Role of SUMOylation in Full Antiestrogenicity

Hilmi, Khalid; Hussein, Nader; Mendoza-Sanchez, Rodrigo; El-Ezzy, Mohamed; Ismail, Houssam; Durette, Chantal; Bail, Martine; Rozendaal, Maria Johanna; Bouvier, Michel; Thibault, Pierre; Gleason, James L.; Mader, Sylvie

doi:10.1128/mcb.00290-12

Cited by 23 publications

(73 citation statements)

References 96 publications

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“…Proteomics also identified K299 in the hinge region and K472 in the steroid-binding domain to be sumoylated. The selective estrogen receptor downregulator fulvestrant induces rapid and strong sumoylation of ERα at K171, K180, K299, and K472 residue [151]. These results indicate that ERα sumoylation contributes to full antiestrogenicity in the absence of accelerated receptor turnover.…”

Section: Sumoylation Of Estrogen Receptormentioning

confidence: 86%

RETRACTED ARTICLE: Regulation of estrogen receptor signaling in breast carcinogenesis and breast cancer therapy

Zhou

Qiao

Shetty

et al. 2013

Cell. Mol. Life Sci.

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Estrogen and estrogen receptors (ERs) are critical regulators of breast epithelial cell proliferation, differentiation, and apoptosis. Compromised signaling vis-à-vis the estrogen receptor is believed © Springer Basel 2013 yow4@pitt.edu. ), which predicts for response to endocrine-based therapy; however, innate or acquired resistance to endocrinebased drugs remains a serious challenge. The complexity of regulation for estrogen signaling coupled with the crosstalk of other oncogenic signaling pathways is a reason for endocrine therapy resistance. Alternative strategies that target novel molecular mechanisms are necessary to overcome this current and urgent gap in therapy. A thorough analysis of estrogen-signaling regulation is critical. In this review article, we will summarize current insights into the regulation of estrogen signaling as related to breast carcinogenesis and breast cancer therapy. NIH Public Access

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Section: Sumoylation Of Estrogen Receptormentioning

confidence: 86%

RETRACTED ARTICLE: Regulation of estrogen receptor signaling in breast carcinogenesis and breast cancer therapy

Zhou

Qiao

Shetty

et al. 2013

Cell. Mol. Life Sci.

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“…2007, Kocanova et al . 2010, Hilmi et al . 2012), decreased steady-state levels of ERα were observed to variable extents in the presence of endoxifen (a tamoxifen metabolite), raloxifene and bazedoxifene.…”

Section: Role Of Post-translational Modifications Of Erα By Ubi-like mentioning

confidence: 99%

“…Further, although the steady-state levels of transfected ERα were not decreased but rather increased in the presence of ICI 182,780 in HepG2 cells, ICI 182,780 still acted as an inverse agonist in these cells, whereas tamoxifen had partial agonist activity (Lupien et al . 2007, Hilmi et al . 2012).…”

Section: Role Of Post-translational Modifications Of Erα By Ubi-like mentioning

confidence: 99%

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Antiestrogens: structure-activity relationships and use in breast cancer treatment

Traboulsi

Ezzy

Gleason

et al. 2017

Journal of Molecular Endocrinology

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About 70% of breast tumors express estrogen receptor alpha (ERα), which mediates the proliferative effects of estrogens on breast epithelial cells, and are candidates for treatment with antiestrogens, steroidal or non-steroidal molecules designed to compete with estrogens and antagonize ERs. The variable patterns of activity of antiestrogens (AEs) in estrogen target tissues and the lack of systematic cross-resistance between different types of molecules have provided evidence for different mechanisms of action. AEs are typically classified as selective estrogen receptor modulators (SERMs), which display tissue-specific partial agonist activity (e.g. tamoxifen and raloxifene), or as pure AEs (e.g. fulvestrant), which enhance ERα post-translational modification by ubiquitin-like molecules and accelerate its proteasomal degradation. Characterization of second- and third-generation AEs, however, suggests the induction of diverse ERα structural conformations, resulting in variable degrees of receptor downregulation and different patterns of systemic properties in animal models and in the clinic.

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“…Involvement of the F-domain in the antagonist-dependent LBD dimerization occurred not only with the AF-2-mutated ERα but also with WT ERα (28). A portion of the antagonistic effect of ICI on WT ERα results from the stimulation of ERα proteolysis (28)(29)(30), and it was recently reported that ICI induces SUMOylation of human ERα protein and that the mutations of H12 reduced SUMOylation in the presence of ICI (31). These results suggest that the prevention of ICI-dependent proteolysis maintains the dimer formation of AF-2-mutated ERα and that this increases ERE binding and transcription activation.…”

Section: Ici Acts As An Erα Agonist On Trabecular Bone Mass and Uterumentioning

confidence: 99%

The estrogen receptor antagonist ICI 182,780 can act both as an agonist and an inverse agonist when estrogen receptor α AF-2 is modified

Movérare‐Skrtic

Börjesson

Farman

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

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Significance Estrogen exerts important effects in the skeleton, which are primarily mediated via estrogen receptor (ER)α, which stimulates target gene transcription through two activation functions (AFs), AF-1 in the N-terminal and AF-2 in the ligand-binding domain. Previous studies demonstrate that ERα ligands might act as agonists, partial agonists, or antagonists. We demonstrate that the ERα antagonist ICI 182,780 (ICI) acts in a tissue-dependent manner in mice lacking ERαAF-2, resulting in no effect, agonistic activity, or inverse agonistic activity. Importantly, ICI exerted a pronounced inverse agonistic activity in the growth plate of mice lacking ERαAF-2. We propose that ERα lacking AF-2 is constitutively active in the absence of ligand in the growth plate, enabling ICI to act as an inverse agonist.

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Role of SUMOylation in Full Antiestrogenicity

Cited by 23 publications

References 96 publications

RETRACTED ARTICLE: Regulation of estrogen receptor signaling in breast carcinogenesis and breast cancer therapy

RETRACTED ARTICLE: Regulation of estrogen receptor signaling in breast carcinogenesis and breast cancer therapy

Antiestrogens: structure-activity relationships and use in breast cancer treatment

The estrogen receptor antagonist ICI 182,780 can act both as an agonist and an inverse agonist when estrogen receptor α AF-2 is modified

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