1. Computational modeling of early T-cell precursor acute lymphoblastic leukemia (ETP-ALL) to identify personalized therapy using genomics
- Author
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Leylah Drusbosky, Shireen Vali, Shahabuddin Usmani, Shivgonda C. Birajdar, Ansu Kumar, Christopher R. Cogle, P. R. K. Bhargav, Anuj Tyagi, Aftab Alam, Taher Abbasi, Amy Meacham, Deepak Anil Lala, Anusha Pampana, Kunal Ghosh Roy, Sumanth Vasista, Girish Chinnaswamy, Madeleine Turcotte, Swaminathan Rajagopalan, Manju Sengar, Bijal D. Shah, and Kabya Basu
- Subjects
Drug ,Cancer Research ,NPM1 ,media_common.quotation_subject ,T cell ,Lymphoblastic Leukemia ,Genomics ,Computational biology ,Biology ,Precursor T-Cell Lymphoblastic Leukemia-Lymphoma ,Sensitivity and Specificity ,03 medical and health sciences ,0302 clinical medicine ,Biomarkers, Tumor ,medicine ,Humans ,Computer Simulation ,Precision Medicine ,Personalized therapy ,media_common ,Computational Biology ,Myeloid leukemia ,Hematology ,medicine.disease ,Leukemia ,medicine.anatomical_structure ,Oncology ,030220 oncology & carcinogenesis ,Nucleophosmin ,030215 immunology - Abstract
Early T-cell precursor acute lymphoblastic leukemia (ETP-ALL) is an aggressive hematological malignancy for which optimal therapeutic approaches are poorly characterized. Using computational biology modeling (CBM) in conjunction with genomic data from cell lines and individual patients, we generated disease-specific protein network maps that were used to identify unique characteristics associated with the mutational profiles of ETP-ALL compared to non-ETP-ALL (T-ALL) cases and simulated cellular responses to a digital library of FDA-approved and investigational agents. Genomics-based classification of ETP-ALL patients using CBM had a prediction sensitivity and specificity of 93% and 87%, respectively. This analysis identified key genomic and pathway characteristics that are distinct in ETP-ALL including deletion of nucleophosmin-1 (NPM1), mutations of which are used to direct therapeutic decisions in acute myeloid leukemia. Computational simulations based on mutational profiles of 62 ETP-ALL patient models identified 87 unique targeted combination therapies in 56 of the 62 patients despite actionable mutations being present in only 37% of ETP-ALL patients. Shortlisted two-drug combinations were predicted to be synergistic in 11 profiles and were validated by in vitro chemosensitivity assays. In conclusion, computational modeling was able to identify unique biomarkers and pathways for ETP-ALL, and identify new drug combinations for potential clinical testing.
- Published
- 2019
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