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المؤلفKhan, Abbas
المؤلفZahid, Muhammad Ammar
المؤلفShahab, Muhammad
المؤلفAl-Zoubi, Raed M.
المؤلفShkoor, Mohanad
المؤلفBenameur, Tarek
المؤلفAgouni, Abdelali
تاريخ الإتاحة2024-09-26T10:55:21Z
تاريخ النشر2024-04-30
اسم المنشورJournal of Biomolecular Structure and Dynamics
المعرّفhttp://dx.doi.org/10.1080/07391102.2024.2335289
الاقتباسKhan, A., Zahid, M. A., Shahab, M., Al-Zoubi, R. M., Shkoor, M., Benameur, T., & Agouni, A. (2024). Investigating the role of functional mutations in leucine binding to Sestrin2 in aging and age-associated degenerative pathologies using structural and molecular simulation approaches. Journal of Biomolecular Structure and Dynamics, 1-13.
الرقم المعياري الدولي للكتاب0739-1102
معرّف المصادر الموحدhttps://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=85192086559&origin=inward
معرّف المصادر الموحدhttp://hdl.handle.net/10576/59370
الملخصLeucine is the native known ligand of Sestrin2 (Sesn2) and its interaction with Sesn2 is particularly important, as it influences the activity of mTOR in aging and its associated pathologies. It is important to find out how leucine interacts with Sesn2 and how mutations in the binding pocket of leucine affect the binding of leucine. Therefore, this study was committed to investigating the impact of non-synonymous mutations by incorporating a broad spectrum of simulation techniques, from molecular dynamics to free energy calculations. Our study was designed to model the atomic-scale interactions between leucine and mutant forms of Sesn2. Our results demonstrated that the interaction paradigm for the mutants has been altered thus showing a significant decline in the hydrogen bonding network. Moreover, these mutations compromised the dynamic stability by altering the conformational flexibility, sampling time, and leucine-induced structural constraints that consequently caused variation in the binding and structural stability. Molecular dynamics-based flexibility analysis revealed that the regions 217–339 and 371–380 demonstrated a higher fluctuation. Noteworthy, these regions correspond to a linker (217–339) and a loop (371–380) that cover the leucine binding cavity that is critical for the ‘latch’ mechanism in the N-terminal, which is essential for leucine binding. Further validation of reduced binding and modified internal motions caused by the mutants was obtained through binding free energy calculations, principal components analysis (PCA), and free energy landscape (FEL) analysis. By unraveling the molecular intricacies of Sesn2-leucine interactions and their mutations, we hope to pave the way for innovative strategies to combat the inevitable tide of aging and its associated diseases. Communicated by Ramaswamy H. Sarma.
راعي المشروعOpen Access funding provided by the Qatar National Library. This work was funded by Qatar National Research Fund (Qatar Research Development and Innovation Council) [grant No. NPRP14S-0406-210150].
اللغةen
الناشرTaylor & Francis
الموضوعaging
free energy calculations
molecular interactions
molecular simulation
Sestrin2
العنوانInvestigating the role of functional mutations in leucine binding to Sestrin2 in aging and age-associated degenerative pathologies using structural and molecular simulation approaches
النوعArticle
الصفحات1-13
ESSN1538-0254
dc.accessType Open Access


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