An Androgen Receptor NH2-terminal Conserved Motif Interacts with the COOH Terminus of the Hsp70-interacting Protein (CHIP)

He, Bin; Bai, Suxia; Hnat, Andrew T.; Kalman, Rebecca I.; Minges, John T.; Patterson, Cam; Wilson, Elizabeth M.

doi:10.1074/jbc.m403117200

Cited by 122 publications

(116 citation statements)

References 69 publications

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“…AR-E231G exhibits increased responsiveness to androgens [testosterone and 5a-dihydrotestosterone (DHT)] and estrogens (estradiol) in the presence of the co-activators, ARA70 and ARA160, 13 and decreased responsiveness to the co-repressor, CHIP. 19 Using enforced overexpression of wtAR, AR-T857A (described earlier), or AR-E231G specifically in the prostate of mice, we previously demonstrated the oncogenic capacity of the AR-E231G variant. 8 Although overexpression of wtAR or AR-T857A had no discernable phenotype, mice expressing AR-E231G recapitulated all stages of disease, developing prostatic intraepithelial neoplasia (PIN)-like lesions at 12 weeks of age and advanced prostate cancer with lung metastases by 50 weeks.…”

mentioning

confidence: 86%

A gene signature identified using a mouse model of androgen receptor‐dependent prostate cancer predicts biochemical relapse in human disease

Thompson

Day

Bianco‐Miotto

et al. 2012

Intl Journal of Cancer

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Mutations in the androgen receptor (AR) have been detected in experimental and clinical prostate tumors. Mice with enforced prostate-specific expression of one such receptor variant, AR-E231G, invariably develop prostatic intraepithelial neoplasia by 12 weeks and metastatic prostate cancer by 52 weeks. The aim of this study was to identify genes with altered expression in the prostates of AR-E231G mice at an early stage of disease that may act as drivers of AR-mediated tumorigenesis. The gene expression profile of AR-E231G prostate tissue from 12-week-old mice was compared to an equivalent profile from mice expressing the AR-T857A receptor variant (analogous to the AR-T877A variant in LNCaP cells), which do not develop prostate tumors. One hundred and thirty-two genes were differentially expressed in AR-E231G prostates. Classification of these genes revealed enrichment for cellular pathways known to be involved in prostate cancer, including cell cycle and lipid metabolism. Suppression of two genes upregulated in the AR-E231G model, ADM and CITED1, increased cell death and reduced proliferation of human prostate cancer cells. Many genes differentially expressed in AR-E231G prostates are also deregulated in human tumors. Three of these genes, ID4, NR2F1 and PTGDS, which were expressed at consistently lower levels in clinical prostate cancer compared to nonmalignant tissues, formed a signature that predicted biochemical relapse (hazard ratio 2.2, p 5 0.038). We believe that our findings support the value of this novel mouse model of prostate cancer to identify candidate therapeutic targets and/or biomarkers of human disease.

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mentioning

confidence: 86%

A gene signature identified using a mouse model of androgen receptor‐dependent prostate cancer predicts biochemical relapse in human disease

Thompson

Day

Bianco‐Miotto

et al. 2012

Intl Journal of Cancer

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“…Wild-type AR is one of the CHIP substrates (Cardozo et al, 2003;He et al, 2004). CHIP also interacts with misfolded proteins trapped by molecular chaperones and degrades them, thus acting as a "quality control" E3 (Cyr et al, 2002;Murata et al, 2003).…”

Section: Introductionmentioning

confidence: 99%

CHIP Overexpression Reduces Mutant Androgen Receptor Protein and Ameliorates Phenotypes of the Spinal and Bulbar Muscular Atrophy Transgenic Mouse Model

Adachi¹,

Waza²,

Tokui³

et al. 2007

J. Neurosci.

131

143

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Spinal and bulbar muscular atrophy (SBMA) is an inherited motor neuron disease caused by the expansion of a polyglutamine tract within the androgen receptor (AR). The pathologic features of SBMA are motor neuron loss in the spinal cord and brainstem and diffuse nuclear accumulation and nuclear inclusions of the mutant AR in the residual motor neurons and certain visceral organs. Many components of the ubiquitin-proteasome and molecular chaperones are also sequestered in the inclusions, suggesting that they may be actively engaged in an attempt to degrade or refold the mutant AR. C terminus of Hsc70 (heat shock cognate protein 70)-interacting protein (CHIP), a U-box type E3 ubiquitin ligase, has been shown to interact with heat shock protein 90 (Hsp90) or Hsp70 and ubiquitylates unfolded proteins trapped by molecular chaperones and degrades them. Here, we demonstrate that transient overexpression of CHIP in a neuronal cell model reduces the monomeric mutant AR more effectively than it does the wild type, suggesting that the mutant AR is more sensitive to CHIP than is the wild type. High expression of CHIP in an SBMA transgenic mouse model also ameliorated motor symptoms and inhibited neuronal nuclear accumulation of the mutant AR. When CHIP was overexpressed in transgenic SBMA mice, mutant AR was also preferentially degraded over wild-type AR. These findings suggest that CHIP overexpression ameliorates SBMA phenotypes in mice by reducing nuclear-localized mutant AR via enhanced mutant AR degradation. Thus, CHIP overexpression would provide a potential therapeutic avenue for SBMA.

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“…Other vectors used were as follows: VP-AR-(1-660) (11,14); transcriptional intermediary factor 2 (TIF2)-AR fusion protein TIF2(LXXLL) 3 AR-(172-919) (18); pSG5-TIF2 and VP-TIF2-(624 -1287) (VP-TIF2.1) (23); wild-type and mutant pcDNA3-AR-(624 -919) (10,14); and 5XGAL4Luc3 (16). GST-SRC1-IV (GST-SRC1-(1139 -1441)) was created by digesting GAL-SRC1-(1139 -1441) with XbaI (blunt-ended) and BamHI, and the fragment was subcloned into pGEX-3X digested with EcoRI (blunt-ended) and BamHI.…”

Section: Methodsmentioning

confidence: 99%

mentioning

confidence: 99%

“…Like other steroid receptors, the androgen receptor (AR) 3 mediates transcriptional activation primarily through two domains. Activation function 1 (AF1) in the NH 2 -terminal region is the major transactivation domain (2) but is not well conserved across species (3). Activation function 2 (AF2) in the ligand binding domain is a highly conserved hydrophobic surface that is stabilized by agonist binding and required for SRC/p160 coactivator recruitment.…”

mentioning

confidence: 99%

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Probing the Functional Link between Androgen Receptor Coactivator and Ligand-binding Sites in Prostate Cancer and Androgen Insensitivity

Gampe

Hnat

et al. 2006

Journal of Biological Chemistry

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An Androgen Receptor NH2-terminal Conserved Motif Interacts with the COOH Terminus of the Hsp70-interacting Protein (CHIP)

Cited by 122 publications

References 69 publications

A gene signature identified using a mouse model of androgen receptor‐dependent prostate cancer predicts biochemical relapse in human disease

A gene signature identified using a mouse model of androgen receptor‐dependent prostate cancer predicts biochemical relapse in human disease

CHIP Overexpression Reduces Mutant Androgen Receptor Protein and Ameliorates Phenotypes of the Spinal and Bulbar Muscular Atrophy Transgenic Mouse Model

Probing the Functional Link between Androgen Receptor Coactivator and Ligand-binding Sites in Prostate Cancer and Androgen Insensitivity

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