The Landscape of microRNA Targeting in Prostate Cancer Defined by AGO-PAR-CLIP

Mark P. Hamilton; Kimal I. Rajapakshe; David A. Bader; Jasmina Z. Cerne; Eric A. Smith; Cristian Coarfa; Sean M. Hartig; Sean E. McGuire

doi:10.1016/j.neo.2016.04.008

The Landscape of microRNA Targeting in Prostate Cancer Defined by AGO-PAR-CLIP

Mark P. Hamilton, Kimal I. Rajapakshe, David A. Bader, Jasmina Z. Cerne, Eric A. Smith, Cristian Coarfa, Sean M. Hartig, Sean E. McGuire

Radiation Oncology

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

40 Scopus citations

Abstract

MicroRNA (miRNA) deregulation in prostate cancer (PCa) contributes to PCa initiation and metastatic progression. To comprehensively define the cancer-associated changes in miRNA targeting and function in commonly studied models of PCa, we performed photoactivatable ribonucleoside-enhanced cross-linking immunoprecipitation of the Argonaute protein in a panel of PCa cell lines modeling different stages of PCa progression. Using this comprehensive catalogue of miRNA targets, we analyzed miRNA targeting on known drivers of PCa and examined tissue-specific and stage-specific pathway targeting by miRNAs. We found that androgen receptor is the most frequently targeted PCa oncogene and that miR-148a targets the largest number of known PCa drivers. Globally, tissue-specific and stage-specific changes in miRNA targeting are driven by homeostatic response to active oncogenic pathways. Our findings indicate that, even in advanced PCa, the miRNA pool adapts to regulate continuing alterations in the cancer genome to balance oncogenic molecular changes. These findings are important because they are the first to globally characterize miRNA changes in PCa and demonstrate how the miRNA target spectrum responds to staged tumorigenesis.

Original language	English (US)
Pages (from-to)	356-370
Number of pages	15
Journal	Neoplasia (United States)
Volume	18
Issue number	6
DOIs	https://doi.org/10.1016/j.neo.2016.04.008
State	Published - Jun 1 2016

ASJC Scopus subject areas

Cancer Research

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@article{c2a957465f444dfcb0a33b68f5aee252,

title = "The Landscape of microRNA Targeting in Prostate Cancer Defined by AGO-PAR-CLIP",

abstract = "MicroRNA (miRNA) deregulation in prostate cancer (PCa) contributes to PCa initiation and metastatic progression. To comprehensively define the cancer-associated changes in miRNA targeting and function in commonly studied models of PCa, we performed photoactivatable ribonucleoside-enhanced cross-linking immunoprecipitation of the Argonaute protein in a panel of PCa cell lines modeling different stages of PCa progression. Using this comprehensive catalogue of miRNA targets, we analyzed miRNA targeting on known drivers of PCa and examined tissue-specific and stage-specific pathway targeting by miRNAs. We found that androgen receptor is the most frequently targeted PCa oncogene and that miR-148a targets the largest number of known PCa drivers. Globally, tissue-specific and stage-specific changes in miRNA targeting are driven by homeostatic response to active oncogenic pathways. Our findings indicate that, even in advanced PCa, the miRNA pool adapts to regulate continuing alterations in the cancer genome to balance oncogenic molecular changes. These findings are important because they are the first to globally characterize miRNA changes in PCa and demonstrate how the miRNA target spectrum responds to staged tumorigenesis.",

author = "Hamilton, {Mark P.} and Rajapakshe, {Kimal I.} and Bader, {David A.} and Cerne, {Jasmina Z.} and Smith, {Eric A.} and Cristian Coarfa and Hartig, {Sean M.} and McGuire, {Sean E.}",

note = "Funding Information: This work was supported by the Caroline Weiss Law Foundation (S. E. M.), the Baylor Research Advocates for Student Scientists, and the Robert and Janice McNair Foundation (M. P. H.). S. E. McGuire is a Dan L. Duncan Scholar and member of the Dan L. Duncan Cancer Center supported by National Cancer Institute Cancer Center Support Grant (P30CA125123). We acknowledge the joint participation by the Diana Helis Henry Medical Research Foundation through its direct engagement in the continuous active conduct of medical research. The National Institutes of Health (K01DK096093 to S. M. H., 1F30CA196108-01 to D. A. B.), the American Heart Association Beginning Grant-in-Aid (15BGIA25850025 to S. M. H.), the Cancer Prevention Research Institute of Texas (CPRIT RP150232 to C. C. and K. I. R.), and the Alkek Center for Molecular Discovery also funded portions of the work. Publisher Copyright: {\textcopyright} 2016 The Authors",

year = "2016",

month = jun,

day = "1",

doi = "10.1016/j.neo.2016.04.008",

language = "English (US)",

volume = "18",

pages = "356--370",

journal = "Neoplasia (United States)",

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T1 - The Landscape of microRNA Targeting in Prostate Cancer Defined by AGO-PAR-CLIP

AU - Hamilton, Mark P.

AU - Rajapakshe, Kimal I.

AU - Bader, David A.

AU - Cerne, Jasmina Z.

AU - Smith, Eric A.

AU - Coarfa, Cristian

AU - Hartig, Sean M.

AU - McGuire, Sean E.

N1 - Funding Information: This work was supported by the Caroline Weiss Law Foundation (S. E. M.), the Baylor Research Advocates for Student Scientists, and the Robert and Janice McNair Foundation (M. P. H.). S. E. McGuire is a Dan L. Duncan Scholar and member of the Dan L. Duncan Cancer Center supported by National Cancer Institute Cancer Center Support Grant (P30CA125123). We acknowledge the joint participation by the Diana Helis Henry Medical Research Foundation through its direct engagement in the continuous active conduct of medical research. The National Institutes of Health (K01DK096093 to S. M. H., 1F30CA196108-01 to D. A. B.), the American Heart Association Beginning Grant-in-Aid (15BGIA25850025 to S. M. H.), the Cancer Prevention Research Institute of Texas (CPRIT RP150232 to C. C. and K. I. R.), and the Alkek Center for Molecular Discovery also funded portions of the work. Publisher Copyright: © 2016 The Authors

PY - 2016/6/1

Y1 - 2016/6/1

N2 - MicroRNA (miRNA) deregulation in prostate cancer (PCa) contributes to PCa initiation and metastatic progression. To comprehensively define the cancer-associated changes in miRNA targeting and function in commonly studied models of PCa, we performed photoactivatable ribonucleoside-enhanced cross-linking immunoprecipitation of the Argonaute protein in a panel of PCa cell lines modeling different stages of PCa progression. Using this comprehensive catalogue of miRNA targets, we analyzed miRNA targeting on known drivers of PCa and examined tissue-specific and stage-specific pathway targeting by miRNAs. We found that androgen receptor is the most frequently targeted PCa oncogene and that miR-148a targets the largest number of known PCa drivers. Globally, tissue-specific and stage-specific changes in miRNA targeting are driven by homeostatic response to active oncogenic pathways. Our findings indicate that, even in advanced PCa, the miRNA pool adapts to regulate continuing alterations in the cancer genome to balance oncogenic molecular changes. These findings are important because they are the first to globally characterize miRNA changes in PCa and demonstrate how the miRNA target spectrum responds to staged tumorigenesis.

AB - MicroRNA (miRNA) deregulation in prostate cancer (PCa) contributes to PCa initiation and metastatic progression. To comprehensively define the cancer-associated changes in miRNA targeting and function in commonly studied models of PCa, we performed photoactivatable ribonucleoside-enhanced cross-linking immunoprecipitation of the Argonaute protein in a panel of PCa cell lines modeling different stages of PCa progression. Using this comprehensive catalogue of miRNA targets, we analyzed miRNA targeting on known drivers of PCa and examined tissue-specific and stage-specific pathway targeting by miRNAs. We found that androgen receptor is the most frequently targeted PCa oncogene and that miR-148a targets the largest number of known PCa drivers. Globally, tissue-specific and stage-specific changes in miRNA targeting are driven by homeostatic response to active oncogenic pathways. Our findings indicate that, even in advanced PCa, the miRNA pool adapts to regulate continuing alterations in the cancer genome to balance oncogenic molecular changes. These findings are important because they are the first to globally characterize miRNA changes in PCa and demonstrate how the miRNA target spectrum responds to staged tumorigenesis.

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DO - 10.1016/j.neo.2016.04.008

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SN - 1522-8002

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EP - 370

JO - Neoplasia (United States)

JF - Neoplasia (United States)

IS - 6

ER -

The Landscape of microRNA Targeting in Prostate Cancer Defined by AGO-PAR-CLIP

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