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المؤلفThirumal Kumar, D
المؤلفJain, Nikita
المؤلفEvangeline, Judith
المؤلفKamaraj, Balu
المؤلفSiva, R
المؤلفZayed, Hatem
المؤلفGeorge Priya Doss, C
تاريخ الإتاحة2019-11-13T05:51:41Z
تاريخ النشر2019-10-01
اسم المنشورComputers in Biology and Medicine
المعرّفhttp://dx.doi.org/10.1016/j.compbiomed.2019.103513
الاقتباس: T. Kumar D, N. Jain, J. Evangeline, B. Kamaraj, S. R, H. Zayed, G.P.Doss C, A computational approach for investigating the mutational landscape of RAC-alpha serine/threonine-protein kinase (AKT1) and screening inhibitors against the oncogenic E17K mutationcausing breast cancer, Computers in Biology and Medicine (2019), doi: https://doi.org/10.1016/j.compbiomed.2019.103513.
الرقم المعياري الدولي للكتاب0010-4825
المعرّف103513
معرّف المصادر الموحدhttp://hdl.handle.net/10576/12317
الملخصBreast cancer (BC) is the most commonly diagnosed cancer among females worldwide, and among the BC-associated mutations in various proteins, mutations in the RAC-alpha serine/threonine-protein kinase (AKT1) remain the most dominant. We thus attempted to understand the potential molecular pathogenicity profile of the mutations in AKT1 using a comprehensive computational protocol involving analyses of biochemistry-disruption and destabilizing properties and conservation. Our predictions revealed that E17K, R67W, V164G, E319G, R391G, D32Y, L52H, L52R, and W80R were the most pathogenic mutations. In addition, the change of glutamate to lysine at position 17 of AKT1 (E17K) was found to be highly predominant. An extensive two-step molecular dynamics (simple and complex) simulation (MDS) using GROMACS (GROningen MAchine for Chemical Simulations) was then initiated to analyze and understand the structural impact of the E17K mutation on the function of AKT1. The simple MDS analysis revealed that the E17K mutation decreases the compactness and intramolecular hydrogen bonds of the protein. We also performed a virtual screening analysis with 19 AKT inhibitors obtained from the Selleck Chemicals website those satisfied the Lipinski rule of 5. Among these 19 compounds, Akti-1/2 exhibited the best binding affinity with both native AKT1 and the E17K mutant. The molecular interaction study also revealed that the co-crystallized AKT1 inhibitor N-(4-(5-(3-acetamidophenyl)-2-(2-aminopyridin-3-yl)-3H-imidazo [4,5-b]pyridin-3-yl)benzyl)-3-fluorobenzamide (12j) exhibited a better interaction with native AKT1 compared with the E17K mutant AKT1 protein, whereas, Akti-1/2 exhibited the opposite effects, i.e., a better interaction with the E17K mutant AKT1 than the native AKT1. These findings from the interaction analysis were further supported by the complex MDS, which measured the compactness and intermolecular hydrogen bonds of the proteins. The results obtained in this study suggest that Akti-1/2 might be a better inhibitor for the treatment of BC caused by the E17K mutation in AKT1.
اللغةen
الناشرElsevier
الموضوعAKT1
E17K
Molecular dynamics simulation analysis
Variant classification
Virtual screening analysis
العنوانA computational approach for investigating the mutational landscape of RAC-alpha serine/threonine-protein kinase (AKT1) and screening inhibitors against the oncogenic E17K mutation causing breast cancer.
النوعArticle
ESSN1879-0534
dc.accessType Abstract Only


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