Naringenina inhibe proliferación a través de apoptosis dependiente de la expresión transcripcional de re en células de cáncer de colon SW480 expuestas a BPA.

S.J. Lozano Herrera; Tusié AA Sánchez; Puga AC Hernández; HA Vergara Castañeda

Vol. 14 No. 1 (2021), Artículos

Vol. 14 No. 1 (2021)

Naringenina inhibe proliferación a través de apoptosis dependiente de la expresión transcripcional de re en células de cáncer de colon SW480 expuestas a BPA.

Artículos

Published 2021-07-01

S.J. Lozano Herrera⁺⁻
Tusié AA Sánchez⁺⁻
Puga AC Hernández⁺⁻
HA Vergara Castañeda⁺⁻

S.J. Lozano Herrera

Departamento de Investigación Biomédica, Facultad de Medicina, Universidad Autónoma de Querétaro

Tusié AA Sánchez

Departamento de Investigación Biomédica, Facultad de Medicina, Universidad Autónoma de Querétaro, Querétaro

Puga AC Hernández

Departamento de Investigación Biomédica, Facultad de Medicina, Universidad Autónoma de Querétaro, Querétaro

HA Vergara Castañeda

Departamento de Investigación Biomédica, Facultad de Medicina, Universidad Autónoma de Querétaro

PDF (Spanish)

Keywords

BPA
naringenin
colon cancer
receptors
GPR30
DNMT1

How to Cite

Naringenina inhibe proliferación a través de apoptosis dependiente de la expresión transcripcional de re en células de cáncer de colon SW480 expuestas a BPA. (2021). Digital Ciencia@UAQRO, 14(1), 118-127. https://revistas.uaq.mx/index.php/ciencia/article/view/112

Abstract

Naringenin (NAR) is a flavonoid that activates various mechanisms to inhibit the development of colon cancer, one of them is its affinity to various estrogen receptors (ERs). Bisphenol A (BPA) is a xenoestrogen that promotes proliferation mechanisms, binding ER type α (ERα). Colon cancer is characterized by a decrease in ER type β (ERβ) and estrogen-sensitive membrane receptors, such as GPR30, which also play an important role. On the other hand, overexpression of the DNMT1 gene have been related to unfavorable prognosis in colon cancer. The objective of the present study was to evaluate the mechanisms involved in the effect of NAR and BPA on the proliferation of human colon cancer cells. The results show that NAR promotes cell death by apoptosis and necrosis, and BPA by necrosis. The effect of BPA and NAR on the transcriptional expression of REs, GPR30 and DNMT1 was measured by qPCR. BPA decreases the expression of REβ, while NAR increases the expression of REα, REβ and GPR30 in co-exposure with BPA. The present study concludes that BPA promotes proliferative mechanisms through transcriptional expression decrease of REβ, and NAR reduces cell proliferation through mechanisms dependent on REβ and GPR30 expression.

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Naringenina inhibe proliferación a través de apoptosis dependiente de la expresión transcripcional de re en células de cáncer de colon SW480 expuestas a BPA.

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