TY - JOUR A1 - Wolter, Patrick A1 - Hanselmann, Steffen A1 - Pattschull, Grit A1 - Schruf, Eva A1 - Gaubatz, Stefan T1 - Central spindle proteins and mitotic kinesins are direct transcriptional targets of MuvB, B-MYB and FOXM1 in breast cancer cell lines and are potential targets for therapy JF - Oncotarget N2 - The MuvB multiprotein complex, together with B-MYB and FOXM1 (MMB-FOXM1), plays an essential role in cell cycle progression by regulating the transcription of genes required for mitosis and cytokinesis. In many tumors, B-MYB and FOXM1 are overexpressed as part of the proliferation signature. However, the transcriptional targets that are important for oncogenesis have not been identified. Given that mitotic kinesins are highly expressed in cancer cells and that selected kinesins have been reported as target genes of MMB-FOXM1, we sought to determine which mitotic kinesins are directly regulated by MMB-FOXM1. We demonstrate that six mitotic kinesins and two microtubule-associated non-motor proteins (MAPs) CEP55 and PRC1 are direct transcriptional targets of MuvB, B-MYB and FOXM1 in breast cancer cells. Suppression of KIF23 and PRC1 strongly suppressed proliferation of MDA-MB-231 cells. The set of MMB-FOXM1 regulated kinesins genes and 4 additional kinesins which we referred to as the mitotic kinesin signature (MKS) is linked to poor outcome in breast cancer patients. Thus, mitotic kinesins could be used as prognostic biomarker and could be potential therapeutic targets for the treatment of breast cancer. KW - breast cancer KW - kinesin KW - cell cycle KW - cytokinesis Y1 - 2017 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-171851 VL - 8 IS - 7 ER - TY - THES A1 - Weinstock [geb. Pattschull], Grit T1 - Crosstalk between the MMB complex and YAP in transcriptional regulation of cell cycle genes T1 - Interaktion zwischen dem MMB-Komplex und YAP bei der transkriptionellen Regulation von Zellzyklusgenen N2 - The Myb-MuvB (MMB) multiprotein complex is a master regulator of cell cycle-dependent gene expression. Target genes of MMB are expressed at elevated levels in several different cancer types and are included in the chromosomal instability (CIN) signature of lung, brain, and breast tumors. This doctoral thesis showed that the complete loss of the MMB core subunit LIN9 leads to strong proliferation defects and nuclear abnormalities in primary lung adenocarcinoma cells. Transcriptome profiling and genome-wide DNA-binding analyses of MMB in lung adenocarcinoma cells revealed that MMB drives the expression of genes linked to cell cycle progression, mitosis, and chromosome segregation by direct binding to promoters of these genes. Unexpectedly, a previously unknown overlap between MMB-dependent genes and several signatures of YAP-regulated genes was identified. YAP is a transcriptional co-activator acting downstream of the Hippo signaling pathway, which is deregulated in many tumor types. Here, MMB and YAP were found to physically interact and co-regulate a set of mitotic and cytokinetic target genes, which are important in cancer. Furthermore, the activation of mitotic genes and the induction of entry into mitosis by YAP were strongly dependent on MMB. By ChIP-seq and 4C-seq, the genome-wide binding of MMB upon YAP overexpression was analyzed and long-range chromatin interaction sites of selected MMB target gene promoters were identified. Strikingly, YAP strongly promoted chromatin-association of B-MYB through binding to distal enhancer elements that interact with MMB-regulated promoters through chromatin looping. Together, the findings of this thesis provide a so far unknown molecular mechanism by which YAP and MMB cooperate to regulate mitotic gene expression and suggest a link between two cancer-relevant signaling pathways. N2 - Der Myb-MuvB (MMB) Multiproteinkomplex spielt eine wichtige Rolle in der Expression Zellzyklus abhängiger Gene, welche erhöhte Expressionsraten in verschiedenen Krebsarten aufweisen und Teil der sogenannten chromosomalen Instabilitätssignatur (CIN) von Lungen-, Gehirn- und Brusttumoren sind. In dieser Arbeit konnte gezeigt werden, dass die Deletion von LIN9, einer zentralen Untereinheit des MMB-Komplexes, in primären Lungenkarzinomzellen der Maus zu starken Proliferationsdefekten und Anomalitäten des Zellkerns führt. Analysen des gesamten Transkriptoms mit Hilfe von RNA-Seq ergaben, dass der MMB-Komplex die Expression einer Gruppe von Genen reguliert, die mit dem Voranschreiten des Zellzyklus, der Mitose und der Trennung der Chromosomen in Verbindung stehen. Die Regulation dieser Gene erfolgt durch direkte Bindung des MMB-Komplexes an die dazugehörigen Promotoren, wie die Analyse der genomweiten DNA-Bindung des MMB-Komplexes durch ChIP-Seq erkennbar werden ließ. Weiterhin wurde in dieser Arbeit eine neuartige Interaktion zwischen MMB und YAP, einem transkriptionellen Co-Aktivator und Effektorprotein des Hippo-Signalweges, gefunden. Die Dysregulation von Hippo/YAP ist an der Entstehung verschiedener Tumorentitäten beteiligt. Die Ergebnisse dieser Arbeit zeigen, dass YAP mit Untereinheiten von MMB interagiert und dass beide Signalwege ein überlappendes Set von Zielgenen, die für die Entstehung von Tumoren relevant sind, regulieren. Es konnte außerdem nachgewiesen werden, dass YAP den MMB-Komplex benötigt, um die Expression mitotischer Gene zu aktivieren und dass der durch YAP induzierte Eintritt in die Mitose vom MMB-Komplex abhängig ist. In einem weiteren Teil der Arbeit wurden mittels ChIP-Seq und 4C-Seq Chromatin-Interaktionen von Promotoren der MMB-Zielgene mit weiter entfernt liegenden Bereichen des Genoms identifiziert. Hierbei konnte festgestellt werden, dass YAP die Bindung der MMB-Untereinheit B-MYB an die Promotoren der MMB-Zielgene verstärkt, indem es an weiter entfernte Enhancer bindet. Diese von YAP gebundenen Enhancer interagieren über Schleifenbildung des Chromatins mit den Promotoren MMB-regulierter Gene. Zusammengefasst konnten die Ergebnisse dieser Arbeit einen bisher unbekannten molekularen Mechanismus für die gemeinsame Regulation von Genen durch den MMB Komplex und YAP enthüllen und somit einen Zusammenhang zwischen zwei krebsrelevanten Signalwegen aufdecken. KW - Krebs KW - Zellteilung KW - Genexpression KW - MMB complex KW - Hippo pathway KW - mitosis KW - cytokinesis KW - mitotic gene expression KW - Lungenkrebs KW - Mitose Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-170866 ER - TY - JOUR A1 - Pattschull, Grit A1 - Walz, Susanne A1 - Gründl, Marco A1 - Schwab, Melissa A1 - Rühl, Eva A1 - Baluapuri, Apoorva A1 - Cindric-Vranesic, Anita A1 - Kneitz, Susanne A1 - Wolf, Elmar A1 - Ade, Carsten P. A1 - Rosenwald, Andreas A1 - von Eyss, Björn A1 - Gaubatz, Stefan T1 - The Myb-MuvB complex is required for YAP-dependent transcription of mitotic genes JF - Cell Reports N2 - YAP and TAZ, downstream effectors of the Hippo pathway, are important regulators of proliferation. Here, we show that the ability of YAP to activate mitotic gene expression is dependent on the Myb-MuvB (MMB) complex, a master regulator of genes expressed in the G2/M phase of the cell cycle. By carrying out genome-wide expression and binding analyses, we found that YAP promotes binding of the MMB subunit B-MYB to the promoters of mitotic target genes. YAP binds to B-MYB and stimulates B-MYB chromatin association through distal enhancer elements that interact with MMB-regulated promoters through chromatin looping. The cooperation between YAP and B-MYB is critical for YAP-mediated entry into mitosis. Furthermore, the expression of genes coactivated by YAP and B-MYB is associated with poor survival of cancer patients. Our findings provide a molecular mechanism by which YAP and MMB regulate mitotic gene expression and suggest a link between two cancer-relevant signaling pathways. KW - YAP KW - B-MYB KW - Myb-MuvB KW - mitotic genes KW - enhancer KW - transcription Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-202039 VL - 27 IS - 12 ER -