The homeoprotein Dlx5 drives murine T-cell lymphomagenesis by directly transactivating Notch and upregulating Akt signaling

Homeobox genes play a critical role in embryonic development, but they have also been implicated in cancer through mechanisms that are largely unknown. While not expressed during normal T-cell development, homeobox transcription factor genes can be reactivated via recurrent chromosomal rearrangement...

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Veröffentlicht in:	Oncotarget 2017-02, Vol.8 (9), p.14941-14956
Hauptverfasser:	Tan, Yinfei, Sementino, Eleonora, Xu, Jinfei, Pei, Jianming, Liu, Zemin, Ito, Timothy K, Cai, Kathy Q, Peri, Suraj, Klein-Szanto, Andres J P, Wiest, David L, Testa, Joseph R
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Sprache:	eng
Schlagworte:	Animals Apoptosis Cell Proliferation Gene Expression Regulation, Neoplastic Homeodomain Proteins - physiology Humans Lymphocyte Specific Protein Tyrosine Kinase p56(lck) - physiology Lymphoma, T-Cell - genetics Lymphoma, T-Cell - metabolism Lymphoma, T-Cell - pathology Mice Mice, Transgenic Promoter Regions, Genetic Proto-Oncogene Proteins c-akt - physiology Receptor, Notch1 - genetics Research Paper Signal Transduction Transcriptional Activation Tumor Cells, Cultured
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creator	Tan, Yinfei Sementino, Eleonora Xu, Jinfei Pei, Jianming Liu, Zemin Ito, Timothy K Cai, Kathy Q Peri, Suraj Klein-Szanto, Andres J P Wiest, David L Testa, Joseph R
description	Homeobox genes play a critical role in embryonic development, but they have also been implicated in cancer through mechanisms that are largely unknown. While not expressed during normal T-cell development, homeobox transcription factor genes can be reactivated via recurrent chromosomal rearrangements in human T-cell acute leukemia/lymphoma (T-ALL), a malignancy often associated with activated Notch and Akt signaling. To address how epigenetic reprogramming via an activated homeobox gene might contribute to T-lymphomagenesis, we investigated a transgenic mouse model with thymocyte-specific overexpression of the Dlx5 homeobox gene. We demonstrate for the first time that Dlx5 induces T-cell lymphomas with high penetrance. Integrated ChIP-seq and mRNA microarray analyses identified Notch1/3 and Irs2 as direct transcriptional targets of Dlx5, a gene signature unique to lymphomas from Lck-Dlx5 mice as compared to T-cell lymphomas from Lck-MyrAkt2 mice, which were previously reported by our group. Moreover, promoter/enhancer studies confirmed that Dlx5 directly transactivates Notch expression. Notch1/3 expression and Irs2-induced Akt signaling were upregulated throughout early stages of T-cell development, which promoted cell survival during β-selection of T lymphocytes. Dlx5 was required for tumor maintenance via its activation of Notch and Akt, as tumor cells were highly sensitive to Notch and Akt inhibitors. Together, these findings provide unbiased genetic and mechanistic evidence that Dlx5 acts as an oncogene when aberrantly expressed in T cells, and that it is a novel discovery that Notch is a direct target of Dlx5. These experimental findings provide mechanistic insights about how reactivation of the Dlx5 gene can drive T-ALL by aberrant epigenetic reprogramming of the T-cell genome.
doi_str_mv	10.18632/oncotarget.14784
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Notch1/3 expression and Irs2-induced Akt signaling were upregulated throughout early stages of T-cell development, which promoted cell survival during β-selection of T lymphocytes. Dlx5 was required for tumor maintenance via its activation of Notch and Akt, as tumor cells were highly sensitive to Notch and Akt inhibitors. Together, these findings provide unbiased genetic and mechanistic evidence that Dlx5 acts as an oncogene when aberrantly expressed in T cells, and that it is a novel discovery that Notch is a direct target of Dlx5. 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Notch1/3 expression and Irs2-induced Akt signaling were upregulated throughout early stages of T-cell development, which promoted cell survival during β-selection of T lymphocytes. Dlx5 was required for tumor maintenance via its activation of Notch and Akt, as tumor cells were highly sensitive to Notch and Akt inhibitors. Together, these findings provide unbiased genetic and mechanistic evidence that Dlx5 acts as an oncogene when aberrantly expressed in T cells, and that it is a novel discovery that Notch is a direct target of Dlx5. These experimental findings provide mechanistic insights about how reactivation of the Dlx5 gene can drive T-ALL by aberrant epigenetic reprogramming of the T-cell genome.</description><subject>Animals</subject><subject>Apoptosis</subject><subject>Cell Proliferation</subject><subject>Gene Expression Regulation, Neoplastic</subject><subject>Homeodomain Proteins - physiology</subject><subject>Humans</subject><subject>Lymphocyte Specific Protein Tyrosine Kinase p56(lck) - physiology</subject><subject>Lymphoma, T-Cell - genetics</subject><subject>Lymphoma, T-Cell - metabolism</subject><subject>Lymphoma, T-Cell - pathology</subject><subject>Mice</subject><subject>Mice, Transgenic</subject><subject>Promoter Regions, Genetic</subject><subject>Proto-Oncogene Proteins c-akt - physiology</subject><subject>Receptor, Notch1 - genetics</subject><subject>Research Paper</subject><subject>Signal Transduction</subject><subject>Transcriptional Activation</subject><subject>Tumor Cells, Cultured</subject><issn>1949-2553</issn><issn>1949-2553</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2017</creationdate><recordtype>article</recordtype><sourceid>EIF</sourceid><recordid>eNpVkU1P3DAQhi1UBAj4AVyQj70E_BFnnUslRFuohOCynC3Hns26dezUdlZd9c8TWEphLjMev_N65AehM0ouqGw4u4zBxKJTD-WC1gtZ76Ej2tZtxYTgn97Vh-g0559kDjHLWHuADpmkjHHOjtDf5RrwOg4QxxQLuIC_-j8C2-Q2kPEwJRcALysD3mO_HcZZqnsIkF3G3RZbl8AUv8Ul6ZC1KW6jiws9vo_FrLEOFk9jgn7yu_bVr4Kz64P28-kE7a-0z3D6mo_R4_dvy-vb6u7h5sf11V1luGhK1TYCFq2QjbZmxVpuqZXcdA2BzjaatLbltSS21obxlV5YQQSVhEgtZa2ha_gx-rLzHaduAGsgzNt6NSY36LRVUTv18Sa4terjRgnesFo8G3x-NUjx9wS5qMHl5y_RAeKU1cyDMVkvKJmldCc1KeacYPX2DCXqhZv6z029cJtnzt_v9zbxjxJ_AtNemq4</recordid><startdate>20170228</startdate><enddate>20170228</enddate><creator>Tan, Yinfei</creator><creator>Sementino, Eleonora</creator><creator>Xu, Jinfei</creator><creator>Pei, Jianming</creator><creator>Liu, Zemin</creator><creator>Ito, Timothy K</creator><creator>Cai, Kathy Q</creator><creator>Peri, Suraj</creator><creator>Klein-Szanto, Andres J P</creator><creator>Wiest, David L</creator><creator>Testa, Joseph R</creator><general>Impact Journals LLC</general><scope>CGR</scope><scope>CUY</scope><scope>CVF</scope><scope>ECM</scope><scope>EIF</scope><scope>NPM</scope><scope>AAYXX</scope><scope>CITATION</scope><scope>7X8</scope><scope>5PM</scope></search><sort><creationdate>20170228</creationdate><title>The homeoprotein Dlx5 drives murine T-cell lymphomagenesis by directly transactivating Notch and upregulating Akt signaling</title><author>Tan, Yinfei ; 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While not expressed during normal T-cell development, homeobox transcription factor genes can be reactivated via recurrent chromosomal rearrangements in human T-cell acute leukemia/lymphoma (T-ALL), a malignancy often associated with activated Notch and Akt signaling. To address how epigenetic reprogramming via an activated homeobox gene might contribute to T-lymphomagenesis, we investigated a transgenic mouse model with thymocyte-specific overexpression of the Dlx5 homeobox gene. We demonstrate for the first time that Dlx5 induces T-cell lymphomas with high penetrance. Integrated ChIP-seq and mRNA microarray analyses identified Notch1/3 and Irs2 as direct transcriptional targets of Dlx5, a gene signature unique to lymphomas from Lck-Dlx5 mice as compared to T-cell lymphomas from Lck-MyrAkt2 mice, which were previously reported by our group. Moreover, promoter/enhancer studies confirmed that Dlx5 directly transactivates Notch expression. Notch1/3 expression and Irs2-induced Akt signaling were upregulated throughout early stages of T-cell development, which promoted cell survival during β-selection of T lymphocytes. Dlx5 was required for tumor maintenance via its activation of Notch and Akt, as tumor cells were highly sensitive to Notch and Akt inhibitors. Together, these findings provide unbiased genetic and mechanistic evidence that Dlx5 acts as an oncogene when aberrantly expressed in T cells, and that it is a novel discovery that Notch is a direct target of Dlx5. These experimental findings provide mechanistic insights about how reactivation of the Dlx5 gene can drive T-ALL by aberrant epigenetic reprogramming of the T-cell genome.</abstract><cop>United States</cop><pub>Impact Journals LLC</pub><pmid>28122332</pmid><doi>10.18632/oncotarget.14784</doi><tpages>16</tpages><oa>free_for_read</oa></addata></record>
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subjects	Animals Apoptosis Cell Proliferation Gene Expression Regulation, Neoplastic Homeodomain Proteins - physiology Humans Lymphocyte Specific Protein Tyrosine Kinase p56(lck) - physiology Lymphoma, T-Cell - genetics Lymphoma, T-Cell - metabolism Lymphoma, T-Cell - pathology Mice Mice, Transgenic Promoter Regions, Genetic Proto-Oncogene Proteins c-akt - physiology Receptor, Notch1 - genetics Research Paper Signal Transduction Transcriptional Activation Tumor Cells, Cultured
title	The homeoprotein Dlx5 drives murine T-cell lymphomagenesis by directly transactivating Notch and upregulating Akt signaling
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