4.5 Article

A novel approach for the identification of efficient combination therapies in primary human acute myeloid leukemia specimens

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BLOOD CANCER JOURNAL
卷 7, 期 -, 页码 -

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SPRINGERNATURE
DOI: 10.1038/bcj.2017.10

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资金

  1. Government of Canada through Genome Canada
  2. Ministere de l'Economie, de l'Innovation et des Exportations du Quebec through Genome Quebec
  3. Amorchem
  4. Canada Research Chair program
  5. Industrielle-Alliance (Universite de Montreal)
  6. Cancer Research Network of the Fonds de recherche du Quebec-Sante
  7. Canada Foundation for Innovation (CFI)
  8. NanoQuebec
  9. RMGA
  10. Fonds de recherche du Quebec-Nature et technologies (FRQ-NT)
  11. Cole foundation
  12. Human Frontier Science Program (HFSP)

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Appropriate culture methods for the interrogation of primary leukemic samples were hitherto lacking and current assays for compound screening are not adapted for large-scale investigation of synergistic combinations. In this study, we report a novel approach that efficiently distills synthetic lethal interactions between small molecules active on primary human acute myeloid leukemia (AML) specimens. In single-dose experiments and under culture conditions preserving leukemia stem cell activity, our strategy considerably reduces the number of tests needed for the identification of promising compound combinations. Initially conducted with a selected library of 5000 small molecules and 20 primary AML specimens, it reveals 5 broad classes of sensitized therapeutic target pathways along with their synergistic patient-specific fingerprints. This novel method opens new avenues for the development of AML personalized therapeutics and may be generalized to other tumor types, for which in vitro cancer stem cell cultures have been developed.

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