Intracellular gonadotropin-releasing hormone receptors in breast cancer and gonadotrope lineage cells

Sedgley, Kathleen R.; Finch, Ann R.; Caunt, Christopher J.; McArdle, Craig A.

doi:10.1677/joe.1.07067

Cited by 27 publications

(37 citation statements)

References 60 publications

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“…Our spatial observations are consistent with those previously reported by Sedgley et al [26] who also observed that in mammary (MCF7) cells the wild-type human GnRH-RI is inefficiently expressed at the plasma membrane. Our study is also consistent with previous biochemical data [8], [11], [27]–[31] that suggest both the wild-type and naturally occurring mutant human GnRH-RI are expressed inefficiently at the plasma membrane and are retained intracellularly, both in the presence and absence of agonist.…”

Section: Discussionsupporting

confidence: 93%

“…It also seems that in HEK 293 cells, Xenopus cytoplasmic tail sequences are not sufficient to visibly increase plasma membrane expression of the hGnRH-RI. This observation was unexpected since studies have demonstrated that cytoplasmic tail sequences potentiate the plasma membrane expression of GPCRs [50], [51], including that of the human GnRH-RI [26]. The differences observed in our HEK 293 cell-based study compared to the MCF7 cell-based study by Sedgley et al [26] suggests that nuclear localization might be cell type-dependent.…”

Section: Discussioncontrasting

confidence: 60%

“…This observation was unexpected since studies have demonstrated that cytoplasmic tail sequences potentiate the plasma membrane expression of GPCRs [50], [51], including that of the human GnRH-RI [26]. The differences observed in our HEK 293 cell-based study compared to the MCF7 cell-based study by Sedgley et al [26] suggests that nuclear localization might be cell type-dependent. This conclusion is in full agreement with those of Finch et al [52] who show variations in surface expression of the human GnRH-RI and chimeric HX-GnRH-RI among various cell lines reported to endogenously express GnRH-RI.…”

Section: Discussioncontrasting

confidence: 60%

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The Human Gonadotropin Releasing Hormone Type I Receptor Is a Functional Intracellular GPCR Expressed on the Nuclear Membrane

Pampillo

Savard

et al. 2010

PLoS ONE

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The mammalian type I gonadotropin releasing hormone receptor (GnRH-R) is a structurally unique G protein-coupled receptor (GPCR) that lacks cytoplasmic tail sequences and displays inefficient plasma membrane expression (PME). Compared to its murine counterparts, the primate type I receptor is inefficiently folded and retained in the endoplasmic reticulum (ER) leading to a further reduction in PME. The decrease in PME and concomitant increase in intracellular localization of the mammalian GnRH-RI led us to characterize the spatial distribution of the human and mouse GnRH receptors in two human cell lines, HEK 293 and HTR-8/SVneo. In both human cell lines we found the receptors were expressed in the cytoplasm and were associated with the ER and nuclear membrane. A molecular analysis of the receptor protein sequence led us to identify a putative monopartite nuclear localization sequence (NLS) in the first intracellular loop of GnRH-RI. Surprisingly, however, neither the deletion of the NLS nor the addition of the Xenopus GnRH-R cytoplasmic tail sequences to the human receptor altered its spatial distribution. Finally, we demonstrate that GnRH treatment of nuclei isolated from HEK 293 cells expressing exogenous GnRH-RI triggers a significant increase in the acetylation and phosphorylation of histone H3, thereby revealing that the nuclear-localized receptor is functional. Based on our findings, we conclude that the mammalian GnRH-RI is an intracellular GPCR that is expressed on the nuclear membrane. This major and novel discovery causes us to reassess the signaling potential of this physiologically and clinically important receptor.

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Section: Discussionsupporting

confidence: 93%

Section: Discussioncontrasting

confidence: 60%

Section: Discussioncontrasting

confidence: 60%

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The Human Gonadotropin Releasing Hormone Type I Receptor Is a Functional Intracellular GPCR Expressed on the Nuclear Membrane

Pampillo

Savard

et al. 2010

PLoS ONE

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“…2D). In addition, cellular proliferation decreased after addition of Buserelin or other GnRH agonists, this depended either on the amount of GnRH at cell surfaces or on receptor functionality (61,124). Concerning the molecular mechanism employed by GnRHR in breast cancer cells to reduce cell proliferation in MCF-7 cells, the direct inhibitory effects of Buserelin on breast cancer cells was mediated, at least in part, by an antagonists effect on the EGF receptor (125) and IGF receptor (126) (Fig.…”

Section: Gnrhr and Ovarian Cancermentioning

confidence: 95%

Human gonadotropin-releasing hormone receptor-activated cellular functions and signaling pathways in extra-pituitary tissues and cancer cells (Review)

Aguilar-Rojas¹

2009

Oncol Rep

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Abstract. Human gonadotropin-releasing hormone receptor (GnRHR) and its natural ligand human gonadotropin-releasing hormone (GnRH) were initially described as signaling complexes that play a key role in reproductive functions. By binding to specific receptors present on pituitary gonadotropes, GnRH regulates the sperm and ovum maturation, as well as steroidogenesis within the context of the hypothalamushypophysis axis. The expression of GnRH and its receptor has clearly been established in many extra-pituitary organs.

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“…Growth effects of GnRH analogs on breast cancer cells depend on the amount of GnRH at cell surfaces and on receptor functionality [12,31], therefore quantification of expression levels holds a specific interest to predict cellular responses. Furthermore, GnRH receptors may contribute to the breast tumor responsiveness to pharmacotherapy with GnRH analogs and thus estimation of expression levels could define a more sensitive patient subpopulation.…”

Section: Discussionmentioning

confidence: 99%

Gonadotropin-releasing hormone neuropeptides and receptor in human breast cancer: Correlation to poor prognosis parameters

et al. 2013

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a b s t r a c tExpression of the two gonadotropin-releasing hormone homologue peptides GnRHI and GnRHII and their receptor GnRHR has been demonstrated in a number of malignancies. In hormone-dependent breast cancer, GnRH analogs are used for therapy in premenopausal women. Gene expression of GnRHI, II and R was studied in breast biopsies from primary breast adenocarcinoma obtained from the tumor and the adjacent benign tissue. Levels were evaluated by a multiplex real-time RT-PCR. GnRHI transcripts were detected in 14.7% of the benign and 29.4% malignant biopsies and GnRHII in 21.2% benign and 44.1% malignant biopsies. GnRHR was also more frequent in the malignant (54.2%) than in the benign (24.0%) biopsies, at similar expression levels. No transcripts were detected in biopsies from healthy individuals. There was a strong correlation between the presence of GnRHI and GnRHII transcripts and their receptor in the benign and the malignant biopsies. GnRHI, II and R expression correlated significantly with poor prognosis pathological parameters. Immunohistochemistry for GnRHR revealed expression in malignant cells and in epithelial cells of mammary ducts of the adjacent area with pre-cancerous features. In contrast, GnRH I and II peptides were rarely expressed at low levels in breast cancer cells. In conclusion GnRH peptides and receptor are expressed more frequently in breast tumors than in the adjacent mammary tissue, representing a malignant feature. Their expression correlated to tumor characteristics of poor prognosis and was therefore related to more aggressive malignancies. Concomitant expression of peptides and receptor supports an autocrine/paracrine regulating role.

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Intracellular gonadotropin-releasing hormone receptors in breast cancer and gonadotrope lineage cells

Cited by 27 publications

References 60 publications

The Human Gonadotropin Releasing Hormone Type I Receptor Is a Functional Intracellular GPCR Expressed on the Nuclear Membrane

The Human Gonadotropin Releasing Hormone Type I Receptor Is a Functional Intracellular GPCR Expressed on the Nuclear Membrane

Human gonadotropin-releasing hormone receptor-activated cellular functions and signaling pathways in extra-pituitary tissues and cancer cells (Review)

Gonadotropin-releasing hormone neuropeptides and receptor in human breast cancer: Correlation to poor prognosis parameters

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