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Implementation of Docking, Molecular Dynamics and Free Energy to Investigate Drug Potency of Novel Bcr-Ablt315i Inhibitors As an Alternative to Ponatinib Publisher



Mahmoudi Gomari M1, 2 ; Rostami N3 ; Ghodrati A4 ; Hernandez Y5 ; Fadaie M6 ; Sadegh Eslami S2 ; Tarighi P2
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Authors Affiliations
  1. 1. Student Research Committee, School of Allied Medical Sciences, Iran University of Medical Sciences, Tehran, Iran
  2. 2. Department of Medical Biotechnology, Faculty of Allied Medicine, Iran University of Medical Sciences, Tehran, Iran
  3. 3. Department of Chemical Engineering, Faculty of Engineering, Arak University, Iran
  4. 4. Department of Chemistry and Biochemistry, University of Windsor, Windsor, Canada
  5. 5. Department of Cellular and Molecular Medicine, University of Arizona, Tucson, United States
  6. 6. Department of Genetics and Molecular Biology, School of Medicine, Isfahan University of Medical Sciences, Isfahan, Iran

Source: Computational Toxicology Published:2021


Abstract

Today, a significant proportion of health costs is dedicated to cancer diagnosis and treatment. Despite considerable advances made in cancer research, the treatment of this disease is still facing numerous challenges. One of the main problems in this field is drug resistance, which in most cases, incidence of mutations in the target molecules is responsible for not responding to prescribed treatments. Chronic myeloid leukemia (CML), is a cancer that is not exempt to this rule. It has been shown that BCR-ABL plays a central role in the emergence of CML and targeting this molecule is a part of all the related therapies. Some mutations in BCR-ABL protein such as T315I reduces the effectiveness of drugs in patients. Compounds such as PBA2, CD-200 and JNJ-26854165 have been introduced as novel candidates for CML treatment in different in vitro/in vivo studies and show potential inhibitory impacts on BCR-ABLT315I. In the present study, our group utilizes computational analysis to investigated interactions and compare the efficiency of designed small molecules to inhibit the BCR-ABLT315I functional domain. Results obtained during docking, analysis of hydrogen bonds and free energy calculation indicated that JNJ-26854165 is a more suitable agent to BCR-ABLT315I inhibition than the other two candidates. However, ponatinib (control agent) shows a higher BCR-ABLT315I inhibitory potency than JNJ-26854165 in the present investigation. Our study demonstrates that none of the three candidate drugs is as potent as ponatinib in terms of targeting the mutant BCR-ABLT315I. © 2021 Elsevier B.V.
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