Hey1, a Mediator of Notch Signaling, Is an Androgen Receptor Corepressor

Belandia, Borja; Powell, Susan; García-Pedrero, Juana M.; Walker, Marjorie M.; Bevan, Charlotte L.; Parker, Malcolm G.

doi:10.1128/mcb.25.4.1425-1436.2005

Cited by 126 publications

(143 citation statements)

References 31 publications

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“…However, recent reports aimed to define possible mechanisms leading to hormone resistance in prostate cancer identified specific alterations (cytoplasmic vs nuclear localization) of Notch modulators in prostate cancer, namely Hey1, which acts as corepressor of androgen receptor-mediated signaling and represses bHLH transcription factors, such as hASH1. 32 Abnormalities of Notch itself or Notch-positive effectors might be responsible for both the development of androgen-independent prostate cancers as well as of the de-repression of hASH1 transcriptional activities with the development of neuroendocrine-differentiated tumor clones. In this respect, our data on the lack of correlation between Notch1 and Hes1 and the presence of neuroendocrine phenotype in prostate tissues is inconclusive, and more detailed experiments are needed to clarify the activation status of such molecules in prostate cancer with neuroendocrine differentiation.…”

Section: Discussionmentioning

confidence: 99%

Human ASH1 expression in prostate cancer with neuroendocrine differentiation

et al. 2008

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Neuroendocrine differentiation in prostate cancer correlates with overall prognosis and disease progression after androgen-deprivation therapy, although its specific mechanisms are currently poorly understood. A role of Notch pathway has been reported in determining neuroendocrine phenotype of normal and neoplastic tissues. The aim of this study was to analyze whether this pathway might affect neuroendocrine differentiation in prostate cancer. Human achaete-scute homolog 1 (hASH1), a pivotal member of the Notch pathway, was investigated in 80 prostate cancers selected and grouped according to chromogranin A immunohistochemistry, as follows: prostate cancers without neuroendocrine differentiation, untreated (25 cases); prostate cancers with neuroendocrine differentiation, untreated (40 cases); prostate cancers with previous androgen-deprivation therapy, all having neuroendocrine differentiation (15 cases). Human ASH1 protein was analyzed by immunohistochemistry, whereas the presence of hASH1 mRNA transcripts was investigated on paraffin material by real-time PCR. By immunohistochemistry, hASH1 was colocalized with chromogranin A in neuroendocrine cells of normal prostatic gland. It was absent in all but one prostate cancers without neuroendocrine differentiation, whereas it was positive in 25% of prostate cancers with neuroendocrine differentiation/ untreated, with a significant correlation with the extent of neuroendocrine features (P ¼ 0.02). Moreover, comparing untreated and treated prostate cancers with neuroendocrine differentiation, a positive association with androgen-deprivation therapy was observed (P ¼ 0.01). In prostate cancers with neuroendocrine differentiation, RNA analysis confirmed the association of higher transcript levels in androgen deprivationtreated compared with untreated patients (P ¼ 0.01). In addition, hASH1 mRNA analysis in microdissected chromogranin A-positive and chromogranin A-negative areas within the same tumor demonstrated a two-to sevenfold increase of hASH1 mRNA expression in chromogranin A-positive tumor cell populations.

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Section: Discussionmentioning

confidence: 99%

Human ASH1 expression in prostate cancer with neuroendocrine differentiation

et al. 2008

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“…In prostate cancer tissue, Hey1 localization was predominantly restricted to the cytoplasm. This localization is thought to abolish the repressive function of Hey1 on AR transcriptional activity (8). Prohibitin, another repressor of AR signaling, was shown to be downregulated by androgen treatment.…”

Section: Introductionmentioning

confidence: 99%

Inability of NCoR/SMRT to repress androgen receptor transcriptional activity in prostate cancer cell lines

Laschak

Bechtel²,

Spindler³

et al. 2011

Int J Mol Med

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Abstract. The molecular mechanisms leading to castrationresistant prostate cancer (CRPC) are poorly understood. Among several mechanisms leading to CRPC growth a dysregulation of androgen receptor (AR) co-regulators (i.e. up-regulation of co-activators or down-regulation of co-repressors) is discussed. There are numerous reports demonstrating an increased expression of co-activators during prostate cancer progression. On the contrary, the impact of co-repressors on tumor growth and development is less clear. In this study we compared the effects of two known co-repressors, NCoR and SMRT, on AR transcriptional activity in prostate cancer (PCa) cell lines and compared them to that in COS-1 cells. Interestingly, we found that NCoR/SMRT overexpression did not repress AR-dependent gene expression in the PCa cell lines, but rather activated it. This finding is probably due to an impaired AR-co-repressor interaction in the prostate cancer cell lines. In conclusion, we provide evidence that up-regulation of NCoR or SMRT may increase transcriptional activity of the AR in a cell type-specific context.

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“…Interestingly, the dimerization of AR, like other nuclear receptors, is driven by the D box in the second zincfinger of the DNA-binding domain (Haelens et al, 2003). Other AR repressors include histone deacetylase 1 (HDAC1) (Korkmaz et al, 2004), Hey1 (Belandia et al, 2005), PIASg (Gross et al, 2004), silencing mediator for retinoic acid and thyroid hormone receptor (SMRT) (Dotzlaw et al, 2002), and HBO1 (Sharma et al, 2000). AR coactivators include SRC-1 (Onate et al, 1998), TIF2 (Berrevoets et al, 1998), SRC-3 (also known as RAC3 or AIB1) (Zhou et al, 2005), and CBP (Aarnisalo et al, 1998), all of which are overexpressed in prostate cancer (Culig et al, 2004).…”

Section: Introductionmentioning

confidence: 99%

c-Jun enhancement of androgen receptor transactivation is associated with prostate cancer cell proliferation

Cai

et al. 2006

Oncogene

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Hey1, a Mediator of Notch Signaling, Is an Androgen Receptor Corepressor

Cited by 126 publications

References 31 publications

Human ASH1 expression in prostate cancer with neuroendocrine differentiation

Human ASH1 expression in prostate cancer with neuroendocrine differentiation

Inability of NCoR/SMRT to repress androgen receptor transcriptional activity in prostate cancer cell lines

c-Jun enhancement of androgen receptor transactivation is associated with prostate cancer cell proliferation

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