[No authors listed]
The muscleâassociated respiratory protein myoglobin (MB) is expressed in multiple types of cancer, including breast and prostate tumors. In KaplanâMeier analyses of the two tumor types, MB positivity is associated with favorable prognoses. Despite its wellâcharacterized function in myocytes, the role of MB in cancer remains unclear. To study the impact of endogenous MB expression, small interfering RNA MBâknockdown cells were engineered using breast, prostate and colon cancer cell lines (MDAâMB468, LNCaP, DLDâ1), and their transcriptomes were investigated using RNAâSeq at different oxygen levels. In MBâpositive cells, increased expression of glycolytic genes was observed, which was possibly mediated by a higher activity of hypoxiaâinducible factor 1α. In addition, the results of the gene set enrichment analysis suggested that MB contributed to fatty acid transport and turnover. MBâpositive, wildâtypeâp53 LNCaP cells also exhibited increased expression of p53 target genes involved in cell cycle checkpoint control and prevention of cell migration. MBâpositive cells expressing mutant p53 exhibited upregulation of genes associated with prolonged cancer cell viability and motility. Therefore, it was hypothesized that these transcriptomic differences may result from MBâmediated generation of nitric oxide or reactive oxygen species, thus employing established enzymatic activities of the globin. In summary, the transcriptome comparisons identified potential molecular functions of MB in carcinogenesis by highlighting the interaction of MB with key metabolic and regulatory processes.
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