Literature DB >> 33562431

Reciprocal Changes in miRNA Expression with Pigmentation and Decreased Proliferation Induced in Mouse B16F1 Melanoma Cells by L-Tyrosine and 5-Bromo-2'-Deoxyuridine.

Hernán Mauricio Rivera1,2, Esther Natalia Muñoz1,2, Daniel Osuna3, Mauro Florez3, Michael Carvajal3, Luis Alberto Gómez2,4.   

Abstract

Background: Many microRNAs have been identified as critical mediators in the progression of melanoma through its regulation of genes involved in different cellular processes such as melanogenesis, cell cycle control, and senescence. However, microRNAs' concurrent participation in syngeneic mouse B16F1 melanoma cells simultaneously induced decreased proliferation and differential pigmentation by exposure to 5-Brd-2'-dU (5'Bromo-2-deoxyuridine) and L-Tyr (L-Tyrosine) respectively, is poorly understood. Aim: To evaluate changes in the expression of microRNAs and identify which miRNAs in-network may contribute to the functional bases of phenotypes of differential pigmentation and reduction of proliferation in B16F1 melanoma cells exposed to 5-Brd-2'-dU and L-Tyr.
Methods: Small RNAseq evaluation of the expression profiles of miRNAs in B16F1 melanoma cells exposed to 5-Brd-2'-dU (2.5 μg/mL) and L-Tyr (5 mM), as well as the expression by qRT-PCR of some molecular targets related to melanogenesis, cell cycle, and senescence. By bioinformatic analysis, we constructed network models of regulation and co-expression of microRNAs.
Results: We confirmed that stimulation or repression of melanogenesis with L-Tyr or 5-Brd-2'-dU, respectively, generated changes in melanin concentration, reduction in proliferation, and changes in expression of microRNAs 470-3p, 470-5p, 30d-5p, 129-5p, 148b-3p, 27b-3p, and 211-5p, which presented patterns of coordinated and reciprocal co-expression, related to changes in melanogenesis through their putative targets Mitf, Tyr and Tyrp1, and control of cell cycle and senescence: Cyclin D1, Cdk2, Cdk4, p21, and p27. Conclusions: These findings provide insights into the molecular biology of melanoma of the way miRNAs are coordinated and reciprocal expression that may operate in a network as molecular bases for understanding changes in pigmentation and decreased proliferation induced in B16F1 melanoma cells exposed to L-Tyr and 5-Brd-2'-dU.

Entities:  

Keywords:  5-bromo-2′-deoxyuridine; l-tyrosine; melanin; melanoma; miRNAs; pigmentation; senescence

Year:  2021        PMID: 33562431      PMCID: PMC7914888          DOI: 10.3390/ijms22041591

Source DB:  PubMed          Journal:  Int J Mol Sci        ISSN: 1422-0067            Impact factor:   5.923


  117 in total

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2.  miRNA-205 suppresses melanoma cell proliferation and induces senescence via regulation of E2F1 protein.

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3.  MicroRNA miR-125b induces senescence in human melanoma cells.

Authors:  Martin Glud; Valentina Manfé; Edyta Biskup; Line Holst; Anne Marie Ahlburg Dirksen; Nina Hastrup; Finn C Nielsen; Krzysztof T Drzewiecki; Robert Gniadecki
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Authors:  Manfred Kunz
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7.  Cell cycle inhibitor p21/ WAF1/ CIP1 as a cofactor of MITF expression in melanoma cells.

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9.  Suppression of pigmentation in mouse melanoma cells by 5-bromodeoxyuridine: effects on tyrosinase activity and melanosome formation.

Authors:  J R Wrathall; C Oliver; S Silagi; E Essner
Journal:  J Cell Biol       Date:  1973-05       Impact factor: 10.539

10.  PCAT-1 promotes cell growth by sponging miR-129 via MAP3K7/NF-κB pathway in multiple myeloma.

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  2 in total

1.  UVB irradiation differential regulate miRNAs expression in skin photoaging.

Authors:  Yuan Fang; Lei Chen; Xin Wang; Xu Li; Wu Xiong; Xi Zhang; Yufang Zhang; Lu Han; Ke Cao; Xiang Chen; Haibo Li; Jianda Zhou
Journal:  An Bras Dermatol       Date:  2022-05-31       Impact factor: 2.113

2.  Changes in cytoarchitecture and mobility in B16F1 melanoma cells induced by 5-Br-2'-dU coincide with Rock2, miRNAs 138-5p and 455-3p reciprocal expressions.

Authors:  Esther Natalia Muñoz; Hernán Mauricio Rivera; Luis Alberto Gómez
Journal:  Biochem Biophys Rep       Date:  2021-06-11
  2 in total

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