• الصفحة الرئيسية
  • The Molecular Docking and Molecular Dynamics Simulation of Some HIV-1 protease Inhibitors For the treatment of Coronavirus Disease-19

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عنوان URL للمقالة


رقم المقالة : JPTC-2201-1233 (R1) زيارة : 113 الصفحة: 1 - 7

10.30495/jptc.2023.65656.1233

نوع المخطوط: ابحاث

The Molecular Docking and Molecular Dynamics Simulation of Some HIV-1 protease Inhibitors For the treatment of Coronavirus Disease-19

الموضوعات : Journal of Physical & Theoretical Chemistry

ghasem ghasemi 1 , babak motahary 2 , robabe Sayadikordabadi 3 , Asghar Alizadehdakhel 4

1 - Department of Chemistry and Chemical Engineering, Rasht Branch, Islamic Azad University, Rasht, Iran
2 - Depatment of Computer Engineering, Rasht Branch, Islamic Azad University, Rasht, Iran
3 - Department of Chemistry and Chemical Engineering, Rasht Branch, Islamic Azad University, Rasht, Iran
4 - Department of Chemistry and Chemical Engineering, Rasht Branch, Islamic Azad University, Rasht, Iran

تاريخ الإرسال : 22 الثلاثاء , جمادى الثانية, 1443 تاريخ التأكيد : 22 الإثنين , رجب, 1444 تاريخ الإصدار : 28 الثلاثاء , رجب, 1443

الکلمات المفتاحية: Covid-19, Autodock-vina, Molecular dynamics simulation, Molecular docking, Gromacs,

ملخص المقالة :

In this manuscript; Molecular dynamics simulation was tested on COVID -19 main protease (PDB: 6LU7) with the docking studies have been employed using autodock-vina-1.1.2-4 and autodock- mgltools-1.5.6 (flex) programs to evaluate the interactions. HIV-1 Protease is a prerequisite for viral replication. In this manuscript; Molecular dynamics simulation was tested on COVID -19 main protease (PDB: 6LU7) with the docking studies have been employed using autodock-vina-1.1.2-4 and autodock- mgltools-1.5.6 (flex) programs to evaluate the interactions. Regular and Flexible docking approaches were run. Molecular dynamics simulation was tested on COVID -19 main protease (PDB: 6LU7) with molecule 7. Drug-likeness descriptors of compounds such as logP (partition coefficient), H-Bond Acceptor (HBA), H-Bond Donor (HBD), number of Rotable Bond (nRB), and nHB calculated by DruLiTo. In the molecular docking study, the maximum binding affinity of -5.9 kcal/mol was obtained between each of COVID -19 main protease (PDB: 6LU7) enzyme systems and the geometric-optimized molecules, representing a strong interaction. The reference molecule PRD_002214 of Mpro forms four hydrogen bonds with Glu 166, Phe 140, Gln 189, His 163, and some hydrophobic bonds. In this study, molecules 7 (Amprenavir) and 15 were presented as the most stable ones that may be introduced for further investigations, including clinical experiments.

المصادر:

 

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