Literature DB >> 22740892

SNRPE is involved in cell proliferation and progression of high-grade prostate cancer through the regulation of androgen receptor expression.

Takashi Anchi1, Kenji Tamura, Mutsuo Furihata, Hirofumi Satake, Hatsune Sakoda, Chiaki Kawada, Maiko Kamei, Tsutomu Shimamoto, Hideo Fukuhara, Satoshi Fukata, Shingo Ashida, Takashi Karashima, Ichiro Yamasaki, Masaharu Yasuda, Masayuki Kamada, Keiji Inoue, Taro Shuin.   

Abstract

Clinically high-grade prostate cancers (PC) with high Gleason scores of 8-10 exhibit rapid growth and are more likely to spread beyond the prostate. These cancer types demonstrate a poor response to androgen deprivation therapy and eventually acquire a castration-resistant phenotype. To identify novel molecular cancer drug targets, we previously analyzed the gene expression profiles of high-grade PC using a cDNA microarray combined with laser microbeam microdissection and found a number of genes that are transactivated in high-grade PC. Among these genes, we report the identification of a novel molecular target, small nuclear ribonucleoprotein polypeptide E (SNRPE). Semi-quantitative RT-PCR confirmed that SNRPE is overexpressed in high-grade PC cells compared with normal prostatic epithelial cells. Knockdown of SNRPE expression by short interfering RNA (siRNA) resulted in the marked suppression of PC cell proliferation. By contrast, SNRPE overexpression promoted PC cell proliferation, indicating its oncogenic effects. Furthermore, we demonstrated that SNRPE regulates androgen receptor (AR) mRNA expression in PC cells. Knockdown of SNRPE expression by siRNA resulted in the marked suppression of AR and its downstream target genes at the mRNA level. We suggest that the regulation of AR expression by SNRPE is essential for cell proliferation and progression of high-grade PC and that it may be a novel molecular target for cancer drugs.

Entities:  

Year:  2011        PMID: 22740892      PMCID: PMC3362443          DOI: 10.3892/ol.2011.505

Source DB:  PubMed          Journal:  Oncol Lett        ISSN: 1792-1074            Impact factor:   2.967


  18 in total

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Review 2.  Trends and patterns of prostate cancer: what do they suggest?

Authors:  A W Hsing; S S Devesa
Journal:  Epidemiol Rev       Date:  2001       Impact factor: 6.222

3.  Novel Sm-like proteins with long C-terminal tails and associated methyltransferases.

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Review 4.  Biology of progressive, castration-resistant prostate cancer: directed therapies targeting the androgen-receptor signaling axis.

Authors:  Howard I Scher; Charles L Sawyers
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5.  Disruption of androgen receptor function inhibits proliferation of androgen-refractory prostate cancer cells.

Authors:  Ofelia L Zegarra-Moro; Lucy J Schmidt; Haojie Huang; Donald J Tindall
Journal:  Cancer Res       Date:  2002-02-15       Impact factor: 12.701

Review 6.  The development of androgen-independent prostate cancer.

Authors:  B J Feldman; D Feldman
Journal:  Nat Rev Cancer       Date:  2001-10       Impact factor: 60.716

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Authors:  Henrik Grönberg
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8.  Molecular determinants of resistance to antiandrogen therapy.

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9.  Molecular features of hormone-refractory prostate cancer cells by genome-wide gene expression profiles.

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Journal:  Cancer Res       Date:  2007-06-01       Impact factor: 12.701

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Authors:  B Séraphin
Journal:  EMBO J       Date:  1995-05-01       Impact factor: 11.598

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6.  SNRPD1/E/F/G Serve as Potential Prognostic Biomarkers in Lung Adenocarcinoma.

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Journal:  Front Genet       Date:  2022-03-03       Impact factor: 4.599

7.  The comprehensive expression and functional analysis of m6A modification "readers" in hepatocellular carcinoma.

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8.  SHISA2 enhances the aggressive phenotype in prostate cancer through the regulation of WNT5A expression.

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Journal:  Oncol Lett       Date:  2017-09-28       Impact factor: 2.967

9.  Stromal regulation of prostate cancer cell growth by mevalonate pathway enzymes HMGCS1 and HMGCR.

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Journal:  Oncol Lett       Date:  2017-09-22       Impact factor: 2.967

10.  Comparison of regulatory networks of E74-like factor 1 and cold-shock domain-containing E1 in breast cancer cell lines using ChIP datasets.

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Journal:  Exp Ther Med       Date:  2020-10-22       Impact factor: 2.447

  10 in total

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