MiR-21 Regulates Growth and Migration of Cervical Cancer Cells by RECK Signaling Pathway

Seidy Y. Aguilar-Martínez; Gabriela E. Campos-Viguri; Selma E. Medina-García; Ricardo J. García-Flores; Jessica Deas; Claudia Gómez-Cerón; Abraham Pedroza-Torres; Elizabeth Bautista-Rodríguez; Gloria Fernández-Tilapa; Mauricio Rodríguez-Dorantes; Carlos Pérez-Plasencia; Oscar Peralta-Zaragoza

doi:10.3390/ijms25074086

International Journal of Molecular Sciences (Apr 2024)

MiR-21 Regulates Growth and Migration of Cervical Cancer Cells by RECK Signaling Pathway

Seidy Y. Aguilar-Martínez,
Gabriela E. Campos-Viguri,
Selma E. Medina-García,
Ricardo J. García-Flores,
Jessica Deas,
Claudia Gómez-Cerón,
Abraham Pedroza-Torres,
Elizabeth Bautista-Rodríguez,
Gloria Fernández-Tilapa,
Mauricio Rodríguez-Dorantes,
Carlos Pérez-Plasencia,
Oscar Peralta-Zaragoza

Affiliations

Seidy Y. Aguilar-Martínez: Direction of Chronic Infections and Cancer, Research Center in Infection Diseases, Instituto Nacional de Salud Pública, Cuernavaca 62100, Mexico
Gabriela E. Campos-Viguri: Direction of Chronic Infections and Cancer, Research Center in Infection Diseases, Instituto Nacional de Salud Pública, Cuernavaca 62100, Mexico
Selma E. Medina-García: Direction of Chronic Infections and Cancer, Research Center in Infection Diseases, Instituto Nacional de Salud Pública, Cuernavaca 62100, Mexico
Ricardo J. García-Flores: Direction of Chronic Infections and Cancer, Research Center in Infection Diseases, Instituto Nacional de Salud Pública, Cuernavaca 62100, Mexico
Jessica Deas: Direction of Chronic Infections and Cancer, Research Center in Infection Diseases, Instituto Nacional de Salud Pública, Cuernavaca 62100, Mexico
Claudia Gómez-Cerón: Department of Epidemiology of Cancer, Research Center Population Health, Instituto Nacional de Salud Pública, Cuernavaca 62100, Mexico
Abraham Pedroza-Torres: Programa Investigadoras e Investigadores por México, Consejo Nacional de Humanidades, Ciencias y Tecnologías, México City 14080, Mexico
Elizabeth Bautista-Rodríguez: Clinical Chemistry, Faculty of Health Sciences, Universidad Autónoma de Tlaxcala, Zacatelco 90750, Mexico
Gloria Fernández-Tilapa: Clinical Research Laboratory, Faculty of Chemical Biological Sciences, Universidad Autónoma de Guerrero, Chilpancingo 39070, Mexico
Mauricio Rodríguez-Dorantes: Oncogenomics Laboratory, Instituto Nacional de Medicina Genómica, Tlalpan, México City 14610, Mexico
Carlos Pérez-Plasencia: Oncogenomics Laboratory, Instituto Nacional de Cancerología, México City 14080, Mexico
Oscar Peralta-Zaragoza: Direction of Chronic Infections and Cancer, Research Center in Infection Diseases, Instituto Nacional de Salud Pública, Cuernavaca 62100, Mexico

DOI: https://doi.org/10.3390/ijms25074086
Journal volume & issue: Vol. 25, no. 7
p. 4086

Abstract

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Expression of miR-21 has been found to be altered in almost all types of cancers, and it has been classified as an oncogenic microRNA. In addition, the expression of tumor suppressor gene RECK is associated with miR-21 overexpression in high-grade cervical lesions. In the present study, we analyze the role of miR-21 in RECK gene regulation in cervical cancer cells. To identify the downstream cellular target genes of upstream miR-21, we silenced endogenous miR-21 expression using siRNAs. We analyzed the expression of miR-21 and RECK, as well as functional effects on cell proliferation and migration. We found that in cervical cancer cells, there was an inverse correlation between miR-21 expression and RECK mRNA and protein expression. SiRNAs to miR-21 increased luciferase reporter activity in construct plasmids containing the RECK-3′-UTR microRNA response elements MRE21-1, MRE21-2, and MRE21-3. The role of miR-21 in cell proliferation was also analyzed, and cancer cells transfected with siRNAs exhibited a markedly reduced cell proliferation and migration. Our findings indicate that miR-21 post-transcriptionally down-regulates the expression of RECK to promote cell proliferation and cell migration inhibition in cervical cancer cell survival. Therefore, miR-21 and RECK may be potential therapeutic targets in gene therapy for cervical cancer.

Published in International Journal of Molecular Sciences

ISSN: 1661-6596 (Print); 1422-0067 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: Science: Biology (General); Science: Chemistry
Website: http://www.mdpi.com/journal/ijms

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