Augmentation of tumor angiogenesis by a Myc-activated microRNA cluster

Michael Dews; Asal Homayouni; Duonan Yu; Danielle Murphy; Cinzia Sevignani; Erik Wentzel; Emma E. Furth; William M. Lee; Greg H. Enders; Joshua T. Mendell; Andrei Thomas-Tikhonenko

doi:10.1038/ng1855

Augmentation of tumor angiogenesis by a Myc-activated microRNA cluster

Michael Dews, Asal Homayouni, Duonan Yu, Danielle Murphy, Cinzia Sevignani, Erik Wentzel, Emma E. Furth, William M. Lee, Greg H. Enders, Joshua T. Mendell, Andrei Thomas-Tikhonenko

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

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Abstract

Human adenocarcinomas commonly harbor mutations in the KRAS and MYC proto-oncogenes and the TP53 tumor suppressor gene. All three genetic lesions are potentially pro-angiogenic, as they sustain production of vascular endothelial growth factor (VEGF). Yet Kras-transformed mouse colonocytes lacking p53 formed indolent, poorly vascularized tumors, whereas additional transduction with a Myc-encoding retrovirus promoted vigorous vascularization and growth. In addition, VEGF levels were unaffected by Myc, but enhanced neovascularization correlated with downregulation of anti-angiogenic thrombospondin-1 (Tsp1) and related proteins, such as connective tissue growth factor (CTGF). Both Tsp1 and CTGF are predicted targets for repression by the miR-17-92 microRNA cluster, which was upregulated in colonocytes coexpressing K-Ras and c-Myc. Indeed, miR-17-92 knockdown with antisense 2′-O-methyl oligoribonucleotides partly restored Tsp1 and CTGF expression; in addition, transduction of Ras-only cells with a miR-17-92-encoding retrovirus reduced Tsp1 and CTGF levels. Notably, miR-17-92-transduced cells formed larger, better-perfused tumors. These findings establish a role for microRNAs in non-cell-autonomous Myc-induced tumor phenotypes.

Original language	English (US)
Pages (from-to)	1060-1065
Number of pages	6
Journal	Nature genetics
Volume	38
Issue number	9
DOIs	https://doi.org/10.1038/ng1855
State	Published - Sep 4 2006
Externally published	Yes

ASJC Scopus subject areas

Genetics

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@article{1c991dbcf50e482eba86364996762116,

title = "Augmentation of tumor angiogenesis by a Myc-activated microRNA cluster",

abstract = "Human adenocarcinomas commonly harbor mutations in the KRAS and MYC proto-oncogenes and the TP53 tumor suppressor gene. All three genetic lesions are potentially pro-angiogenic, as they sustain production of vascular endothelial growth factor (VEGF). Yet Kras-transformed mouse colonocytes lacking p53 formed indolent, poorly vascularized tumors, whereas additional transduction with a Myc-encoding retrovirus promoted vigorous vascularization and growth. In addition, VEGF levels were unaffected by Myc, but enhanced neovascularization correlated with downregulation of anti-angiogenic thrombospondin-1 (Tsp1) and related proteins, such as connective tissue growth factor (CTGF). Both Tsp1 and CTGF are predicted targets for repression by the miR-17-92 microRNA cluster, which was upregulated in colonocytes coexpressing K-Ras and c-Myc. Indeed, miR-17-92 knockdown with antisense 2′-O-methyl oligoribonucleotides partly restored Tsp1 and CTGF expression; in addition, transduction of Ras-only cells with a miR-17-92-encoding retrovirus reduced Tsp1 and CTGF levels. Notably, miR-17-92-transduced cells formed larger, better-perfused tumors. These findings establish a role for microRNAs in non-cell-autonomous Myc-induced tumor phenotypes.",

author = "Michael Dews and Asal Homayouni and Duonan Yu and Danielle Murphy and Cinzia Sevignani and Erik Wentzel and Furth, {Emma E.} and Lee, {William M.} and Enders, {Greg H.} and Mendell, {Joshua T.} and Andrei Thomas-Tikhonenko",

note = "Funding Information: We are indebted to C. Dang (Johns Hopkins University) for fostering collaborations between the investigators. We are grateful to C. Simon and C.-J. Hu (University of Pennsylvania) for providing HIF1a-overexpressing cell lysates for protein blot analysis and J. Tobias (University of Pennsylvania) for his help with microarray data analysis. We thank W. El-Deiry, A. Rustgi, and S. Fuchs (University of Pennsylvania) for stimulating discussions and comments on the manuscript. M. Goldschmidt and J. Burns (University of Pennsylvania) are acknowledged for their help with histopathological analyses. This work was supported by US National Institutes of Health grants CA 097932 and DK 050306 and a University of Pennsylvania Research Foundation grant to A.T.-T.",

year = "2006",

month = sep,

day = "4",

doi = "10.1038/ng1855",

language = "English (US)",

volume = "38",

pages = "1060--1065",

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T1 - Augmentation of tumor angiogenesis by a Myc-activated microRNA cluster

AU - Dews, Michael

AU - Homayouni, Asal

AU - Yu, Duonan

AU - Murphy, Danielle

AU - Sevignani, Cinzia

AU - Wentzel, Erik

AU - Furth, Emma E.

AU - Lee, William M.

AU - Enders, Greg H.

AU - Mendell, Joshua T.

AU - Thomas-Tikhonenko, Andrei

N1 - Funding Information: We are indebted to C. Dang (Johns Hopkins University) for fostering collaborations between the investigators. We are grateful to C. Simon and C.-J. Hu (University of Pennsylvania) for providing HIF1a-overexpressing cell lysates for protein blot analysis and J. Tobias (University of Pennsylvania) for his help with microarray data analysis. We thank W. El-Deiry, A. Rustgi, and S. Fuchs (University of Pennsylvania) for stimulating discussions and comments on the manuscript. M. Goldschmidt and J. Burns (University of Pennsylvania) are acknowledged for their help with histopathological analyses. This work was supported by US National Institutes of Health grants CA 097932 and DK 050306 and a University of Pennsylvania Research Foundation grant to A.T.-T.

PY - 2006/9/4

Y1 - 2006/9/4

N2 - Human adenocarcinomas commonly harbor mutations in the KRAS and MYC proto-oncogenes and the TP53 tumor suppressor gene. All three genetic lesions are potentially pro-angiogenic, as they sustain production of vascular endothelial growth factor (VEGF). Yet Kras-transformed mouse colonocytes lacking p53 formed indolent, poorly vascularized tumors, whereas additional transduction with a Myc-encoding retrovirus promoted vigorous vascularization and growth. In addition, VEGF levels were unaffected by Myc, but enhanced neovascularization correlated with downregulation of anti-angiogenic thrombospondin-1 (Tsp1) and related proteins, such as connective tissue growth factor (CTGF). Both Tsp1 and CTGF are predicted targets for repression by the miR-17-92 microRNA cluster, which was upregulated in colonocytes coexpressing K-Ras and c-Myc. Indeed, miR-17-92 knockdown with antisense 2′-O-methyl oligoribonucleotides partly restored Tsp1 and CTGF expression; in addition, transduction of Ras-only cells with a miR-17-92-encoding retrovirus reduced Tsp1 and CTGF levels. Notably, miR-17-92-transduced cells formed larger, better-perfused tumors. These findings establish a role for microRNAs in non-cell-autonomous Myc-induced tumor phenotypes.

AB - Human adenocarcinomas commonly harbor mutations in the KRAS and MYC proto-oncogenes and the TP53 tumor suppressor gene. All three genetic lesions are potentially pro-angiogenic, as they sustain production of vascular endothelial growth factor (VEGF). Yet Kras-transformed mouse colonocytes lacking p53 formed indolent, poorly vascularized tumors, whereas additional transduction with a Myc-encoding retrovirus promoted vigorous vascularization and growth. In addition, VEGF levels were unaffected by Myc, but enhanced neovascularization correlated with downregulation of anti-angiogenic thrombospondin-1 (Tsp1) and related proteins, such as connective tissue growth factor (CTGF). Both Tsp1 and CTGF are predicted targets for repression by the miR-17-92 microRNA cluster, which was upregulated in colonocytes coexpressing K-Ras and c-Myc. Indeed, miR-17-92 knockdown with antisense 2′-O-methyl oligoribonucleotides partly restored Tsp1 and CTGF expression; in addition, transduction of Ras-only cells with a miR-17-92-encoding retrovirus reduced Tsp1 and CTGF levels. Notably, miR-17-92-transduced cells formed larger, better-perfused tumors. These findings establish a role for microRNAs in non-cell-autonomous Myc-induced tumor phenotypes.

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Augmentation of tumor angiogenesis by a Myc-activated microRNA cluster

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