Affiliation:
1. Graduate Program in Translational Biology, Medicine, and Health, Virginia Tech, Blacksburg, VA 24061, USA
2. Department of Human Nutrition, Foods and Exercise, Virginia Tech, Blacksburg, VA 24061, USA
Abstract
The aggregation of cancer cells provides a survival signal for disseminating cancer cells; however, the underlying molecular mechanisms have yet to be elucidated. Using qPCR gene arrays, this study investigated the changes in cancer-specific genes as well as genes regulating mitochondrial quality control, metabolism, and oxidative stress in response to aggregation and hypoxia in our progressive ovarian cancer models representing slow- and fast-developing ovarian cancer. Aggregation increased the expression of anti-apoptotic, stemness, epithelial-mesenchymal transition (EMT), angiogenic, mitophagic, and reactive oxygen species (ROS) scavenging genes and functions, and decreased proliferation, apoptosis, metabolism, and mitochondrial content genes and functions. The incorporation of stromal vascular cells (SVF) from obese mice into the spheroids increased DNA repair and telomere regulatory genes that may represent a link between obesity and ovarian cancer risk. While glucose had no effect, glutamine was essential for aggregation and supported proliferation of the spheroid. In contrast, low glucose and hypoxic culture conditions delayed adhesion and outgrowth capacity of the spheroids independent of their phenotype, decreased mitochondrial mass and polarity, and induced a shift of mitochondrial dynamics towards mitophagy. However, these conditions did not reduce the appearance of polarized mitochondria at adhesion sites, suggesting that adhesion signals that either reversed mitochondrial fragmentation or induced mitobiogenesis can override the impact of low glucose and oxygen levels. Thus, the plasticity of the spheroids’ phenotype supports viability during dissemination, allows for the adaptation to changing conditions such as oxygen and nutrient availability. This may be critical for the development of an aggressive cancer phenotype and, therefore, could represent druggable targets for clinical interventions.
Funder
USDA National Institute of Food and Agriculture
CEH seed funds
NCI Ruth L. Kirschstein NRSA individual fellowship
Subject
Inorganic Chemistry,Organic Chemistry,Physical and Theoretical Chemistry,Computer Science Applications,Spectroscopy,Molecular Biology,General Medicine,Catalysis
Reference75 articles.
1. American Cancer Society (2008). Cancer Facts & Figures, American Cancer Society.
2. The clonal evolution of metastases from primary serous epithelial ovarian cancers;Khalique;Int. J. Cancer,2009
3. Distinct evolutionary trajectories of primary high-grade serous ovarian cancers revealed through spatial mutational profiling;Bashashati;J. Pathol.,2013
4. Kim, Y.-N., Koo, K.H., Sung, J.Y., Yun, U.-J., and Kim, H. (2012). Anoikis resistance: An essential prerequisite for tumor metastasis. Int. J. Cell Biol., 2012.
5. Adaptation of metabolism to multicellular aggregation, hypoxia and obese stromal cell incorporation as potential measure of survival of ovarian metastases;Compton;Exp. Cell Res.,2021
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