| Literature DB >> 29042365 |
Margaret Nieborowska-Skorska1, Silvia Maifrede1, Yashodhara Dasgupta1, Katherine Sullivan1, Sylwia Flis1,2, Bac Viet Le1,3, Martyna Solecka1, Elizaveta A Belyaeva4, Lucia Kubovcakova5, Morgan Nawrocki1, Martin Kirschner6, Huaqing Zhao7, Josef T Prchal8, Katarzyna Piwocka3, Alison R Moliterno9, Mariusz Wasik4, Steffen Koschmieder6, Tony R Green10,11,12, Radek C Skoda5, Tomasz Skorski1,13.
Abstract
Myeloproliferative neoplasms (MPNs) often carry JAK2(V617F), MPL(W515L), or CALR(del52) mutations. Current treatment options for MPNs include cytoreduction by hydroxyurea and JAK1/2 inhibition by ruxolitinib, both of which are not curative. We show here that cell lines expressing JAK2(V617F), MPL(W515L), or CALR(del52) accumulated reactive oxygen species-induced DNA double-strand breaks (DSBs) and were modestly sensitive to poly-ADP-ribose polymerase (PARP) inhibitors olaparib and BMN673. At the same time, primary MPN cell samples from individual patients displayed a high degree of variability in sensitivity to these drugs. Ruxolitinib inhibited 2 major DSB repair mechanisms, BRCA-mediated homologous recombination and DNA-dependent protein kinase-mediated nonhomologous end-joining, and, when combined with olaparib, caused abundant accumulation of toxic DSBs resulting in enhanced elimination of MPN primary cells, including the disease-initiating cells from the majority of patients. Moreover, the combination of BMN673, ruxolitinib, and hydroxyurea was highly effective in vivo against JAK2(V617F)+ murine MPN-like disease and also against JAK2(V617F)+, CALR(del52)+, and MPL(W515L)+ primary MPN xenografts. In conclusion, we postulate that ruxolitinib-induced deficiencies in DSB repair pathways sensitized MPN cells to synthetic lethality triggered by PARP inhibitors.Entities:
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Year: 2017 PMID: 29042365 PMCID: PMC5746670 DOI: 10.1182/blood-2017-05-784942
Source DB: PubMed Journal: Blood ISSN: 0006-4971 Impact factor: 25.476