The cistrome and gene signature of androgen receptor splice variants in castration resistant prostate cancer cells

Ji Lu; Peter E. Lonergan; Lucas P. Nacusi; Liguo Wang; Lucy J. Schmidt; Zhifu Sun; Travis Van Der Steen; Stephen A. Boorjian; Farhad Kosari; George Vasmatzis; George G. Klee; Steven P. Balk; Haojie Huang; Chunxi Wang; Donald J. Tindall

doi:10.1016/j.juro.2014.08.043

The cistrome and gene signature of androgen receptor splice variants in castration resistant prostate cancer cells

Ji Lu, Peter E. Lonergan, Lucas P. Nacusi, Liguo Wang, Lucy J. Schmidt, Zhifu Sun, Travis Van Der Steen, Stephen A. Boorjian, Farhad Kosari, George Vasmatzis, George G. Klee, Steven P. Balk, Haojie Huang, Chunxi Wang, Donald J. Tindall

Research output: Contribution to journal › Article › peer-review

40 Scopus citations

Abstract

Purpose Spliced variant forms of androgen receptor were recently identified in castration resistant prostate cancer cell lines and clinical samples. We identified the cistrome and gene signature of androgen receptor splice variants in castration resistant prostate cancer cell lines and determined the clinical significance of androgen receptor splice variant regulated genes. Materials and Methods The castration resistant prostate cancer cell line 22Rv1, which expresses full-length androgen receptor and androgen receptor splice variants endogenously, was used as the research model. We established 22Rv1-ARFL^-/ARV⁺ and 22Rv1-ARFL^-/ARV^- through RNA interference. Chromatin immunoprecipitation coupled with next generation sequencing and microarray techniques were used to identify the cistrome and gene expression profiles of androgen receptor splice variants in the absence of androgen. Results Androgen receptor splice variant binding sites were identified in 22Rv1-ARFL^-/ARV⁺. A gene set was regulated uniquely by androgen receptor splice variants but not by full-length androgen receptor in the absence of androgen. Integrated analysis revealed that some genes were directly modulated by androgen receptor splice variants. Unsupervised clustering analysis showed that the androgen receptor splice variant gene signature differentiated benign from malignant prostate tissue as well as localized prostate cancer from metastatic castration resistant prostate cancer specimens. Some genes that were modulated uniquely by androgen receptor splice variants also correlated with histological grade and biochemical failure. Conclusions Androgen receptor splice variants can bind to DNA independent of full-length androgen receptor in the absence of androgen and modulate a unique set of genes that is not regulated by full-length androgen receptor. The androgen receptor splice variant gene signature correlates with disease progression. It distinguishes primary cancer from castration resistant prostate cancer specimens and benign from malignant prostate specimens.

Original language	English (US)
Pages (from-to)	690-698
Number of pages	9
Journal	Journal of Urology
Volume	193
Issue number	2
DOIs	https://doi.org/10.1016/j.juro.2014.08.043
State	Published - Feb 1 2015

Keywords

alternative splicing
disease progression
prostatic neoplasms, castration-resistant
receptors, androgen
transcriptome

ASJC Scopus subject areas

Urology

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10.1016/j.juro.2014.08.043

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Lu, J., Lonergan, P. E., Nacusi, L. P., Wang, L., Schmidt, L. J., Sun, Z., Van Der Steen, T., Boorjian, S. A., Kosari, F., Vasmatzis, G., Klee, G. G., Balk, S. P., Huang, H., Wang, C., & Tindall, D. J. (2015). The cistrome and gene signature of androgen receptor splice variants in castration resistant prostate cancer cells. Journal of Urology, 193(2), 690-698. https://doi.org/10.1016/j.juro.2014.08.043

Lu, J, Lonergan, PE, Nacusi, LP, Wang, L, Schmidt, LJ, Sun, Z, Van Der Steen, T, Boorjian, SA, Kosari, F , Vasmatzis, G, Klee, GG, Balk, SP, Huang, H, Wang, C & Tindall, DJ 2015, 'The cistrome and gene signature of androgen receptor splice variants in castration resistant prostate cancer cells', Journal of Urology, vol. 193, no. 2, pp. 690-698. https://doi.org/10.1016/j.juro.2014.08.043

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title = "The cistrome and gene signature of androgen receptor splice variants in castration resistant prostate cancer cells",

abstract = "Purpose Spliced variant forms of androgen receptor were recently identified in castration resistant prostate cancer cell lines and clinical samples. We identified the cistrome and gene signature of androgen receptor splice variants in castration resistant prostate cancer cell lines and determined the clinical significance of androgen receptor splice variant regulated genes. Materials and Methods The castration resistant prostate cancer cell line 22Rv1, which expresses full-length androgen receptor and androgen receptor splice variants endogenously, was used as the research model. We established 22Rv1-ARFL-/ARV+ and 22Rv1-ARFL-/ARV- through RNA interference. Chromatin immunoprecipitation coupled with next generation sequencing and microarray techniques were used to identify the cistrome and gene expression profiles of androgen receptor splice variants in the absence of androgen. Results Androgen receptor splice variant binding sites were identified in 22Rv1-ARFL-/ARV+. A gene set was regulated uniquely by androgen receptor splice variants but not by full-length androgen receptor in the absence of androgen. Integrated analysis revealed that some genes were directly modulated by androgen receptor splice variants. Unsupervised clustering analysis showed that the androgen receptor splice variant gene signature differentiated benign from malignant prostate tissue as well as localized prostate cancer from metastatic castration resistant prostate cancer specimens. Some genes that were modulated uniquely by androgen receptor splice variants also correlated with histological grade and biochemical failure. Conclusions Androgen receptor splice variants can bind to DNA independent of full-length androgen receptor in the absence of androgen and modulate a unique set of genes that is not regulated by full-length androgen receptor. The androgen receptor splice variant gene signature correlates with disease progression. It distinguishes primary cancer from castration resistant prostate cancer specimens and benign from malignant prostate specimens.",

keywords = "alternative splicing, disease progression, prostatic neoplasms, castration-resistant, receptors, androgen, transcriptome",

author = "Ji Lu and Lonergan, {Peter E.} and Nacusi, {Lucas P.} and Liguo Wang and Schmidt, {Lucy J.} and Zhifu Sun and {Van Der Steen}, Travis and Boorjian, {Stephen A.} and Farhad Kosari and George Vasmatzis and Klee, {George G.} and Balk, {Steven P.} and Haojie Huang and Chunxi Wang and Tindall, {Donald J.}",

note = "Publisher Copyright: {\textcopyright} 2015 American Urological Association Education and Research, Inc.",

year = "2015",

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doi = "10.1016/j.juro.2014.08.043",

language = "English (US)",

volume = "193",

pages = "690--698",

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T1 - The cistrome and gene signature of androgen receptor splice variants in castration resistant prostate cancer cells

AU - Lu, Ji

AU - Lonergan, Peter E.

AU - Nacusi, Lucas P.

AU - Wang, Liguo

AU - Schmidt, Lucy J.

AU - Sun, Zhifu

AU - Van Der Steen, Travis

AU - Boorjian, Stephen A.

AU - Kosari, Farhad

AU - Vasmatzis, George

AU - Klee, George G.

AU - Balk, Steven P.

AU - Huang, Haojie

AU - Wang, Chunxi

AU - Tindall, Donald J.

PY - 2015/2/1

Y1 - 2015/2/1

N2 - Purpose Spliced variant forms of androgen receptor were recently identified in castration resistant prostate cancer cell lines and clinical samples. We identified the cistrome and gene signature of androgen receptor splice variants in castration resistant prostate cancer cell lines and determined the clinical significance of androgen receptor splice variant regulated genes. Materials and Methods The castration resistant prostate cancer cell line 22Rv1, which expresses full-length androgen receptor and androgen receptor splice variants endogenously, was used as the research model. We established 22Rv1-ARFL-/ARV+ and 22Rv1-ARFL-/ARV- through RNA interference. Chromatin immunoprecipitation coupled with next generation sequencing and microarray techniques were used to identify the cistrome and gene expression profiles of androgen receptor splice variants in the absence of androgen. Results Androgen receptor splice variant binding sites were identified in 22Rv1-ARFL-/ARV+. A gene set was regulated uniquely by androgen receptor splice variants but not by full-length androgen receptor in the absence of androgen. Integrated analysis revealed that some genes were directly modulated by androgen receptor splice variants. Unsupervised clustering analysis showed that the androgen receptor splice variant gene signature differentiated benign from malignant prostate tissue as well as localized prostate cancer from metastatic castration resistant prostate cancer specimens. Some genes that were modulated uniquely by androgen receptor splice variants also correlated with histological grade and biochemical failure. Conclusions Androgen receptor splice variants can bind to DNA independent of full-length androgen receptor in the absence of androgen and modulate a unique set of genes that is not regulated by full-length androgen receptor. The androgen receptor splice variant gene signature correlates with disease progression. It distinguishes primary cancer from castration resistant prostate cancer specimens and benign from malignant prostate specimens.

AB - Purpose Spliced variant forms of androgen receptor were recently identified in castration resistant prostate cancer cell lines and clinical samples. We identified the cistrome and gene signature of androgen receptor splice variants in castration resistant prostate cancer cell lines and determined the clinical significance of androgen receptor splice variant regulated genes. Materials and Methods The castration resistant prostate cancer cell line 22Rv1, which expresses full-length androgen receptor and androgen receptor splice variants endogenously, was used as the research model. We established 22Rv1-ARFL-/ARV+ and 22Rv1-ARFL-/ARV- through RNA interference. Chromatin immunoprecipitation coupled with next generation sequencing and microarray techniques were used to identify the cistrome and gene expression profiles of androgen receptor splice variants in the absence of androgen. Results Androgen receptor splice variant binding sites were identified in 22Rv1-ARFL-/ARV+. A gene set was regulated uniquely by androgen receptor splice variants but not by full-length androgen receptor in the absence of androgen. Integrated analysis revealed that some genes were directly modulated by androgen receptor splice variants. Unsupervised clustering analysis showed that the androgen receptor splice variant gene signature differentiated benign from malignant prostate tissue as well as localized prostate cancer from metastatic castration resistant prostate cancer specimens. Some genes that were modulated uniquely by androgen receptor splice variants also correlated with histological grade and biochemical failure. Conclusions Androgen receptor splice variants can bind to DNA independent of full-length androgen receptor in the absence of androgen and modulate a unique set of genes that is not regulated by full-length androgen receptor. The androgen receptor splice variant gene signature correlates with disease progression. It distinguishes primary cancer from castration resistant prostate cancer specimens and benign from malignant prostate specimens.

KW - alternative splicing

KW - disease progression

KW - prostatic neoplasms, castration-resistant

KW - receptors, androgen

KW - transcriptome

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The cistrome and gene signature of androgen receptor splice variants in castration resistant prostate cancer cells

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