Your search keyword '"Döhner, Konstanze"' showing total 24 results

1. Genomic characterization of AML with aberrations of chromosome 7:a multinational cohort of 519 patients

Author

Halik, Adriane, Tilgner, Marlon, Silva, Patricia, Estrada, Natalia, Altwasser, Robert, Jahn, Ekaterina, Heuser, Michael, Hou, Hsin An, Pratcorona, Marta, Hills, Robert K., Metzeler, Klaus H., Fenwarth, Laurene, Dolnik, Anna, Terre, Christine, Kopp, Klara, Blau, Olga, Szyska, Martin, Christen, Friederike, Krönke, Jan, Vasseur, Loïc, Löwenberg, Bob, Esteve, Jordi, Valk, Peter J.M., Duchmann, Matthieu, Chou, Wen Chien, Linch, David C., Döhner, Hartmut, Gale, Rosemary E., Döhner, Konstanze, Bullinger, Lars, Yoshida, Kenichi, Damm, Frederik, Halik, Adriane, Tilgner, Marlon, Silva, Patricia, Estrada, Natalia, Altwasser, Robert, Jahn, Ekaterina, Heuser, Michael, Hou, Hsin An, Pratcorona, Marta, Hills, Robert K., Metzeler, Klaus H., Fenwarth, Laurene, Dolnik, Anna, Terre, Christine, Kopp, Klara, Blau, Olga, Szyska, Martin, Christen, Friederike, Krönke, Jan, Vasseur, Loïc, Löwenberg, Bob, Esteve, Jordi, Valk, Peter J.M., Duchmann, Matthieu, Chou, Wen Chien, Linch, David C., Döhner, Hartmut, Gale, Rosemary E., Döhner, Konstanze, Bullinger, Lars, Yoshida, Kenichi, and Damm, Frederik

Abstract

Background: Deletions and partial losses of chromosome 7 (chr7) are frequent in acute myeloid leukemia (AML) and are linked to dismal outcome. However, the genomic landscape and prognostic impact of concomitant genetic aberrations remain incompletely understood. Methods: To discover genetic lesions in adult AML patients with aberrations of chromosome 7 [abn(7)], 60 paired diagnostic/remission samples were investigated by whole-exome sequencing in the exploration cohort. Subsequently, a gene panel including 66 genes and a SNP backbone for copy-number variation detection was designed and applied to the remaining samples of the validation cohort. In total, 519 patients were investigated, of which 415 received intensive induction treatment, typically containing a combination of cytarabine and anthracyclines. Results: In the exploration cohort, the most frequently mutated gene was TP53 (33%), followed by epigenetic regulators (DNMT3A, KMT2C, IDH2) and signaling genes (NRAS, PTPN11). Thirty percent of 519 patients harbored ≥ 1 mutation in genes located in commonly deleted regions of chr7—most frequently affecting KMT2C (16%) and EZH2 (10%). KMT2C mutations were often subclonal and enriched in patients with del(7q), de novo or core-binding factor AML (45%). Cancer cell fraction analysis and reconstruction of mutation acquisition identified TP53 mutations as mainly disease-initiating events, while del(7q) or −7 appeared as subclonal events in one-third of cases. Multivariable analysis identified five genetic lesions with significant prognostic impact in intensively treated AML patients with abn(7). Mutations in TP53 and PTPN11 (11%) showed the strongest association with worse overall survival (OS, TP53: hazard ratio [HR], 2.53 [95% CI 1.66–3.86]; P < 0.001; PTPN11: HR, 2.24 [95% CI 1.56–3.22]; P < 0.001) and relapse-free survival (RFS, TP53: HR, 2.3 [95% CI 1.25–4.26]; P = 0.008; PTPN11: HR, 2.32 [95% CI 1.33–

Published

2024

2. Precision hematology:Navigating the evolution of diagnostic classifications in the era of globalized medicine

Author

Macintyre, Elizabeth, Döhner, Konstanze, Grønbæk, Kirsten, Dreyling, Martin, Huntly, Brian, Almeida, Antonio, Gribben, John, Macintyre, Elizabeth, Döhner, Konstanze, Grønbæk, Kirsten, Dreyling, Martin, Huntly, Brian, Almeida, Antonio, and Gribben, John

Published

2024

3. Precision hematology:Navigating the evolution of diagnostic classifications in the era of globalized medicine

Author

Macintyre, Elizabeth, Döhner, Konstanze, Grønbæk, Kirsten, Dreyling, Martin, Huntly, Brian, Almeida, Antonio, Gribben, John, Macintyre, Elizabeth, Döhner, Konstanze, Grønbæk, Kirsten, Dreyling, Martin, Huntly, Brian, Almeida, Antonio, and Gribben, John

Published

2024

4. Experience with IVDR Implementation in Three Diagnostic Laboratories: Messages to EU Health Institutions, Diagnostic Healthcare Payers, and Authorities

Author

Lubbers, Bart R., Dombrink, Isabel, Kalina, Tomas, Hofmans, Mattias, Bruun, Morten S., Stanworth, Simon J., Béne, Marie C., Döhner, Konstanze, Brüggemann, Monika, Macintyre, Elizabeth A., Dongen, J. J. M. van, Lubbers, Bart R., Dombrink, Isabel, Kalina, Tomas, Hofmans, Mattias, Bruun, Morten S., Stanworth, Simon J., Béne, Marie C., Döhner, Konstanze, Brüggemann, Monika, Macintyre, Elizabeth A., and Dongen, J. J. M. van

Abstract

Regulation (EU) 2017/746 on in vitro diagnostic medical devices1 (IVDR) has been implemented with the aim to safeguard the quality of diagnostic tests in the EU, for example, by requiring robust proof of safety and performance. The IVDR is a product regulation mainly aimed at industry manufacturing and marketing medical devices. While IVDR-compliant diagnostic tests should predominantly be supplied by manufacturers, health institutions have the possibility of manufacturing and using in-house devices (IH-IVDs), provided they meet the Article 5(5) conditions and relevant general safety and performance requirements in Annex I. This “health institution exemption” concerns, for example, their quality management system (QMS), risk management, performance evaluation, and justification of IH-IVD use.2 The first significant task for diagnostic laboratories at health institutions, compliance with Annex I, has been applicable since May 2022, whereas other implementation timelines are shifted based on the December 2021 amendment of the IVDR.3,4

Published

2023

5. A Lack of Diversity, Equity, and Inclusion in Clinical Research Has Direct Impact on Patient Care

Author

El-Galaly, Tarec Christoffer, Gaidzik, Verena I., Gaman, Mihnea Alexandru, Antic, Darko, Okosun, Jessica, Copland, Mhairi, Sexl, Veronika, Fielding, Adele K., Doeswijk, Robin, Parker, Helen, Dreyling, Martin, Döhner, Konstanze, Almeida, António Medina, Macintyre, Elizabeth, Gribben, John G., Grønbæk, Kirsten, El-Galaly, Tarec Christoffer, Gaidzik, Verena I., Gaman, Mihnea Alexandru, Antic, Darko, Okosun, Jessica, Copland, Mhairi, Sexl, Veronika, Fielding, Adele K., Doeswijk, Robin, Parker, Helen, Dreyling, Martin, Döhner, Konstanze, Almeida, António Medina, Macintyre, Elizabeth, Gribben, John G., and Grønbæk, Kirsten

Abstract

Diversity, equity, and inclusion (DEI) in research is important. This is the case not only because it is simply the right thing to do but also because DEI fosters collaboration, empathy, and psychological safety between scientists and clinicians as well as in our attitudes to and relations with patients. Inclusion of patient samples from diverse populations is critical to ensure that the full range of biological variabilities are represented in basic and clinical research.

Published

2023

6. A Lack of Diversity, Equity, and Inclusion in Clinical Research Has Direct Impact on Patient Care

Author

El-Galaly, Tarec Christoffer, Gaidzik, Verena I., Gaman, Mihnea Alexandru, Antic, Darko, Okosun, Jessica, Copland, Mhairi, Sexl, Veronika, Fielding, Adele K., Doeswijk, Robin, Parker, Helen, Dreyling, Martin, Döhner, Konstanze, Almeida, António Medina, Macintyre, Elizabeth, Gribben, John G., Grønbæk, Kirsten, El-Galaly, Tarec Christoffer, Gaidzik, Verena I., Gaman, Mihnea Alexandru, Antic, Darko, Okosun, Jessica, Copland, Mhairi, Sexl, Veronika, Fielding, Adele K., Doeswijk, Robin, Parker, Helen, Dreyling, Martin, Döhner, Konstanze, Almeida, António Medina, Macintyre, Elizabeth, Gribben, John G., and Grønbæk, Kirsten

Abstract

Diversity, equity, and inclusion (DEI) in research is important. This is the case not only because it is simply the right thing to do but also because DEI fosters collaboration, empathy, and psychological safety between scientists and clinicians as well as in our attitudes to and relations with patients. Inclusion of patient samples from diverse populations is critical to ensure that the full range of biological variabilities are represented in basic and clinical research.

Published

2023

7. TET2 deficiency cooperates with CBFB-MYH11 to induce acute myeloid leukaemia and represents an early leukaemogenic event

Author

Reckzeh, Kristian, Estruch, Montserrat, Ali, Mina, Helbo, Alexandra Søgaard, Mosbech, Anna, Won, Kyoung Jae, Rücker, Frank, Döhner, Konstanze, Theilgaard-Monch, Kim, Reckzeh, Kristian, Estruch, Montserrat, Ali, Mina, Helbo, Alexandra Søgaard, Mosbech, Anna, Won, Kyoung Jae, Rücker, Frank, Döhner, Konstanze, and Theilgaard-Monch, Kim

Published

2022

8. Association of FLT3-internal tandem duplication length with overall survival in acute myeloid leukemia:a systematic review and meta-analysis

Author

Polak, Tobias B., van Rosmalen, Joost, Dirven, Stijn, Herzig, Julia K., Cloos, Jacqueline, Meshinchi, Soheil, Döhner, Konstanze, Janssen, Jeroen J.W.M., Cucchi, David G.J., Polak, Tobias B., van Rosmalen, Joost, Dirven, Stijn, Herzig, Julia K., Cloos, Jacqueline, Meshinchi, Soheil, Döhner, Konstanze, Janssen, Jeroen J.W.M., and Cucchi, David G.J.

Published

2022

9. Molecular landscape and prognostic impact of FLT3 -ITD insertion site in acute myeloid leukemia : RATIFY study results

Author

Rücker, Frank G., Du, Ling, Luck, Tamara J., Benner, Axel, Krzykalla, Julia, Gathmann, Insa, Voso, Maria Teresa, Amadori, Sergio, Prior, Thomas W., Brandwein, Joseph M., Appelbaum, Frederick R., Medeiros, Bruno, Tallman, Martin S., Savoie, Lynn, Sierra, Jorge, Pallaud, Celine, Sanz, Miguel A., Jansen, Joop H., Niederwieser, Dietger, Fischer, Thomas, Ehninger, Gerhard, Heuser, Michael, Ganser, Arnold, Bullinger, Lars, Larson, Richard A., Bloomfield, Clara D., Stone, Richard M., Döhner, Hartmut, Thiede, Christian, Döhner, Konstanze, Universitat Autònoma de Barcelona, Rücker, Frank G., Du, Ling, Luck, Tamara J., Benner, Axel, Krzykalla, Julia, Gathmann, Insa, Voso, Maria Teresa, Amadori, Sergio, Prior, Thomas W., Brandwein, Joseph M., Appelbaum, Frederick R., Medeiros, Bruno, Tallman, Martin S., Savoie, Lynn, Sierra, Jorge, Pallaud, Celine, Sanz, Miguel A., Jansen, Joop H., Niederwieser, Dietger, Fischer, Thomas, Ehninger, Gerhard, Heuser, Michael, Ganser, Arnold, Bullinger, Lars, Larson, Richard A., Bloomfield, Clara D., Stone, Richard M., Döhner, Hartmut, Thiede, Christian, Döhner, Konstanze, and Universitat Autònoma de Barcelona

Abstract

In acute myeloid leukemia (AML) internal tandem duplications of the FLT3 gene (FLT3- ITD) are associated with poor prognosis. Retrospectively, we investigated the prognostic and predictive impact of FLT3 -ITD insertion site (IS) in 452 patients randomized within the RATIFY trial, which evaluated midostaurin additionally to intensive chemotherapy. Next-generation sequencing identified 908 ITDs, with 643 IS in the juxtamembrane domain (JMD) and 265 IS in the tyrosine kinase domain-1 (TKD1). According to IS, patients were categorized as JMDsole (n = 251, 55%), JMD and TKD1 (JMD/TKD1; n = 117, 26%), and TKD1sole (n = 84, 19%). While clinical variables did not differ among the 3 groups, NPM1 mutation was correlated with JMDsole (P = 0.028). Overall survival (OS) differed significantly, with estimated 4-year OS probabilities of 0.44, 0.50, and 0.30 for JMDsole, JMD/TKD1, and TKD1sole, respectively (P = 0.032). Multivariate (cause-specific) Cox models for OS and cumulative incidence of relapse using allogeneic hematopoietic cell transplantation (HCT) in first complete remission as a time-dependent variable identified TKD1sole as unfavorable and HCT as favorable factors. In addition, Midostaurin exerted a significant benefit only for JMDsole. Our results confirm the distinct molecular heterogeneity of FLT3 -ITD and the negative prognostic impact of TKD1 IS in AML that was not overcome by midostaurin.

Published

2021

10. Impact of PPM1D mutations in patients with myelodysplastic syndrome and deletion of chromosome 5q

Author

Panagiota, Victoria, Meggendorfer, Manja, Kubasch, Anne Sophie, Gabdoulline, Razif, Krönke, Jan, Mies, Anna, Shahswar, Rabia, Kandziora, Christian, Klement, Piroska, Schiller, Johannes, Göhring, Gudrun, Haferlach, Claudia, Ganster, Christina, Shirneshan, Katayoon, Gutermuth, Annika, Thiede, Christian, Germing, Ulrich, Schroeder, Thomas, Kobbe, Guido, Klesse, Sabrina, Koenecke, Christian, Schlegelberger, Brigitte, Kröger, Nicolaus, Haase, Detlef, Döhner, Konstanze, Sperr, Wolfgang R., Valent, Peter, Ganser, Arnold, Thol, Felicitas, Haferlach, Torsten, Platzbecker, Uwe, Heuser, Michael, Panagiota, Victoria, Meggendorfer, Manja, Kubasch, Anne Sophie, Gabdoulline, Razif, Krönke, Jan, Mies, Anna, Shahswar, Rabia, Kandziora, Christian, Klement, Piroska, Schiller, Johannes, Göhring, Gudrun, Haferlach, Claudia, Ganster, Christina, Shirneshan, Katayoon, Gutermuth, Annika, Thiede, Christian, Germing, Ulrich, Schroeder, Thomas, Kobbe, Guido, Klesse, Sabrina, Koenecke, Christian, Schlegelberger, Brigitte, Kröger, Nicolaus, Haase, Detlef, Döhner, Konstanze, Sperr, Wolfgang R., Valent, Peter, Ganser, Arnold, Thol, Felicitas, Haferlach, Torsten, Platzbecker, Uwe, and Heuser, Michael

Published

2021

11. Impact of PPM1D mutations in patients with myelodysplastic syndrome and deletion of chromosome 5q

Author

Panagiota, Victoria, Meggendorfer, Manja, Kubasch, Anne Sophie, Gabdoulline, Razif, Krönke, Jan, Mies, Anna, Shahswar, Rabia, Kandziora, Christian, Klement, Piroska, Schiller, Johannes, Göhring, Gudrun, Haferlach, Claudia, Ganster, Christina, Shirneshan, Katayoon, Gutermuth, Annika, Thiede, Christian, Germing, Ulrich, Schroeder, Thomas, Kobbe, Guido, Klesse, Sabrina, Koenecke, Christian, Schlegelberger, Brigitte, Kröger, Nicolaus, Haase, Detlef, Döhner, Konstanze, Sperr, Wolfgang R., Valent, Peter, Ganser, Arnold, Thol, Felicitas, Haferlach, Torsten, Platzbecker, Uwe, Heuser, Michael, Panagiota, Victoria, Meggendorfer, Manja, Kubasch, Anne Sophie, Gabdoulline, Razif, Krönke, Jan, Mies, Anna, Shahswar, Rabia, Kandziora, Christian, Klement, Piroska, Schiller, Johannes, Göhring, Gudrun, Haferlach, Claudia, Ganster, Christina, Shirneshan, Katayoon, Gutermuth, Annika, Thiede, Christian, Germing, Ulrich, Schroeder, Thomas, Kobbe, Guido, Klesse, Sabrina, Koenecke, Christian, Schlegelberger, Brigitte, Kröger, Nicolaus, Haase, Detlef, Döhner, Konstanze, Sperr, Wolfgang R., Valent, Peter, Ganser, Arnold, Thol, Felicitas, Haferlach, Torsten, Platzbecker, Uwe, and Heuser, Michael

Published

2021

12. Kidney dysfunction is associated with thrombosis and disease severity in myeloproliferative neoplasms: implications from the German Study Group for MPN Bioregistry

Author

Gecht, Judith, Tsoukakis, Ioannis, Kricheldorf, Kim, Stegelmann, Frank, Klausmann, Martine, Griesshammer, Martin, Schulz, Holger, Hollburg, Wiebke, Göthert, Joachim Rudolf, Sockel, Katja, Heidel, Florian, Gattermann, Norbert, Maintz, Christoph, Al-Ali, Haifa Kathrin, Platzbecker, Uwe, Hansen, Richard, Hänel, Mathias, Parmentier, Stefani Barbara, Bommer, Martin, Pahl, Heike L., Lang, Fabian Magnus Eugen, Kirschner, Martin, Isfort, Susanne, Brümmendorf, Tim Henrik, Döhner, Konstanze, Koschmieder, Steffen, Gecht, Judith, Tsoukakis, Ioannis, Kricheldorf, Kim, Stegelmann, Frank, Klausmann, Martine, Griesshammer, Martin, Schulz, Holger, Hollburg, Wiebke, Göthert, Joachim Rudolf, Sockel, Katja, Heidel, Florian, Gattermann, Norbert, Maintz, Christoph, Al-Ali, Haifa Kathrin, Platzbecker, Uwe, Hansen, Richard, Hänel, Mathias, Parmentier, Stefani Barbara, Bommer, Martin, Pahl, Heike L., Lang, Fabian Magnus Eugen, Kirschner, Martin, Isfort, Susanne, Brümmendorf, Tim Henrik, Döhner, Konstanze, and Koschmieder, Steffen

Abstract

Simple Summary: In patients with myeloproliferative neoplasms (MPN) and in patients with kidney dysfunction, a higher rate of thrombosis has been reported compared with the general population. Furthermore, MPN patients are more prone to develop kidney dysfunction. In our study, we assessed the importance of specific risk factors for kidney dysfunction and thrombosis in MPN patients. We found that the rate of thrombosis is correlated with the degree of kidney dysfunction, especially in myelofibrosis. Significant associations for kidney dysfunction included arterial hypertension, MPN treatment, and increased inflammation, and those for thrombosis comprised arterial hypertension, non-excessive platelet counts, and antithrombotic therapy. The identified risk factor associations varied between MPN subtypes. Our data suggest that kidney dysfunction in MPN patients is associated with an increased risk of thrombosis, mandating closer monitoring, and, possibly, early thromboprophylaxis. Abstract: Inflammation-induced thrombosis represents a severe complication in patients with myeloproliferative neoplasms (MPN) and in those with kidney dysfunction. Overlapping disease-specific attributes suggest common mechanisms involved in MPN pathogenesis, kidney dysfunction, and thrombosis. Data from 1420 patients with essential thrombocythemia (ET, 33.7%), polycythemia vera (PV, 38.5%), and myelofibrosis (MF, 27.9%) were extracted from the bioregistry of the German Study Group for MPN. The total cohort was subdivided according to the calculated estimated glomerular filtration rate (eGFR, (mL/min/1.73 m2)) into eGFR1 (≥90, 21%), eGFR2 (60–89, 56%), and eGFR3 (<60, 22%). A total of 29% of the patients had a history of thrombosis. A higher rate of thrombosis and longer MPN duration was observed in eGFR3 than in eGFR2 and eGFR1. Kidney dysfunction occurred earlier in ET than in PV or MF. Multiple logistic regression analysis identified arterial hypertension, MPN treatment, increased uric ac

Published

2021

13. Mutant CEBPA directly drives the expression of the targetable tumor-promoting factor CD73 in AML

Author

Jakobsen, Janus S, Laursen, Linea G, Schuster, Mikkel B, Pundhir, Sachin, Schoof, Erwin, Ge, Ying, d'Altri, Teresa, Vitting-Seerup, Kristoffer, Rapin, Nicolas, Gentil, Coline, Jendholm, Johan, Theilgaard-Mönch, Kim, Reckzeh, Kristian, Bullinger, Lars, Döhner, Konstanze, Hokland, Peter, Fitzgibbon, Jude, Porse, Bo T, Jakobsen, Janus S, Laursen, Linea G, Schuster, Mikkel B, Pundhir, Sachin, Schoof, Erwin, Ge, Ying, d'Altri, Teresa, Vitting-Seerup, Kristoffer, Rapin, Nicolas, Gentil, Coline, Jendholm, Johan, Theilgaard-Mönch, Kim, Reckzeh, Kristian, Bullinger, Lars, Döhner, Konstanze, Hokland, Peter, Fitzgibbon, Jude, and Porse, Bo T

Abstract

The key myeloid transcription factor (TF), CEBPA, is frequently mutated in acute myeloid leukemia (AML), but the direct molecular effects of this leukemic driver mutation remain elusive. To investigate CEBPA mutant AML, we performed microscale, in vivo chromatin immunoprecipitation sequencing and identified a set of aberrantly activated enhancers, exclusively occupied by the leukemia-associated CEBPA-p30 isoform. Comparing gene expression changes in human CEBPA mutant AML and the corresponding CebpaLp30 mouse model, we identified Nt5e, encoding CD73, as a cross-species AML gene with an upstream leukemic enhancer physically and functionally linked to the gene. Increased expression of CD73, mediated by the CEBPA-p30 isoform, sustained leukemic growth via the CD73/A2AR axis. Notably, targeting of this pathway enhanced survival of AML-transplanted mice. Our data thus indicate a first-in-class link between a cancer driver mutation in a TF and a druggable, direct transcriptional target.

Published

2019

14. Mutant CEBPA directly drives the expression of the targetable tumor-promoting factor CD73 in AML

Author

Jakobsen, Janus S, Laursen, Linea G, Schuster, Mikkel B, Pundhir, Sachin, Schoof, Erwin, Ge, Ying, d'Altri, Teresa, Vitting-Seerup, Kristoffer, Rapin, Nicolas, Gentil, Coline, Jendholm, Johan, Theilgaard-Mönch, Kim, Reckzeh, Kristian, Bullinger, Lars, Döhner, Konstanze, Hokland, Peter, Fitzgibbon, Jude, Porse, Bo T, Jakobsen, Janus S, Laursen, Linea G, Schuster, Mikkel B, Pundhir, Sachin, Schoof, Erwin, Ge, Ying, d'Altri, Teresa, Vitting-Seerup, Kristoffer, Rapin, Nicolas, Gentil, Coline, Jendholm, Johan, Theilgaard-Mönch, Kim, Reckzeh, Kristian, Bullinger, Lars, Döhner, Konstanze, Hokland, Peter, Fitzgibbon, Jude, and Porse, Bo T

Abstract

The key myeloid transcription factor (TF), CEBPA, is frequently mutated in acute myeloid leukemia (AML), but the direct molecular effects of this leukemic driver mutation remain elusive. To investigate CEBPA mutant AML, we performed microscale, in vivo chromatin immunoprecipitation sequencing and identified a set of aberrantly activated enhancers, exclusively occupied by the leukemia-associated CEBPA-p30 isoform. Comparing gene expression changes in human CEBPA mutant AML and the corresponding CebpaLp30 mouse model, we identified Nt5e, encoding CD73, as a cross-species AML gene with an upstream leukemic enhancer physically and functionally linked to the gene. Increased expression of CD73, mediated by the CEBPA-p30 isoform, sustained leukemic growth via the CD73/A2AR axis. Notably, targeting of this pathway enhanced survival of AML-transplanted mice. Our data thus indicate a first-in-class link between a cancer driver mutation in a TF and a druggable, direct transcriptional target.

Published

2019

15. Cancer specific changes in DNA methylation reveal aberrant silencing and activation of enhancers in leukemia

Author

Qu, Ying, Siggens, Lee, Cordeddu, Lina, Gaidzik, Verena I, Karlsson, Kasper, Bullinger, Lars, Döhner, Konstanze, Ekwall, Karl, Lehmann, Sören, Lennartsson, Andreas, Qu, Ying, Siggens, Lee, Cordeddu, Lina, Gaidzik, Verena I, Karlsson, Kasper, Bullinger, Lars, Döhner, Konstanze, Ekwall, Karl, Lehmann, Sören, and Lennartsson, Andreas

Abstract

Acute myeloid leukemia (AML) is characterized by an impaired differentiation process leading to an accumulation of immature blasts in the blood. One feature of cytogenetically normal AML is alterations to the DNA methylome. Here we have analyzed 57 AML patients with normal karyotype using Illuminas 450 k array and show that aberrant DNA methylation is significantly altered at enhancer regions and that the methylation levels at specific enhancers predict overall survival of AML patients. The majority of sites that become differentially methylated in AML occur in regulatory elements of the human genome. Hypermethylation associates with enhancer silencing. In addition, ChIP-seq analyses showed that a subset of hypomethylated sites correlate with enhancer activation, indicated by increased H3K27 acetylation. DNA hypomethylation is not therefore sufficient for enhancer activation. Some sites of hypomethylation occur at weak / poised enhancers marked with H3K4 monomethylation in hematopoietic progenitor cells. Other hypomethylated regions occur at sites inactive in progenitors and reflect the de novo acquisition of AML specific enhancers. Altered enhancer dynamics are reflected in the gene expression of enhancer target genes including genes involved in oncogenesis and blood cell development. This study demonstrates that histone variants and different histone modifications interact with aberrant DNA methylation, causing perturbed enhancer activity in CN-AML that contributes to a leukemic transcriptome.

Published

2017

16. Symptom burden profile in myelofibrosis patients with thrombocytopenia : Lessons and unmet needs

Author

Scotch, Allison H, Kosiorek, Heidi, Scherber, Robyn, Dueck, Amylou C, Slot, Stefanie, Zweegman, Sonja, Boekhorst, Peter A W Te, Commandeur, Suzan, Schouten, Harry, Sackmann, Federico, Fuentes, Ana Kerguelen, Hernández-Maraver, Dolores, Pahl, Heike L, Griesshammer, Martin, Stegelmann, Frank, Döhner, Konstanze, Lehmann, Thomas, Bonatz, Karin, Reiter, Andreas, Boyer, Francoise, Etienne, Gabriel, Ianotto, Jean-Christophe, Ranta, Dana, Roy, Lydia, Cahn, Jean-Yves, Harrison, Claire N, Radia, Deepti, Muxi, Pablo, Maldonado, Norman, Besses, Carlos, Cervantes, Francisco, Johansson, Peter L, Barbui, Tiziano, Barosi, Giovanni, Vannucchi, Alessandro M, Paoli, Chiara, Passamonti, Francesco, Andreasson, Bjorn, Ferrari, Maria L, Rambaldi, Alessandro, Samuelsson, Jan, Birgegård, Gunnar, Xiao, Zhijian, Xu, Zefeng, Zhang, Yue, Sun, Xiujuan, Xu, Junqing, Kiladjian, Jean-Jacques, Zhang, Peihong, Gale, Robert Peter, Mesa, Ruben A, Geyer, Holly L, Scotch, Allison H, Kosiorek, Heidi, Scherber, Robyn, Dueck, Amylou C, Slot, Stefanie, Zweegman, Sonja, Boekhorst, Peter A W Te, Commandeur, Suzan, Schouten, Harry, Sackmann, Federico, Fuentes, Ana Kerguelen, Hernández-Maraver, Dolores, Pahl, Heike L, Griesshammer, Martin, Stegelmann, Frank, Döhner, Konstanze, Lehmann, Thomas, Bonatz, Karin, Reiter, Andreas, Boyer, Francoise, Etienne, Gabriel, Ianotto, Jean-Christophe, Ranta, Dana, Roy, Lydia, Cahn, Jean-Yves, Harrison, Claire N, Radia, Deepti, Muxi, Pablo, Maldonado, Norman, Besses, Carlos, Cervantes, Francisco, Johansson, Peter L, Barbui, Tiziano, Barosi, Giovanni, Vannucchi, Alessandro M, Paoli, Chiara, Passamonti, Francesco, Andreasson, Bjorn, Ferrari, Maria L, Rambaldi, Alessandro, Samuelsson, Jan, Birgegård, Gunnar, Xiao, Zhijian, Xu, Zefeng, Zhang, Yue, Sun, Xiujuan, Xu, Junqing, Kiladjian, Jean-Jacques, Zhang, Peihong, Gale, Robert Peter, Mesa, Ruben A, and Geyer, Holly L

Abstract

Myelofibrosis is a myeloproliferative neoplasm associated with progressive cytopenias and high symptom burden. MF patients with thrombocytopenia have poor prognosis but the presence of thrombocytopenia frequently precludes the use of JAK2 inhibitors. In this study, we assessed quality of life and symptom burden in 418 MF patients with (n = 89) and without (n = 329) thrombocytopenia using prospective data from the MPN-QOL study group database, including the Myeloproliferative Neoplasm Symptom Assessment Form (MPN-SAF) and Total Symptom Score (MPN10). Thrombocytopenia, defined as platelet count < 100 x10(9)/L (moderate 51-100 x 10(9)/L; severe <= 50 x10(9)/L), was associated with anemia (76% vs. 45%, p < 0.001), leukopenia (29% vs. 11%, p < 0.001), and need for red blood cell transfusion (35% vs. 19%, p = 0.002). Thrombocytopenic patients had more fatigue, early satiety, inactivity, dizziness, sad mood, cough, night sweats, itching, fever, and weight loss; total symptom scores were also higher (33 vs. 24, p < 0.001). Patients with severe thrombocytopenia were more likely to have anemia (86% vs. 67%, p = 0.04), leukopenia (40% vs. 20%, p = 0.04), and transfusion requirements (51% vs. 20%, p = 0.002) but few differences in symptoms when compared to patients with moderate thrombocytopenia. These results suggest that MF patients with thrombocytopenia experience greater symptomatic burden than MF patients without thrombocytopenia and may benefit from additional therapies.

Published

2017

17. Symptomatic Profiles of Patients With Polycythemia Vera : Implications of Inadequately Controlled Disease

Author

Geyer, Holly, Scherber, Robyn, Kosiorek, Heidi, Dueck, Amylou C, Kiladjian, Jean-Jacques, Xiao, Zhijian, Slot, Stefanie, Zweegman, Sonja, Sackmann, Federico, Fuentes, Ana Kerguelen, Hernández-Maraver, Dolores, Döhner, Konstanze, Harrison, Claire N, Radia, Deepti, Muxi, Pablo, Besses, Carlos, Cervantes, Francisco, Johansson, Peter L, Andreasson, Bjorn, Rambaldi, Alessandro, Barbui, Tiziano, Bonatz, Karin, Reiter, Andreas, Boyer, Francoise, Etienne, Gabriel, Ianotto, Jean-Christophe, Ranta, Dana, Roy, Lydia, Cahn, Jean-Yves, Maldonado, Norman, Barosi, Giovanni, Ferrari, Maria L, Gale, Robert Peter, Birgegard, Gunnar, Xu, Zefeng, Zhang, Yue, Sun, Xiujuan, Xu, Junqing, Zhang, Peihong, Te Boekhorst, Peter A W, Commandeur, Suzan, Schouten, Harry, Pahl, Heike L, Griesshammer, Martin, Stegelmann, Frank, Lehmann, Thomas, Senyak, Zhenya, Vannucchi, Alessandro M, Passamonti, Francesco, Samuelsson, Jan, Mesa, Ruben A, Geyer, Holly, Scherber, Robyn, Kosiorek, Heidi, Dueck, Amylou C, Kiladjian, Jean-Jacques, Xiao, Zhijian, Slot, Stefanie, Zweegman, Sonja, Sackmann, Federico, Fuentes, Ana Kerguelen, Hernández-Maraver, Dolores, Döhner, Konstanze, Harrison, Claire N, Radia, Deepti, Muxi, Pablo, Besses, Carlos, Cervantes, Francisco, Johansson, Peter L, Andreasson, Bjorn, Rambaldi, Alessandro, Barbui, Tiziano, Bonatz, Karin, Reiter, Andreas, Boyer, Francoise, Etienne, Gabriel, Ianotto, Jean-Christophe, Ranta, Dana, Roy, Lydia, Cahn, Jean-Yves, Maldonado, Norman, Barosi, Giovanni, Ferrari, Maria L, Gale, Robert Peter, Birgegard, Gunnar, Xu, Zefeng, Zhang, Yue, Sun, Xiujuan, Xu, Junqing, Zhang, Peihong, Te Boekhorst, Peter A W, Commandeur, Suzan, Schouten, Harry, Pahl, Heike L, Griesshammer, Martin, Stegelmann, Frank, Lehmann, Thomas, Senyak, Zhenya, Vannucchi, Alessandro M, Passamonti, Francesco, Samuelsson, Jan, and Mesa, Ruben A

Abstract

PURPOSE: Polycythemia vera (PV) is a myeloproliferative neoplasm (MPN) associated with disabling symptoms and a heightened risk of life-threatening complications. Recent studies have demonstrated the effectiveness of JAK inhibitor therapy in patients with PV patients who have a history of prior hydroxyurea (HU) use (including resistance or intolerance), phlebotomy requirements, and palpable splenomegaly. We aimed to determine how these features contribute alone and in aggregate to the PV symptom burden. PATIENTS AND METHODS: Through prospective evaluation of 1,334 patients with PV who had characterized symptom burden, we assessed patient demographics, laboratory data, and the presence of splenomegaly by disease feature (ie, known HU use, known phlebotomy requirements, splenomegaly). RESULTS: The presence of each feature in itself is associated with a moderately high symptom burden (MPN symptom assessment form [SAF] total symptom score [TSS] range, 27.7 to 29.2) that persists independent of PV risk category. In addition, symptoms incrementally increase in severity with the addition of other features. Patients with PV who had all three features (PV-HUPS) faced the highest total score (MPN-SAF TSS, 32.5) but had similar individual symptom scores to patients with known HU use (PV-HU), known phlebotomy (PV-P), and splenomegaly (PV-S). CONCLUSION: The results of this study suggest that patients with PV who have any one of the features in question (known HU use, known phlebotomy, or splenomegaly) have significant PV-associated symptoms. Furthermore, it demonstrates that many PV symptoms remain severe independent of the number of features present.

Published

2016

18. All-trans retinoic acid as adjunct to intensive treatment in younger adult patients with acute myeloid leukemia : results of the randomized AMLSG 07-04 study

Author

German-Austrian Acute Myeloid Leukemia Study Group, Schlenk, Richard Friedrich, Lübbert, Michael, Benner, Axel, Lamparter, Alexander, Krauter, Jürgen, Herr, Wolfgang, Martin, Hans, Salih, Helmut Rainer, Kündgen, Andrea, Horst, Heinz August, Brossart, Peter, Götze, Katharina, Nachbaur, David, Wattad, Mohammed, Köhne, Claus-Henning, Fiedler, Walter, Bentz, Martin, Wulf, Gerald, Held, Gerhard, Hertenstein, Bernd, Salwender, Hans, Gaidzik, Verena I., Schlegelberger, Brigitte, Weber, Daniela, Döhner, Konstanze, Ganser, Arnold, Döhner, Hartmut, German-Austrian Acute Myeloid Leukemia Study Group, Schlenk, Richard Friedrich, Lübbert, Michael, Benner, Axel, Lamparter, Alexander, Krauter, Jürgen, Herr, Wolfgang, Martin, Hans, Salih, Helmut Rainer, Kündgen, Andrea, Horst, Heinz August, Brossart, Peter, Götze, Katharina, Nachbaur, David, Wattad, Mohammed, Köhne, Claus-Henning, Fiedler, Walter, Bentz, Martin, Wulf, Gerald, Held, Gerhard, Hertenstein, Bernd, Salwender, Hans, Gaidzik, Verena I., Schlegelberger, Brigitte, Weber, Daniela, Döhner, Konstanze, Ganser, Arnold, and Döhner, Hartmut

Abstract

The aim of this clinical trial was to evaluate the impact of all-trans retinoic acid (ATRA) in combination with chemotherapy and to assess the NPM1 status as biomarker for ATRA therapy in younger adult patients (18-60 years) with acute myeloid leukemia (AML). Patients were randomized for intensive chemotherapy with or without open-label ATRA (45 mg/m2, days 6-8; 15 mg/m2, days 9-21). Two cycles of induction therapy were followed by risk-adapted consolidation with high-dose cytarabine or allogeneic hematopoietic cell transplantation. Due to the open label character of the study, analysis was performed on an intention-to-treat (ITT) and a per-protocol (PP) basis. One thousand one hundred patients were randomized (556, STANDARD; 544, ATRA) with 38 patients treated vice versa. Median follow-up for survival was 5.2 years. ITT analyses revealed no difference between ATRA and STANDARD for the total cohort and for the subset of NPM1-mutated AML with respect to event-free (EFS; p = 0.93, p = 0.17) and overall survival (OS; p = 0.24 and p = 0.32, respectively). Pre-specified PP analyses revealed better EFS in NPM1-mutated AML (p = 0.05) and better OS in the total cohort (p = 0.03). Explorative subgroup analyses on an ITT basis revealed better OS (p = 0.05) in ATRA for genetic low-risk patients according to ELN recommendations. The clinical trial is registered at clinicaltrialsregister.eu (EudraCT Number: 2004-004321-95).

Published

2016

19. Disease evolution and outcomes in familial AML with germline CEBPA mutations

Author

Tawana, Kiran, Wang, Jun, Renneville, Aline, Bödör, Csaba, Hills, Robert, Loveday, Chey, Savic, Aleksandar, Van Delft, Frederik W, Treleaven, Jennifer, Georgiades, Panayiotis, Uglow, Elizabeth, Asou, Norio, Uike, Naokuni, Debeljak, Maruša, Jazbec, Janez, Ancliff, Philip, Gale, Rosemary, Thomas, Xavier, Mialou, Valerie, Döhner, Konstanze, Bullinger, Lars, Mueller, Beatrice, Pabst, Thomas, Stelljes, Matthias, Schlegelberger, Brigitte, Wozniak, Eva, Iqbal, Sameena, Okosun, Jessica, Araf, Shamzah, Frank, Anne-Katrine, Lauridsen, Felicia B, Porse, Bo, Nerlov, Claus, Owen, Carolyn, Dokal, Inderjeet, Gribben, John, Smith, Matthew, Preudhomme, Claude, Chelala, Claude, Cavenagh, Jamie, Fitzgibbon, Jude, Tawana, Kiran, Wang, Jun, Renneville, Aline, Bödör, Csaba, Hills, Robert, Loveday, Chey, Savic, Aleksandar, Van Delft, Frederik W, Treleaven, Jennifer, Georgiades, Panayiotis, Uglow, Elizabeth, Asou, Norio, Uike, Naokuni, Debeljak, Maruša, Jazbec, Janez, Ancliff, Philip, Gale, Rosemary, Thomas, Xavier, Mialou, Valerie, Döhner, Konstanze, Bullinger, Lars, Mueller, Beatrice, Pabst, Thomas, Stelljes, Matthias, Schlegelberger, Brigitte, Wozniak, Eva, Iqbal, Sameena, Okosun, Jessica, Araf, Shamzah, Frank, Anne-Katrine, Lauridsen, Felicia B, Porse, Bo, Nerlov, Claus, Owen, Carolyn, Dokal, Inderjeet, Gribben, John, Smith, Matthew, Preudhomme, Claude, Chelala, Claude, Cavenagh, Jamie, and Fitzgibbon, Jude

Abstract

In-depth molecular investigation of familial leukemia has been limited by the rarity of recognized cases. This study examines the genetic events initiating leukemia and details the clinical progression of disease across multiple families harboring germ-line CEBPA mutations. Clinical data were collected from 10 CEBPA-mutated families, representing 24 members with acute myeloid leukemia (AML). Whole-exome (WES) and deep sequencing were performed to genetically profile tumors and define patterns of clonal evolution. Germline CEBPA mutations clustered within the N-terminal and were highly penetrant, with AML presenting at a median age of 24.5 years (range, 1.75-46 years). In all diagnostic tumors tested (n = 18), double CEBPA mutations (CEBPAdm) were detected, with acquired (somatic) mutations preferentially targeting the C-terminal. Somatic CEBPA mutations were unstable throughout the disease course, with different mutations identified at recurrence. Deep sequencing of diagnostic and relapse paired samples confirmed that relapse-associated CEBPA mutations were absent at diagnosis, suggesting recurrence was triggered by novel, independent clones. Integrated WES and deep sequencing subsequently revealed an entirely new complement of mutations at relapse, verifying the presentation of a de novo leukemic episode. The cumulative incidence of relapse in familial AML was 56% at 10 years (n = 11), and 3 patients experienced ≥3 disease episodes over a period of 17 to 20 years. Durable responses to secondary therapies were observed, with prolonged median survival after relapse (8 years) and long-term overall survival (10-year overall survival, 67%). Our data reveal that familial CEBPA-mutated AML exhibits a unique model of disease progression, associated with favorable long-term outcomes.

Published

2015

20. A single oncogenic enhancer rearrangement causes concomitant EVI1 and GATA2 deregulation in leukemia

Author

Gröschel, Stefan, Sanders, Mathijs A, Hoogenboezem, Remco, de Wit, Elzo, Bouwman, Britta A M, Erpelinck, Claudia, van der Velden, Vincent H J, Havermans, Marije, Avellino, Roberto, van Lom, Kirsten, Rombouts, Elwin J, van Duin, Mark, Döhner, Konstanze, Beverloo, H Berna, Bradner, James E, Döhner, Hartmut, Löwenberg, Bob, Valk, Peter J M, Bindels, Eric M J, de Laat, Wouter, Delwel, Ruud, Gröschel, Stefan, Sanders, Mathijs A, Hoogenboezem, Remco, de Wit, Elzo, Bouwman, Britta A M, Erpelinck, Claudia, van der Velden, Vincent H J, Havermans, Marije, Avellino, Roberto, van Lom, Kirsten, Rombouts, Elwin J, van Duin, Mark, Döhner, Konstanze, Beverloo, H Berna, Bradner, James E, Döhner, Hartmut, Löwenberg, Bob, Valk, Peter J M, Bindels, Eric M J, de Laat, Wouter, and Delwel, Ruud

Abstract

Chromosomal rearrangements without gene fusions have been implicated in leukemogenesis by causing deregulation of proto-oncogenes via relocation of cryptic regulatory DNA elements. AML with inv(3)/t(3;3) is associated with aberrant expression of the stem-cell regulator EVI1. Applying functional genomics and genome-engineering, we demonstrate that both 3q rearrangements reposition a distal GATA2 enhancer to ectopically activate EVI1 and simultaneously confer GATA2 functional haploinsufficiency, previously identified as the cause of sporadic familial AML/MDS and MonoMac/Emberger syndromes. Genomic excision of the ectopic enhancer restored EVI1 silencing and led to growth inhibition and differentiation of AML cells, which could be replicated by pharmacologic BET inhibition. Our data show that structural rearrangements involving the chromosomal repositioning of a single enhancer can cause deregulation of two unrelated distal genes, with cancer as the outcome.

Published

2014

21. A single oncogenic enhancer rearrangement causes concomitant EVI1 and GATA2 deregulation in leukemia

Author

Gröschel, Stefan, Sanders, Mathijs A, Hoogenboezem, Remco, de Wit, Elzo, Bouwman, Britta A M, Erpelinck, Claudia, van der Velden, Vincent H J, Havermans, Marije, Avellino, Roberto, van Lom, Kirsten, Rombouts, Elwin J, van Duin, Mark, Döhner, Konstanze, Beverloo, H Berna, Bradner, James E, Döhner, Hartmut, Löwenberg, Bob, Valk, Peter J M, Bindels, Eric M J, de Laat, Wouter, Delwel, Ruud, Gröschel, Stefan, Sanders, Mathijs A, Hoogenboezem, Remco, de Wit, Elzo, Bouwman, Britta A M, Erpelinck, Claudia, van der Velden, Vincent H J, Havermans, Marije, Avellino, Roberto, van Lom, Kirsten, Rombouts, Elwin J, van Duin, Mark, Döhner, Konstanze, Beverloo, H Berna, Bradner, James E, Döhner, Hartmut, Löwenberg, Bob, Valk, Peter J M, Bindels, Eric M J, de Laat, Wouter, and Delwel, Ruud

Abstract

Chromosomal rearrangements without gene fusions have been implicated in leukemogenesis by causing deregulation of proto-oncogenes via relocation of cryptic regulatory DNA elements. AML with inv(3)/t(3;3) is associated with aberrant expression of the stem-cell regulator EVI1. Applying functional genomics and genome-engineering, we demonstrate that both 3q rearrangements reposition a distal GATA2 enhancer to ectopically activate EVI1 and simultaneously confer GATA2 functional haploinsufficiency, previously identified as the cause of sporadic familial AML/MDS and MonoMac/Emberger syndromes. Genomic excision of the ectopic enhancer restored EVI1 silencing and led to growth inhibition and differentiation of AML cells, which could be replicated by pharmacologic BET inhibition. Our data show that structural rearrangements involving the chromosomal repositioning of a single enhancer can cause deregulation of two unrelated distal genes, with cancer as the outcome.

Published

2014

22. Prognostic DNA methylation patterns in cytogenetically normal acute myeloid leukemia are predefined by stem cell chromatin marks

Author

Deneberg, Stefan, Guardiola, Philippe, Lennartsson, Andreas, Qu, Ying, Gaidzik, Verena, Blanchet, Odile, Karimi, Mohsen, Bengtzén, Sofia, Nahi, Hareth, Uggla, Bertil, Tidefelt, Ulf, Höglund, Martin, Paul, Christer, Ekwall, Karl, Döhner, Konstanze, Lehmann, Sören, Deneberg, Stefan, Guardiola, Philippe, Lennartsson, Andreas, Qu, Ying, Gaidzik, Verena, Blanchet, Odile, Karimi, Mohsen, Bengtzén, Sofia, Nahi, Hareth, Uggla, Bertil, Tidefelt, Ulf, Höglund, Martin, Paul, Christer, Ekwall, Karl, Döhner, Konstanze, and Lehmann, Sören

Abstract

Cytogenetically normal acute myeloid leukemia (CN-AML) compose between 40% and 50% of all adult acute myeloid leukemia (AML) cases. In this clinically diverse group, molecular aberrations, such as FLT3-ITD, NPM1, and CEBPA mutations, recently have added to the prognostic accuracy. Aberrant DNA methylation is a hallmark of cancer, including AML. We investigated in total 118 CN-AML samples in a test and a validation cohort for genome-wide promoter DNA methylation with Illumina Methylation Bead arrays and compared them with normal myeloid precursors and global gene expression. IDH and NPM1 mutations were associated with different methylation patterns (P = .0004 and .04, respectively). Genome-wide methylation levels were elevated in IDH-mutated samples (P = .006). We observed a negative impact of DNA methylation on transcription. Genes targeted by Polycomb group (PcG) proteins and genes associated with bivalent histone marks in stem cells showed increased aberrant methylation in AML (P < .0001). Furthermore, high methylation levels of PcG target genes were independently associated with better progression-free survival (odds ratio = 0.47, P = .01) and overall survival (odds ratio = 0.36, P = .001). In summary, genome-wide methylation patterns show preferential methylation of PcG targets with prognostic impact in CN-AML.

Published

2011

23. Prognostic DNA methylation patterns in cytogenetically normal acute myeloid leukemia are predefined by stem cell chromatin marks

Author

Deneberg, Stefan, Guardiola, Philippe, Lennartsson, Andreas, Qu, Ying, Gaidzik, Verena E., Blanchet, Odile, Karimi, Mohsen, Bengtzén, Sofia, Nahi, Hareth, Uggla, Bertil, Tidefelt, Ulf, Höglund, Martin, Paul, Christer, Ekwall, Karl, Döhner, Konstanze, Lehmann, Sören, Deneberg, Stefan, Guardiola, Philippe, Lennartsson, Andreas, Qu, Ying, Gaidzik, Verena E., Blanchet, Odile, Karimi, Mohsen, Bengtzén, Sofia, Nahi, Hareth, Uggla, Bertil, Tidefelt, Ulf, Höglund, Martin, Paul, Christer, Ekwall, Karl, Döhner, Konstanze, and Lehmann, Sören

Abstract

Cytogenetically normal acute myeloid leukemia (CN-AML) comprise between forty and fifty percent of all adult acute myeloid leukemia (AML) cases. In this clinically diverse group molecular aberrations such as FLT3ITD, NPM1 and CEBPA mutations recently have added to the prognostic accuracy. Aberrant DNA methylation is a hallmark of cancer including AML. We investigated in total 118 CN-AML samples in a test and a validation cohort for genome-wide promoter DNA methylation with Illumina Methylation Bead arrays and compared them to normal myeloid precursors and global gene expression. IDH and NPM1 mutations were associated with different methylation patterns (p=0.0004 and 0.04, respectively). Genome-wide methylation levels were elevated in IDH mutated samples (p=0.006). We observed a negative impact of DNA methylation on transcription. Genes targeted by Polycomb group (PcG) proteins and genes associated with bivalent histone marks in stem cells showed increased aberrant methylation in AML (p<0.0001). Furthermore, high methylation levels of PcG target genes were independently associated with better progression free (OR 0.47, p=0.01) and overall survival (OR 0.36, p=0.001). In summary, genome wide methylation patterns show preferential methylation of PcG targets with prognostic impact in CN-AML., Funding Agencies:Göran Gustafssons Foundation for Research in Natural Sciences Sigurd och Elsa Golje Foundation Ligue Contre le Cancer La Region Pays de la Loire/Appel a Projets du Canceropole Grand-Ouest

Published

2011

24. Prognostic DNA methylation patterns in cytogenetically normal acute myeloid leukemia are predefined by stem cell chromatin marks

Author

Deneberg, Stefan, Guardiola, Philippe, Lennartsson, Andreas, Qu, Ying, Gaidzik, Verena E., Blanchet, Odile, Karimi, Mohsen, Bengtzén, Sofia, Nahi, Hareth, Uggla, Bertil, Tidefelt, Ulf, Höglund, Martin, Paul, Christer, Ekwall, Karl, Döhner, Konstanze, Lehmann, Sören, Deneberg, Stefan, Guardiola, Philippe, Lennartsson, Andreas, Qu, Ying, Gaidzik, Verena E., Blanchet, Odile, Karimi, Mohsen, Bengtzén, Sofia, Nahi, Hareth, Uggla, Bertil, Tidefelt, Ulf, Höglund, Martin, Paul, Christer, Ekwall, Karl, Döhner, Konstanze, and Lehmann, Sören

Abstract

Cytogenetically normal acute myeloid leukemia (CN-AML) comprise between forty and fifty percent of all adult acute myeloid leukemia (AML) cases. In this clinically diverse group molecular aberrations such as FLT3ITD, NPM1 and CEBPA mutations recently have added to the prognostic accuracy. Aberrant DNA methylation is a hallmark of cancer including AML. We investigated in total 118 CN-AML samples in a test and a validation cohort for genome-wide promoter DNA methylation with Illumina Methylation Bead arrays and compared them to normal myeloid precursors and global gene expression. IDH and NPM1 mutations were associated with different methylation patterns (p=0.0004 and 0.04, respectively). Genome-wide methylation levels were elevated in IDH mutated samples (p=0.006). We observed a negative impact of DNA methylation on transcription. Genes targeted by Polycomb group (PcG) proteins and genes associated with bivalent histone marks in stem cells showed increased aberrant methylation in AML (p<0.0001). Furthermore, high methylation levels of PcG target genes were independently associated with better progression free (OR 0.47, p=0.01) and overall survival (OR 0.36, p=0.001). In summary, genome wide methylation patterns show preferential methylation of PcG targets with prognostic impact in CN-AML., Funding Agencies:Göran Gustafssons Foundation for Research in Natural Sciences Sigurd och Elsa Golje Foundation Ligue Contre le Cancer La Region Pays de la Loire/Appel a Projets du Canceropole Grand-Ouest

Published

2011