums.mazums.ac.ir/article-1-16302-en.html
Abstract: (1635 Views)
Background and purpose: Autophagy is lysosomal degradation pathway that contributes to tumor development through metabolic support, especially at final stages. The purpose of this study was to evaluate the effect of 12 weeks endurance training on autophagy-related gene expression levels in tumors of breast cancer-bearing BALB/c mice.
Materials and methods: Twenty-two female BALB/c mice were randomly divided into control (n= 11) and experimental (n= 11) groups. Breast cancer was induced by injecting MC4-L2 cancer cells into the right dorsal mammary fat pad. The experimental group underwent training protocol for 12 weeks. Expression levels of autophagy-related genes were measured by real-time PCR and quantified by
method. Data analysis was done applying Student t-test.
Results: Endurance training led to significant decrease in tumor weight (P= 0.038) and volume (P= 0.043) in experimental group compared to the control group. Expression levels of Beclin1 (11%), Atg7 (53%), p62 (37%), gabarapl (76%), LC3-I (35%), and LC3-II (62%) in tumors of experimental group were lower compared to the controls. In addition, training protocol resulted in a decrease in LC3-II/LC3-I ratio (42%) and increase in p62 expression level (157%) (all P< 0.05).
Conclusion: Endurance training-induced reduction in tumor weight and volume was coincided with substantial reduction in expression levels of autophagy-related genes. This may suggest that beneficial effects of endurance training in breast cancer, at least in part, could be mediated through suppression of autophagy process in solid tumors.
Materials and methods: Twenty-two female BALB/c mice were randomly divided into control (n= 11) and experimental (n= 11) groups. Breast cancer was induced by injecting MC4-L2 cancer cells into the right dorsal mammary fat pad. The experimental group underwent training protocol for 12 weeks. Expression levels of autophagy-related genes were measured by real-time PCR and quantified by
method. Data analysis was done applying Student t-test.Results: Endurance training led to significant decrease in tumor weight (P= 0.038) and volume (P= 0.043) in experimental group compared to the control group. Expression levels of Beclin1 (11%), Atg7 (53%), p62 (37%), gabarapl (76%), LC3-I (35%), and LC3-II (62%) in tumors of experimental group were lower compared to the controls. In addition, training protocol resulted in a decrease in LC3-II/LC3-I ratio (42%) and increase in p62 expression level (157%) (all P< 0.05).
Conclusion: Endurance training-induced reduction in tumor weight and volume was coincided with substantial reduction in expression levels of autophagy-related genes. This may suggest that beneficial effects of endurance training in breast cancer, at least in part, could be mediated through suppression of autophagy process in solid tumors.
Type of Study: Research(Original) |
Subject:
Sport Physiology
Send email to the article author
| Rights and permissions | |
 |
This work is licensed under a Creative Commons Attribution-NonCommercial 4.0 International License. |
Articles Copyright © The Author(s). Owned by Mazandaran University of Medical Sciences.
Contact Us
Address: Journal Office, Building No. 2, Mazandaran University of Medical Sciences, Moallem Square, Sari.Tel: +98 (011)34484874 Postal code: 48175-866 E-Mail: jmums@mazums.ac.ir Telefax: +98 (011)33262679
