一种新三维描述子用于Nevirapine类抗艾滋病药物定量构效关系的研究

运用三维全息原子场作用矢量(3D-HoVAIF)对33个Nevirapine类抗艾滋病药物进行了定量构效关系(QSAR)研究。采用偏最小二乘回归(PLSR)建立定量构效关系模型,同时采用内部及外部双重验证的方法对所得模型稳定性能进行深入分析和检验,所建模型的复相关系数(Rcum2)、留一法(LOO)交互校验(CV)复相关系数(Qcum2)和外部样本校验复相关系数(Qext2)分别为0·835、0·530和0·518。结果表明,3D-HoVAIF能较好表征Nevirapine类抗艾滋病药物分子结构信息,且所建模型具有较好稳定性能和预测能力。     

Physicochemical properties of nevirapine-loaded solid lipid nanoparticles and nanostructured lipid carriers

Solid lipid nanoparticles (SLNs) and nanostructured lipid carriers (NLCs) coated with human serum albumin (HSA) were fabricated for formulating nevirapine (NVP). Here, NLCs contained low-melting-point oleic acid (OA) in the internal lipid phase. The results revealed that the two nanoparticles were uniformly distributed with the average diameter ranging from 145 to 180 nm. The surface HSA neutralized the positive charge of dimethyldioctadecyl ammonium bromide (DODAB) on SLNs and NLCs and reduced their zeta potential. In a fixed ratio of solid lipids, SLNs entrapped more NVP than NLCs. The incorporation of OA also reduced the thermal resistance of NLCs and accelerated the release of NVP from the nanocarriers. When incubated with DODAB-stabilized SLNs, the viability of human brain-microvascular endothelial cells (HBMECs) reduced. However, the surface HSA increased the viability of HBMECs about 10% when the concentration of SLNs was higher than 0.8 mg/mL. HSA-grafted SLNs and NLCs can be effective formulations in the delivery of NVP for viral therapy.     

密度泛函理论研究奈韦拉平结构,芳香性和电荷性质

利用密度泛函理论(DFT)和Hartree-Fock方法,分别在B3LPY/6-31G和HF/6-31G基组水平上优化了奈韦拉平的几何和电子结构.从奈韦拉平的几何结构出发,分析了其稳定性、芳香性和电子结构特性.计算结果表明,C_1点群对称性为基态奈韦拉平结构.对于奈韦拉平,芳香性大小按环4环3环1的顺序依次降低;环1、环3、环4具有芳香性,环2具有反芳香性.氮原子和碳原子形成sp~2杂化,氧原子形成sp杂化.     

Bulk Modification of Carbon Paste Electrode with Bi2O3 Nanoparticles and Its Application as an Electrochemical Sensor for Selective Sensing of AntiHIV Drug Nevirapine

Bi₂O₃ nanoparticles were synthesized by solution combustion method and utilized for fabrication of an electrochemical sensor [carbon paste electrode modified with Bi₂O₃ (CPE‐Bi₂O₃)] for nevirapine (NVP). Electrode materials were characterized by XRD, FTIR, TG‐DTA, AFM and SEM‐EDS methods. CPE‐Bi₂O₃ was electroreduced (Er) in KOH in the potential range of ?1.3–0 V to obtain CPE‐ErBi₂O₃. CPE‐ErBi₂O₃ exhibited electrocatalytic activity towards the oxidation of NVP. Under optimized conditions, linearity between the peak current and NVP concentration was observed in the range of 0.05–50 µM. Further, the sensor was used for the assay of NVP in tablets and biological samples.     

Electrodeposition of Copper Oxide Nanoparticles on Precasted Carbon Nanoparticles Film for Electrochemical Investigation of anti‐HIV Drug Nevirapine

This work describes the development of a novel electrochemical sensor based on electrodeposition of copper oxide nanoparticles onto carbon nanoparticle (CNP) film modified electrode for the analysis of the anti‐HIV drug, nevirapine (NEV). The electrochemical experiments were performed using linear sweep and cyclic voltammetry. Atomic force microscopy was applied for surface characterization of the deposited modifier film (CuO‐CNP) on glassy carbon electrode (GCE). No oxidation peak was observed for NEV on the bare GCE, but both CNP‐GCE and CuO‐CNP‐GCE showed a distinctive anodic response towards NEV with considerable enhancement (276‐fold and 350‐fold, respectively) compared to CuO‐GCE. The mechanism of the electrocatalytic process on the modified electrode surface was investigated by cyclic and linear sweep voltammetry at various potential sweep rates and pHs of the buffer solutions. The modified electrode exhibited linear dynamic range in three concentration intervals (0.1–0.8, 1–10 and 10–100 µM) with a detection limit of 66 nM. The stability, reproducibility, and repetitive usability exhibited by the proposed modified electrode are good enough to make it a suitable sensor for the determination of NEV in real samples with complex matrices such as human blood serum.     

Antiviral drug nevirapine as a template for hydrated imidazoline ring expansion (HIRE): Rapid access to the diarene-fused 1,4,7-triazecine ring system

The tricyclic ring system of the antiviral drug nevirapine has been employed to test the workability of the hydrated imidazoline ring expansion (HIRE) reaction which was previously exemplified for [1.4]oxazepine and [1.4]thiazepine counterparts. The imidazoline nucleus was grafted onto the lactam moiety of nevirapine in two high-yielding steps. Subsequent N-alkylation and the HIRE reaction proceeded as envisioned and delivered rare ring-expanded diarene-fused 1,4,7-triazecines with a diversity of alkyl substituents at the lactam nitrogen atom. These findings extend the scope of the HIRE reaction to the medicinally prominent [1.4]diazepine chemical space.