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ASP210: a potent oligonucleotide-based inhibitor effective against TKI-resistant CML cells
V. Nemethova, P. Babiakova, B. Teglasova, L. Uhelska, A. Babelova, M. Selc, K. Jakic, O. Mitrovsky, D. Myslivcova, M. Zackova, A. Poturnayova, A. Batorova, L. Drgona, F. Razga
Jazyk angličtina Země Spojené státy americké
Typ dokumentu časopisecké články
Grantová podpora
APVV-15-0215
Agentúra na Podporu Výskumu a Vývoja (APVV)
APVV-19-0070
Agentúra na Podporu Výskumu a Vývoja (APVV)
1/0069/20
Vedecká Grantová Agentúra MŠVVaŠ SR a SAV (VEGA)
2/0160/21
Vedecká Grantová Agentúra MŠVVaŠ SR a SAV (VEGA)
2/0116/22
Vedecká Grantová Agentúra MŠVVaŠ SR a SAV (VEGA)
00023736
Ministerstvo Zdravotnictví Ceské Republiky (MZCR)
313021T081
Slovenská Akadémia Vied (SAV)
NLK
American Physiological Society
od 2024-03-01
Open Access Digital Library
od 1997-10-01
- MeSH
- apoptóza * účinky léků MeSH
- bcr-abl fúzní proteiny * genetika antagonisté a inhibitory metabolismus MeSH
- chemorezistence * účinky léků MeSH
- chronická myeloidní leukemie * farmakoterapie genetika patologie MeSH
- dasatinib farmakologie MeSH
- imatinib mesylát * farmakologie terapeutické užití MeSH
- inhibitory proteinkinas * farmakologie MeSH
- lidé MeSH
- messenger RNA genetika metabolismus MeSH
- nádorové buněčné linie MeSH
- oligonukleotidy * farmakologie MeSH
- protinádorové látky farmakologie MeSH
- viabilita buněk účinky léků MeSH
- Check Tag
- lidé MeSH
- Publikační typ
- časopisecké články MeSH
Clinical experience with tyrosine kinase inhibitors (TKIs) over the past two decades has shown that, despite the apparent therapeutic benefit, nearly 30% of patients with chronic myelogenous leukemia (CML) display primary resistance or intolerance to TKIs, and approximately 25% of those treated are forced to switch TKIs at least once during therapy due to acquired resistance. Safe and effective treatment modalities targeting leukemic clones that escape TKI therapy could hence be game changers in the professional management of these patients. Here, we aimed to investigate the efficacy of a novel therapeutic oligonucleotide of unconventional design, called ASP210, to reduce BCR-ABL1 mRNA levels in TKI-resistant CML cells, with the assumption of inducing their apoptosis. Imatinib- and dasatinib-resistant sublines of BCR-ABL1-positive MOLM-7 and CML-T1 cells were established and exposed to 0.25 and 2.5 μM ASP210 for 10 days. RT-qPCR showed a remarkable reduction of the target mRNA level by >99% after a single application. Cell viability was monitored daily by trypan blue staining. In response to the lack of driver oncoprotein BCR-ABL1, TKI-resistant CML cells underwent apoptosis regardless of the presence of the clinically relevant T315I mutation by day 5 after redosing with ASP210. The effect was selective for cancer cells, indicating a favorable safety profile for this therapeutic modality. Furthermore, the spontaneous uptake and high intracellular concentrations of ASP210 suggest its potential to be effective at relatively low doses. The present findings suggest that ASP210 is a promising therapeutic avenue for patients with CML who fail to respond to TKI therapy.NEW & NOTEWORTHY Effective treatment modalities targeting leukemic clones that escape tyrosine kinase inhibitor (TKI) therapy could be game changers in the professional management of patients displaying primary resistance, intolerance, or acquired resistance to TKIs. Although delivering authentic innovations today is more complex than ever, we developed a highly potent and safe oligonucleotide-based modality against BCR-ABL1 mRNA named ASP210 that effectively induces cell death in BCR-ABL1-positive TKI-resistant cells while sparing BCR-ABL1-negative healthy cells.
Centre for Advanced Materials Application Slovak Academy of Sciences Bratislava Slovakia
Department of Biochemistry Faculty of Science Charles University Prague Czech Republic
Department of Oncohematology Comenius University and National Cancer Institute Bratislava Slovakia
Department of Proteomics Institute of Hematology and Blood Transfusion Prague Czech Republic
Citace poskytuje Crossref.org
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