Activation of the Src/p21ras/Erk pathway by progesterone receptor via cross-talk with estrogen receptor

Migliaccio, Antimo; Piccolo, Domenico; Castoria, Gabriella; Domenico, Marina Di; Bilancio, Antonio; Lombardi, Maria; Gong, Wenrong; Beato, Miguel; Auricchio, Ferdinando

doi:10.1093/emboj/17.7.2008

Cited by 573 publications

(522 citation statements)

References 64 publications

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“…This is in agreement with reports of ER and PR activating MAP kinase through the Ras-Raf-1-MEK pathway (Migliaccio et al, , 1998. In addition, we have shown for the AR that PI3 kinase and PKC also contribute to the DHT-mediated activation of MAP kinase.…”

Section: Discussionsupporting

confidence: 93%

“…In addition, a number of steroid hormones are reported to rapidly and reversibly activate important intermediates in signal transduction pathways known to trigger cell proliferation (Migliaccio et al, , 1998Endoh et al, 1997;Marcinkowska et al, 1997). For example estrogens activate two members in the family of c-srcrelated tyrosine kinases, c-src and c-yes as well as the MAP kinases Erk-1 and -2 (Di .…”

Section: Introductionmentioning

confidence: 99%

“…For example estrogens activate two members in the family of c-srcrelated tyrosine kinases, c-src and c-yes as well as the MAP kinases Erk-1 and -2 (Di . Progestins also activate MAP kinase, a reaction that has been correlated with an indirect association of the progesterone receptor (PR) with c-src through the intermediary role of the estrogen receptor (ER) (Migliaccio et al, 1998). Interaction of the PR and ER with c-src either directly or indirectly enhances the kinase activity of this protein which then activates MAP kinase via the Ras-Raf-1 pathway (Castoria et al, 1999).…”

Section: Introductionmentioning

confidence: 99%

“…We therefore report here a rapid cellular signalling response which appears to be speci®c for the AR. a novel non-conventional mechanism (Migliaccio et al, , 1998Endoh et al, 1997;Marcinkowska et al, 1997). In this study we have asked whether androgens also mediate this response using two primary androgen responsive cells: human genital skin ®broblasts and prostatic stromal cells.…”

Section: Introductionmentioning

confidence: 99%

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Rapid signalling by androgen receptor in prostate cancer cells

Peterziel¹,

Mink²,

Schonert³

et al. 1999

Oncogene

234

157

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Androgens are important growth regulators in prostate cancer. Their known mode of action in target cells requires binding to a cytoplasmic androgen receptor followed by a nuclear translocation event and modulation of the expression of speci®c genes. Here, we report another mode of action of this receptor. Treatment of androgen responsive prostate cancer cells with dihydrotestosterone leads to a rapid and reversible activation of mitogen-activated protein kinases MAPKs (also called extracellular signal-regulated kinases or Erks). Transient transfection assays demonstrated that the androgen receptor-mediated activation of MAP kinase results in enhanced activity of the transcription factor Elk-1. This action of the androgen receptor di ers from its known transcriptional activity since it is rapid and insensitive to androgen antagonists such as hydroxy¯utamide or casodex. Biochemical studies as well as analyses with dominant negative mutants showed the involvement of kinases such as MAPK/Erk kinase, phosphatidyl-inositol 3-kinase and protein kinase C in the androgen receptormediated activation of MAP kinase. These results demonstrate a novel regulatory action of the androgen receptor and prove that in addition to its known transcriptional e ects, it also uses non-conventional means to modulate several cellular signalling processes.

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Section: Discussionsupporting

confidence: 93%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Rapid signalling by androgen receptor in prostate cancer cells

Peterziel¹,

Mink²,

Schonert³

et al. 1999

Oncogene

234

157

View full text Add to dashboard Cite

show abstract

“…Western blotting using phospho-specific antibodies indicated that EGF stimulation of T47D cells induces phosphorylation of PR Ser294 at 5-10 min, similar to that induced by R5020 at early time points (15,16). Both agents are known to activate MAPKs within 5-15 minutes (25,26). However, EGF is a stronger activator of MAPK relative to progestins at this time point, and liganded PRs are relatively transient, most likely due to the rapid down-regulation of liganded and Ser294 phosphorylated species (14).…”

Section: Egf Induces Pr Nuclear Association and Pre Bindingmentioning

confidence: 88%

Linkage of progestin and epidermal growth factor signaling: Phosphorylation of progesterone receptors mediates transcriptional hypersensitivity and increased ligand-independent breast cancer cell growth

et al. 2007

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Progesterone receptor (PR) action is linked to epidermal growth factor (EGF) initiated signaling pathways at multiple levels; mitogen-activated protein kinases (MAPKs) are key mediators of this important cross-talk. Herein, we probed the effects of EGF on PR function and regulation of breast cancer cell growth. EGF stimulated rapid and transient phosphorylation of PR-B Ser294 relative to persistent phosphorylation of this site induced by the synthetic progestin, R5020. EGF induced nuclear translocation and DNA binding of unliganded wild-type, but not mutant PRs containing an Ala at position 294 (S294A). However, EGF alone induced little to no PR-B transcriptional activity; S294A PR-B was transcriptionally impaired. In contrast, pretreatment of cells with EGF (30 min) significantly increased the potency and efficacy of wild-type, but not S294A PR transcriptional activity in response to progestin, and enhanced ligand-dependent downregulation of wild-type but not S294A PR. Replacement of Ser294 with aspartic acid (S294D) to mimic phosphorylation at this site decreased receptor stability and, as predicted, heightened progestin-induced transcription relative to wild-type PR-B. RT-PCR demonstrated the Ser294 phosphorylation-dependence of selected PR target genes (TGFα and HB-EGF). Surprisingly, PR-B expressing cells growing in soft agar were highly responsive to EGF or progestin, and this was further stimulated by the combination of both hormones. Cells expressing S294A PR exhibited reduced soft agar growth, and were also sensitive to R5020 alone, but failed to respond to EGF. These results suggest that PR Ser294 is an important "sensor" for growth factor inputs that affects PR function and breast cancer cell growth in the absence of progestin or in the presence of low or "sub-threshold" progestin concentrations. PR function likely contributes to breast cancer progression when EGFR family members or their ligands are overexpressed, a condition that predicts low abundance, but highly active and nuclear PR.

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Steroid Hormone Receptors

Beato

Klug

2002

Encyclopedia of Molecular Biology

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Activation of the Src/p21ras/Erk pathway by progesterone receptor via cross-talk with estrogen receptor

Cited by 573 publications

References 64 publications

Rapid signalling by androgen receptor in prostate cancer cells

Rapid signalling by androgen receptor in prostate cancer cells

Linkage of progestin and epidermal growth factor signaling: Phosphorylation of progesterone receptors mediates transcriptional hypersensitivity and increased ligand-independent breast cancer cell growth

Steroid Hormone Receptors

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