&lt;p&gt;The synergistic antileukemic effects of eltrombopag and decitabine in myeloid leukemia cells&lt;/p&gt;

Shi, Mingyue; Xu, Fangfang; Yang, Xinrong; Bai, Yanliang; Niu, Junwei; Drokow, Emmanuel Kwateng; Chen, Mingyi; Chen, Yuqing; Sun, Kai

doi:10.2147/cmar.s213931

Cited by 10 publications

(15 citation statements)

References 35 publications

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“…Instead, we identified that the growth inhibitory effect of eltrombopag is due, in part, to the iron chelation properties of the drug, which provides further support for our previous work that identified iron chelator drugs as a unique vulnerability of Ewing sarcoma tumor in vitro and in vivo [7]. Notably, eltrombopag has also been reported to target additional cancer types, including leukemia and hepatocellular carcinoma, via an iron chelation mechanism [12,13,55].…”

Section: Discussionsupporting

confidence: 81%

Eltrombopag inhibits the proliferation of Ewing sarcoma cells via iron chelation and impaired DNA replication

et al. 2020

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Background The treatment of Ewing sarcoma, an aggressive bone and soft tissue sarcoma, is associated with suboptimal outcomes and significant side-effects. Consequently, there is an urgent need to identify novel therapies that will improve outcomes for children and adults with Ewing sarcoma tumors while also decreasing treatment-related toxicities. Methods We analyzed data from the PRISM drug repurposing screen, which tested the activity of 4518 drugs across 578 cancer cell lines, to identify drugs that selectively inhibit the growth of Ewing sarcoma cell lines. We then tested the effects of a top hit from the screen on cell proliferation, cell cycle progression, and activation of the DNA damage pathway using Ewing sarcoma cell lines. We also used a CRISPR/Cas9 gene knockout approach to investigate the role of Schlafen 11 (SLFN11), a restriction factor for DNA replication stress that is overexpressed in Ewing sarcoma tumors, in mediating the sensitivity of Ewing sarcoma cells to the drug. Results We found that eltrombopag, an FDA-approved thrombopoietin-receptor agonist (TPO-RA) that is currently being evaluated as a treatment for chemotherapy-induced thrombocytopenia, inhibits the growth of Ewing sarcoma cell lines in vitro in proliferation and colony formation assays. However, from a mechanistic standpoint, the thrombopoietin receptor is not expressed in Ewing sarcoma cells and we show that eltrombopag impairs DNA replication and causes DNA damage in Ewing sarcoma cells by chelating iron, a known “off-target” effect of the drug. We also found that the sensitivity of Ewing sarcoma cells to eltrombopag is mediated, in part, by SLFN11, which regulates the cellular response to DNA replication stress. Conclusions Ewing sarcoma cell lines are sensitive to eltrombopag and this drug could improve outcomes for patients with Ewing sarcoma tumors by both targeting the tumor, via chelation of iron and inhibition of DNA replication, and reducing chemotherapy-induced thrombocytopenia, via stimulation of the thrombopoietin receptor.

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Section: Discussionsupporting

confidence: 81%

Eltrombopag inhibits the proliferation of Ewing sarcoma cells via iron chelation and impaired DNA replication

et al. 2020

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“…This controversial aspect on iron overload management could depend on the considered cell type and health condition. As regards cell cycle progression, we observed a block in S phase after cytarabine administration in THP-1 cells, as also reported for decitabine, another chemotherapy drug currently used in AML not eligible for standard protocols [37]. But, when we combined it with ELT, the arrest shifted in G0/G1 phase, consistently with the already documented effects of ELT used alone [37,40].…”

Section: Figure 5: Effect Of 48-hour Treatments On Proliferation Nfkb Protein Expression Level In Thp-1 Cell Line Was Determined Bysupporting

confidence: 88%

“…As regards cell cycle progression, we observed a block in S phase after cytarabine administration in THP-1 cells, as also reported for decitabine, another chemotherapy drug currently used in AML not eligible for standard protocols [37]. But, when we combined it with ELT, the arrest shifted in G0/G1 phase, consistently with the already documented effects of ELT used alone [37,40]. Several authors demonstrated that iron chelators reduce cyclin-dependent kinase 2 (CDK2) activity [41][42][43], a protein normally responsible for cell cycle progression from G0/G1 phase to S one.…”

Section: Figure 5: Effect Of 48-hour Treatments On Proliferation Nfkb Protein Expression Level In Thp-1 Cell Line Was Determined Bysupporting

confidence: 85%

“…This difference could be due to biological differences between cancers and also to differences in therapy strategies. Even though the role of ferroportin in cancer need to be better clarified, in literature it is clear the potential anticancer role of iron chelation and in particular ELT seems to be a very promising agent in this field [ 36 , 37 ].…”

Section: Discussionmentioning

confidence: 99%

“…All treatments we administered caused a significative increase in CDK2 expression, which is not in accordance with the arrest actually observed by cytofluorimetry. Therefore, it could be interesting to investigate on the hypothesis formulated by Shi et al ., which observed an arrest in G0/G1 phase after treating leukemia cells with ELT and decitabine [ 37 ] and attributed this anticancer effect to the alteration in intracellular ROS levels caused by ELT [ 40 ]. We also evaluated the effect of treatments on cell proliferation by analyzing the expression levels of nuclear transcription factor-kappa beta (NFkB), one of the principal mediators of inflammation, carcinogenesis [ 45 , 46 ] and chemotherapy resistance [ 38 ].…”

Section: Discussionmentioning

confidence: 99%

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Eltrombopag and its iron chelating properties in pediatric acute myeloid leukemia

et al. 2021

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Pediatric acute myeloid leukemia (AML) represents 20% of total childhood leukemia diagnoses and is characterized by poor prognosis with a long-term survival rate around the 50%, when patients are properly treated. The standard treatment for pediatric AML currently consists in a combination of cytarabine (Ara-C) and antracycline. Iron plays an important role in cancer development and progression. Targeting iron and its metabolism mediators could be a novel therapeutic strategy in cancer.Deferasirox (DFX) inhibits cancer cell proliferation and its use as an antiblastic drug could be suggested. Eltrombopag (ELT), a thrombopoietin receptor agonist used in immunethrombocytopenia, shows anticancer properties related to its emerging iron chelating properties. We compare the anticancer effect of classically used cytarabine with DFX and ELT effects in a pediatric AML cell line, THP-1, in order to identify innovative and more effective therapeutic strategies. ELT and DFX reduce intracellular iron concentration by inhibiting its uptake and by promoting its release.In particular, even though further investigations are needed to better understand the extact underlying action mechanisms, we demonstrated that ELT improves cytarabine antineoplastic activity in pediatric AML cell line.

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Decitabine and all-trans retinoic acid synergistically exhibit cytotoxicity against elderly AML patients via miR-34a/MYCN axis

Cao

Liu

Shang

et al. 2020

Biomedicine & Pharmacotherapy

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<p>The synergistic antileukemic effects of eltrombopag and decitabine in myeloid leukemia cells</p>

Cited by 10 publications

References 35 publications

Eltrombopag inhibits the proliferation of Ewing sarcoma cells via iron chelation and impaired DNA replication

Eltrombopag inhibits the proliferation of Ewing sarcoma cells via iron chelation and impaired DNA replication

Eltrombopag and its iron chelating properties in pediatric acute myeloid leukemia

Decitabine and all-trans retinoic acid synergistically exhibit cytotoxicity against elderly AML patients via miR-34a/MYCN axis

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