Literature DB >> 23677930

ERα-targeted therapy in ovarian cancer cells by a novel estradiol-platinum(II) hybrid.

K Brasseur1, V Leblanc, F Fabi, S Parent, C Descôteaux, G Bérubé, E Asselin.   

Abstract

As we previously showed, we have synthesized a new family of 17β-estradiol-platinum(II) hybrids. Earlier studies revealed the VP-128 hybrid to show high efficiency compared with cisplatin toward hormone-dependent breast cancer cells. In the present research, we have studied the antitumor activity of VP-128 in vitro and in vivo against ovarian cancer. In nude mice with ovarian xenografts, VP-128 displayed selective activity toward hormone-dependent tumors and showed higher efficiency than cisplatin to inhibit tumor growth. Similarly, in vitro, transient transfection of estrogen receptor (ER)-α in ERα-negative A2780 cells increased their sensitivity to VP-128-induced apoptosis, confirming the selectivity of VP-128 toward hormone-dependent tumor cells. In agreement, Western blot analysis revealed that VP-128 induced higher caspase-9, caspase-3, and poly (ADP-ribose) polymerase cleavage compared with cisplatin. The activation of caspase-independent apoptosis was also observed in ERα-negative A2780 cells, in which VP-128 rapidly induced the translocation of apoptosis-inducing factor to the nucleus. Conversely, subcellular localization of apoptosis-inducing factor was not modified in ERα-positive Ovcar-3 cells. We also discovered that VP-128 induces autophagy in ovarian cancer cells because of the formation of acidic vesicular organelles (AVOs) and increase of Light Chain 3B-II protein responsible for the formation of autophagosomes; pathways related to autophagy (AKT and mammalian target of rapamycin) were also down-regulated, supporting this mechanism. Finally, the inhibition of autophagy using chloroquine increased VP-128 efficiency, indicating a possible combination therapy. Altogether these results highlight the beneficial value of VP-128 for the treatment of hormone-dependent ovarian cancers and provide preliminary proof of concept for the efficient targeting of ERα- by 17β-estradiol-Pt(II)-linked chemotherapeutic hybrids in these tumors.

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Year:  2013        PMID: 23677930     DOI: 10.1210/en.2013-1083

Source DB:  PubMed          Journal:  Endocrinology        ISSN: 0013-7227            Impact factor:   4.736


  7 in total

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Journal:  Oncotarget       Date:  2014-09-15

Review 3.  Chemoresistance and targeted therapies in ovarian and endometrial cancers.

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Journal:  Oncotarget       Date:  2017-01-17

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Review 6.  Antitumor Activity of Pt(II), Ru(III) and Cu(II) Complexes.

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Journal:  Molecules       Date:  2020-07-31       Impact factor: 4.411

7.  Oestrogen-activated autophagy has a negative effect on the anti-osteoclastogenic function of oestrogen.

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Journal:  Cell Prolif       Date:  2020-03-11       Impact factor: 6.831

  7 in total

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