Abstract
In recent, millions of people are living with the human immunodeficiency virus type 1 (HIV-1), which causes acquired immunodeficiency syndrome. HIV-1 reverse transcriptase (RT) is one of the main viral targets for HIV-1 inhibition. Pyrimidine nucleoside derivative, 3′-azido-3′-deoxythymidine (AZT) is a highly active nucleoside inhibitor of human immunodeficiency virus type 1 (HIV-1) reverse transcriptase (RT). In this work, hydroxyl (-OH) groups of cytidine structure were modified with different aliphatic and aromatic groups to get 5´-O-acyl- and 2´,3´-di-O-acyl derivatives and then employed for molecular modeling, molecular docking, biological prediction, and pharmacological studies. Herein, we relate the optimization of cytidine and its acylated analogues applying density functional theory (DFT) with B3LYP/3-21G level theory to explore their thermochemical and molecular electrostatic potential (MEP) properties. Prediction of activity spectra for substances (PASS) indicated promising antiviral, anti-carcinogenic, and antifungal functionality of these cytidine esters compared to the antibacterial activities. To support this observation, their cytotoxic prediction and molecular docking studies have been performed against HIV-1 reverse transcriptase (RT) (PDB: 3V4I). Most of the molecules studied out here could bind near the crucial catalytic binding site, Tyr181, Ile94, Ile382, Lys374, Val381, Val90, and Tyr34 of the HIV-1 reverse transcriptase (RT), and the molecules were surrounded by other active site residues like Gln332, Trp406, Asn265, Gly93, His96, Pro95, and Thr165. Finally, these novel molecules were analyzed for their pharmacokinetic properties which expressed that the combination of in silico ADMET prediction, toxicity prediction, and drug-likeness had shown a promising result. The study discusses the performance of molecular docking to suggest the novel molecules active against resistance mutants of RT and/or recombinant strains of HIV-1.
Highlights
Nucleoside antibiotics have been under investigation for many years [1]
It was realized that the analyzed cytidine derivatives bound within some of the catalytic binding sites such as Valine (Val35, Val90, Val381, and val179), Tyr181, Tyr144, His96, Pro95, Lys101, Lys172, Ile31, Ile94, Asn135, Gln91, and Gln161 of the human immunodeficiency virus type 1 (HIV-1) reverse transcriptase (RT), which is responsible for which causes acquired immunodeficiency syndrome
Several cytidine derivatives were analyzed in silico for their antimicrobial, physicochemical, molecular docking, pharmacokinetic, and drug-likeness properties
Summary
Some of the most clinically effective antiviral agents currently in use are purine or pyrimidine nucleoside analogs [2]. Alteration of hydroxyl (-OH) group at 3՛ and 5՛ position increases the antimicrobial activity of pyrimidine nucleoside and brings about some potent antimicrobial agents [4, 5]. As a result of screening synthetic compounds for potential antimicrobial activity, a study reported that azidothymidine (AZT) has potent bactericidal in vitro activity against various members of the family Enterobacteriaceae [6]. Azidothymidine (AZT) is one of the most popular nucleoside derivatives (antiviral drug) in which 3՛ hydroxyl (-OH) of thymidine was replaced by an azide group and it’s used worldwide for the treatment of HIV infection [7]
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