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1. Multinational proficiency tests for EGFR exon 20 insertions reveal that the assay design matters

Author

Ihle, Michaela A., Heydt, Carina, Schultheis, Anne Maria, Stöhr, Robert, Haller, Florian, Herold, Sylvia, Aust, Daniela, Dietmaier, Wolfgang, Evert, Matthias, Eszlinger, Markus, Haak, Anja, Laßmann, Silke, Vorholt, Daniela, Breitenbücher, Frank, Werner, Martin, Streubel, Anna, Mairinger, Thomas, Grassow-Narlik, Maja, and Merkelbach-Bruse, Sabine

Published
2024
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3. Resistance to MET inhibition in MET-dependent NSCLC and therapeutic activity after switching from type I to type II MET inhibitors

Author

Riedel, Richard, Fassunke, Jana, Tumbrink, Hannah L., Scheel, Andreas H., Heydt, Carina, Hieggelke, Lena, Scheffler, Matthias, Heimsoeth, Alena, Nogova, Lucia, Michels, Sebastian, Weber, Jan-Phillip, Fischer, Rieke N., Eisert, Anna, Westphal, Theresa, Schaufler, Diana, Siemanowski, Janna, Ihle, Michaela A., Wagener-Ryczek, Svenja, Castiglione, Roberta, Pappesch, Roberto, Rehker, Jan, Jürgens, Jessica, Stoelben, Erich, Bunck, Anne, Kobe, Carsten, Merkelbach-Bruse, Sabine, Sos, Martin L., Büttner, Reinhard, and Wolf, Jürgen

Published
2023
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4. BMP signaling promotes heart regeneration via alleviation of replication stress

Author

Dalvoy Vasudevarao, Mohankrishna, primary, Posadas-pena, Denise Silvia, additional, Ihle, Michaela, additional, Bongiovanni, Chiara, additional, Maity, Pallab, additional, Redaelli, Simone, additional, Happ, Kathrin, additional, Geissler, Dominik, additional, Mohammadi, Hossein Falah, additional, Rall-Scharpf, Melanie, additional, Wu, Chi-Chung, additional, Beisaw, Arica, additional, Scharffetter-Kochanek, Karin, additional, D'Uva, Gabriele, additional, Wiesmueller, Lisa, additional, and Weidinger, Gilbert, additional

Published
2024
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5. K-ras Mutation Subtypes in NSCLC and Associated Co-occuring Mutations in Other Oncogenic Pathways

Author

Scheffler, Matthias, Ihle, Michaela A., Hein, Rebecca, Merkelbach-Bruse, Sabine, Scheel, Andreas H., Siemanowski, Janna, Brägelmann, Johannes, Kron, Anna, Abedpour, Nima, Ueckeroth, Frank, Schüller, Merle, Koleczko, Sophia, Michels, Sebastian, Fassunke, Jana, Pasternack, Helen, Heydt, Carina, Serke, Monika, Fischer, Rieke, Schulte, Wolfgang, Gerigk, Ulrich, Nogova, Lucia, Ko, Yon-Dschun, Abdulla, Diana S.Y., Riedel, Richard, Kambartel, Karl-Otto, Lorenz, Joachim, Sauerland, Imke, Randerath, Winfried, Kaminsky, Britta, Hagmeyer, Lars, Grohé, Christian, Eisert, Anna, Frank, Rieke, Gogl, Leonie, Schaepers, Carsten, Holzem, Alessandra, Hellmich, Martin, Thomas, Roman K., Peifer, Martin, Sos, Martin L., Büttner, Reinhard, and Wolf, Jürgen

Published
2019
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6. MET Fusions in NSCLC: Clinicopathologic Features and Response to MET Inhibition

Author

Riedel, Richard, primary, Fassunke, Jana, additional, Scheel, Andreas H., additional, Scheffler, Matthias, additional, Heydt, Carina, additional, Nogova, Lucia, additional, Michels, Sebastian, additional, Fischer, Rieke N., additional, Eisert, Anna, additional, Scharpenseel, Heather, additional, John, Felix, additional, Ruge, Lea, additional, Schaufler, Diana, additional, Siemanowski, Janna, additional, Ihle, Michaela A., additional, Wagener-Ryczek, Svenja, additional, Pappesch, Roberto, additional, Rehker, Jan, additional, Bunck, Anne, additional, Kobe, Carsten, additional, Keil, Felix, additional, Merkelbach-Bruse, Sabine, additional, Büttner, Reinhard, additional, and Wolf, Jürgen, additional

Published
2023
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11. Supplementary Figure 3 from Heterogeneous Mechanisms of Primary and Acquired Resistance to Third-Generation EGFR Inhibitors

Author

Ortiz-Cuaran, Sandra, primary, Scheffler, Matthias, primary, Plenker, Dennis, primary, Dahmen, llona, primary, Scheel, Andreas H., primary, Fernandez-Cuesta, Lynnette, primary, Meder, Lydia, primary, Lovly, Christine M., primary, Persigehl, Thorsten, primary, Merkelbach-Bruse, Sabine, primary, Bos, Marc, primary, Michels, Sebastian, primary, Fischer, Rieke, primary, Albus, Kerstin, primary, König, Katharina, primary, Schildhaus, Hans-Ulrich, primary, Fassunke, Jana, primary, Ihle, Michaela A., primary, Pasternack, Helen, primary, Heydt, Carina, primary, Becker, Christian, primary, Altmüller, Janine, primary, Ji, Hongbin, primary, Müller, Christian, primary, Florin, Alexandra, primary, Heuckmann, Johannes M., primary, Nuernberg, Peter, primary, Ansén, Sascha, primary, Heukamp, Lukas C., primary, Berg, Johannes, primary, Pao, William, primary, Peifer, Martin, primary, Buettner, Reinhard, primary, Wolf, Jürgen, primary, Thomas, Roman K., primary, and Sos, Martin L., primary

Published
2023
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12. Figure S5 Tumour growth upon ATRi and Gemcitabine Treatment in Allografts model from ATM Deficiency Generating Genomic Instability Sensitizes Pancreatic Ductal Adenocarcinoma Cells to Therapy-Induced DNA Damage

Author

Perkhofer, Lukas, primary, Schmitt, Anna, primary, Romero Carrasco, Maria Carolina, primary, Ihle, Michaela, primary, Hampp, Stephanie, primary, Ruess, Dietrich Alexander, primary, Hessmann, Elisabeth, primary, Russell, Ronan, primary, Lechel, André, primary, Azoitei, Ninel, primary, Lin, Qiong, primary, Liebau, Stefan, primary, Hohwieler, Meike, primary, Bohnenberger, Hanibal, primary, Lesina, Marina, primary, Algül, Hana, primary, Gieldon, Laura, primary, Schröck, Evelin, primary, Gaedcke, Jochen, primary, Wagner, Martin, primary, Wiesmüller, Lisa, primary, Sipos, Bence, primary, Seufferlein, Thomas, primary, Reinhardt, Hans Christian, primary, Frappart, Pierre-Olivier, primary, and Kleger, Alexander, primary

Published
2023
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13. Supplemental Table 8 from Clinical and Pathological Characteristics of KEAP1- and NFE2L2-Mutated Non–Small Cell Lung Carcinoma (NSCLC)

Author

Frank, Rieke, primary, Scheffler, Matthias, primary, Merkelbach-Bruse, Sabine, primary, Ihle, Michaela A., primary, Kron, Anna, primary, Rauer, Michael, primary, Ueckeroth, Frank, primary, König, Katharina, primary, Michels, Sebastian, primary, Fischer, Rieke, primary, Eisert, Anna, primary, Fassunke, Jana, primary, Heydt, Carina, primary, Serke, Monika, primary, Ko, Yon-Dschun, primary, Gerigk, Ulrich, primary, Geist, Thomas, primary, Kaminsky, Britta, primary, Heukamp, Lukas C., primary, Clement-Ziza, Mathieu, primary, Büttner, Reinhard, primary, and Wolf, Jürgen, primary

Published
2023
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14. Figure S2 from ATM Deficiency Generating Genomic Instability Sensitizes Pancreatic Ductal Adenocarcinoma Cells to Therapy-Induced DNA Damage

Author

Perkhofer, Lukas, primary, Schmitt, Anna, primary, Romero Carrasco, Maria Carolina, primary, Ihle, Michaela, primary, Hampp, Stephanie, primary, Ruess, Dietrich Alexander, primary, Hessmann, Elisabeth, primary, Russell, Ronan, primary, Lechel, André, primary, Azoitei, Ninel, primary, Lin, Qiong, primary, Liebau, Stefan, primary, Hohwieler, Meike, primary, Bohnenberger, Hanibal, primary, Lesina, Marina, primary, Algül, Hana, primary, Gieldon, Laura, primary, Schröck, Evelin, primary, Gaedcke, Jochen, primary, Wagner, Martin, primary, Wiesmüller, Lisa, primary, Sipos, Bence, primary, Seufferlein, Thomas, primary, Reinhardt, Hans Christian, primary, Frappart, Pierre-Olivier, primary, and Kleger, Alexander, primary

Published
2023
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15. Figure S1 GSEA Analysis from ATM Deficiency Generating Genomic Instability Sensitizes Pancreatic Ductal Adenocarcinoma Cells to Therapy-Induced DNA Damage

Author

Perkhofer, Lukas, primary, Schmitt, Anna, primary, Romero Carrasco, Maria Carolina, primary, Ihle, Michaela, primary, Hampp, Stephanie, primary, Ruess, Dietrich Alexander, primary, Hessmann, Elisabeth, primary, Russell, Ronan, primary, Lechel, André, primary, Azoitei, Ninel, primary, Lin, Qiong, primary, Liebau, Stefan, primary, Hohwieler, Meike, primary, Bohnenberger, Hanibal, primary, Lesina, Marina, primary, Algül, Hana, primary, Gieldon, Laura, primary, Schröck, Evelin, primary, Gaedcke, Jochen, primary, Wagner, Martin, primary, Wiesmüller, Lisa, primary, Sipos, Bence, primary, Seufferlein, Thomas, primary, Reinhardt, Hans Christian, primary, Frappart, Pierre-Olivier, primary, and Kleger, Alexander, primary

Published
2023
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16. Table S1 from ATM Deficiency Generating Genomic Instability Sensitizes Pancreatic Ductal Adenocarcinoma Cells to Therapy-Induced DNA Damage

Author

Perkhofer, Lukas, primary, Schmitt, Anna, primary, Romero Carrasco, Maria Carolina, primary, Ihle, Michaela, primary, Hampp, Stephanie, primary, Ruess, Dietrich Alexander, primary, Hessmann, Elisabeth, primary, Russell, Ronan, primary, Lechel, André, primary, Azoitei, Ninel, primary, Lin, Qiong, primary, Liebau, Stefan, primary, Hohwieler, Meike, primary, Bohnenberger, Hanibal, primary, Lesina, Marina, primary, Algül, Hana, primary, Gieldon, Laura, primary, Schröck, Evelin, primary, Gaedcke, Jochen, primary, Wagner, Martin, primary, Wiesmüller, Lisa, primary, Sipos, Bence, primary, Seufferlein, Thomas, primary, Reinhardt, Hans Christian, primary, Frappart, Pierre-Olivier, primary, and Kleger, Alexander, primary

Published
2023
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17. Supplementary Figure 2 from Heterogeneous Mechanisms of Primary and Acquired Resistance to Third-Generation EGFR Inhibitors

Author

Ortiz-Cuaran, Sandra, primary, Scheffler, Matthias, primary, Plenker, Dennis, primary, Dahmen, llona, primary, Scheel, Andreas H., primary, Fernandez-Cuesta, Lynnette, primary, Meder, Lydia, primary, Lovly, Christine M., primary, Persigehl, Thorsten, primary, Merkelbach-Bruse, Sabine, primary, Bos, Marc, primary, Michels, Sebastian, primary, Fischer, Rieke, primary, Albus, Kerstin, primary, König, Katharina, primary, Schildhaus, Hans-Ulrich, primary, Fassunke, Jana, primary, Ihle, Michaela A., primary, Pasternack, Helen, primary, Heydt, Carina, primary, Becker, Christian, primary, Altmüller, Janine, primary, Ji, Hongbin, primary, Müller, Christian, primary, Florin, Alexandra, primary, Heuckmann, Johannes M., primary, Nuernberg, Peter, primary, Ansén, Sascha, primary, Heukamp, Lukas C., primary, Berg, Johannes, primary, Pao, William, primary, Peifer, Martin, primary, Buettner, Reinhard, primary, Wolf, Jürgen, primary, Thomas, Roman K., primary, and Sos, Martin L., primary

Published
2023
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18. Data from ATM Deficiency Generating Genomic Instability Sensitizes Pancreatic Ductal Adenocarcinoma Cells to Therapy-Induced DNA Damage

Author

Perkhofer, Lukas, primary, Schmitt, Anna, primary, Romero Carrasco, Maria Carolina, primary, Ihle, Michaela, primary, Hampp, Stephanie, primary, Ruess, Dietrich Alexander, primary, Hessmann, Elisabeth, primary, Russell, Ronan, primary, Lechel, André, primary, Azoitei, Ninel, primary, Lin, Qiong, primary, Liebau, Stefan, primary, Hohwieler, Meike, primary, Bohnenberger, Hanibal, primary, Lesina, Marina, primary, Algül, Hana, primary, Gieldon, Laura, primary, Schröck, Evelin, primary, Gaedcke, Jochen, primary, Wagner, Martin, primary, Wiesmüller, Lisa, primary, Sipos, Bence, primary, Seufferlein, Thomas, primary, Reinhardt, Hans Christian, primary, Frappart, Pierre-Olivier, primary, and Kleger, Alexander, primary

Published
2023
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19. Supplementary Data from Heterogeneous Mechanisms of Primary and Acquired Resistance to Third-Generation EGFR Inhibitors

Author

Ortiz-Cuaran, Sandra, primary, Scheffler, Matthias, primary, Plenker, Dennis, primary, Dahmen, llona, primary, Scheel, Andreas H., primary, Fernandez-Cuesta, Lynnette, primary, Meder, Lydia, primary, Lovly, Christine M., primary, Persigehl, Thorsten, primary, Merkelbach-Bruse, Sabine, primary, Bos, Marc, primary, Michels, Sebastian, primary, Fischer, Rieke, primary, Albus, Kerstin, primary, König, Katharina, primary, Schildhaus, Hans-Ulrich, primary, Fassunke, Jana, primary, Ihle, Michaela A., primary, Pasternack, Helen, primary, Heydt, Carina, primary, Becker, Christian, primary, Altmüller, Janine, primary, Ji, Hongbin, primary, Müller, Christian, primary, Florin, Alexandra, primary, Heuckmann, Johannes M., primary, Nuernberg, Peter, primary, Ansén, Sascha, primary, Heukamp, Lukas C., primary, Berg, Johannes, primary, Pao, William, primary, Peifer, Martin, primary, Buettner, Reinhard, primary, Wolf, Jürgen, primary, Thomas, Roman K., primary, and Sos, Martin L., primary

Published
2023
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20. Supplement from Clinical and Pathological Characteristics of KEAP1- and NFE2L2-Mutated Non–Small Cell Lung Carcinoma (NSCLC)

Author

Frank, Rieke, primary, Scheffler, Matthias, primary, Merkelbach-Bruse, Sabine, primary, Ihle, Michaela A., primary, Kron, Anna, primary, Rauer, Michael, primary, Ueckeroth, Frank, primary, König, Katharina, primary, Michels, Sebastian, primary, Fischer, Rieke, primary, Eisert, Anna, primary, Fassunke, Jana, primary, Heydt, Carina, primary, Serke, Monika, primary, Ko, Yon-Dschun, primary, Gerigk, Ulrich, primary, Geist, Thomas, primary, Kaminsky, Britta, primary, Heukamp, Lukas C., primary, Clement-Ziza, Mathieu, primary, Büttner, Reinhard, primary, and Wolf, Jürgen, primary

Published
2023
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21. Figure S3 Tumour growth upon Olaparib and Gemcitabine Treatment in Allografts model from ATM Deficiency Generating Genomic Instability Sensitizes Pancreatic Ductal Adenocarcinoma Cells to Therapy-Induced DNA Damage

Author

Perkhofer, Lukas, primary, Schmitt, Anna, primary, Romero Carrasco, Maria Carolina, primary, Ihle, Michaela, primary, Hampp, Stephanie, primary, Ruess, Dietrich Alexander, primary, Hessmann, Elisabeth, primary, Russell, Ronan, primary, Lechel, André, primary, Azoitei, Ninel, primary, Lin, Qiong, primary, Liebau, Stefan, primary, Hohwieler, Meike, primary, Bohnenberger, Hanibal, primary, Lesina, Marina, primary, Algül, Hana, primary, Gieldon, Laura, primary, Schröck, Evelin, primary, Gaedcke, Jochen, primary, Wagner, Martin, primary, Wiesmüller, Lisa, primary, Sipos, Bence, primary, Seufferlein, Thomas, primary, Reinhardt, Hans Christian, primary, Frappart, Pierre-Olivier, primary, and Kleger, Alexander, primary

Published
2023
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22. Supplementary Figure 4 from Heterogeneous Mechanisms of Primary and Acquired Resistance to Third-Generation EGFR Inhibitors

Author

Ortiz-Cuaran, Sandra, primary, Scheffler, Matthias, primary, Plenker, Dennis, primary, Dahmen, llona, primary, Scheel, Andreas H., primary, Fernandez-Cuesta, Lynnette, primary, Meder, Lydia, primary, Lovly, Christine M., primary, Persigehl, Thorsten, primary, Merkelbach-Bruse, Sabine, primary, Bos, Marc, primary, Michels, Sebastian, primary, Fischer, Rieke, primary, Albus, Kerstin, primary, König, Katharina, primary, Schildhaus, Hans-Ulrich, primary, Fassunke, Jana, primary, Ihle, Michaela A., primary, Pasternack, Helen, primary, Heydt, Carina, primary, Becker, Christian, primary, Altmüller, Janine, primary, Ji, Hongbin, primary, Müller, Christian, primary, Florin, Alexandra, primary, Heuckmann, Johannes M., primary, Nuernberg, Peter, primary, Ansén, Sascha, primary, Heukamp, Lukas C., primary, Berg, Johannes, primary, Pao, William, primary, Peifer, Martin, primary, Buettner, Reinhard, primary, Wolf, Jürgen, primary, Thomas, Roman K., primary, and Sos, Martin L., primary

Published
2023
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23. METFusions in NSCLC: Clinicopathologic Features and Response to MET Inhibition

Author

Riedel, Richard, Fassunke, Jana, Scheel, Andreas H., Scheffler, Matthias, Heydt, Carina, Nogova, Lucia, Michels, Sebastian, Fischer, Rieke N., Eisert, Anna, Scharpenseel, Heather, John, Felix, Ruge, Lea, Schaufler, Diana, Siemanowski, Janna, Ihle, Michaela A., Wagener-Ryczek, Svenja, Pappesch, Roberto, Rehker, Jan, Bunck, Anne, Kobe, Carsten, Keil, Felix, Merkelbach-Bruse, Sabine, Büttner, Reinhard, and Wolf, Jürgen

Abstract

METfusions have been described only rarely in NSCLC. Thus, data on patient characteristics and treatment response are limited. We here report histopathologic data, patient demographics, and treatment outcome including response to MET tyrosine kinase inhibitor (TKI) therapy in METfusion-positive NSCLC.

Published
2024
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24. EGFR T790M mutation testing of non-small cell lung cancer tissue and blood samples artificially spiked with circulating cell-free tumor DNA: results of a round robin trial

Author

Fassunke, Jana, Ihle, Michaela Angelika, Lenze, Dido, Lehmann, Annika, Hummel, Michael, Vollbrecht, Claudia, Penzel, Roland, Volckmar, Anna-Lena, Stenzinger, Albrecht, Endris, Volker, Jung, Andreas, Lehmann, Ulrich, Zeugner, Silke, Baretton, Gustavo, Kreipe, Hans, Schirmacher, Peter, Kirchner, Thomas, Dietel, Manfred, Büttner, Reinhard, and Merkelbach-Bruse, Sabine

Published
2017
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25. Overcoming EGFRG724S-mediated osimertinib resistance through unique binding characteristics of second-generation EGFR inhibitors

Author

Fassunke, Jana, Müller, Fabienne, Keul, Marina, Michels, Sebastian, Dammert, Marcel A., Schmitt, Anna, Plenker, Dennis, Lategahn, Jonas, Heydt, Carina, Brägelmann, Johannes, Tumbrink, Hannah L., Alber, Yannic, Klein, Sebastian, Heimsoeth, Alena, Dahmen, Ilona, Fischer, Rieke N., Scheffler, Matthias, Ihle, Michaela A., Priesner, Vanessa, Scheel, Andreas H., Wagener, Svenja, Kron, Anna, Frank, Konrad, Garbert, Katia, Persigehl, Thorsten, Püsken, Michael, Haneder, Stefan, Schaaf, Bernhard, Rodermann, Ernst, Engel-Riedel, Walburga, Felip, Enriqueta, Smit, Egbert F., Merkelbach-Bruse, Sabine, Reinhardt, H. Christian, Kast, Stefan M., Wolf, Jürgen, Rauh, Daniel, Büttner, Reinhard, and Sos, Martin L.

Published
2018
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26. Clinicopathological Characteristics of RET Rearranged Lung Cancer in European Patients

Author

Michels, Sebastian, Scheel, Andreas Hans, Scheffler, Matthias, Schultheis, Anne Maria, Gautschi, Oliver, Aebersold, Franziska, Diebold, Joachim, Pall, Georg, Rothschild, Sacha, Bubendorf, Lukas, Hartmann, Wolfgang, Heukamp, Lukas, Schildhaus, Hans-Ulrich, Fassunke, Jana, Ihle, Michaela Angelika, Künstlinger, Helen, Heydt, Carina, Fischer, Rieke, Nogovà, Lucia, Mattonet, Christian, Hein, Rebecca, Adams, Anne, Gerigk, Ulrich, Schulte, Wolfgang, Lüders, Heike, Grohé, Christian, Graeven, Ullrich, Müller-Naendrup, Clemens, Draube, Andreas, Kambartel, Karl-Otto, Krüger, Stefan, Schulze-Olden, Susanne, Serke, Monika, Engel-Riedel, Walburga, Kaminsky, Britta, Randerath, Winfried, Merkelbach-Bruse, Sabine, Büttner, Reinhard, and Wolf, Jürgen

Published
2016
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27. Impact of the interplay between stemness features, p53 and pol iota on replication pathway choices

Author

Ihle, Michaela, Biber, Stephanie, Schroeder, Insa S, Blattner, Christine, Deniz, Miriam, Damia, Giovanna, Gottifredi, Vanesa, and Wiesmüller, Lisa

Subjects
Life sciences, biology, DNA Replication, AcademicSubjects/SCI00010, Replikation, DNA-Directed DNA Polymerase, Genome Integrity, Repair and Replication, DNA replication, Repair and replication, DDC 570 / Life sciences, Stress, Physiological, ddc:570, Humans, Cells, Cultured, Embryonic Stem Cells, integumentary system, Stem Cells, DNA Helicases, Cell Differentiation, Genome integrity, nervous system, ddc:540, DNA Polymerase iota, Neoplastic Stem Cells, Tumor Suppressor Protein p53, tissues
Abstract

Using human embryonic, adult and cancer stem cells/stem cell-like cells (SCs), we demonstrate that DNA replication speed differs in SCs and their differentiated counterparts. While SCs decelerate DNA replication, differentiated cells synthesize DNA faster and accumulate DNA damage. Notably, both replication phenotypes depend on p53 and polymerase iota (POL ). By exploring protein interactions and newly synthesized DNA, we show that SCs promote complex formation of p53 and POL at replication sites. Intriguingly, in SCs the translocase ZRANB3 is recruited to POL and required for slow-down of DNA replication. The known role of ZRANB3 in fork reversal suggests that the p53–POL complex mediates slow but safe bypass of replication barriers in SCs. In differentiated cells, POL localizes more transiently to sites ofDNA synthesis and no longer interactswith p53 facilitating fast POL -dependent DNA replication. In this alternative scenario, POL associates with the p53 target p21, which antagonizes PCNA polyubiquitination and, thereby potentially disfavors the recruitment of translocases. Altogether, we provide evidence for diametrically opposed DNA replication phenotypes in SCs and their differentiated counterparts putting DNA replication-based strategies in the spotlight for the creation of therapeutic opportunities targeting SCs., publishedVersion

Published
2021

29. Implementation of Amplicon Parallel Sequencing Leads to Improvement of Diagnosis and Therapy of Lung Cancer Patients

Author

König, Katharina, Peifer, Martin, Fassunke, Jana, Ihle, Michaela A., Künstlinger, Helen, Heydt, Carina, Stamm, Katrin, Ueckeroth, Frank, Vollbrecht, Claudia, Bos, Marc, Gardizi, Masyar, Scheffler, Matthias, Nogova, Lucia, Leenders, Frauke, Albus, Kerstin, Meder, Lydia, Becker, Kerstin, Florin, Alexandra, Rommerscheidt-Fuss, Ursula, Altmüller, Janine, Kloth, Michael, Nürnberg, Peter, Henkel, Thomas, Bikár, Sven-Ernö, Sos, Martin L., Geese, William J., Strauss, Lewis, Ko, Yon-Dschun, Gerigk, Ulrich, Odenthal, Margarete, Zander, Thomas, Wolf, Jürgen, Merkelbach-Bruse, Sabine, Buettner, Reinhard, and Heukamp, Lukas C.

Published
2015
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30. Connections between stem cell features, EMT, DNA Replication and DNA damage response : mechanisms and therapeutic implication

Author

Ihle, Michaela, Wiesmüller, Lisa, Gottifredi, Vanesa, and Kleger, Alexander

Subjects
Replikation, ddc:610, Stem cells, DNA replication, Genes, p53, DDC 610 / Medicine & health, Stammzelle, Polymerase Iota, Protein p53
Abstract

Up to date the impact of stemness features as well as epithelial to mesenchymal transition (EMT) on DNA repair and vice versa was intensively studied. On the contrary the effect of stemness and EMT on DNA replication and therefore, on DNA damage tolerance (DDT) pathways remained almost unknown. Hence, the aim of my dissertation was to elucidate replication phenotype differences between human stem and differentiated (diff) cells and determine the underlying mechanisms. To this end, I applied DNA Fiber Spreading Assay to three human cell models: embryonic, adult as well as cancer stem cell-like cells and their corresponding diff counterparts for determining the impact of stemness features on replication. Furthermore, proximity ligation assay as well as co-immunoprecipiation assays were used to demonstrate protein associations. Additionally, cell survival assays and immunofluorescence as well as protein expression analysis were performed to determine the impact of stemness on durg as well as DNA damage response. Interestingly, the results of my dissertation revealed that in human cells differentiation causes accelerated DNA replication. Notably, replication in stem as well as diff cells depends on p53 and translesion synthesis (TLS) polymerase iota (POLι) but neither on doubling time nor on the metabolism. I could elucidate that in stem cells the p53-POLι idling complex is formed, guaranteeing poly-ubiquitination of proliferating cell nuclear antigen (PCNA) by helicaselike transcription factor (HLTF) and error-free lesion bypass via recruitment of zinc finger Ran-binding domain containing protein 3 (ZRANB3). This translocase then mediates fork reversal to overcome the barrier by change of the template strand and new DNA synthesis by POLι. In diff cells, p53 plays a more regulatory role and impacts DNA replication most probably due to transcriptional transactivation. This cell type shows elevated ratios of mono- to poly-ubiquitinated PCNA levels consistent with lesion bypass via TLS by POLι. Beside p53 and POLι replication also relies on the p53 targets p21, mouse double minute 2 (MDM2) and ribonucleotide reductase (RNR) regulatory p53 inducible subunit M2B (p53R2) whose functions have not been fully elucidated yet and will need further investigation. Based on the current literature together with my results p21 most likely regulates loading of proteins like POLι to PCNA and possibly influence PCNA ubiquitination pattern and therefore, DDT pathway choice in both cell types. MDM2 remodels chromatin and removes R-loops in both cell types. Furthermore, in stem cells MDM2 binds p53 to probably scaffold formation of the p53-POLι complex. p53R2 ensures in association with the large subunit of the RNR R1 the deoxyribonucleoside triphosphate supply and possibly promotes MDM2 replacement at p53 by POLι, guaranteeing the formation of the idling complex. Remarkably, I also obtained hints indicating a major impact of p53 or p21 levels on DDT pathway choice. Nevertheless, also these findings will need further investigation, to fully disclose the impact of p53 amounts. Up to date it is not known if stemness, p53 levels or both determine DDT pathway choice. Importantly, my results imply that DDT selection could affect DNA double-strand break levels and that stem cells prevent DNA damage accumulation and most likely maintain their genome stability and hence cell survival by choosing idling-DDT. Furthermore, the outcomes of my experiments indicate that cancer cells hi-jack this DDT preferred by stem cells resulting in resistance against DNA damage inducing agents, which are often applied in chemotherapy. Overall, this dissertation represents a solid basis for continuative experiments evolving the detailed mechanistical switch in replication between stem as well as differentiated cells. In the future, this knowledge could then be used for the development of personalized therapies of cancer stem cell-like cells as well as stem cell therapies.

Published
2021
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31. Synergistic targeting and resistance to PARP inhibition in DNA damage repair-deficient pancreatic cancer

Author

Gout, Johann, Perkhofer, Lukas, Morawe, Mareen, Arnold, Frank, Ihle, Michaela, Lange, Sebastian, Roger, Elodie, Kraus, Johann M., Stifter, Katja, Hahn, Stephan A., Zamperone, Andrea, Engleitner, Thomas, Müller, Martin, Walter, Karolin, Rodriguez-Aznar, Eva, Sainz Jr, Bruno, Hermann, Patrick C., Hessmann, Elisabeth, Müller, Sebastian, Azoitei, Ninel, Lechel, Andre, Liebau, Stefan, Wagner, Martin, Simeone, Diane M., Kestler, Hans A., Seufferlein, Thomas, Wiesmüller, Lisa, Rad, Roland, Frappart, Pierre-Olivier, and Kleger, Alexander

Subjects
ddc:610, DNS-Schädigung, DDC 610 / Medicine & health, DNA Damage
Abstract

Objective ATM serine/threonine kinase (ATM) is the most frequently mutated DNA damage response gene, involved in homologous recombination (HR), in pancreatic ductal adenocarcinoma (PDAC). Design Combinational synergy screening was performed to endeavour a genotype-tailored targeted therapy. Results Synergy was found on inhibition of PARP, ATR and DNA-PKcs (PAD) leading to synthetic lethality in ATM-deficient murine and human PDAC. Mechanistically, PAD-induced PARP trapping, replication fork stalling and mitosis defects leading to P53-mediated apoptosis. Most importantly, chemical inhibition of ATM sensitises human PDAC cells toward PAD with long-term tumour control in vivo. Finally, we anticipated and elucidated PARP inhibitor resistance within the ATM-null background via whole exome sequencing. Arising cells were aneuploid, underwent epithelial-mesenchymal-transition and acquired multidrug resistance (MDR) due to upregulation of drug transporters and a bypass within the DNA repair machinery. These functional observations were mirrored in copy number variations affecting a region on chromosome 5 comprising several of the upregulated MDR genes. Using these findings, we ultimately propose alternative strategies to overcome the resistance. Conclusion Analysis of the molecular susceptibilities triggered by ATM deficiency in PDAC allow elaboration of an efficient mutation-specific combinational therapeutic approach that can be also implemented in a genotype-independent manner by ATM inhibition., publishedVersion

Published
2020

32. Co-occurrence of targetable mutations in Non-small cell lung cancer (NSCLC) patients harboring MAP2K1 mutations

Author

Scheffler, Matthias, Holzem, Alessandra, Kron, Anna, Nogova, Lucia, Ihle, Michaela A., von Levetzow, Cornelia, Fassunke, Jana, Woempner, Claudia, Bitter, Elisabeth, Koleczko, Sophia, Abdulla, Diana S. Y., Michels, Sebastian, Fischer, Rieke, Riedel, Richard, Weber, Jan-Philipp, Westphal, Theresa, Gerigk, Ulrich, Kern, Jens, Kaminsky, Britta, Randerath, Winfried, Kambartel, Karl-Otto, Merkelbach-Bruse, Sabine, Buttner, Reinhard, Wolf, Juergen, Scheffler, Matthias, Holzem, Alessandra, Kron, Anna, Nogova, Lucia, Ihle, Michaela A., von Levetzow, Cornelia, Fassunke, Jana, Woempner, Claudia, Bitter, Elisabeth, Koleczko, Sophia, Abdulla, Diana S. Y., Michels, Sebastian, Fischer, Rieke, Riedel, Richard, Weber, Jan-Philipp, Westphal, Theresa, Gerigk, Ulrich, Kern, Jens, Kaminsky, Britta, Randerath, Winfried, Kambartel, Karl-Otto, Merkelbach-Bruse, Sabine, Buttner, Reinhard, and Wolf, Juergen

Abstract

Background: MAP2K1 mutations are rare in non-small cell lung cancer (NSCLC) and considered to be mutually exclusive from known driver mutations. Activation of the MEK1-cascade is considered pivotal in resistance to targeted therapy approaches, and MAP2K1 K57 N mutation could be linked to resistance in preclinical models. We set out this study to detect MAP2K1 mutations and potentially targetable co-mutations using a molecular multiplex approach. Methods: Between 2012 and 2018, we routinely analyzed 14.512 NSCLC patients with two next-generation sequencing (NGS) panels. In a subset of patients, fluorescence in-situ hybridization was performed to detect rearrangements or amplifications. We assessed clinical parameters and co-occurring mutations and compared treatment outcomes of different forms of systemic therapy. Results: We identified 66 (0.5%) patients with MAP2K1 mutations. Both adenocarcinoma (n = 62) and squamous cell carcinoma (n = 4) histology. The presence of the mutations was linked to smoking, and transversions were more common than transitions. K57 N was the most frequent MAP2K1 mutation (n = 25). Additional mutations were found in 57 patients (86.4%). Mutations of TP53 were detected in 33 patients, followed by KEAP1 mutations in 28.1%. 24 patients (36.4%) had either MAP2K1-only or a co-occurring aberration considered targetable, including EGFR mutations, a BRAF V600E mutation and ROS1 rearrangements. Outcome analyses revealed a trend toward benefit from pemetrexed treatment. Conclusion: Our analysis shows that MAP2K1-mutated NSCLC patients might frequently present with potentially targetable aberrations. Their role in providing resistance in these subtypes and the possible therapeutic opportunities justify further analyses of this rare NSCLC subgroup.

Published
2020

33. Synergistic targeting and resistance to PARP inhibition in DNA damage repair-deficient pancreatic cancer

Author

German Cancer Aid, German Research Foundation, Ulm University, Ministry for Science and Culture of Lower Saxony, Deutsche Krebshilfe, Gout, Johann, Perkhofer, Lukas, Morawe, Mareen, Arnold, Frank, Ihle, Michaela, Biber, Stephanie, Lange, Sebastian, Roger, Elodie, Kraus, Johann M., Stifter, Katja, Hahn, Stephan A., Zamperone, Andrea, Engleitner, Thomas, Müller, Martin, Walter, Karolin, Rodriguez-Aznar, Eva, Sainz, Bruno Jr., Hermann, Patrick C., Hessmann, Elisabeth, Müller, Sebastian, Azoitei, Ninel, Lechel, André, Liebau, Stefan, Wagner, Martin, Simeone, Diane M., Kestler, Hans A., Seufferlein, Thomas, Wiesmüller, Lisa, Rad, Roland, Frappart, Pierre-Olivier, Kleger, Alexander, German Cancer Aid, German Research Foundation, Ulm University, Ministry for Science and Culture of Lower Saxony, Deutsche Krebshilfe, Gout, Johann, Perkhofer, Lukas, Morawe, Mareen, Arnold, Frank, Ihle, Michaela, Biber, Stephanie, Lange, Sebastian, Roger, Elodie, Kraus, Johann M., Stifter, Katja, Hahn, Stephan A., Zamperone, Andrea, Engleitner, Thomas, Müller, Martin, Walter, Karolin, Rodriguez-Aznar, Eva, Sainz, Bruno Jr., Hermann, Patrick C., Hessmann, Elisabeth, Müller, Sebastian, Azoitei, Ninel, Lechel, André, Liebau, Stefan, Wagner, Martin, Simeone, Diane M., Kestler, Hans A., Seufferlein, Thomas, Wiesmüller, Lisa, Rad, Roland, Frappart, Pierre-Olivier, and Kleger, Alexander

Abstract

[Objective]: ATM serine/threonine kinase (ATM) is the most frequently mutated DNA damage response gene, involved in homologous recombination (HR), in pancreatic ductal adenocarcinoma (PDAC)., [Design]: Combinational synergy screening was performed to endeavour a genotype-tailored targeted therapy., [Results]: Synergy was found on inhibition of PARP, ATR and DNA-PKcs (PAD) leading to synthetic lethality in ATM-deficient murine and human PDAC. Mechanistically, PAD-induced PARP trapping, replication fork stalling and mitosis defects leading to P53-mediated apoptosis. Most importantly, chemical inhibition of ATM sensitises human PDAC cells toward PAD with long-term tumour control in vivo. Finally, we anticipated and elucidated PARP inhibitor resistance within the ATM-null background via whole exome sequencing. Arising cells were aneuploid, underwent epithelial-mesenchymal-transition and acquired multidrug resistance (MDR) due to upregulation of drug transporters and a bypass within the DNA repair machinery. These functional observations were mirrored in copy number variations affecting a region on chromosome 5 comprising several of the upregulated MDR genes. Using these findings, we ultimately propose alternative strategies to overcome the resistance., [Conclusion]: Analysis of the molecular susceptibilities triggered by ATM deficiency in PDAC allow elaboration of an efficient mutation-specific combinational therapeutic approach that can be also implemented in a genotype-independent manner by ATM inhibition.

Published
2020

34. Synergistic targeting and resistance to PARP inhibition in DNA damage repair-deficient pancreatic cancer

Author

Gout, Johann, primary, Perkhofer, Lukas, additional, Morawe, Mareen, additional, Arnold, Frank, additional, Ihle, Michaela, additional, Biber, Stephanie, additional, Lange, Sebastian, additional, Roger, Elodie, additional, Kraus, Johann M, additional, Stifter, Katja, additional, Hahn, Stephan A, additional, Zamperone, Andrea, additional, Engleitner, Thomas, additional, Müller, Martin, additional, Walter, Karolin, additional, Rodriguez-Aznar, Eva, additional, Sainz Jr, Bruno, additional, Hermann, Patrick C, additional, Hessmann, Elisabeth, additional, Müller, Sebastian, additional, Azoitei, Ninel, additional, Lechel, André, additional, Liebau, Stefan, additional, Wagner, Martin, additional, Simeone, Diane M, additional, Kestler, Hans A, additional, Seufferlein, Thomas, additional, Wiesmüller, Lisa, additional, Rad, Roland, additional, Frappart, Pierre-Olivier, additional, and Kleger, Alexander, additional

Published
2020
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35. Co-occurrence of targetable mutations in Non-small cell lung cancer (NSCLC) patients harboring MAP2K1 mutations

Author

Scheffler, Matthias, primary, Holzem, Alessandra, additional, Kron, Anna, additional, Nogova, Lucia, additional, Ihle, Michaela A., additional, von Levetzow, Cornelia, additional, Fassunke, Jana, additional, Wömpner, Claudia, additional, Bitter, Elisabeth, additional, Koleczko, Sophia, additional, Abdulla, Diana S.Y., additional, Michels, Sebastian, additional, Fischer, Rieke, additional, Riedel, Richard, additional, Weber, Jan-Philipp, additional, Westphal, Theresa, additional, Gerigk, Ulrich, additional, Kern, Jens, additional, Kaminsky, Britta, additional, Randerath, Winfried, additional, Kambartel, Karl-Otto, additional, Merkelbach-Bruse, Sabine, additional, Büttner, Reinhard, additional, and Wolf, Jürgen, additional

Published
2020
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36. Genomic Profiling Identifies Outcome-Relevant Mechanisms of Innate and Acquired Resistance to Third-Generation Epidermal Growth Factor Receptor Tyrosine Kinase Inhibitor Therapy in Lung Cancer

Author

Michels, Sebastian, primary, Heydt, Carina, additional, van Veggel, Bianca, additional, Deschler-Baier, Barbara, additional, Pardo, Nuria, additional, Monkhorst, Kim, additional, Rüsseler, Vanessa, additional, Stratmann, Jan, additional, Griesinger, Frank, additional, Steinhauser, Susanne, additional, Kostenko, Anna, additional, Diebold, Joachim, additional, Fassunke, Jana, additional, Fischer, Rieke, additional, Engel-Riedel, Walburga, additional, Gautschi, Oliver, additional, Geissinger, Eva, additional, Haneder, Stefan, additional, Ihle, Michaela A., additional, Kopp, Hans-Georg, additional, de Langen, Adrianus J., additional, Martinez-Marti, Alex, additional, Nogova, Lucia, additional, Persigehl, Thorsten, additional, Plenker, Dennis, additional, Puesken, Michael, additional, Rodermann, Ernst, additional, Rosenwald, Andreas, additional, Scheel, Andreas H., additional, Scheffler, Matthias, additional, Spengler, Werner, additional, Seggewiss-Bernhardt, Ruth, additional, Brägelmann, Johannes, additional, Sebastian, Martin, additional, Vrugt, Bart, additional, Hellmich, Martin, additional, Sos, Martin L., additional, Heukamp, Lukas C., additional, Felip, Enriqueta, additional, Merkelbach-Bruse, Sabine, additional, Smit, Egbert F., additional, Büttner, Reinhard, additional, and Wolf, Jürgen, additional

Published
2019
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37. Genomic Profiling Identifies Outcome-Relevant Mechanisms of Innate and Acquired Resistance to Third-Generation Epidermal Growth Factor Receptor Tyrosine Kinase Inhibitor Therapy in Lung Cancer

Author

Michels, Sebastian, Heydt, Carina, van Veggel, Bianca, Deschler-Baier, Barbara, Pardo, Nuria, Monkhorst, Kim, Ruesseler, Vanessa, Stratmann, Jan, Griesinger, Frank, Steinhauser, Susanne, Kostenko, Anna, Diebold, Joachim, Fassunke, Jana, Fischer, Rieke, Engel-Riedel, Walburga, Gautschi, Oliver, Geissinger, Eva, Haneder, Stefan, Ihle, Michaela A., Kopp, Hans-Georg, de Langen, Adrianus J., Martinez-Marti, Alex, Nogova, Lucia, Persigehl, Thorsten, Plenker, Dennis, Puesken, Michael, Rodermann, Ernst, Rosenwald, Andreas, Scheel, Andreas H., Scheffler, Matthias, Spengler, Werner, Seggewiss-Bernhardt, Ruth, Braegelmann, Johannes, Sebastian, Martin, Vrugt, Bart, Hellmich, Martin, Sos, Martin L., Heukamp, Lukas C., Felip, Enriqueta, Merkelbach-Bruse, Sabine, Smit, Egbert F., Buettner, Reinhard, Wolf, Juergen, Michels, Sebastian, Heydt, Carina, van Veggel, Bianca, Deschler-Baier, Barbara, Pardo, Nuria, Monkhorst, Kim, Ruesseler, Vanessa, Stratmann, Jan, Griesinger, Frank, Steinhauser, Susanne, Kostenko, Anna, Diebold, Joachim, Fassunke, Jana, Fischer, Rieke, Engel-Riedel, Walburga, Gautschi, Oliver, Geissinger, Eva, Haneder, Stefan, Ihle, Michaela A., Kopp, Hans-Georg, de Langen, Adrianus J., Martinez-Marti, Alex, Nogova, Lucia, Persigehl, Thorsten, Plenker, Dennis, Puesken, Michael, Rodermann, Ernst, Rosenwald, Andreas, Scheel, Andreas H., Scheffler, Matthias, Spengler, Werner, Seggewiss-Bernhardt, Ruth, Braegelmann, Johannes, Sebastian, Martin, Vrugt, Bart, Hellmich, Martin, Sos, Martin L., Heukamp, Lukas C., Felip, Enriqueta, Merkelbach-Bruse, Sabine, Smit, Egbert F., Buettner, Reinhard, and Wolf, Juergen

Abstract

PURPOSE Third-generation epidermal growth factor receptor (EGFR) tyrosine kinase inhibitors (TKIs) are effective in acquired resistance (AR) to early-generation EGFR TKIs in EGFR-mutant lung cancer. However, efficacy is marked by interindividual heterogeneity. We present the molecular profiles of pretreatment and post-treatment samples from patients treated with third-generation EGFR TKIs and their impact on treatment outcomes. METHODS Using the databases of two lung cancer networks and two lung cancer centers, we molecularly characterized 124 patients with EGFR p. T790M-positive AR to early-generation EGFR TKIs. In 56 patients, correlative analyses of third-generation EGFR TKI treatment outcomes and molecular characteristics were feasible. In addition, matched post-treatment biopsy samples were collected for 29 patients with progression to third-generation EGFR TKIs. RESULTS Co-occurring genetic aberrations were found in 74.4% of EGFR p. T790-positive samples (n = 124). Mutations in TP53 were the most frequent aberrations detected (44.5%; n = 53) and had no significant impact on third-generation EGFR TKI treatment. Mesenchymal-epithelial transition factor (MET) amplifications were found in 5% of samples (n = 6) and reduced efficacy of third-generation EGFR TKIs significantly (eg, median progression-free survival, 1.0 months; 95% CI, 0.37 to 1.72 v 8.2 months; 95% CI, 1.69 to 14.77 months; P <= .001). Genetic changes in the 29 samples with AR to third-generation EGFR TKIs were found in EGFR (eg, p.T790M loss, acquisition of p.C797S or p.G724S) or in other genes (eg, MET amplification, KRAS mutations). CONCLUSION Additional genetic aberrations are frequent in EGFR-mutant lung cancer and may mediate innate and AR to third-generation EGFR TKIs. MET amplification was strongly associated with primary treatment failure and was a common mechanism of AR to third-generation EGFR TKIs. Thus, combining EGFR inhibitors with TKIs targeting common mechanisms of resistance may del

Published
2019

38. Synergistic targeting and resistance to PARP inhibition in DNA damage repair-deficient pancreatic cancer.

Author

Gout, Johann, Perkhofer, Lukas, Morawe, Mareen, Arnold, Frank, Ihle, Michaela, Biber, Stephanie, Lange, Sebastian, Roger, Elodie, Kraus, Johann M., Stifter, Katja, Hahn, Stephan A., Zamperone, Andrea, Engleitner, Thomas, Müller, Martin, Walter, Karolin, Rodriguez-Aznar, Eva, Jr, Bruno Sainz, Hermann, Patrick C., Hessmann, Elisabeth, and Müller, Sebastian

Subjects
DNA damage, PANCREATIC cancer, POLY(ADP-ribose) polymerase, DNA polymerases, SERINE/THREONINE kinases, CIRCULATING tumor DNA, PANCREATIC intraepithelial neoplasia, LYMPHOBLASTOID cell lines
Published
2021
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39. Expression of cell cycle regulators and frequency of TP53 mutations in high risk gastrointestinal stromal tumors prior to adjuvant imatinib treatment

Author

Ihle, Michaela Angelika, Huss, Sebastian, Jeske, Wiebke, Hartmann, Wolfgang, Merkelbach-Bruse, Sabine, Schildhaus, Hans-Ulrich, Buettner, Reinhard, Sihto, Harri, Hall, Kirsten Sundby, Eriksson, Mikael, Reichardt, Peter, Joensuu, Heikki, Wardelmann, Eva, Ihle, Michaela Angelika, Huss, Sebastian, Jeske, Wiebke, Hartmann, Wolfgang, Merkelbach-Bruse, Sabine, Schildhaus, Hans-Ulrich, Buettner, Reinhard, Sihto, Harri, Hall, Kirsten Sundby, Eriksson, Mikael, Reichardt, Peter, Joensuu, Heikki, and Wardelmann, Eva

Abstract

Despite of multitude investigations no reliable prognostic immunohistochemical biomarkers in GIST have been established so far with added value to predict the recurrence risk of high risk GIST besides mitotic count, primary location and size. In this study, we analyzed the prognostic relevance of eight cell cycle and apoptosis modulators and of TP53 mutations for prognosis in GIST with high risk of recurrence prior to adjuvant treatment with imatinib. In total, 400 patients with high risk for GIST recurrence were randomly assigned for adjuvant imatinib either for one or for three years following laparotomy. 320 primary tumor samples with available tumor tissue were immunohistochemically analyzed prior to treatment for the expression of cell cycle regulators and apoptosis modulators cyclin D1, p21, p16, CDK4, E2F1, MDM2, p53 and p-RB1. TP53 mutational analysis was possible in 245 cases. A high expression of CDK4 was observed in 32.8% of all cases and was associated with a favorable recurrence free survival (RFS), whereas high expression of MDM2 (12.2%) or p53 (35.3%) was associated with a shorter RFS. These results were independent from the primary KIT or PDGFRA mutation. In GISTs with higher mitotic counts was a significantly increased expression of cyclin D1, p53 and E2F1. The expression of p16 and E2F1 significantly correlated to a non-gastric localization. Furthermore, we observed a significant higher expression of p21 and E2F1 in KIT mutant GISTs compared to PDGFRA mutant and wt GISTs. The overall frequency of TP53 mutations was low (n = 8; 3.5%) and could not be predicted by the immunohistochemical expression of p53. In summary, mutation analysis in TP53 plays a minor role in the subgroup of high-risk GIST before adjuvant treatment with imatinib. Strong expression of MDM2 and p53 correlated with a shorter recurrence free survival, whereas a strong expression of CDK4 correlated to a better recurrence free survival.

Published
2018

40. ClinicalandPathological Characteristics of KEAP1- and NFE2L2-Mutated Non-Small Cell Lung Carcinoma (NSCLC)

Author

Frank, Rieke, Scheffler, Matthias, Merkelbach-Bruse, Sabine, Ihle, Michaela A., Kron, Anna, Rauer, Michael, Ueckeroth, Frank, Koenig, Katharina, Michels, Sebastian, Fischer, Rieke, Eisert, Anna, Fassunke, Jana, Heydt, Carina, Serke, Monika, Ko, Yon-Dschun, Gerigk, Ulrich, Geist, Thomas, Kaminsky, Britta, Heukamp, Lukas C., Clement-Ziza, Mathieu, Buettner, Reinhard, Wolf, Juergen, Frank, Rieke, Scheffler, Matthias, Merkelbach-Bruse, Sabine, Ihle, Michaela A., Kron, Anna, Rauer, Michael, Ueckeroth, Frank, Koenig, Katharina, Michels, Sebastian, Fischer, Rieke, Eisert, Anna, Fassunke, Jana, Heydt, Carina, Serke, Monika, Ko, Yon-Dschun, Gerigk, Ulrich, Geist, Thomas, Kaminsky, Britta, Heukamp, Lukas C., Clement-Ziza, Mathieu, Buettner, Reinhard, and Wolf, Juergen

Abstract

Purpose: KEAP1 and NFE2L2 mutations are associated with impaired prognosis in a variety of cancers and with squamous cell carcinoma formation in non-small cell lung cancer (NSCLC). However, little is known about frequency, histology dependence, molecular and clinical presentation as well as response to systemic treatment in NSCLC. Experimental Design: Tumor tissue of 1,391 patients with NSCLC was analyzed using next-generation sequencing (NGS). Clinical and pathologic characteristics, survival, and treatment outcome of patients with KEAP1 or NFE2L2 mutations were assessed. Results: KEAP1 mutations occurred with a frequency of 11.3% (n = 157) and NFE2L2 mutations with a frequency of 3.5% (n = 49) in NSCLC patients. In the vast majority of patients, both mutations did not occur simultaneously. KEAP1 mutations were found mainly in adenocarcinoma (AD; 72%), while NFE2L2 mutations were more common in squamous cell carcinoma (LSCC; 59%). KEAP1 mutations were spread over the whole protein, whereas NFE2L2 mutations were clustered in specific hotspot regions. In over 80% of the patients both mutations co-occurred with other cancer-related mutations, among them also targetable aberrations like activating EGFR mutations or MET amplification. Both patient groups showed different patterns of metastases, stage distribution and performance state. No patient with KEAP1 mutation had a response on systemic treatment in first-, second-, or third-line setting. Of NFE2L2-mutated patients, none responded to second-or third-line therapy. Conclusions: KEAP1- and NFE2L2-mutated NSCLC patients represent a highly heterogeneous patient cohort. Both are associated with different histologies and usually are found together with other cancer-related, partly targetable, genetic aberrations. In addition, both markers seem to be predictive for chemotherapy resistance. (C) 2018 AACR.

Published
2018

41. Genetic instability and recurrent MYC amplification in ALK-translocated NSCLC: a central role of TP53 mutations

Author

Alidousty, Christina, Baar, Till, Martelotto, Luciano G., Heydt, Carina, Wagener, Svenja, Fassunke, Jana, Duerbaum, Nicolai, Scheel, Andreas H., Frank, Sandra, Holz, Barbara, Binot, Elke, Kron, Anna, Merkelbach-Bruse, Sabine, Ihle, Michaela A., Wolf, Juergen, Buettner, Reinhard, Schultheis, Anne Maria, Alidousty, Christina, Baar, Till, Martelotto, Luciano G., Heydt, Carina, Wagener, Svenja, Fassunke, Jana, Duerbaum, Nicolai, Scheel, Andreas H., Frank, Sandra, Holz, Barbara, Binot, Elke, Kron, Anna, Merkelbach-Bruse, Sabine, Ihle, Michaela A., Wolf, Juergen, Buettner, Reinhard, and Schultheis, Anne Maria

Abstract

The anaplastic lymphoma kinase (ALK) rearrangement defines a distinct molecular subtype of non-small cell lung cancer (NSCLC). Despite the excellent initial efficacy of ALK inhibitors in patients with ALK+ lung cancer, resistance occurs almost inevitably. To date, there is no reliable biomarker allowing the identification of patients at higher risk of relapse. Here, we analysed a subset of 53 ALK+ tumors with and without TP53 mutation and ALK+ NSCLC cell lines by NanoString nCounter technology. We found that the co-occurrence of early TP53 mutations in ALK+ NSCLC can lead to chromosomal instability: 24% of TP53-mutated patients showed amplifications of known cancer genes such as MYC (14%), CCND1 (10%), TERT (5%), BIRC2 (5%), ORAOV1 (5%), and YAP1 (5%). MYC-overexpressing ALK+ TP53-mutated cells had a proliferative advantage compared to wild-type cells. ChIP-Seq data revealed MYC-binding sites within the promoter region of EML4, and MYC overexpression in ALK+ TP53-mutated cells resulted in an upregulation of EML4-ALK, indicating a potential MYC-dependent resistance mechanism in patients with increased MYC copy number. Our study reveals that ALK+ NSCLC represents a more heterogeneous subgroup of tumors than initially thought, and that TP53 mutations in that particular cancer type define a subset of tumors that harbour chromosomal instability, leading to the co-occurrence of pathogenic aberrations. (c) 2018 The Authors. The Journal of Pathology published by John Wiley & Sons Ltd on behalf of Pathological Society of Great Britain and Ireland.

Published
2018

42. Impact of TP53 mutation status on systemic treatment outcome in ALK-rearranged non-small-cell lung cancer

Author

Kron, Anna, Alidousty, Christina, Scheffler, Matthias, Merkelbach-Bruse, Sabine, Seidel, Danila, Riedel, Richard, Ihle, Michaela A., Michels, Sebastian Yves Friedrich, Nogova, Lucia, Fassunke, Jana, Heydt, Carina, Kron, Florian, Ueckeroth, Frank, Serke, Monika, Krüger, Stefan, Grohé, Christian, Koschel, Dirk, Benedikter, Josef, Kaminsky, Britta, Schaaf, Bernhard, Braess, Jan, Sebastian, Martin, Kambartel, Karl-Otto, Thomas, Roman, Zander, Thomas, Schultheis, Anne Maria, Büttner, Reinhard, Wolf, Jürgen, Kron, Anna, Alidousty, Christina, Scheffler, Matthias, Merkelbach-Bruse, Sabine, Seidel, Danila, Riedel, Richard, Ihle, Michaela A., Michels, Sebastian Yves Friedrich, Nogova, Lucia, Fassunke, Jana, Heydt, Carina, Kron, Florian, Ueckeroth, Frank, Serke, Monika, Krüger, Stefan, Grohé, Christian, Koschel, Dirk, Benedikter, Josef, Kaminsky, Britta, Schaaf, Bernhard, Braess, Jan, Sebastian, Martin, Kambartel, Karl-Otto, Thomas, Roman, Zander, Thomas, Schultheis, Anne Maria, Büttner, Reinhard, and Wolf, Jürgen

Abstract

Background: We analyzed whether co-occurring mutations influence the outcome of systemic therapy in ALK-rearranged non-small-cell lung cancer (NSCLC). Patients and methods: ALK-rearranged stage IIIB/IV NSCLC patients were analyzed with next-generation sequencing and fluorescence in situ hybridization analyses on a centralized diagnostic platform. Median progression-free survival (PFS) and overall survival (OS) were determined in the total cohort and in treatment-related sub-cohorts. Cox regression analyses were carried out to exclude confounders. Results: Among 216 patients with ALK-rearranged NSCLC, the frequency of pathogenic TP53 mutations was 23.8%, while other co-occurring mutations were rare events. In ALK/TP53 co-mutated patients, median PFS and OS were significantly lower compared with TP53 wildtype patients [PFS 3.9 months (95% CI: 2.4–5.6) versus 10.3 months (95% CI: 8.6–12.0), P < 0.001; OS 15.0 months (95% CI: 5.0–24.9) versus 50.0 months (95% CI: 22.9–77.1), P = 0.002]. This difference was confirmed in all treatment-related subgroups including chemotherapy only [PFS first-line chemotherapy 2.6 months (95% CI: 1.3–4.1) versus 6.2 months (95% CI: 1.8–10.5), P = 0.021; OS 2.0 months (95% CI: 0.0–4.6) versus 9.0 months (95% CI: 6.1–11.9), P = 0.035], crizotinib plus chemotherapy [PFS crizotinib 5.0 months (95% CI: 2.9–7.2) versus 14.0 months (95% CI: 8.0–20.1), P < 0.001; OS 17.0 months (95% CI: 6.7–27.3) versus not reached, P = 0.049] and crizotinib followed by next-generation ALK-inhibitor [PFS next-generation inhibitor 5.4 months (95% CI: 0.1–10.7) versus 9.9 months (95% CI: 6.4–13.5), P = 0.039; OS 7.0 months versus 50.0 months (95% CI: not reached), P = 0.001). Conclusions: In ALK-rearranged NSCLC co-occurring TP53 mutations predict an unfavorable outcome of systemic therapy. Our observations encourage future research to understand the underlying molecular mechanisms and to improve treatment outcome of the ALK/TP53 co-mutated subgroup.

Published
2018

43. Genetic instability and recurrent MYC amplification in ALK- translocated NSCLC: a central role of TP53 mutations

Author

Alidousty, Christina, primary, Baar, Till, additional, Martelotto, Luciano G, additional, Heydt, Carina, additional, Wagener, Svenja, additional, Fassunke, Jana, additional, Duerbaum, Nicolai, additional, Scheel, Andreas H, additional, Frank, Sandra, additional, Holz, Barbara, additional, Binot, Elke, additional, Kron, Anna, additional, Merkelbach-Bruse, Sabine, additional, Ihle, Michaela A, additional, Wolf, Jürgen, additional, Buettner, Reinhard, additional, and Schultheis, Anne Maria, additional

Published
2018
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44. Clinical and Pathological Characteristics of KEAP1- and NFE2L2-Mutated Non–Small Cell Lung Carcinoma (NSCLC)

Author

Frank, Rieke, primary, Scheffler, Matthias, additional, Merkelbach-Bruse, Sabine, additional, Ihle, Michaela A., additional, Kron, Anna, additional, Rauer, Michael, additional, Ueckeroth, Frank, additional, König, Katharina, additional, Michels, Sebastian, additional, Fischer, Rieke, additional, Eisert, Anna, additional, Fassunke, Jana, additional, Heydt, Carina, additional, Serke, Monika, additional, Ko, Yon-Dschun, additional, Gerigk, Ulrich, additional, Geist, Thomas, additional, Kaminsky, Britta, additional, Heukamp, Lukas C., additional, Clement-Ziza, Mathieu, additional, Büttner, Reinhard, additional, and Wolf, Jürgen, additional

Published
2018
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45. Expression of cell cycle regulators and frequency of TP53 mutations in high risk gastrointestinal stromal tumors prior to adjuvant imatinib treatment

Author

Ihle, Michaela Angelika, primary, Huss, Sebastian, additional, Jeske, Wiebke, additional, Hartmann, Wolfgang, additional, Merkelbach-Bruse, Sabine, additional, Schildhaus, Hans-Ulrich, additional, Büttner, Reinhard, additional, Sihto, Harri, additional, Sundby Hall, Kirsten, additional, Eriksson, Mikael, additional, Reichardt, Peter, additional, Joensuu, Heikki, additional, and Wardelmann, Eva, additional

Published
2018
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46. MAP2K1 Mutations in NSCLC: Clinical Presentation and Co-Occurrence of Additional Genetic Aberrations

Author

Holzem, Alessandra, Nogova, Lucia, Ihle, Michaela, Woempner, Claudia, Bitter, Elisabeth, Michels, Sebastian, Lamanna, Alessandra, Christensen, Britt-Marie, Fischer, Rieke, Kaminsky, Britta, Kern, Jens, Graeven, Ullrich, Kostenko, Anna, Merkelbach-Bruse, Sabine, Buettner, Reinhard, Scheffler, Matthias, Wolf, Jurgen, Holzem, Alessandra, Nogova, Lucia, Ihle, Michaela, Woempner, Claudia, Bitter, Elisabeth, Michels, Sebastian, Lamanna, Alessandra, Christensen, Britt-Marie, Fischer, Rieke, Kaminsky, Britta, Kern, Jens, Graeven, Ullrich, Kostenko, Anna, Merkelbach-Bruse, Sabine, Buettner, Reinhard, Scheffler, Matthias, and Wolf, Jurgen

Published
2017

47. Analysis of Potentially Targetable Mutations in 821 Patients with Squamous cell Lung Cancer Undergoing Routine NGS-Based Molecular Diagnostics

Author

Koleczko, Sophia, Schaepers, Carsten, Scheffler, Matthias, Ihle, Michaela, Kostenko, Anna, Michels, Sebastian, Fischer, Rieke, Nogova, Lucia, Serke, Monika, Kaminsky, Britta, Gerigk, Ulrich, Benedikter, Josef, Bruemmendorf, Tim, Ficker, Joachim, Kruis, Wolfgang, Lorenz, Joachim, Schulte, Clemens, Schulze-Olden, Susanne, Merkelbach-Bruse, Sabine, Ueckeroth, Frank, Buttner, Reinhard, Wolf, Juergen, Koleczko, Sophia, Schaepers, Carsten, Scheffler, Matthias, Ihle, Michaela, Kostenko, Anna, Michels, Sebastian, Fischer, Rieke, Nogova, Lucia, Serke, Monika, Kaminsky, Britta, Gerigk, Ulrich, Benedikter, Josef, Bruemmendorf, Tim, Ficker, Joachim, Kruis, Wolfgang, Lorenz, Joachim, Schulte, Clemens, Schulze-Olden, Susanne, Merkelbach-Bruse, Sabine, Ueckeroth, Frank, Buttner, Reinhard, and Wolf, Juergen

Published
2017

48. ATM Deficiency Generating Genomic Instability Sensitizes Pancreatic Ductal Adenocarcinoma Cells to Therapy-Induced DNA Damage

Author

Perkhofer, Lukas, Schmitt, Anna, Carrasco, Maria Carolina Romero, Ihle, Michaela, Hampp, Stephanie, Ruess, Dietrich Alexander, Hessmann, Elisabeth, Russell, Ronan, Lechel, Andre, Azoitei, Ninel, Lin, Qiong, Liebau, Stefan, Hohwieler, Meike, Bohnenberger, Hanibal, Lesina, Marina, Alguel, Hana, Gieldon, Laura, Schroeck, Evelin, Gaedcke, Jochen, Wagner, Martin, Wiesmueller, Lisa, Sipos, Bence, Seufferlein, Thomas, Reinhardt, Hans Christian, Frappart, Pierre-Olivier, Kleger, Alexander, Perkhofer, Lukas, Schmitt, Anna, Carrasco, Maria Carolina Romero, Ihle, Michaela, Hampp, Stephanie, Ruess, Dietrich Alexander, Hessmann, Elisabeth, Russell, Ronan, Lechel, Andre, Azoitei, Ninel, Lin, Qiong, Liebau, Stefan, Hohwieler, Meike, Bohnenberger, Hanibal, Lesina, Marina, Alguel, Hana, Gieldon, Laura, Schroeck, Evelin, Gaedcke, Jochen, Wagner, Martin, Wiesmueller, Lisa, Sipos, Bence, Seufferlein, Thomas, Reinhardt, Hans Christian, Frappart, Pierre-Olivier, and Kleger, Alexander

Abstract

Pancreatic ductal adenocarcinomas (PDAC) harbor recurrent functional mutations of the master DNA damage response kinase ATM, which has been shown to accelerate tumorigenesis and epithelial-mesenchymal transition. To study how ATMdeficiency affects genome integrity in this setting, we evaluated the molecular and functional effects of conditional Atm deletion in a mouse model of PDAC. ATM deficiency was associated with increased mitotic defects, recurrent genomic rearrangements, and deregulated DNA integrity checkpoints, reminiscent of human PDAC. We hypothesized that altered genome integrity might allow synthetic lethality-based options for targeted therapeutic intervention. Supporting this possibility, we found that the PARP inhibitor olaparib or ATR inhibitors reduced the viability of PDAC cells in vitro and in vivo associated with a genotype-selective increase in apoptosis. Overall, our results offered a preclinical mechanistic rationale for the use of PARP and ATR inhibitors to improve treatment of ATM-mutant PDAC. (C) 2017 AACR.

Published
2017

49. Copy number variations in atypical fibroxanthomas and pleomorphic dermal sarcomas

Author

Helbig, Doris, Quaas, Alexander, Mauch, Cornelia, Merkelbach-Bruse, Sabine, Buettner, Reinhard, Emberger, Michael, Wobser, Marion, Ruesseler, Vanessa, Puetz, Katharina, Binot, Elke, Rehker, Jan, Budczies, Jan, Ihle, Michaela Angelika, Helbig, Doris, Quaas, Alexander, Mauch, Cornelia, Merkelbach-Bruse, Sabine, Buettner, Reinhard, Emberger, Michael, Wobser, Marion, Ruesseler, Vanessa, Puetz, Katharina, Binot, Elke, Rehker, Jan, Budczies, Jan, and Ihle, Michaela Angelika

Abstract

Atypical fibroxanthomas (AFX) and pleomorphic dermal sarcomas (PDS) are frequent cutaneous sarcomas typically arising on sun-exposed skin in elderly patients. In contrast to AFX, which generally do not recur after complete excision, PDS locally recur in up to 50% and metastasize in up to 20%. We recently detected characteristic UV-induced TP53 mutations as potential driver mutation in almost all PDS investigated as well as activating PIK3CA and RAS gene mutations in around one third of our tumors representing targets for personalized treatments in patients with unresectable or metastasized PDS. In the present study, we identified amplifications and deletions in a small part of the PDS (6 of 27 cases) but not in AFX suggesting that copy number variations (CNV) might not be an initial event in tumor development but rather important during tumor progression. In addition to BRAF, KNSTRN, IDH1 and PDGFRA amplification, CNV analyses revealed deletions in the CDKN2A, KIT and PDGFRA genes. In cases where an appropriate FISH assay was established, the CNV results could be verified by FISH analysis. Amplification of BRAF, KIT or PDGFRA and/or losses of CDKN2A might represent bad prognostic markers, although larger studies are needed to clarify their association with prognosis or progression in PDS.

Published
2017

50. Copy number variations in atypical fibroxanthomas and pleomorphic dermal sarcomas

Author

Helbig, Doris, primary, Quaas, Alexander, additional, Mauch, Cornelia, additional, Merkelbach-Bruse, Sabine, additional, Büttner, Reinhard, additional, Emberger, Michael, additional, Wobser, Marion, additional, Rüsseler, Vanessa, additional, Pütz, Katharina, additional, Binot, Elke, additional, Rehker, Jan, additional, Budczies, Jan, additional, and Ihle, Michaela Angelika, additional

Published
2017
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