Mifepristone Treatment Promotes Testicular Leydig Cell Tumor Progression in Transgenic Mice

SIMPLE SUMMARY: Recently, the antiprogestin activity of selective progesterone receptor (PR) modulator mifepristone (MF) has proven unsuccessful as a potential anti-cancer agent in various clinical trials. Herein, we analyzed the effects of MF treatment on Leydig cell tumor (LCT) progression in a tr...

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Autores principales: Ponikwicka-Tyszko, Donata, Chrusciel, Marcin, Pulawska, Kamila, Bernaczyk, Piotr, Sztachelska, Maria, Guo, Peilan, Li, Xiangdong, Toppari, Jorma, Huhtaniemi, Ilpo T., Wołczyński, Slawomir, Rahman, Nafis A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2020
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7694279/
https://www.ncbi.nlm.nih.gov/pubmed/33158280
http://dx.doi.org/10.3390/cancers12113263
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author Ponikwicka-Tyszko, Donata
Chrusciel, Marcin
Pulawska, Kamila
Bernaczyk, Piotr
Sztachelska, Maria
Guo, Peilan
Li, Xiangdong
Toppari, Jorma
Huhtaniemi, Ilpo T.
Wołczyński, Slawomir
Rahman, Nafis A.
author_facet Ponikwicka-Tyszko, Donata
Chrusciel, Marcin
Pulawska, Kamila
Bernaczyk, Piotr
Sztachelska, Maria
Guo, Peilan
Li, Xiangdong
Toppari, Jorma
Huhtaniemi, Ilpo T.
Wołczyński, Slawomir
Rahman, Nafis A.
author_sort Ponikwicka-Tyszko, Donata
collection PubMed
description SIMPLE SUMMARY: Recently, the antiprogestin activity of selective progesterone receptor (PR) modulator mifepristone (MF) has proven unsuccessful as a potential anti-cancer agent in various clinical trials. Herein, we analyzed the effects of MF treatment on Leydig cell tumor (LCT) progression in a transgenic mouse model (inhibin-α promoter-driven SV40 T-antigen), as well as on the proliferation of two Leydig tumor cell lines. MF significantly stimulated the proliferation of LCT in vitro. Similarly, a 1-mo MF or P4 treatment stimulated LCT tumor growth in vivo. Only the abundant membrane Pgrmc1 expression was found in LCTs, but no other classical Pgr or nonclassical membrane PRs. Functional analysis showed that PGRMC1 is required for MF and P4 to stimulate the proliferation and invasiveness of LCTs. Our findings provide novel information that the use of MF as an anti-cancer agent should be considered with caution due to its potential PGRMC1 tumor-promoting pathway activation in cancers. ABSTRACT: The selective progesterone receptor modulator mifepristone (MF) may act as a potent antiproliferative agent in different steroid-dependent cancers due to its strong antagonistic effect on the nuclear progesterone receptor (PGR). Hereby, we analyzed the effects of MF treatment on Leydig cell tumor (LCT) progression in a transgenic mouse model (inhibin-α promoter-driven SV40 T-antigen), as well as on LCT (BLTK-1 and mLTC-1) cell proliferation. MF significantly stimulated the proliferation of LCT in vitro. Similarly, a 1-mo MF or P4 treatment stimulated LCT tumor growth in vivo. Traceable/absent classical Pgr or nonclassical membrane PRs α, β, γ and Pgrmc2, but abundant membrane Pgrmc1 expression, was found in LCTs. MF did not activate glucocorticoid or androgen receptors in LCTs. Functional analysis showed that PGRMC1 is required for MF and P4 to stimulate the proliferation and invasiveness of LCTs. Accordingly, MF and P4 induced PGRMC1 translocation into the nucleus and thereby stimulated the release of TGFβ1 in LCT cells. MF and P4 treatments upregulated Tgfbr1, Tgfbr2, and Alk1 expression and stimulated TGFβ1 release in LCT cells. Our findings provide novel mechanistic insights into the action of MF as a membrane PR agonist that promotes LCT growth through PGRMC1 and the alternative TGFβ1 signaling pathway.
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spelling pubmed-76942792020-11-28 Mifepristone Treatment Promotes Testicular Leydig Cell Tumor Progression in Transgenic Mice Ponikwicka-Tyszko, Donata Chrusciel, Marcin Pulawska, Kamila Bernaczyk, Piotr Sztachelska, Maria Guo, Peilan Li, Xiangdong Toppari, Jorma Huhtaniemi, Ilpo T. Wołczyński, Slawomir Rahman, Nafis A. Cancers (Basel) Article SIMPLE SUMMARY: Recently, the antiprogestin activity of selective progesterone receptor (PR) modulator mifepristone (MF) has proven unsuccessful as a potential anti-cancer agent in various clinical trials. Herein, we analyzed the effects of MF treatment on Leydig cell tumor (LCT) progression in a transgenic mouse model (inhibin-α promoter-driven SV40 T-antigen), as well as on the proliferation of two Leydig tumor cell lines. MF significantly stimulated the proliferation of LCT in vitro. Similarly, a 1-mo MF or P4 treatment stimulated LCT tumor growth in vivo. Only the abundant membrane Pgrmc1 expression was found in LCTs, but no other classical Pgr or nonclassical membrane PRs. Functional analysis showed that PGRMC1 is required for MF and P4 to stimulate the proliferation and invasiveness of LCTs. Our findings provide novel information that the use of MF as an anti-cancer agent should be considered with caution due to its potential PGRMC1 tumor-promoting pathway activation in cancers. ABSTRACT: The selective progesterone receptor modulator mifepristone (MF) may act as a potent antiproliferative agent in different steroid-dependent cancers due to its strong antagonistic effect on the nuclear progesterone receptor (PGR). Hereby, we analyzed the effects of MF treatment on Leydig cell tumor (LCT) progression in a transgenic mouse model (inhibin-α promoter-driven SV40 T-antigen), as well as on LCT (BLTK-1 and mLTC-1) cell proliferation. MF significantly stimulated the proliferation of LCT in vitro. Similarly, a 1-mo MF or P4 treatment stimulated LCT tumor growth in vivo. Traceable/absent classical Pgr or nonclassical membrane PRs α, β, γ and Pgrmc2, but abundant membrane Pgrmc1 expression, was found in LCTs. MF did not activate glucocorticoid or androgen receptors in LCTs. Functional analysis showed that PGRMC1 is required for MF and P4 to stimulate the proliferation and invasiveness of LCTs. Accordingly, MF and P4 induced PGRMC1 translocation into the nucleus and thereby stimulated the release of TGFβ1 in LCT cells. MF and P4 treatments upregulated Tgfbr1, Tgfbr2, and Alk1 expression and stimulated TGFβ1 release in LCT cells. Our findings provide novel mechanistic insights into the action of MF as a membrane PR agonist that promotes LCT growth through PGRMC1 and the alternative TGFβ1 signaling pathway. MDPI 2020-11-04 /pmc/articles/PMC7694279/ /pubmed/33158280 http://dx.doi.org/10.3390/cancers12113263 Text en © 2020 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Ponikwicka-Tyszko, Donata
Chrusciel, Marcin
Pulawska, Kamila
Bernaczyk, Piotr
Sztachelska, Maria
Guo, Peilan
Li, Xiangdong
Toppari, Jorma
Huhtaniemi, Ilpo T.
Wołczyński, Slawomir
Rahman, Nafis A.
Mifepristone Treatment Promotes Testicular Leydig Cell Tumor Progression in Transgenic Mice
title Mifepristone Treatment Promotes Testicular Leydig Cell Tumor Progression in Transgenic Mice
title_full Mifepristone Treatment Promotes Testicular Leydig Cell Tumor Progression in Transgenic Mice
title_fullStr Mifepristone Treatment Promotes Testicular Leydig Cell Tumor Progression in Transgenic Mice
title_full_unstemmed Mifepristone Treatment Promotes Testicular Leydig Cell Tumor Progression in Transgenic Mice
title_short Mifepristone Treatment Promotes Testicular Leydig Cell Tumor Progression in Transgenic Mice
title_sort mifepristone treatment promotes testicular leydig cell tumor progression in transgenic mice
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7694279/
https://www.ncbi.nlm.nih.gov/pubmed/33158280
http://dx.doi.org/10.3390/cancers12113263
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