Glycoside-based niosomal nanocarrier for enhanced in-vivo performance of Cefixime
المؤلف | Imran, Muhammad |
المؤلف | Shah, Muhammad Raza |
المؤلف | Ullah, Farhat |
المؤلف | Ullah, Shafi |
المؤلف | Elhissi, Abdelbary M. A. |
المؤلف | Nawaz, Waqas |
المؤلف | Ahmad, Farid |
المؤلف | Sadiq, Abdul |
المؤلف | Ali, Imdad |
تاريخ الإتاحة | 2021-09-01T10:03:32Z |
تاريخ النشر | 2016 |
اسم المنشور | International Journal of Pharmaceutics |
المصدر | Scopus |
الملخص | This study aimed to evaluate the potential of a novel glycoside non-ionic surfactant synthesized and characterized in our laboratory for increased oral bioavailability of Cefixime. The surfactant was synthesized by simple etherification of bergenin with bromoundecane and characterized by 1H NMR and mass spectroscopy (MS). Biocompatibility of the surfactant (BRM-BG) was assessed by in-vitro cytotoxicity against NIH/3T3 cells and human blood hemolysis. In-vivo acute toxicity was evaluated in mices. Cefixime loaded BRM-BG niosomes were investigated for drug entrapment efficiency using HPLC and surface morphology and vesicle size by atomic force microscopy (AFM) and dynamic light scattering (DLS). The in-vivo oral bioavailability and pharmacokinetics studies were carried out using rabbits. Cefixime loaded BRM-BG vesicles were spherical in the size range of 178.66 ± 8.17 nm with a polydipersity index (PDI) of 0.20 ± 0.01, offering an entrapment efficiency as high as 78.4 ± 0.83%. When the surfactant was applied on NIH 3T3 tissue culture, as high as 90.77 ± 3.15% and 86.86 ± 3.02%, cell viability at 1000 μg/mL concentration after 24 and 48 h respectively were observed. The surfactant also caused 5.49 ± 1.62% haemolysis and was found to be safe at a dose up to 2000 mg/kg. In-vivo drug plasma concentration (Cmax) was found to be 9.69 ± 1.22 μg/mL, much higher than that resulting from the intake of commercial suspension and capsules. BRM-BG demonstrated to be safe and effective as carrier of Cefixime following oral dosing in rabbits. The BRM-BG surfactant delivery nano-system is relatively safe and in animal models it is an appropriate carrier for Cefixime, offering enhanced bioavailability compared to commercially available formulations of the drug. |
راعي المشروع | Authors are thankful to Higher Education Commission (HEC) , Pakistan, for financial support provided for PhD scholarship of Mr. Muhammad Imran, under indigenous PhD scholarships program (PIN NO: 112-23671-2BM1-136). Authors are also thankful to Mr. Fahad Siddiqui, Manager Department of Bioanalysis, Center for Bioequivalence Studies and Clinical Research (CBSCR), International Center for Chemical and Biological Sciences (ICCBS) University of Karachi, Pakistan, for his help in-vivo studies of this research |
اللغة | en |
الناشر | Elsevier B.V. |
الموضوع | bergenin bromoundecane cefixime glycoside nanocarrier niosome surfactant unclassified drug antiinfective agent benzopyran derivative cefixime drug carrier glycoside liposome surfactant acute toxicity animal cell animal experiment area under the curve Article atomic force microscopy cell viability controlled study drug blood level drug clearance drug delivery system drug formulation embryo etherification experimental rabbit hemolysis high performance liquid chromatography in vivo study male mass spectrometry mouse nonhuman photon correlation spectroscopy priority journal proton nuclear magnetic resonance suspension tissue culture 3T3 cell line animal bioavailability chemistry comparative study female human medicinal chemistry oral drug administration particle size procedures rabbit Administration, Oral Animals Anti-Bacterial Agents Benzopyrans Biological Availability Cefixime Chemistry, Pharmaceutical Drug Carriers Dynamic Light Scattering Female Glycosides Humans Liposomes Male Mice Microscopy, Atomic Force NIH 3T3 Cells Particle Size Rabbits Surface-Active Agents |
النوع | Article |
الصفحات | 122-132 |
رقم العدد | 2-Jan |
رقم المجلد | 505 |
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