The neuronal repellent SLIT2 is a target for repression by EZH2 in prostate cancer

J Yu; Q Cao; J Yu; L Wu; Ashraf Dallol; J Li; G Chen; C Grasso; X Cao; RJ Lonigro; S Varambally; R Mehra; N Palanisamy; JY Wu; Farida Latif; AM Chinnaiyan

doi:10.1038/onc.2010.269

The neuronal repellent SLIT2 is a target for repression by EZH2 in prostate cancer

J Yu, Q Cao, J Yu, L Wu, Ashraf Dallol, J Li, G Chen, C Grasso, X Cao, RJ Lonigro, S Varambally, R Mehra, N Palanisamy, JY Wu, Farida Latif, AM Chinnaiyan

Birmingham Medical School

Research output: Contribution to journal › Article

62 Citations (Scopus)

Abstract

The neuronal repellent SLIT2 is repressed in a number of cancer types primarily through promoter hypermethylation. SLIT2, however, has not been studied in prostate cancer. Through genome-wide location analysis we identified SLIT2 as a target of polycomb group (PcG) protein EZH2. The EZH2-containing polycomb repressive complexes bound to the SLIT2 promoter inhibiting its expression. SLIT2 was downregulated in a majority of metastatic prostate tumors, showing a negative correlation with EZH2. This repressed expression could be restored by methylation inhibitors or EZH2-suppressing compounds. In addition, a low level of SLIT2 expression was associated with aggressive prostate, breast and lung cancers. Functional assays showed that SLIT2 inhibited prostate cancer cell proliferation and invasion. Thus, this study showed for the first time the epigenetic silencing of SLIT2 in prostate tumors, and supported SLIT2 as a potential biomarker for aggressive solid tumors. Importantly, PcG-mediated repression may serve as a precursor for the silencing of SLIT2 by DNA methylation in cancer. Oncogene (2010) 29, 5370-5380; doi: 10.1038/onc.2010.269; published online 12 July 2010

Original language	English
Pages (from-to)	5370-5380
Number of pages	11
Journal	Oncogene
Volume	29
Issue number	39
DOIs	https://doi.org/10.1038/onc.2010.269
Publication status	Published - 1 Sept 2010

Keywords

polycomb group proteins
epigenetic silencing
EZH2
DNA hypermethylation
prostate cancer
SLIT2

UN SDGs

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10.1038/onc.2010.269

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title = "The neuronal repellent SLIT2 is a target for repression by EZH2 in prostate cancer",

abstract = "The neuronal repellent SLIT2 is repressed in a number of cancer types primarily through promoter hypermethylation. SLIT2, however, has not been studied in prostate cancer. Through genome-wide location analysis we identified SLIT2 as a target of polycomb group (PcG) protein EZH2. The EZH2-containing polycomb repressive complexes bound to the SLIT2 promoter inhibiting its expression. SLIT2 was downregulated in a majority of metastatic prostate tumors, showing a negative correlation with EZH2. This repressed expression could be restored by methylation inhibitors or EZH2-suppressing compounds. In addition, a low level of SLIT2 expression was associated with aggressive prostate, breast and lung cancers. Functional assays showed that SLIT2 inhibited prostate cancer cell proliferation and invasion. Thus, this study showed for the first time the epigenetic silencing of SLIT2 in prostate tumors, and supported SLIT2 as a potential biomarker for aggressive solid tumors. Importantly, PcG-mediated repression may serve as a precursor for the silencing of SLIT2 by DNA methylation in cancer. Oncogene (2010) 29, 5370-5380; doi: 10.1038/onc.2010.269; published online 12 July 2010",

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author = "J Yu and Q Cao and J Yu and L Wu and Ashraf Dallol and J Li and G Chen and C Grasso and X Cao and RJ Lonigro and S Varambally and R Mehra and N Palanisamy and JY Wu and Farida Latif and AM Chinnaiyan",

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T1 - The neuronal repellent SLIT2 is a target for repression by EZH2 in prostate cancer

AU - Yu, J

AU - Cao, Q

AU - Yu, J

AU - Wu, L

AU - Dallol, Ashraf

AU - Li, J

AU - Chen, G

AU - Grasso, C

AU - Cao, X

AU - Lonigro, RJ

AU - Varambally, S

AU - Mehra, R

AU - Palanisamy, N

AU - Wu, JY

AU - Latif, Farida

AU - Chinnaiyan, AM

PY - 2010/9/1

Y1 - 2010/9/1

N2 - The neuronal repellent SLIT2 is repressed in a number of cancer types primarily through promoter hypermethylation. SLIT2, however, has not been studied in prostate cancer. Through genome-wide location analysis we identified SLIT2 as a target of polycomb group (PcG) protein EZH2. The EZH2-containing polycomb repressive complexes bound to the SLIT2 promoter inhibiting its expression. SLIT2 was downregulated in a majority of metastatic prostate tumors, showing a negative correlation with EZH2. This repressed expression could be restored by methylation inhibitors or EZH2-suppressing compounds. In addition, a low level of SLIT2 expression was associated with aggressive prostate, breast and lung cancers. Functional assays showed that SLIT2 inhibited prostate cancer cell proliferation and invasion. Thus, this study showed for the first time the epigenetic silencing of SLIT2 in prostate tumors, and supported SLIT2 as a potential biomarker for aggressive solid tumors. Importantly, PcG-mediated repression may serve as a precursor for the silencing of SLIT2 by DNA methylation in cancer. Oncogene (2010) 29, 5370-5380; doi: 10.1038/onc.2010.269; published online 12 July 2010

AB - The neuronal repellent SLIT2 is repressed in a number of cancer types primarily through promoter hypermethylation. SLIT2, however, has not been studied in prostate cancer. Through genome-wide location analysis we identified SLIT2 as a target of polycomb group (PcG) protein EZH2. The EZH2-containing polycomb repressive complexes bound to the SLIT2 promoter inhibiting its expression. SLIT2 was downregulated in a majority of metastatic prostate tumors, showing a negative correlation with EZH2. This repressed expression could be restored by methylation inhibitors or EZH2-suppressing compounds. In addition, a low level of SLIT2 expression was associated with aggressive prostate, breast and lung cancers. Functional assays showed that SLIT2 inhibited prostate cancer cell proliferation and invasion. Thus, this study showed for the first time the epigenetic silencing of SLIT2 in prostate tumors, and supported SLIT2 as a potential biomarker for aggressive solid tumors. Importantly, PcG-mediated repression may serve as a precursor for the silencing of SLIT2 by DNA methylation in cancer. Oncogene (2010) 29, 5370-5380; doi: 10.1038/onc.2010.269; published online 12 July 2010

KW - polycomb group proteins

KW - epigenetic silencing

KW - EZH2

KW - DNA hypermethylation

KW - prostate cancer

KW - SLIT2

U2 - 10.1038/onc.2010.269

DO - 10.1038/onc.2010.269

M3 - Article

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JO - Oncogene

JF - Oncogene

IS - 39

ER -

The neuronal repellent SLIT2 is a target for repression by EZH2 in prostate cancer

Abstract

Keywords

UN SDGs

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