4.6 Article

miR-145 inhibits mitochondrial function of ovarian cancer by targeting ARL5B

Journal

JOURNAL OF OVARIAN RESEARCH
Volume 14, Issue 1, Pages -

Publisher

BMC
DOI: 10.1186/s13048-020-00762-0

Keywords

miR-145; ARL5B; Mitochondrial function; Ovarian cancer

Funding

  1. National Natural Science Foundation of China [81702577]
  2. Natural Science Basic Research Program of Shaanxi [2018JQ8035]
  3. Fundamental Research Funds for the Central Universities [XZY012019105]

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The study reveals that miR-145 inhibits mitochondrial function and affects metabolic reprogramming in ovarian cancer cells by directly targeting ARL5B. This finding provides a basis for miR-145 as a potential diagnostic and therapeutic target for ovarian cancer.
Metabolic reprogramming refers to the transformation of the whole metabolic network including glycolysis and mitochondrial metabolism, mainly manifested in Warburg effect and mitochondrial metabolic reprogramming. The roles of miR-145 in glycolysis have been established in ovarian cancer cells. Howerer, its roles in mitochondrial metabolic reprogramming are still unclear. This study aims to identify whether miR-145 regulates mitochondrial metabolic reprogramming in ovarian cancer cells. First, functional experiment showed that overexpression of miR-145 inhibited mitochondrial function in ovarian cancer cells, evident by the decreased mtDNA copy numbers, ATP level, mitochondrial membrane potential, and the expression levels of mitochondrial markers. Mechanistically, miR-145 inhibited mitochondrial function by targeting ARL5B directly. Futhermore, miR-145 overexpression decreased ARL5B expression in ovarian cancer tissue subcutaneous tumors of nude mice. In conclusion, we have highlighted that miR-145 inhibits mitochondrial function and achieves this by targeting ARL5B directly for the first time. The results provides a more adequate theoretical basis for understanding the molecular pathology of ovarian cancer, and provides the necessary basic data for miR-145 as a potential diagnosis and treatment target for ovarian cancer.

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