Melanoma cell invasiveness is regulated by miR-211 suppression of the BRN2 transcription factor
journal contribution
posted on 2023-05-17, 07:50authored byBoyle, GM, Woods, SL, Bonazzi, VF, Stark, MS, Hacker, E, Aoude, LG, Dutton-Regester, K, Anthony CookAnthony Cook, Sturm, RA, Hayward, NK
To identify microRNAs potentially involved in melanomagenesis, we compared microRNA expression profiles between melanoma cell lines and cultured melanocytes. The most differentially expressed microRNA between the normal and tumor cell lines was miR-211. We focused on this pigment-cell-enriched miRNA as it is derived from the microphthalmia-associated transcription factor (MITF)-regulated gene, TRPM1 (melastatin). We find that miR-211 expression is greatly decreased in melanoma cells and melanoblasts compared to melanocytes. Bioinformatic analysis identified a large number of potential targets of miR-211, including POU3F2 (BRN2). Inhibition of miR-211 in normal melanocytes resulted in increased BRN2 protein, indicating that endogenous miR-211 represses BRN2 in differentiated cells. Over-expression of miR-211 in melanoma cell lines changed the invasive potential of the cells in vitro through directly targeting BRN2 translation. We propose a model for the apparent non-overlapping expression levels of BRN2 and MITF in melanoma, mediated by miR-211 expression.
History
Publication title
Pigment Cell & Melanoma Research
Volume
24
Pagination
525-537
ISSN
1755-148X
Department/School
School of Health Sciences
Publisher
John Wiley & Sons
Place of publication
England
Rights statement
The definitive published version is available online at: http://www3.interscience.wiley.com/