Author
Listed:
- Gero Knittel
(University Hospital of Cologne
University of Cologne
University Hospital of Cologne)
- Tim Rehkämper
(University Hospital of Cologne
University of Cologne
University Hospital of Cologne)
- Darya Korovkina
(University Hospital of Cologne
University of Cologne
University Hospital of Cologne)
- Paul Liedgens
(University Hospital of Cologne
University of Cologne
University Hospital of Cologne)
- Christian Fritz
(University Hospital of Cologne
University of Cologne
University Hospital of Cologne)
- Alessandro Torgovnick
(University Hospital of Cologne
University of Cologne
University Hospital of Cologne)
- Yussor Al-Baldawi
(University Hospital of Cologne)
- Mona Al-Maarri
(Max-Planck-Institute for Metabolism Research)
- Yupeng Cun
(University of Cologne)
- Oleg Fedorchenko
(University Hospital of Cologne
University of Cologne
University Hospital of Cologne)
- Arina Riabinska
(University Hospital of Cologne
University of Cologne
University Hospital of Cologne)
- Filippo Beleggia
(University Hospital of Cologne
University of Cologne
University Hospital of Cologne)
- Phuong-Hien Nguyen
(University Hospital of Cologne
University of Cologne
University Hospital of Cologne)
- F. Thomas Wunderlich
(Max-Planck-Institute for Metabolism Research)
- Monika Ortmann
(University Hospital of Cologne)
- Manuel Montesinos-Rongen
(University Hospital of Cologne)
- Eugen Tausch
(Ulm University)
- Stephan Stilgenbauer
(Ulm University)
- Lukas P. Frenzel
(University Hospital of Cologne
University of Cologne
University Hospital of Cologne)
- Marco Herling
(University Hospital of Cologne
University of Cologne
University Hospital of Cologne
University of Cologne)
- Carmen Herling
(University Hospital of Cologne
University Hospital of Cologne)
- Jasmin Bahlo
(University Hospital of Cologne)
- Michael Hallek
(University Hospital of Cologne
University of Cologne
University Hospital of Cologne)
- Martin Peifer
(University of Cologne)
- Reinhard Buettner
(University Hospital of Cologne
University Hospital of Cologne)
- Thorsten Persigehl
(University Hospital of Cologne)
- H. Christian Reinhardt
(University Hospital of Cologne
University of Cologne
University Hospital of Cologne
University of Cologne)
Abstract
Chronic lymphocytic leukemia (CLL) remains an incurable disease. Two recurrent cytogenetic aberrations, namely del(17p), affecting TP53, and del(11q), affecting ATM, are associated with resistance against genotoxic chemotherapy (del17p) and poor outcome (del11q and del17p). Both del(17p) and del(11q) are also associated with inferior outcome to the novel targeted agents, such as the BTK inhibitor ibrutinib. Thus, even in the era of targeted therapies, CLL with alterations in the ATM/p53 pathway remains a clinical challenge. Here we generated two mouse models of Atm- and Trp53-deficient CLL. These animals display a significantly earlier disease onset and reduced overall survival, compared to controls. We employed these models in conjunction with transcriptome analyses following cyclophosphamide treatment to reveal that Atm deficiency is associated with an exquisite and genotype-specific sensitivity against PARP inhibition. Thus, we generate two aggressive CLL models and provide a preclinical rational for the use of PARP inhibitors in ATM-affected human CLL.
Suggested Citation
Gero Knittel & Tim Rehkämper & Darya Korovkina & Paul Liedgens & Christian Fritz & Alessandro Torgovnick & Yussor Al-Baldawi & Mona Al-Maarri & Yupeng Cun & Oleg Fedorchenko & Arina Riabinska & Filipp, 2017.
"Two mouse models reveal an actionable PARP1 dependence in aggressive chronic lymphocytic leukemia,"
Nature Communications, Nature, vol. 8(1), pages 1-13, December.
Handle:
RePEc:nat:natcom:v:8:y:2017:i:1:d:10.1038_s41467-017-00210-6
DOI: 10.1038/s41467-017-00210-6
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