PIM inhibitors target CD25-positive AML cells through concomitant suppression of STAT5 activation and degradation of MYC oncogene

Guo, Zhuyan; Wang, Anlai; Zhang, Weidong; Levit, Mikhail; Gao, Qiang; Barberis, Claude; Tabart, Michel; Zhang, Jingxin; Hoffmann, Dietmar; Wiederschain, Dmitri; Rocnik, Jennifer L.; Sun, Fangxian; Murtie, Josh; Lengauer, Christoph; Größ, Stefan; Zhang, Bailin; Cheng, Hong; Patel, Vinod F.; Schio, Laurent; Adrián, Francisco; Dorsch, Marion; García‐Echeverría, Carlos; Huang, Shih Min A

doi:10.1182/blood-2014-01-551234

Cited by 40 publications

(35 citation statements)

References 45 publications

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“…As expected from cell culture experiments, mice treated with AZD1208 had activated STAT signaling; this activation was significantly inhibited in mice with combination treatment. Following treatment with AZD1208, induction of PIM1 protein levels was increased, as previously reported with other PIM inhibitors [58]. These results support dual inhibitor treatment for a specific subset of T-ALL tumors expressing PIM1.…”

Section: Resultssupporting

confidence: 86%

Targeting the PIM protein kinases for the treatment of a T-cell acute lymphoblastic leukemia subset

Padi

Luevano

et al. 2017

Oncotarget

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New approaches are needed for the treatment of patients with T-cell acute lymphoblastic leukemia (T-ALL) who fail to achieve remission with chemotherapy. Analysis of the effects of pan-PIM protein kinase inhibitors on human T-ALL cell lines demonstrated that the sensitive cell lines expressed higher PIM1 protein kinase levels, whereas T-ALL cell lines with NOTCH mutations tended to have lower levels of PIM1 kinase and were insensitive to these inhibitors. NOTCH-mutant cells selected for resistance to gamma secretase inhibitors developed elevated PIM1 kinase levels and increased sensitivity to PIM inhibitors. Gene profiling using a publically available T-ALL dataset demonstrated overexpression of PIM1 in the majority of early T-cell precursor (ETP)-ALLs and a small subset of non-ETP ALL. While the PIM inhibitors blocked growth, they also stimulated ERK and STAT5 phosphorylation, demonstrating that activation of additional signaling pathways occurs with PIM inhibitor treatment. To block these pathways, Ponatinib, a broadly active tyrosine kinase inhibitor (TKI) used to treat chronic myelogenous leukemia, was added to this PIM-inhibitor regimen. The combination of Ponatinib with a PIM inhibitor resulted in synergistic T-ALL growth inhibition and marked apoptotic cell death. Treatment of mice engrafted with human T-ALL with these two agents significantly decreased the tumor burden and improved the survival of treated mice. This dual therapy has the potential to be developed as a novel approach to treat T-ALL with high PIM expression.

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Section: Resultssupporting

confidence: 86%

Targeting the PIM protein kinases for the treatment of a T-cell acute lymphoblastic leukemia subset

Padi

Luevano

et al. 2017

Oncotarget

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“…PIM inhibitors have been investigated in AML cells as single agents as well as in combination, with varying potencies and cellular consequences[5,7,10,14,17,31,33–44]. Downstream mTOR targets (4E-BP1, PRAS40, eIF4B)[23,45,46] and upstream regulators (TSC2) [47] have been identified as Pim targets, and our RPPA investigations support the reports of Pim activity on mTOR signaling.…”

Section: Discussionmentioning

confidence: 99%

“…Pim-1 kinase also regulates MET receptor tyrosine kinase levels and signaling via translation through phosphorylation of eIF4B[6]. More recently, Pim inhibition has been demonstrated to suppress STAT5 activation and reduce MYC protein half-life in higher CD25-expressing subpopulations of AML cell lines[7]. Thus, inhibition of Pim kinases may be an avenue to target AML cell survival.…”

Section: Introductionmentioning

confidence: 99%

Protein profiling identifies mTOR pathway modulation and cytostatic effects of Pim kinase inhibitor, AZD1208, in acute myeloid leukemia

Chen

Yang

Han

et al. 2016

Leukemia & Lymphoma

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Pim kinases phosphorylate and regulate a number of key AML cell survival proteins, and Pim inhibitors have recently entered clinical trial for hematological malignancies. AZD1208 is a small molecule pan-Pim kinase inhibitor and AZD1208 treatment resulted in growth inhibition and cell size reduction in AML cell lines including FLT3-WT (OCI-AML-3, KG-1a, MOLM-16) and FLT3-ITD mutated (MOLM-13, MV-4-11). There was limited apoptosis induction (<10% increase) in the AML cell lines evaluated with up to 3 μM AZD1208 for 24h, suggesting that growth inhibition is not through apoptosis induction. Using reverse phase protein array (RPPA) and immunoblot analysis, we identified that AZD1208 resulted in suppression of mTOR signaling, including inhibition of protein phosphorylation of mTOR(Ser2448), p70S6K(Thr389), S6(Ser235/236) and 4E-BP1(Ser65). Consistent with mTOR inhibition, there was also a reduction in protein synthesis that correlated with cell size reduction and growth inhibition with AZD1208; our study provide insights into the mechanism of AZD1208.

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“…Several retrospective studies carried out in AML patients have shown that patients with a higher percentage of CD25-positive AML blasts have poor overall survival or relapse-free survival [126,127]. The enhanced CD25 expression in AMLs seems to be induced by STAT5 and MYC hyperactivation occurring in many AMLs: both STAT5 and MYC play a key role in leukemia-initiating activity [128,129].…”

Section: Cd25 and Cd32mentioning

confidence: 96%

Targeting LSCs through membrane antigens selectively or preferentially expressed on these cells

Pelosi

Castelli

Testa

2015

Blood Cells, Molecules, and Diseases

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PIM inhibitors target CD25-positive AML cells through concomitant suppression of STAT5 activation and degradation of MYC oncogene

Cited by 40 publications

References 45 publications

Targeting the PIM protein kinases for the treatment of a T-cell acute lymphoblastic leukemia subset

Targeting the PIM protein kinases for the treatment of a T-cell acute lymphoblastic leukemia subset

Protein profiling identifies mTOR pathway modulation and cytostatic effects of Pim kinase inhibitor, AZD1208, in acute myeloid leukemia

Targeting LSCs through membrane antigens selectively or preferentially expressed on these cells

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