Your search keyword '"In vivo pharmacokinetics"' showing total 127 results

1. Design and evaluation of oseltamivir phosphate dual-phase extended-release tablets for the treatment of influenza

Author

Yu, Liping, Huang, Xin, Jiang, Manhua, Guo, Wentao, Li, Xue, Huang, Fangfang, and You, Jinsong

Published

2024

2. A Visual Raman Nano−Delivery System Based on Thiophene Polymer for Microtumor Detection.

Author

Li, Meng, Luo, Aoxiang, Xu, Wei, Wang, Haoze, Qiu, Yuanyuan, Xiao, Zeyu, and Cui, Kai

Subjects

*THIOPHENES, *DRUG delivery systems, *ABSORPTION spectra

Abstract

A visual Raman nano-delivery system (NS) is a widely used technique for the visualization and diagnosis of tumors and various biological processes. Thiophene-based organic polymers exhibit excellent biocompatibility, making them promising candidates for development as a visual Raman NS. However, materials based on thiophene face limitations due to their absorption spectra not matching with NIR (near-infrared) excitation light, which makes it difficult to achieve enhanced Raman properties and also introduces potential fluorescence interference. In this study, we introduce a donor–acceptor (D-A)-structured thiophene-based polymer, PBDB-T. Due to the D-A molecular modulation, PBDB-T exhibits a narrow bandgap of Eg = 2.63 eV and a red-shifted absorption spectrum, with the absorption edge extending into the NIR region. Upon optimal excitation with 785 nm light, it achieves ultra-strong pre-resonant Raman enhancement while avoiding fluorescence interference. As an intrinsically sensitive visual Raman NS for in vivo imaging, the PBDB-T NS enables the diagnosis of microtumor regions with dimensions of 0.5 mm × 0.9 mm, and also successfully diagnoses deeper tumor tissues, with an in vivo circulation half-life of 14.5 h. This research unveils the potential application of PBDB-T as a NIR excited visual Raman NS for microtumor diagnosis, introducing a new platform for the advancement of "Visualized Drug Delivery Systems". Moreover, the aforementioned platform enables the development of a more diverse range of targeted visual drug delivery methods, which can be tailored to specific regions. [ABSTRACT FROM AUTHOR]

Published

2024

3. The Increased Dissolution and Oral Absorption of Itraconazole by Nanocrystals with an Endogenous Small-Molecule Surfactant as a Stabilizer.

Author

Chang, Sheng, Yang, Qiang, Liu, Jiahuan, Yin, Li, Han, Jihong, Zong, Lanlan, and Pu, Xiaohui

Subjects

*ITRACONAZOLE, *DRUG solubility, *HIGH performance liquid chromatography, *TRANSMISSION electron microscopes, *DIFFERENTIAL scanning calorimetry, *CHOLIC acid

Abstract

The aim of this study was to develop cholic-acid-stabilized itraconazole nanosuspensions (ITZ-Nanos) with the objective of enhancing drug dissolution and oral absorption. A laboratory-scale microprecipitation–high-pressure homogenization method was employed for the preparation of the ITZ-Nanos, while dynamic light scattering, transmission electron microscope analysis, X-ray diffraction, differential scanning calorimetry, and high-performance liquid chromatography analysis were utilized to evaluate their physicochemical properties. The absorption and bioavailability of the ITZ-Nanos were assessed using Caco-2 cells and rats, with Sporanox® pellets as a comparison. Prior to lyophilization, the particle size of the ITZ-Nanos measured approximately 225.7 nm. Both X-ray diffraction and differential scanning calorimetry confirmed that the ITZ remained crystalline within the nanocrystals. Compared to the pellets, the ITZ-Nanos exhibited significantly higher levels of supersaturation dissolution and demonstrated enhanced drug uptake by the Caco-2 cells. The AUC(0–t) value for the ITZ-Nanos in rats was 1.33-fold higher than that observed for the pellets. These findings suggest that cholic acid holds promise as a stabilizer for ITZ nanocrystals, as well as potentially other nanocrystals. [ABSTRACT FROM AUTHOR]

Published

2024

4. Paeoniflorin loaded liposomes modified with glycyrrhetinic acid for liver-targeting: preparation, characterization, and pharmacokinetic study.

Author

Yang, Menghuan, Jiang, Gang, Li, Yumeng, Chen, Weidong, Zhang, Shantang, and Wang, Rulin

Subjects

LIPOSOMES, PHARMACOKINETICS, RESPONSE surfaces (Statistics), DRUG delivery systems, TRANSMISSION electron microscopy, THERAPEUTICS

Abstract

To enhance the retention times and therapeutic efficacy of paeoniflorin (PF), a liver-targeted drug delivery system has been developed using glycyrrhetinic acid (GA) as a ligand. The development and optimization of GA-modified PF liposomes (GPLs) have shown promising potential for targeted delivery to the liver, opening up new possibilities for liver disease treatment. This study aimed to identify the best prescriptions using single-factor experiments and response surface methodology. The formulation morphology was determined using transmission electron microscopy. Tissue distribution was observed through in vivo imaging, and pharmacokinetic studies were conducted. The results indicated that GPLs, prepared using the thin film dispersion method and response surface optimization, exhibited well-dispersed and uniformly sized particles. The in vitro release rate of GPLs was slower compared to PF monomers, suggesting a sustained release effect. The liver-targeting ability of GA resulted in stronger fluorescence signals in the liver for targeted liposomes compared to non-targeted liposomes. Furthermore, pharmacokinetic studies demonstrated that GPLs significantly prolonged the residence time of PF in the bloodstream, thereby contributing to prolonged efficacy. These findings suggest that GPLs are more effective than PF monomers in terms of controlling drug release and delivering drugs to specific targets, highlighting the potential of PF as a liver-protective drug. [ABSTRACT FROM AUTHOR]

Published

2024

5. Mixed Pluronic/lecithin micelles formulation for oral bioavailability of candesartan cilexetil drug: in vitro characterization and in vivo pharmacokinetic investigations.

Author

Mahajan, Homraj, Patel, Hemil S., Ray, Debes, Aswal, Vinod K., Sharma, Rakesh K., and Tandel, Hemal

Subjects

CANDESARTAN, LECITHIN, MICELLES, PHARMACOKINETICS, BIOAVAILABILITY, DRUG delivery systems

Abstract

This study aimed to develop a mixed polymeric micelle formulation incorporating candesartan cilexetil (CAND) drug to enhance its oral bioavailability for the better treatment of hypertension. A Box–Behnken design was utilized to optimize the CAND-incorporated mixed polymeric micelles formulation (CAND-PFLC) consisting of Pluronics (P123 and F68) and lecithin (LC). The optimized CAND-PFLC micelles formulation was characterized for size, shape, zeta potential, polydispersity index (PDI), and entrapment efficiency (%EE). An in vitro release study, ex vivo permeability investigation, and an in vivo pharmacokinetic analysis were carried out to evaluate the performance of the formulation. The optimized CAND-PFLC micelles formulation demonstrated a spherical shape, a particle size of 44 ± 2.03 nm, a zeta potential of −7.07 ± 1.39 mV, a PDI of 0.326 ± 0.06, and an entrapment efficiency of 87 ± 3.12%. The formulation exhibited excellent compatibility, better stability, and a noncrystalline nature. An in vitro release study revealed a faster drug release of 7.98% at gastric pH in 2 hrs and 94.45% at intestinal pH within 24 hrs. The ex vivo investigation demonstrated a significantly enhanced permeability of CAND, with 94.86% in the micelle formulation compared to 9.03% of the pure drug. In vivo pharmacokinetic analysis showed a 4.11-fold increase in oral bioavailability of CAND compared to the marketed formulation. The CAND-PFLC mixed micelle formulation demonstrated improved performance compared to pure CAND, indicating its potential as a promising oral drug delivery system for the effective treatment of hypertension. [ABSTRACT FROM AUTHOR]

Published

2024

6. Mannose-Functionalized Isoniazid-Loaded Nanostructured Lipid Carriers for Pulmonary Delivery: In Vitro Prospects and In Vivo Therapeutic Efficacy Assessment.

Author

Ahalwat, Shaveta, Bhatt, Dinesh Chandra, Rohilla, Surbhi, Jogpal, Vikas, Sharma, Kirti, Virmani, Tarun, Kumar, Girish, Alhalmi, Abdulsalam, Alqahtani, Ali S., Noman, Omar M., and Almoiliqy, Marwan

Subjects

*TREATMENT effectiveness, *MULTIDRUG-resistant tuberculosis, *TUBERCULOSIS, *LIPIDS, *ZETA potential, *DRUG efficacy

Abstract

Resistance to isoniazid (INH) is common and increases the possibility of acquiring multidrug-resistant tuberculosis. For this study, isoniazid-loaded nanostructured lipid carriers (INH-NLCs) were developed and effectively functionalized with mannose (Man) to enhance the residence time of the drug within the lungs via specific delivery and increase the therapeutic efficacy of the formulation. The mannose-functionalized isoniazid-loaded nanostructured lipid carrier (Man-INH-NLC) formulation was evaluated with respect to various formulation parameters, namely, encapsulation efficiency (EE), drug loading (DL), average particle size (PS), zeta potential (ZP), polydispersity index (PDI), in vitro drug release (DR), and release kinetics. The in vitro inhalation behavior of the developed formulation after nebulization was investigated using an Andersen cascade impactor via the estimation of the mass median aerosolized diameter (MMAD) and geometric aerodynamic diameter (GAD) and subsequently found to be suitable for effective lung delivery. An in vivo pharmacokinetic study was carried out in a guinea pig animal model, and it was demonstrated that Man-INH-NLC has a longer residence time in the lungs with improved pharmacokinetics when compared with unfunctionalized INH-NLC, indicating the enhanced therapeutic efficacy of the Man-INH-NLC formulation. Histopathological analysis led us to determine that the extent of tissue damage was more severe in the case of the pure drug solution of isoniazid compared to the Man-INH-NLC formulation after nebulization. Thus, the nebulization of Man-INH-NLC was found to be safe, forming a sound basis for enhancing the therapeutic efficacy of the drug for improved management in the treatment of pulmonary tuberculosis. [ABSTRACT FROM AUTHOR]

Published

2023

7. In Vitro Release and In Vivo Pharmacokinetics of Praziquantel Loaded in Different Polymer Particles.

Author

Pereira, Emiliane Daher, da Silva Dutra, Luciana, Paiva, Thamiris Franckini, de Almeida Carvalho, Larissa Leite, Rocha, Helvécio Vinícius Antunes, and Pinto, José Carlos

Subjects

*PRAZIQUANTEL, *ORAL drug administration, *PHARMACOKINETICS, *SCHISTOSOMA mansoni, *SUMATRIPTAN, *NEGLECTED diseases, *ITRACONAZOLE

Abstract

Approximately 1 billion people are affected by neglected diseases around the world. Among these diseases, schistosomiasis constitutes one of the most important public health problems, being caused by Schistosoma mansoni and treated through the oral administration of praziquantel (PZQ). Despite being a common disease in children, the medication is delivered in the form of large, bitter-tasting tablets, which makes it difficult for patients to comply with the treatment. In order to mask the taste of the drug, allow more appropriate doses for children, and enhance the absorption by the body, different polymer matrices based on poly(methyl methacrylate) (PMMA) were developed and used to encapsulate PZQ. Polymer matrices included PMMA nano- and microparticles, PMMA-co-DEAEMA (2-(diethylamino)ethyl methacrylate), and PMMA-co-DMAEMA (2-(dimethylamino)ethyl methacrylate) microparticles. The performances of the drug-loaded particles were characterized in vitro through dissolution tests and in vivo through pharmacokinetic analyses in rats for the first time. The in vitro dissolution studies were carried out in accordance with the Brazilian Pharmacopeia and revealed a good PZQ release profile in an acidic medium for the PMMA-DEAEMA copolymer, reaching values close to 100 % in less than 3 h. The in vivo pharmacokinetic analyses were conducted using free PZQ as the control group that was compared with the investigated matrices. The drug was administered orally at doses of 60 mg/kg, and the PMMA-co-DEAEMA copolymer microparticles were found to be the most efficient release system among the investigated ones, reaching a Cmax value of 1007 ± 83 ng/mL, even higher than that observed for free PZQ, which displayed a Cmax value of 432 ± 98 ng/mL. [ABSTRACT FROM AUTHOR]

Published

2023

8. Characterization of a polychromatic microfocus X-ray fluorescence imaging setup with metallic contrast agents in a microphysiological tumor model

Author

Kunal Kumar, Melanie Fachet, Marwah Al-Maatoq, Amit Chakraborty, Rahul S. Khismatrao, Shreyas V. Oka, Theresa Staufer, Florian Grüner, Thilo Michel, Heike Walles, and Christoph Hoeschen

Subjects

tissue engineering, X-ray fluorescence computed tomography, in vivo pharmacokinetics, in vitro cancer models, nanoparticle contrast agents, molecular imaging, Physics, QC1-999

Abstract

Introduction: Accurate diagnosis and personalized treatments involving site-targeted cancer localization, drug delivery, therapeutic strategy, and disease pathways identification, rely on a precise understanding of biomarker kinetics, drug pharmacokinetics, and mechanistic behaviour of functionalized tracers through in vitro and in vivo studies. X-ray fluorescence (XRF) computed tomography (XFCT) offers a potential alternative to current 3D imaging techniques for spatiotemporal localization of nanoparticle-tracers with high spatial resolution and sensitivity. In this work, the applicability of a benchtop cone-beam system with a polychromatic X-ray source was examined with regard to physical constraints of engineered tissue models.Methods: A tissue engineering approach based on a decellularized scaffold was used to establish a 3D breast cancer model with MDA-MB-231 cells in co-culture with primary human fibroblasts. The 3D breast cancer system, in combination with small-animal-sized phantoms, was used to demonstrate the novel integrated pre-clinical imaging approach to perform in vitro surrogate investigations and non-destructive analysis on biophantoms. These models are adopted to evaluate the functionality and optimize the setup for high-spatial-resolution, fast, and fully-3D quantitative imaging. Polychromatic X-rays from a microfocus source are used for XRF stimulation from conventional Gadolinium (Gd) and nanoparticle-based Molybdenum (MoNPs) contrast agents.Results and Discussion: The intestinal scaffold allowed the invasion of the breast cancer cells over this barrier and therefore provides a valuable tool to study metastasis formation of tumor cells from epithelial origin. The breast cancer model was well suited for the development and validation of the proposed XRF imaging, with spatial resolution under

Published

2023

9. New 5-Aryl-1,3,4-Thiadiazole-Based Anticancer Agents: Design, Synthesis, In Vitro Biological Evaluation and In Vivo Radioactive Tracing Studies.

Author

El-Masry, Rana M., Essa, Basma M., Selim, Adli A., El-Emam, Soad Z., Mohamed, Khaled O., Sakr, Tamer M., Kadry, Hanan H., Taher, Azza T., and Abou-Seri, Sahar M.

Subjects

*THIADIAZOLES, *CELL death, *ANTINEOPLASTIC agents, *CELL cycle, *PYRIDINIUM compounds, *CANCER cells, *CELL analysis

Abstract

A new series of 5-(4-chlorophenyl)-1,3,4-thiadiazole-based compounds featuring pyridinium (3), substituted piperazines (4a–g), benzyl piperidine (4i), and aryl aminothiazoles (5a–e) heterocycles were synthesized. Evaluation of the cytotoxicity potential of the new compounds against MCF-7 and HepG2 cancer cell lines indicated that compounds 4e and 4i displayed the highest activity toward the tested cancer cells. A selectivity study demonstrated the high selective cytotoxicity of 4e and 4i towards cancerous cells over normal mammalian Vero cells. Cell cycle analysis revealed that treatment with either compound 4e or 4i induced cell cycle arrest at the S and G2/M phases in HepG2 and MCF-7 cells, respectively. Moreover, the significant increase in the Bax/Bcl-2 ratio and caspase 9 levels in HepG2 and MCF-7 cells treated with either 4e or 4i indicated that their cytotoxic effect is attributed to the ability to induce apoptotic cell death. Finally, an in vivo radioactive tracing study of compound 4i proved its targeting ability to sarcoma cells in a tumor-bearing mice model. [ABSTRACT FROM AUTHOR]

Published

2022

10. Improved uptake and bioavailability of cinnamaldehyde via solid lipid nanoparticles for oral delivery.

Author

Wu, Long, Meng, Yun, Xu, Yuhang, and Chu, Xiaoqin

Subjects

BIOAVAILABILITY, ORAL drug administration, DIFFERENTIAL scanning calorimetry, NANOPARTICLES, ZETA potential, CAVEOLAE

Abstract

The purpose of this experiment was to explore the effect of Solid lipid nanoparticles (SLNs) on improving the oral absorption and bioavailability of cinnamaldehyde (CA). CA-SLNs were prepared by high-pressure homogenization and characterized by particle size, entrapment efficiency, and morphology, thermal behavior and attenuated total reflection Fourier transform infrared (ATR-FTIR). In vitro characteristics of release, stability experiments, cytotoxicity, uptake and transport across Caco-2 cell monolayer of CA-SLNs were studied as well. In addition, CA-SLNs underwent pharmacokinetic and gastrointestinal mucosal irritation studies in rats. CA-SLNs exhibited a spherical shape with a particle size of 44.57 ± 0.27 nm, zeta potential of −27.66 ± 1.9 mV and entrapment efficiency of 83.63% ± 2.16%. Differential scanning calorimetry (DSC) and ATR-FTIR confirmed that CA was well encapsulated. In vitro release of CA-SLNs displayed that most of the drug (90.77% ± 5%) was released in the phosphate buffer, and only a small amount of drug (18.55% ± 5%) was released in the HCl buffer. CA-SLNs were taken up by an energy-dependent, endocytic mechanism mediated by caveolae mediated endocytosis across Caco-2 cells. The CA permeation through Caco-2 cell was facilitated by CA-SLNs. The outcome of the gastrointestinal irritation test demonstrated that CA-SLNs had no irritation to the rats' intestines. Compared with CA dispersions, incorporation of SLNs increased the oral bioavailability of CA more than 1.69-fold. It was concluded that CA-SLNs improved the absorption across Caco-2 cell model and improved the oral administration bioavailability of CA in rats. [ABSTRACT FROM AUTHOR]

Published

2022

11. Toward Optimized 89 Zr-Immuno-PET: Side-by-Side Comparison of [ 89 Zr]Zr-DFO-, [ 89 Zr]Zr-3,4,3-(LI-1,2-HOPO)- and [ 89 Zr]Zr-DFO*-Cetuximab for Tumor Imaging: Which Chelator Is the Most Suitable?

Author

Damerow, Helen, Cheng, Xia, von Kiedrowski, Valeska, Schirrmacher, Ralf, Wängler, Björn, Fricker, Gert, and Wängler, Carmen

Subjects

*CETUXIMAB, *RADIOCHEMICAL purification, *SPLEEN

Abstract

89Zr represents a highly favorable positron emitter for application in immuno-PET (Positron Emission Tomography) imaging. Clinically, the 89Zr4+ ion is introduced into antibodies by complexation with desferrioxamine B. However, producing complexes of limited kinetic inertness. Therefore, several new chelators for 89Zr introduction have been developed over the last years. Of these, the direct comparison of the most relevant ones for clinical translation, DFO* and 3,4,3-(LI-1,2-HOPO), is still missing. Thus, we directly compared DFO with DFO* and 3,4,3-(LI-1,2-HOPO) immunoconjugates to identify the most suitable agent stable 89Zr-complexation. The chelators were introduced into cetuximab, and an optical analysis method was developed, enabling the efficient quantification of derivatization sites per protein. The cetuximab conjugates were efficiently obtained and radiolabeled with 89Zr at 37 °C within 30 min, giving the [89Zr]Zr-cetuximab derivatives in high radiochemical yields and purities of >99% as well as specific activities of 50 MBq/mg. The immunoreactive fraction of all 89Zr-labeled cetuximab derivatives was determined to be in the range of 86.5–88.1%. In vivo PET imaging and ex vivo biodistribution studies in tumor-bearing animals revealed a comparable and significantly higher kinetic inertness for both [89Zr]Zr-3,4,3-(LI-1,2-HOPO)-cetuximab and [89Zr]Zr-DFO*-cetuximab, compared to [89Zr]Zr-DFO-cetuximab. Of these, [89Zr]Zr-DFO*-cetuximab showed a considerably more favorable pharmacokinetic profile with significantly lower liver and spleen retention than [89Zr]Zr-3,4,3-(LI-1,2-HOPO)-cetuximab. Since [89Zr]Zr-DFO* demonstrates a very high kinetic inertness, paired with a highly favorable pharmacokinetic profile of the resulting antibody conjugate, DFO* currently represents the most suitable chelator candidate for stable 89Zr-radiolabeling of antibodies and clinical translation. [ABSTRACT FROM AUTHOR]

Published

2022

12. Hemocompatible and biocompatible hybrid nanocarriers for enhanced oral bioavailability of paclitaxel: in vivo evaluation.

Author

Majeed, Asma, Akhtar, Muhammad, Khan, Mehran, Ijaz, Muhammad, Hussain, Pakeeza, Maqbool, Tahir, and Hanan, Hanasul

Subjects

*ORAL drug administration, *CELL anatomy, *X-ray diffraction, *ANTINEOPLASTIC agents, *SURFACE morphology

Abstract

Oral administration of BCS class IV anticancer agents has always remained challenging and frequently results in poor oral bioavailability. The goal of the current study was to develop hybrid nanoparticles (HNPs) employing cholesterol and poloxamer-407 to boost paclitaxel's (PTX) oral bioavailability. A series of HNPs with different cholesterol and poloxamer-407 ratios were developed utilizing a single-step nanoprecipitation technique. The PTX loaded HNPs were characterized systematically via particle size, zeta potential, polydispersity index, surface morphology, in vitro drug release, FTIR, DSC, XRD, acute oral toxicity analysis, hemolysis evaluation, accelerated stability studies, and in vivo pharmacokinetic analysis. The HNPs were found within the range of 106.6±55.60 – 244.5±88.24 nm diameter with the polydispersity index ranging from 0.20±0.03 – 0.51±0.11. SEM confirmed circular, nonporous, and smooth surfaces of HNPs. PTX loaded HNPs exhibited controlled release profile. The compatibility between the components of formulation, thermal stability, and amorphous nature of HNPs were confirmed by FTIR, DSC, and XRD, respectively. Acute oral toxicity analysis revealed that developed system have no deleterious effects on the animals' cellular structures. HNPs demonstrated notable cytotoxic effects and were hemocompatible at relatively higher concentrations. In vivo pharmacokinetic profile (AUC 0-∞ , AUMC 0-∞ , t 1/2, and MRT 0-∞) of the PTX loaded HNPs was improved as compared to pure PTX. It is concluded from our findings that the developed HNPs are hemocompatible, biocompatible and have significantly enhanced the oral bioavailability of PTX. [Display omitted] • Development of a novel core shell type, PTX loaded Cs-Chol HNPs system. • Aqueous solubility of PTX was significantly enhanced by HNPs. • PTX loaded HNPs exhibited a controlled release profile. • Cs-Chol HNPs are stable, hemocompatible and biocompatible. • PTX loaded Cs-Chol HNPs are safe for oral delivery. [ABSTRACT FROM AUTHOR]

Published

2024

13. Towards wearable and implantable continuous drug monitoring: A review

Author

Sumin Bian, Bowen Zhu, Guoguang Rong, and Mohamad Sawan

Subjects

Continuous drug monitoring, Wearable biosensors, Implantable biosensors, In vivo pharmacokinetics, Electrochemical aptamer-based sensors, Individualised therapy, Therapeutics. Pharmacology, RM1-950

Abstract

Continuous drug monitoring is a promising alternative to current therapeutic drug monitoring strategies and has a strong potential to reshape our understanding of pharmacokinetic variability and to improve individualised therapy. This review highlights recent advances in biosensing technologies that support continuous drug monitoring in real time. We focus primarily on aptamer-based biosensors, wearable and implantable devices. Emphasis is given to the approaches employed in constructing biosensors. We pay attention to sensors’ biocompatibility, calibration performance, long-term characteristics stability and measurement quality. Last, we discuss the current challenges and issues to be addressed in continuous drug monitoring to make it a promising, future tool for individualised therapy. The ongoing efforts are expected to result in fully integrated implantable drug biosensing technology. Thus, we may anticipate an era of advanced healthcare in which wearable and implantable biochips will automatically adjust drug dosing in response to patient health conditions, thus enabling the management of diseases and enhancing individualised therapy.

Published

2021

14. Pharmacokinetics and the Dermal Absorption of Bromochlorophene, a Cosmetic Preservative Ingredient, in Rats.

Author

Lee, Yong-Jae, Kim, Hyang-Yeon, Pham, Quynh-Lien, Lee, Jung-Dae, and Kim, Kyu-Bong

Subjects

SKIN absorption, SKIN permeability, PHARMACOKINETICS, LIQUID chromatography-mass spectrometry, RATS

Abstract

The cosmetic industry has flourished in recent years. Accordingly, the safety of cosmetic ingredients is increasing. Bromochlorophene (BCP) is a commonly used cosmetic preservative. To evaluate the effects of BCP exposure, in vitro dermal absorption and in vivo pharmacokinetic (PK) studies were conducted using gel and cream formulations. The Franz diffusion cell system and rat dorsal skin were used for tests according to the Korea Ministry of Food and Drug Safety guidelines for in vitro skin absorption methods. After the dermal application (1.13 mg/cm2) of BCP in the gel and cream formulations, liquid chromatography–mass spectrometry (LC–MS/MS) was used to evaluate the amount of BCP that remained unabsorbed on the skin (WASH), and that was present in the receptor fluid (RF), stratum corneum (SC), and (epi)dermis (SKIN). The total dermal absorption rate of BCP was 7.42 ± 0.74% for the gel formulation and 1.5 ± 0.9% for the cream formulation. Total recovery in an in vitro dermal absorption study was 109.12 ± 8.79% and 105.43 ± 11.07% for the gel and cream formulations, respectively. In vivo PK and dermal absorption studies of BCP were performed following the Organization for Economic Cooperation and Development guidelines 417 and 427, respectively. When intravenous (i.v.) pharmacokinetics was performed, BCP was dissolved in glycerol formal and injected into the tail vein (n = 3) of the rats at doses of 1 and 0.2 mg/kg. Dermal PK parameters were estimated by the application of the gel and cream formulations (2.34 mg/kg of BCP as an active ingredient) to the dorsal skin of the rats. Intravenous and dermal PK parameters were analyzed using a non-compartmental method. The dermal bioavailability of BCP was determined as 12.20 ± 2.63% and 4.65 ± 0.60% for the gel and cream formulations, respectively. The representative dermal absorption of BCP was evaluated to be 12.20 ± 2.63% based on the results of the in vivo PK study. [ABSTRACT FROM AUTHOR]

Published

2022

15. Investigation of pre-clinical pharmacokinetic parameters of atovaquone nanosuspension prepared using a pH-based precipitation method and its pharmacodynamic properties in a novel artemisinin combination

Author

Harsha Kathpalia, Siddhesh Juvekar, Krishnapriya Mohanraj, Mrunal Apsingekar, and Supriya Shidhaye

Subjects

Triple drug artemisinin combination therapy, Atovaquone, Nanosuspension, Suppressive, Curative, In vivo pharmacokinetics, Microbiology, QR1-502

Abstract

Objectives: Recently, a growing resistance to antimalarial drugs such as chloroquine, sulfadoxine–pyrimethamine, artemisinin derivatives and mefloquine has been observed. The pharmacokinetic limitation of the current therapy and multi-drug resistance has resulted in an urgent need to study the new antimalarial combinations with existing drugs. This study investigated the activity of a novel triple combination of atovaquone (nanosized)–proguanil–artesunate as an alternative artemisinin combination therapy. Atovaquone in this combination was formulated as a freeze–dried nanosuspension and its pharmacokinetic parameters were also evaluated. Methods: The suppressive and curative effect of atovaquone nanosuspension, proguanil, and artesunate were studied in a murine model. The in vivo pharmacokinetics of the newly developed atovaquone nanosuspension with particle size less than 200 nm was investigated. Results: Prophylactic efficacy of atovaquone nanosuspension alone at 1/80th the therapeutic dose was proven. In the curative test, atovaquone nanosuspension and proguanil at 1/10th the therapeutic dose was the minimum effective dose that resulted in complete cure of parasitaemia. As a triple combination, atovaquone nanosuspension in combination with proguanil at 1/80th the therapeutic dose of each and 1/5th the therapeutic dose of artesunate resulted in a complete cure. The in vivo pharmacokinetics of the nanosuspension showed a significant (three times) reduction in Tmax value and the area under the curve of the nanosuspension was 1.9 times greater as compared with the plain suspension. Conclusions: The potential of the synergistic combination of atovaquone nanosuspension–proguanil–artesunate in curing the multi-drug resistant malarial infection at reduced doses of all three drugs could be a solution to pill burden observed with the current therapy.

Published

2020

16. Pharmacokinetics and the Dermal Absorption of Bromochlorophene, a Cosmetic Preservative Ingredient, in Rats

Author

Yong-Jae Lee, Hyang-Yeon Kim, Quynh-Lien Pham, Jung-Dae Lee, and Kyu-Bong Kim

Subjects

bromochlorophene, in vitro dermal absorption, in vivo pharmacokinetics, Chemical technology, TP1-1185

Abstract

The cosmetic industry has flourished in recent years. Accordingly, the safety of cosmetic ingredients is increasing. Bromochlorophene (BCP) is a commonly used cosmetic preservative. To evaluate the effects of BCP exposure, in vitro dermal absorption and in vivo pharmacokinetic (PK) studies were conducted using gel and cream formulations. The Franz diffusion cell system and rat dorsal skin were used for tests according to the Korea Ministry of Food and Drug Safety guidelines for in vitro skin absorption methods. After the dermal application (1.13 mg/cm2) of BCP in the gel and cream formulations, liquid chromatography–mass spectrometry (LC–MS/MS) was used to evaluate the amount of BCP that remained unabsorbed on the skin (WASH), and that was present in the receptor fluid (RF), stratum corneum (SC), and (epi)dermis (SKIN). The total dermal absorption rate of BCP was 7.42 ± 0.74% for the gel formulation and 1.5 ± 0.9% for the cream formulation. Total recovery in an in vitro dermal absorption study was 109.12 ± 8.79% and 105.43 ± 11.07% for the gel and cream formulations, respectively. In vivo PK and dermal absorption studies of BCP were performed following the Organization for Economic Cooperation and Development guidelines 417 and 427, respectively. When intravenous (i.v.) pharmacokinetics was performed, BCP was dissolved in glycerol formal and injected into the tail vein (n = 3) of the rats at doses of 1 and 0.2 mg/kg. Dermal PK parameters were estimated by the application of the gel and cream formulations (2.34 mg/kg of BCP as an active ingredient) to the dorsal skin of the rats. Intravenous and dermal PK parameters were analyzed using a non-compartmental method. The dermal bioavailability of BCP was determined as 12.20 ± 2.63% and 4.65 ± 0.60% for the gel and cream formulations, respectively. The representative dermal absorption of BCP was evaluated to be 12.20 ± 2.63% based on the results of the in vivo PK study.

Published

2022

17. Towards wearable and implantable continuous drug monitoring: A review.

Author

Bian, Sumin, Zhu, Bowen, Rong, Guoguang, and Sawan, Mohamad

Subjects

DRUG monitoring, DISEASE management, ARTIFICIAL implants, CLINICAL trials monitoring

Abstract

Continuous drug monitoring is a promising alternative to current therapeutic drug monitoring strategies and has a strong potential to reshape our understanding of pharmacokinetic variability and to improve individualised therapy. This review highlights recent advances in biosensing technologies that support continuous drug monitoring in real time. We focus primarily on aptamer-based biosensors, wearable and implantable devices. Emphasis is given to the approaches employed in constructing biosensors. We pay attention to sensors' biocompatibility, calibration performance, long-term characteristics stability and measurement quality. Last, we discuss the current challenges and issues to be addressed in continuous drug monitoring to make it a promising, future tool for individualised therapy. The ongoing efforts are expected to result in fully integrated implantable drug biosensing technology. Thus, we may anticipate an era of advanced healthcare in which wearable and implantable biochips will automatically adjust drug dosing in response to patient health conditions, thus enabling the management of diseases and enhancing individualised therapy. Image 1 • The review summarizes biosensing technologies in real-time continuous drug monitoring. • The review focuses on aptamer-based sensors, wearables and implantable sensors. • The review summaries challenges and issues to address in continuous drug monitoring. [ABSTRACT FROM AUTHOR]

Published

2021

18. Toward simplified oral lipid-based drug delivery using mono-/di-glycerides as single component excipients.

Author

Ilie, Alexandra-Roxana, Griffin, Brendan T., Vertzoni, Maria, Kuentz, Martin, Cuyckens, Filip, Wuyts, Koen, Kolakovic, Ruzica, and Holm, René

Subjects

DRUG delivery systems, DRUG abuse, PHARMACOKINETICS, UNCERTAINTY

Abstract

This study aimed to systematically explore compositional effects for a series of lipid systems, on the in vitro drug solubilization and in vivo bioavailability of three poorly water-soluble drugs with different physico-chemical properties. While many lipid-based drug products have successfully reached the market, there is still a level of uncertainty on the design guidelines for such drug products with limited understanding on the influence of composition on in vitro and in vivo performance. Lipid-based drug delivery systems were prepared using either single excipient systems based on partially digested triglycerides (i.e. mono- and/or di-glycerides) or increasingly complex systems by incorporating surfactants and/or triglycerides. These lipid systems were evaluated for both in vitro and in vivo behavior. Results indicated that simple single component long chain lipid systems are more beneficial for the absorption of the weak acid celecoxib and the weak base cinnarizine compared to equivalent single component medium chain lipid systems. Similarly, a two-component system produced by incorporating small amount of hydrophilic surfactant yields similar overall pharmacokinetic effects. The lipid drug delivery systems based on medium chain lipid excipients improved the in vivo exposure of the neutral drug JNJ-2A. The higher in vivo bioavailability of long chain lipid systems compared to medium chain lipid systems was in agreement with in vitro dilution and dispersion studies for celecoxib and cinnarizine. The present study demonstrated the benefits of using mono-/di-glycerides as single component excipients in LBDDS to streamline formulation screening and improve oral bioavailability for the three tested poorly water-soluble drugs. [ABSTRACT FROM AUTHOR]

Published

2020

19. Synthesis and characterization of nanoemulsion-mediated core crosslinked nanoparticles, and in vivo pharmacokinetics depending on the structural characteristics.

Author

Matsuno, Jun, Kanamaru, Takuma, Arai, Koichi, Tanaka, Rena, Lee, Ji Ha, Takahashi, Rintaro, Sakurai, Kazuo, and Fujii, Shota

Subjects

*NANOPARTICLES, *SMALL-angle neutron scattering, *SMALL-angle scattering, *PHARMACOKINETICS, *NEUTRON scattering, *DRUG carriers

Abstract

For designing nanoparticles as drug carriers, a covalently crosslinked structure is necessary for the structural stability in vivo. In this study, we prepared core crosslinked nanoparticles through the formation of nanoemulsions stabilized by poly(ethylene glycol) (PEG)-bearing surfactants. The structural characteristics of these particles were carefully evaluated using small-angle scattering techniques including dynamic, static, X-ray, and neutron scattering. The particles demonstrated high stability even in vivo , with the suppression of premature drug release owing to the crosslinked structure. Interestingly, the ability to retain encapsulated molecules was dependent on the molecular weight of PEG in vivo , presumably due to the difference in the crowding density of PEG chains at the outermost surface. This suggests that conferring structural stability via a core crosslinked structure is surely important, but we also need to consider controlling the crowding density of the hydrophilic polymer chains in the particle shell when designing drug carriers. Unlabelled Image • Synthesizing core crosslinked nanoparticles via the formation of nanoemulsions. • Precise structural characterization of nanoparticles using small angle scattering. • Correlation of the polymer density on nanoparticles with the in vivo stability. [ABSTRACT FROM AUTHOR]

Published

2020

20. Physicochemical and Pharmacokinetic Evaluation of Spray-Dried Coformulation of Salvia miltiorrhiza Polyphenolic Acid and L-Leucine with Improved Bioavailability.

Author

Lu, Peng, Xing, Yue, Peng, Hui, Liu, Zhidong, Zhou, Qi (Tony), Xue, Zhifeng, Ma, Zhe, Kebebe, Dereje, Zhang, Bing, and Liu, Hongfei

Subjects

*SALVIA miltiorrhiza, *PARTICLE size distribution, *BIOAVAILABILITY, *SPRAY drying, *DRUG delivery systems

Abstract

Background:Salvia miltiorrhiza polyphenolic acid (SMPA) is effective in the treatment of cardiovascular diseases and currently it is administered orally or intravenously. However, SMPA is poorly absorbed orally and quickly eliminated in vivo. A long-term frequent intravenous administration leads to poor patient compliance. Therefore, it is urgently demanded to find a new alternative route of noninjection drug delivery system for SMPA. Methods: Two dry powder inhalation (DPI) formulations of spray-dried SMPA formulation (P1) and spray-dried SMPA–L-leucine formulation (P2) were prepared by spray drying method and their physicochemical properties were assessed by thermogravimetric analysis, X-ray diffraction, scanning electron microscopy, particle size distribution analysis, and in vitro aerodynamic analysis. Moreover, In vitro cytotoxicity of SMPA and P2 was conducted with NR8383 cells. In vivo pharmacokinetics were carried out by Penn-Century endotracheal intubation technique to deliver P2 to the lungs of rats. Results and Conclusions: The moisture content of P1 and P2 were 5.81% ± 0.005%, and 4.08% ± 0.002%, respectively. P1 and P2 were in an amorphous state. Moreover, P1 had slightly corrugated surfaces, whereas P2 exhibited severely corrugated surfaces with invagination due to the presence of L-leucine. In addition, there were more hollow particles with smooth surface in P1 than that in P2. Compared with P1, P2 has shown optimal physical particle size and aerosolization behavior with D (v, 50) of 2.64 ± 0.01 μm and fine particle fraction of 37.55% ± 2.63%. The findings of in vitro cytotoxicity showed that P2 did not inhibit cell viability and could be safe for pulmonary administration. The absolute bioavailability of salvianolic acid B (Sal B) for pulmonary administration was 19.15% ± 7.44%, which is significantly higher than the oral bioavailability of Sal B (<5.56%). In this study, we have shown the feasibleness of pulmonary administration of SMPA in the form of DPIs for systemic delivery to treat cardiovascular diseases. [ABSTRACT FROM AUTHOR]

Published

2020

21. Evaluation of the Pharmacokinetics of the Pancreastatin Inhibitor PSTi8 Peptide in Rats: Integration of In Vitro and In Vivo Findings

Author

Guru R. Valicherla, Roshan A. Katekar, Shailesh Dadge, Mohammed Riyazuddin, Anees A. Syed, Sandeep K. Singh, Athar Husain, Muhammad Wahajuddin, and Jiaur R. Gayen

Subjects

antidiabetic drugs, PSTi8, in vitro ADME, in vivo pharmacokinetics, bioavailability, Organic chemistry, QD241-441

Abstract

PSTi8 is a pancreastatin inhibitory peptide that is effective in the treatment of diabetic models. This study investigates the pharmacokinetic (PK) properties of PSTi8 in Sprague Dawley rats, for the first time. In vitro and in vivo PK studies were performed to evaluate the solubility, stability in plasma and liver microsomes, plasma protein binding, blood–plasma partitioning, bioavailability, dose proportionality, and gender difference in PK. Samples were analyzed using the validated LC-MS/MS method. The solubility of PSTi8 was found to be 9.30 and 25.75 mg/mL in simulated gastric and intestinal fluids, respectively. The protein binding of PSTi8 was estimated as >69% in rat plasma. PSTi8 showed high stability in rat plasma and liver microsomes and the blood–plasma partitioning was >2. The bioavailability of PSTi8 after intraperitoneal and subcutaneous administration was found to be 95.00 ± 12.15 and 78.47 ± 17.72%, respectively, in rats. PSTi8 showed non-linear PK in dose proportionality studies, and has no gender difference in the PK behavior in rats. The high bioavailability of PSTi8 can be due to high water solubility and plasma protein binding, low clearance and volume of distribution. Our in vitro and in vivo findings support the development of PSTi8 as an antidiabetic agent.

Published

2022

22. Cholesterol-Based Nanovesicles Enhance the In Vitro Cytotoxicity, Ex Vivo Intestinal Absorption, and In Vivo Bioavailability of Flutamide

Author

Mohamed A. Ali, Magdy I. Mohamed, Mohamed A. Megahed, Tamer M. Abdelghany, and Khalid M. El-Say

Subjects

Draper–Lin small composite design, ex vivo intestinal permeation, flutamide, in vitro cytotoxicity, optimization, in vivo pharmacokinetics, Pharmacy and materia medica, RS1-441

Abstract

Critical adverse effects and frequent administration, three times per day, limit the use of flutamide (FLT) as a chemotherapeutic agent in the treatment of prostate cancer. Therefore, our research aimed to develop new cholesterol-based nanovesicles for delivering FLT to malignant cells in an endeavor to maximize its therapeutic efficacy and minimize undesired adverse effects. Draper–Lin small composite design was used to optimize the critical quality attributes of FLT-loaded niosomes and ensure the desired product quality. The influence of the selected four independent variables on mean particle size (Y1), zeta potential (Y2), drug entrapment efficiency (Y3), and the cumulative drug release after 24 h (Y4) was examined. The optimized nanovesicles were assessed for their in vitro cytotoxicity, ex-vivo absorption via freshly excised rabbit intestine as well as in vivo pharmacokinetics on male rats. TEM confirmed nanovescicles’ spherical shape with bilayer structure. Values of dependent variables were 748.6 nm, −48.60 mV, 72.8% and 72.2% for Y1, Y2, Y3 and Y4, respectively. The optimized FLT-loaded niosomes exerted high cytotoxic efficacy against human prostate cancer cell line (PC-3) with an IC50 value of 0.64 ± 0.04 µg/mL whilst, it was 1.88 ± 0.16 µg/mL for free FLT. Moreover, the IC50 values on breast cancer cell line (MCF-7) were 0.27 ± 0.07 µg/mL and 4.07 ± 0.74 µg/mL for FLT-loaded niosomes and free FLT, respectively. The permeation of the optimized FLT-loaded niosomes through the rabbit intestine showed an enhancement ratio of about 1.5 times that of the free FLT suspension. In vivo pharmacokinetic study displayed an improvement in oral bioavailability of the optimized niosomal formulation with AUC and Cmax values of 741.583 ± 33.557 μg/mL × min and 6.950 ± 0.45 μg/mL compared to 364.536 ± 45.215 μg/mL × min and 2.650 ± 0.55 μg/mL for the oral FLT suspension. With these promising findings, we conclude that encapsulation of FLT in cholesterol-loaded nanovesicles enhanced its anticancer activity and oral bioavailability which endorse its use in the management of prostate cancer.

Published

2021

23. Improved oral bioavailability of the anticancer drug catechin using chitosomes: Design, in-vitro appraisal and in-vivo studies.

Author

Ezzat, Hadeer M., Elnaggar, Yosra S.R., and Abdallah, Ossama Y.

Subjects

*BIOAVAILABILITY, *DRUG bioavailability, *EPICATECHIN, *CATECHIN, *DRUG side effects, *ANTINEOPLASTIC agents, *DRUG abuse, *PATIENT compliance

Abstract

Catechin hydrate is a phytopharmaceutical with promising anticancer effects but poor bioavailability. This study aimed to elaborate catechin loaded chitosan-tethered liposomes (chitosomes) to enhance catechin oral bioavailability. Nanocarriers were optimized via ethanol injection method followed by physicochemical, ex vivo and biological appraisal in male Wistar albino rats. Results demonstrated that chitosomes possessed excellent nanosize of 137 nm, monodispersity (PDI < 0.2) and high Zeta potential of +36.8 mV. Additionally, chitosomes showed significant improvement in digestive stability against bile salt with enhanced ex-vivo intestinal permeation. Pharmacokinetic studies revealed the significant potential of chitosomes to enhance catechin bioavailability (AUC, Cmax) and sustain its effect (Tmax). In conclusion, elaborated chitosomes are promising nanoplatforms to enhance catechin oral efficacy with lower dose, side effects, administration frequency and higher patient compliance. [ABSTRACT FROM AUTHOR]

Published

2019

24. Tailoring novel soft nano-vesicles 'Flexosomes' for enhanced transdermal drug delivery: Optimization, characterization and comprehensive ex vivo – in vivo evaluation.

Author

Abdel-Messih, Hanaa A., Ishak, Rania A.H., Geneidi, Ahmed S., and Mansour, Samar

Subjects

*POLYMERSOMES, *HYDROPHILIC interactions, *TRANSDERMAL medication

Abstract

Graphical abstract Abstract The transdermal route is a convenient non-invasive way for drug delivery, however, the hydrophobic compact nature of stratum corneum (SC) forms an obstacle hindering the diffusion of drugs particularly hydrophilic ones. Hence, the purpose of this study was to develop novel soft nano-vesicles, entitled Flexosomes, amalgamating two penetration enhancers, ethanol and one edge activator (EA) from various types and different hydrophilic-lipophilic balances. The tailored vesicles were loaded with tropisetron hydrochloride (TRO), a potent highly-soluble anti-emetic, and compared with ethosomes. Aiming to preclude the formation of rigid non-deformable mixed micelles, all critical parameters; EA type, phosphatidylcholine-to-EA molar ratio, and cholesterol concentration, were optimized proving their influences on vesicle-to-micelle transitions. The prepared formulations were characterized in terms of visual inspection, particle size, polydispersity, zeta potential, turbidity measurements, entrapment efficiency, and vesicle morphology. The permeation mechanisms were assessed by differential scanning calorimetry on isolated SC. The modified vesicles, based on ethanol and either vitamin E or PEGylated castor oil derivatives exhibited the highest transdermal fluxes confirmed by a deeply tracking to dermis using confocal laser microscopy. Both vesicles demonstrated higher bioavailability relative to ethosomes, topical and oral aqueous solutions. The findings endorsed the effectiveness of tailored nano-vesicles in boosting TRO skin transport suggesting their applicability with various drug entities for enhanced transdermal delivery. [ABSTRACT FROM AUTHOR]

Published

2019

25. Study on Formulation, in vivo Exposure, and Passive Targeting of Intravenous Itraconazole Nanosuspensions

Author

Qi Yuan, Yanling Wang, Rufeng Song, Xianqiao Hou, Keke Yu, Jiaojiao Zheng, Juanmei Zhang, Xiaohui Pu, Jihong Han, and Lanlan Zong

Subjects

itraconazole nanosuspension, process optimization, in vivo pharmacokinetics, tissue distribution, passive targeting, Therapeutics. Pharmacology, RM1-950

Abstract

The pharmacokinetic profile of a drug can be different when delivered as a nanosuspension compared with a true solution, which may in turn affect the therapeutic effect of the drug. The goal of this study was to prepare itraconazole nanosuspensions (ITZ-Nanos) stabilized by an amphipathic polymer, polyethylene glycol-poly (benzyl aspartic acid ester) (PEG-PBLA), by the precipitation-homogenization, and study the pharmacokinetic profile of the ITZ-Nanos. The particle size and morphology of nanosuspensions were determined by Zetasizer and field emission scanning electron microscope (SEM), respectively. The dissolution profile was evaluated using a paddle method according to Chinese Pharmacopoeia 2015. The level of ITZ in plasma and tissues was measured by a HPLC method. The optimized ITZ-Nanos had an average particle size of 268.1 ± 6.5 nm and the particles were in a rectangular form. The dissolution profile of ITZ-Nanos was similar to that of commercial ITZ injections, with nearly 90% ITZ released in the first 5 min. The ITZ-Nanos displayed different pharmacokinetic properties compared with the commercial ITZ injections, including a decreased initial drug concentration, increased plasma half-life and mean residence time (MRT), and increased concentration in the liver, lung, and spleen. The ITZ-Nanos can change the in vivo distribution of ITZ and result in passive targeting to the organs with mononuclear phagocyte systems (MPS).

Published

2019

26. Application of Nanopharmaceutics for Flibanserin Brain Delivery Augmentation Via the Nasal Route

Author

Osama A. A. Ahmed, Usama A. Fahmy, Shaimaa M. Badr-Eldin, Hibah M. Aldawsari, Zuhier A. Awan, Hani Z. Asfour, Ahmed K. Kammoun, Giuseppe Caruso, Filippo Caraci, Anas Alfarsi, Raniyah A. Al-Ghamdi, Rawan A. Al-Ghamdi, and Nabil A. Alhakamy

Subjects

flibanserin, transfersomes, hydrogel, ex vivo permeation, in vivo pharmacokinetics, Chemistry, QD1-999

Abstract

Flibanserin (FLB) is a nonhormonal medicine approved by the Food and Drug Administration (FDA) to treat the hypoactive sexual appetite disorder in females. However, the peroral administration of the medicine is greatly affected by its poor bioavailability as a result of its extensive first-pass effect and poor solubility. Aiming at circumventing these drawbacks, this work involves the formulation of optimized FLB transfersome (TRF) loaded intranasal hydrogel. Box–Behnken design was utilized for the improvement of FLB TRFs with decreased size. The FLB-to-phospholipid molar ratio, the edge activator hydrophilic lipophilic balance, and the pH of the hydration medium all exhibited significant effects on the TRF size. The optimized/developed TRFs were unilamellar in shape. Hydroxypropyl methyl cellulose based hydrogel filled with the optimized FLB TRFs exhibited an improved ex vivo permeation when compared with the control FLB-loaded hydrogel. In addition, the optimized TRF-loaded hydrogel exhibited higher bioavailability and enhanced brain delivery relative to the control hydrogel following intranasal administration in Wistar rats. The results foreshadow the possible potential application of the proposed intranasal optimized FLB-TRF-loaded hydrogel to increase the bioavailability and nose-to-brain delivery of the drug.

Published

2020

27. Study on Formulation, in vivo Exposure, and Passive Targeting of Intravenous Itraconazole Nanosuspensions.

Author

Yuan, Qi, Wang, Yanling, Song, Rufeng, Hou, Xianqiao, Yu, Keke, Zheng, Jiaojiao, Zhang, Juanmei, Pu, Xiaohui, Han, Jihong, and Zong, Lanlan

Subjects

ITRACONAZOLE, FIELD emission electron microscopes, RETICULO-endothelial system, PHARMACOLOGY

Abstract

The pharmacokinetic profile of a drug can be different when delivered as a nanosuspension compared with a true solution, which may in turn affect the therapeutic effect of the drug. The goal of this study was to prepare itraconazole nanosuspensions (ITZ-Nanos) stabilized by an amphipathic polymer, polyethylene glycol-poly (benzyl aspartic acid ester) (PEG-PBLA), by the precipitation-homogenization, and study the pharmacokinetic profile of the ITZ-Nanos. The particle size and morphology of nanosuspensions were determined by Zetasizer and field emission scanning electron microscope (SEM), respectively. The dissolution profile was evaluated using a paddle method according to Chinese Pharmacopoeia 2015. The level of ITZ in plasma and tissues was measured by a HPLC method. The optimized ITZ-Nanos had an average particle size of 268.1 ± 6.5 nm and the particles were in a rectangular form. The dissolution profile of ITZ-Nanos was similar to that of commercial ITZ injections, with nearly 90% ITZ released in the first 5 min. The ITZ-Nanos displayed different pharmacokinetic properties compared with the commercial ITZ injections, including a decreased initial drug concentration, increased plasma half-life and mean residence time (MRT), and increased concentration in the liver, lung, and spleen. The ITZ-Nanos can change the in vivo distribution of ITZ and result in passive targeting to the organs with mononuclear phagocyte systems (MPS). [ABSTRACT FROM AUTHOR]

Published

2019

28. Design and Optimization of Controlled Release Felbamate Tablets by D-optimal Mixture Design: In vitro-in vivo Evaluation.

Author

PARIKH, KINJAL, MUNDADA, P., and SAWANT, KUTIKA

Subjects

*LAMOTRIGINE, *PHARMACOKINETICS, *LENNOX-Gastaut syndrome, *DIFFERENTIAL scanning calorimetry, *PATIENT compliance, *CHILDHOOD epilepsy, *INFRARED spectroscopy

Abstract

Felbamate, an antiepileptic drug is administered multiple times a day to obtain proper restorative action against seizures in childhood onset epilepsy (Lennox-Gastaut syndrome), which usually result in poor therapeutic efficacy because of fluctuating plasma levels and low patient compliance. Hence, controlled release hydroxypropyl methylcellulose matrix tablets of felbamate were formulated to overcome these drawbacks. The results of pre-formulation studies such as differential scanning calorimetry and Fourier-transform infrared spectroscopy showed compatibility of drug with the selected excipients. The formulation variables were optimized using D-optimal design, which can elucidate the effect of all variables simultaneously during formulation optimization. In vitro drug release at the end of 2, 8 and 20 h were taken as the response parameters for the optimization study by D-optimal design. The results enabled selection of the formulation with the desired drug release pattern approaching to zero order. The optimized batch was subjected to in vivo pharmacokinetic studies in rabbits, which showed extended release of drug up to 24 h. Thus, the felbamate controlled release tablets optimized by D-optimal design have potential to reduce the dose and dosing frequency, improve therapy and patient compliance. [ABSTRACT FROM AUTHOR]

Published

2019

29. In vitro and in vivo evaluation of pirfenidone loaded acrylamide grafted pullulan-poly(vinyl alcohol) interpenetrating polymer networks.

Author

Soni, Saundray Raj, Kumari, Nimmy, Bhunia, Bibhas K., Sarkar, Biswatrish, Mandal, Biman B., and Ghosh, Animesh

Subjects

*ACRYLAMIDE, *POLYVINYL alcohol, *POLYMER networks, *DRUG delivery systems, *BIOCOMPATIBILITY, *PHARMACOKINETICS

Abstract

Highlights • Application of acrylamide grafted pullulan as one of the component for controlled release drug delivery system. • Detailed thermal kinetic profile of microsphere using isoconversional model. • In vitro enzymatic degradation of microsphere. • Biocompatibility assessment of microsphere in human hepatocellular carcinoma cell line. • Comparative in vivo pharmacokinetic study of optimized formulation with marketed product. Abstract The aim of present study was to develop controlled release formulation of pirfenidone using acrylamide grafted pullulan. Interpenetrating polymer network (IPN) microspheres were prepared using acrylamide grafted pullulan and PVA utilizing glutaraldehyde assisted water-in-oil emulsion crosslinking method. IPN microspheres were characterized by FTIR, solid state 13C NMR and XRD spectroscopy. In vitro enzymatic degradation study showed 34.30% degradation after 24 h with degradation rate constant of 0.0088 min−1. In vitro biocompatibility test showed no changes in cellular morphology and cell adherence to microspheres, indicating its biocompatible nature. The release exponent value of all formulations was less than 0.45, indicating the release mechanism to be Fickian diffusion. Finally, in vivo pharmacokinetic study showed longer T max (1.16 h) and greater AUC value (10037.76 ng h/mL,) as compared to Pirfenex® (T max = 0.5 h; AUC = 4310.45 ng h/mL,). The results indicated that the prepared formulation could successfully control the drug release for prolonged time period. [ABSTRACT FROM AUTHOR]

Published

2018

30. Combined use of biocompatible nanoemulsions and solid microneedles to improve transport of a model NSAID across the skin: In vitro and in vivo studies.

Author

Ilić, Tanja, Savić, Sanela, Batinić, Bojan, Marković, Bojan, Schmidberger, Markus, Lunter, Dominique, Savić, Miroslav, and Savić, Snežana

Subjects

*LECITHIN, *SUCROSE esters, *DICLOFENAC, *POLYSORBATE 80, *BIOAVAILABILITY, *PHARMACOKINETICS, *DRUG delivery systems, *INTRAVENOUS injections

Abstract

Abstract This study aimed to investigate the potential of lecithin-based nanoemulsions costabilized by sucrose esters, with and without skin pretreatment with stainless steel microneedles, to improve delivery of aceclofenac, as a model drug, into/across the skin. The characterization revealed favorable droplet size (about 180 nm), narrow size distribution (<0.15), high surface charge (about −40 mV) and satisfying long-term stability (one year at 4 ± 1 °C) of the formulation costabilized by sucrose palmitate, demonstrating a similar trend observed for the reference stabilized by widely used lecithin/polysorbate 80 combination. In vitro release/permeation testing and differential stripping on the porcine ear proved the superiority of the sucrose ester- over polysorbate-based nanoemulsion. However, in vitro findings were not fully indicative of the in vivo performances – no significant differences were observed between investigated formulations in pharmacokinetic profile and total amount of aceclofenac deposited in the rat skin 24 h after dosing, simultaneously pointing to delayed aceclofenac delivery into the systemic circulation. In addition, the ratio of plasma concentrations of aceclofenac and its major metabolite in rats, diclofenac, was remarkably changed after topical application of tested nanoemulsions compared to intravenous administration of aceclofenac solution. Finally, skin pretreatment with microneedles improved aceclofenac delivery into/across the rat skin from tested formulations, resulting in 1.4–2.1-fold increased bioavailability and 1.2–1.7-fold enhanced level of aceclofenac retained in the skin, as measured 24 h after administration. Moreover, the plasma concentrations of aceclofenac 24 h after application of tested formulations (lecithin/sucrose palmitate vs. lecithin/polysorbate 80) combined with microneedles (173.37 ± 40.50 ng/ml vs. 259.23 ± 73.18 ng/ml) were significantly higher than those obtained through intact skin (105.69 ± 19.53 ng/ml vs. 88.38 ± 14.46 ng/ml). However, obtained results suggest that combination of microneedles and sucrose palmitate-costabilized nanoemulsion could be useful to attain higher skin concentration, while combination of microneedles with polysorbate 80-costabilized nanoemulsion could be a preferable option for enhancing drug delivery into the bloodstream. Graphical abstract Unlabelled Image [ABSTRACT FROM AUTHOR]

Published

2018

31. A physiologically based pharmacokinetic model for valacyclovir established based on absolute expression quantity of hPEPT1 and its application.

Author

Sun, Le, Wang, Chao, and Zhang, Youxi

Subjects

*PHARMACOKINETICS, *VALACYCLOVIR, *INTESTINES, *BIOAVAILABILITY, *ACYCLOVIR, *THERAPEUTICS

Abstract

Abstract In this study, a physiologically based pharmacokinetic (PBPK) model was established for valacyclovir based on absolute expression quantity of hPEPT1 along the entire length of the human intestine and other reliable in vitro , in vivo observed data. The PBPK model-3 defined acyclovir as metabolite of valacyclovir and simulated the plasma concentration-time profiles of valacyclovir and acyclovir simultaneously. It was validated strictly by a series of observed plasma concentration-time profiles. The average fold error (AFE) and absolute average fold error (AAFE) values were all smaller than 2. Then, it was used to quantitatively evaluate the effect of hPEPT1, luminal degradation rate, drug release rate and gastric residence time on the oral absorption of valacyclovir and acyclovir. The PBPK model-3 suggests that mainly 75% of valacyclovir was absorbed by active transport of hPEPT1. The luminal degradation of valacyclovir in the upper intestinal lumen cannot be considered the only reason for its incomplete bioavailability. The plasma concentration-time profiles of valacyclovir and its metabolite acyclovir were not sensitive to dissolution rate faster than T 85% = 120 min. Prolonged gastric residence time of sustained release tablet can improve the oral absorption of valacyclovir. All in all, the PBPK model-3 in this study is reliable and accurate. It is useful for the research of clinical application and dosage forms design of valacyclovir. Graphical abstract Unlabelled Image [ABSTRACT FROM AUTHOR]

Published

2018

32. Hedgehog pathway inhibitors of the acylthiourea and acylguanidine class show antitumor activity on colon cancer in vitro and in vivo.

Author

Vesci, Loredana, Milazzo, Ferdinando Maria, Stasi, Maria Antonietta, Pace, Silvia, Manera, Francesco, Tallarico, Carlo, Cini, Elena, Petricci, Elena, Manetti, Fabrizio, De Santis, Rita, and Giannini, Giuseppe

Subjects

*GUANIDINE, *THIOUREA, *HEDGEHOG signaling proteins, *ANTINEOPLASTIC agents, *COLON cancer, *ORGANIC synthesis

Abstract

Abstract Small series of acylguanidine and acylthiourea derivatives were synthesized in gram-scale and assayed for their ability to modulate the Hh signalling pathway. In vitro studies showed a low micromolar inhibitory activity toward tumor cell lines, while the oral administration revealed an excellent ADME profile in vivo. Compound 5 emerged as the most active and safe inhibitor of colon cancer cells both in vitro and in a xenograft mouse model. Based on these data, 5 could be prioritized to further development with the perspective of clinical studies. Graphical abstract Image 1 Highlights • Gram-scale synthesis of Hedgehog inhibitors with an Heck coupling. • Cell-based evaluation and ADME profiling with vismodegib as reference. • The phenetyl analogue 5 is a safe inhibitor of a LS180 colon cancer xenograft. [ABSTRACT FROM AUTHOR]

Published

2018

33. Development of a novel conjugatable sunitinib analogue validated through in vitro and in vivo preclinical settings.

Author

El Mubarak, Mohamed A., Leontari, Iliana, Efstathia, Giannopoulou, Vrettos, Eirinaios I., Shaikh, Abdul kadar, Konstantinos, Siatis E., Danika, Charikleia, Kalofonos, Haralabos P., Tzakos, Andreas G., and Sivolapenko, Gregory B.

Subjects

*PROTEIN-tyrosine kinases, *ANTINEOPLASTIC agents, *MASS spectrometry, *PHARMACOKINETICS, *CHEMICAL kinetics

Abstract

Sunitinib is an oral FDA/EMEA approved multi-targeted tyrosine kinase inhibitor. It possesses anti-angiogenic and antitumor activity against a variety of advanced solid tumors. However, its chemical core does not allow a potential linkage to tumor-homing elements that could eventually enhance its potency. Therefore, a novel linkable sunitinib derivative, designated SB1, was rationally designed and synthesized. The pharmaceutical profile of SB1 was explored both in vitro and in vivo . Mass spectrometry and NMR spectroscopy were utilized for characterization, while MTT assays and LC-MS/MS validated protocols were used to explore its antiproliferative effect and stability, respectively. Cytotoxicity evaluation in three glioma cells showed that SB1 preserved the antiproliferative effect of sunitinib. SB1 was stable in vitro after 24 h incubation in mouse plasma, while both agents exhibited bioequivalent pharmacokinetic characteristics after i.v. administration in Balb/c mice. To evaluate the levels of SB1 in mouse plasma, a novel analytical method was developed and validated in accordance to the US FDA and the EU EMA guidelines. We formulated a novel linkable sunitinib analog exhibiting similar antiproliferative and apoptotic properties with native sunitinib in glioma cell lines. Both SB1 and native sunitinib showed identical in vitro stability in mouse plasma and pharmacokinetics after i.v. administration in Balb/c mice. [ABSTRACT FROM AUTHOR]

Published

2018

34. Preparation and <italic>in vitro</italic>–<italic>in vivo</italic> characterization of trans-resveratrol nanosuspensions.

Author

Dong, Qiannian, Yuan, Hui-Ling, Qian, Jia-Jia, Zhang, Cai-Yun, and Chen, Wei-Dong

Subjects

*RESVERATROL, *SATURATION (Chemistry), *METEOROLOGICAL precipitation, *PHARMACOKINETICS, *ZETA potential

Abstract

Nanosuspensions technique is an important tool to enhance the saturation solubility and dissolution velocity of poorly soluble drugs. Trans-resveratrol (t-Res) with extensive pharmacological effects was severely restricted by poor solubility and short biological half-life. In this study, anti-solvent precipitation was employed to development trans-resveratrol nanosuspensions (t-Res NS) with PVPK30 as stabilizer. The physicochemical properties, in vitro release and in vivo pharmacokinetics of t-Res NS were investigated. The mean particle size, zeta potential, encapsulation efficiency and drug loading of t-Res NS prepared by the optimal prescription were 96.9 nm, −20.4mV, 78% and 28.1%, respectively. The morphology of t-Res nanoparticles was spherical indicated by SEM with amorphous phase verified by XRD and DSC. The t-Res NS present a good physical stability as well as enhanced chemical stability. Compared to crude drug, the in vitro dissolution rate of t-Res NS was increased with fitting Higuchi equation ( Q = 0.3215 t 1 / 2 + 0.0070 ). The in vivo pharmacokinetic test in rats showed that the AUC 0 ∼ t of t-Res NS (559.4 μg/mL·min) was about 3.6-fold higher than that of t-Res solution. Meanwhile, the MRT of t-Res nanosuspensions was longer than that of t-Res solution. These results suggested that NS may be a potentially nanocarrier for clinical delivery of t-Res. [ABSTRACT FROM AUTHOR]

Published

2018

35. Cefmetazole as an Alternative to Carbapenems Against Extended-Spectrum Beta-Lactamase-Producing Escherichia coli Infections Based on In Vitro and In Vivo Pharmacokinetics/Pharmacodynamics Experiments

Author

Nana Kojima, Yuki Igarashi, Tomonori Nakamura, Yuta Yokoyama, Wataru Takemura, Marina Hayashi, Yuki Mizukami, Kazuaki Taguchi, Sho Tashiro, Kazuaki Matsumoto, Yuki Enoki, Xiaoxi Liu, and Takumi Morita

Subjects

Neutropenia, medicine.medical_treatment, Pharmaceutical Science, Microbial Sensitivity Tests, Pharmacology, Cefmetazole, medicine.disease_cause, beta-Lactam Resistance, beta-Lactamases, Mice, Pharmacokinetics, In vivo, Escherichia coli, medicine, Animals, Humans, Pharmacology (medical), Escherichia coli Infections, Chemistry, Escherichia coli Proteins, Organic Chemistry, In vitro, Anti-Bacterial Agents, Disease Models, Animal, Carbapenems, Pharmacodynamics, Beta-lactamase, Molecular Medicine, Female, In vivo pharmacokinetics, Biotechnology, medicine.drug

Abstract

PURPOSE Cefmetazole (CMZ) has received attention as a pharmaceutical intervention for extended-spectrum beta-lactamase-producing Escherichia coli (ESBL-EC) infections. This study aimed to investigate the pharmacokinetics/pharmacodynamics (PK/PD) characteristics of CMZ against ESBL-EC. METHODS The susceptibility and time-killing activity of CMZ against clinically isolated ESBL-EC (EC9 and EC19) were determined in vitro. The optimal PK/PD index and its target value were calculated based on the results of a PK study in healthy mice and PD study in neutropenic murine thigh infection model mice. RESULTS The minimum inhibitory concentrations (MICs) of CMZ against EC9 and EC19 were 2.0 and 1.0 µg/mL, respectively. Time-kill studies showed that colony-forming units decreased in a time-dependent manner at CMZ concentrations in the range of 4-64 × MIC. In in vivo PK/PD studies, the antibacterial effect of CMZ showed the better correlation with the time that the free drug concentration remaining above the MIC (fT>MIC), with the target values for a static effect and 1 log10 kill reduction calculated as 57.6% and 69.6%, respectively. CONCLUSION CMZ possesses time-dependent bactericidal activities against ESBL-EC and is required to achieve "fT>MIC" ≥ 69.6% for the treatment of ESBL-EC infections.

Published

2021

36. New 5-Aryl-1,3,4-Thiadiazole-Based Anticancer Agents: Design, Synthesis, In Vitro Biological Evaluation and In Vivo Radioactive Tracing Studies

Author

Rana M. El-Masry, Basma M. Essa, Adli A. Selim, Soad Z. El-Emam, Khaled O. Mohamed, Tamer M. Sakr, Hanan H. Kadry, Azza T. Taher, and Sahar M. Abou-Seri

Subjects

Drug Discovery, Pharmaceutical Science, Molecular Medicine, 1,3,4-thiadiazole, anticancer activity, structure-activity relationship, radiolabeling, in vivo pharmacokinetics

Abstract

A new series of 5-(4-chlorophenyl)-1,3,4-thiadiazole-based compounds featuring pyridinium (3), substituted piperazines (4a–g), benzyl piperidine (4i), and aryl aminothiazoles (5a–e) heterocycles were synthesized. Evaluation of the cytotoxicity potential of the new compounds against MCF-7 and HepG2 cancer cell lines indicated that compounds 4e and 4i displayed the highest activity toward the tested cancer cells. A selectivity study demonstrated the high selective cytotoxicity of 4e and 4i towards cancerous cells over normal mammalian Vero cells. Cell cycle analysis revealed that treatment with either compound 4e or 4i induced cell cycle arrest at the S and G2/M phases in HepG2 and MCF-7 cells, respectively. Moreover, the significant increase in the Bax/Bcl-2 ratio and caspase 9 levels in HepG2 and MCF-7 cells treated with either 4e or 4i indicated that their cytotoxic effect is attributed to the ability to induce apoptotic cell death. Finally, an in vivo radioactive tracing study of compound 4i proved its targeting ability to sarcoma cells in a tumor-bearing mice model.

Published

2022

37. Automated radiosynthesis of [18F]AlF-NOTA-octreotide and PET/CT imaging in NENs

Author

Dong Xu, Wei Xue, Qian Yu, Zhenguang Wang, Dacheng Li, Bin Shi, Xiaojie Tan, and Fengyu Wu

Subjects

Biodistribution, Chemistry, Health, Toxicology and Mutagenesis, Radiochemistry, Public Health, Environmental and Occupational Health, Pet ct imaging, Octreotide, Automated radiosynthesis, Pollution, Analytical Chemistry, Nuclear Energy and Engineering, Reagent, medicine, Somatostatin receptor 2, Radiology, Nuclear Medicine and imaging, Spectroscopy, In vivo pharmacokinetics, medicine.drug

Abstract

[18F]AlF-NOTA-octreotide was evaluated for its biodistribution and dosimetry and demonstrated good safety, good tolerance, in vivo pharmacokinetics, and specific uptake in somatostatin receptor 2 (SSTR2)-positive tumors. This study aimed to improve the automated radiolabeling of NOTA-octreotide with [18F]AlF2+ and optimize the radiochemical yield (RCY) of [18F]AlF-NOTA-octreotide. The labeling procedure was optimized by changing the amounts of peptide and AlCl3, the labeling buffers. To simplify the process of preparing the solution, the reagent of the precursor (NOTA-octreotide 0.2 mg) and AlCl3·6H2O (27 µL 4 mM) were made into freeze-dried kit in advance. NOTA-octreotide was labeled with [18F]AlF2+ with a 55% yield in 40 min. This method can be used to effectively improve RCY and meet clinical requirements.

Published

2021

38. In Silico Absorption Analysis of Valacyclovir in Wildtype and Pept1 Knockout Mice Following Oral Dose Escalation.

Author

Yang, Bei and Smith, David

Subjects

*PHARMACOKINETICS, *ACYCLOVIR, *VALACYCLOVIR, *ILEUM, *COLON (Anatomy)

Abstract

Purpose: We developed simulation and modeling methods to predict the in vivo pharmacokinetic profiles of acyclovir, following escalating oral doses of valacyclovir, in wildtype and Pept1 knockout mice. We also quantitated the contribution of specific intestinal segments in the absorption of valacyclovir in these mice. Methods: Simulations were conducted using a mechanistic advanced compartmental absorption and transit (ACAT) model implemented in GastroPlus™. Simulations were performed for 3 h post-dose in wildtype and Pept1 knockout mice following single oral doses of 10, 25, 50 and 100 nmol/g valacyclovir, and compared to experimentally observed plasma concentration-time profiles of acyclovir. Results: Good fits were obtained in wildtype and Pept1 knockout mice. Valacyclovir was primarily absorbed from duodenum (42%) and jejunum (24%) of wildtype mice, with reduced uptake from ileum (3%) and caecum/colon (1%), for a total of 70% absorption. In contrast, the absorption of valacyclovir in Pept1 knockout mice was slow and sustained throughout the entire intestinal tract in which duodenum (4%), jejunum (14%), ileum (10%) and caecum/colon (12%) accounted for a total of 40% absorption. Conclusion: The ACAT model bridged the gap between in situ and in vivo experimental findings, and facilitated our understanding of the complicated intestinal absorption processes of valacyclovir. [ABSTRACT FROM AUTHOR]

Published

2017

39. Traditional uses, phytochemistry, pharmacology, and toxicology of Pterocephalus hookeri (C. B. Clarke) Höeck: a review

Author

Yi Zhang, Honglin Tao, Xianli Meng, Shi-Ying Luo, Jia Yu, Zhi-Qiang Gan, Ce Tang, and Juan Jiang

Subjects

Toxicology, Iridoid Glycosides, Phytochemistry, Triterpenoid, biology, General Chemical Engineering, Traditional Tibetan Medicine, General Chemistry, Pharmacology, biology.organism_classification, Pterocephalus hookeri, Dipsacaceae, In vivo pharmacokinetics

Abstract

Pterocephalus hookeri (C. B. Clarke) Hoeck is a member of the Dipsacaceae family and has been used in traditional Tibetan medicine for thousands of years. P. hookeri clears heat, detoxifies, stops dysentery, eliminates distemper, dispels wind, and relieves stagnation and is mainly prescribed for heat syndrome, dysentery, arthritis, and plague. Approximately 93 chemical compounds have been isolated and identified from P. hookeri, including iridoid glycosides, lignan and triterpenoids. Meanwhile, modern pharmacological studies have shown that P. hookeri has anti-inflammatory, anti-rheumatoid arthritis, analgesic, anticancer, and neuroprotection activities. However, studies on the in vivo pharmacokinetics and mechanism of action, discovery of quality markers, and qualitative and quantitative analysis are still insufficient. Hence, this paper provides a comprehensive review of the ethnic medicine, phytochemistry, pharmacology, and toxicology of P. hookeri to increase the understanding of the medicinal value of P. hookeri.

Published

2021

40. In vivo pharmacokinetics, distribution, and excretion of an anticancer agent isolated from red ginseng, in rat

Author

Qian Zheng, Pingya Li, Nanqi Zhang, Ruili Wang, and Cuizhu Wang

Subjects

Pharmacology, Health, Toxicology and Mutagenesis, General Medicine, Toxicology, 030226 pharmacology & pharmacy, Biochemistry, Excretion, 03 medical and health sciences, chemistry.chemical_compound, Ginseng, 0302 clinical medicine, chemistry, Pharmacokinetics, Ginsenoside, 030220 oncology & carcinogenesis, Lc ms ms, Distribution (pharmacology), In vivo pharmacokinetics

Abstract

The compound 20(S),25-epoxydammarane-3β,12β,24α-triol (24-hydroxy-panaxadiol or 24-OH-PD), isolated from the red Panax ginseng CA Meyer possesses anticancer activity. Our aim was to study the pharm...

Published

2020

41. Nanosuspensions as delivery system for gambogenic acid: characterization and in vitro/in vivo evaluation.

Author

Yuan, Huiling, Li, Xin, Zhang, Caiyun, Pan, Wenli, Liang, Yumeng, Chen, Yang, Chen, Weidong, Liu, Lulu, and Wang, Xiaomin

Subjects

*NONIONIC surfactants, *SURFACE active agents, *NANOPARTICLES, *ZETA potential, *HYDROGEN bonding

Abstract

Nanosuspensions (NS) can enhance the saturation solubility and dissolution velocity of poorly soluble drugs. PEG as a non-ionic surfactant plays an important role in surface modification of nanoparticles for prolonging in vivo circulation. In this study, anti-solvent precipitation method was introduced to prepare gambogenic acid nanosuspensions (GNA-NS) with PVPK30 and PEG2000 as stabilizers to settle the disadvantages of GNA. The obtained nanoparticles were spherical with a mean particle size of 183.7 nm and a zeta potential of −22.8 mV. The entrapment efficiency and drug loading of the resultant formulation were 97.3 and 29.73%. X-ray diffraction analysis confirmed the amorphous phase of GNA in NS. Fourier transform infrared indicated there may be hydrogen bond interaction between the drug and excipients. After lyophilization of GNA-NS, the freeze-dried powder displayed sufficient long-term physical stability at 4 and 25 °C. In comparison to GNA solution, in vitro studies of GNA-NS showed much slower release and higher cytotoxicity in HepG2 cells. What's more, the pharmacokinetic study in rats revealed that the AUC0–∞ and t1/2 of GNA-NS were increased 2.63- and 1.77-fold than that of the reference formulation. Taken together, in vitro/in vivo evaluations showed NS would be an effectively strategy to change the poor aqueous solubility and prolong the half-life for GNA. The GNA-NS with enhanced bioavailability and drug efficacy provided a promising delivery system for the application of GNA. [ABSTRACT FROM AUTHOR]

Published

2016

42. Formulation, production, in vitro release and in vivo pharmacokinetics of cinnamaldehyde sub-micron emulsions

Author

Huang Jie, Wang Xingqi, Hu Rongfeng, Zhang Yong, and Chu Xiaoqin

Subjects

Chromatography, Production optimization, Pharmaceutical Science, 02 engineering and technology, General Medicine, 021001 nanoscience & nanotechnology, 030226 pharmacology & pharmacy, Box–Behnken design, In vitro, Cinnamaldehyde, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, chemistry, Emulsion, 0210 nano-technology, In vivo pharmacokinetics

Abstract

Objective: The purpose of this study was to study the effects of formulation of cinnamaldehyde submicron emulsion (CA-SME) and optimize the preparation process parameters of CA-SME, characterize CA...

Published

2020

43. [6]-Shogaol/β-CDs inclusion complex: preparation, characterisation, in vivo pharmacokinetics, and in situ intestinal perfusion study

Author

Rui Bao, Qiuxuan Yang, Hao Ji, Ran Li, Jiangnan Yu, Qilong Wang, Toreniyazov Elmurat, Ximing Xu, Qiuyu Wei, and Michael Adu-Frimpong

Subjects

In situ, Intestinal perfusion, Chemistry, Organic Chemistry, Pharmaceutical Science, Bioengineering, 02 engineering and technology, Absorption (skin), Shogaol, Pharmacology, 021001 nanoscience & nanotechnology, 030226 pharmacology & pharmacy, In vitro, Bioavailability, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Colloid and Surface Chemistry, In vivo, Physical and Theoretical Chemistry, 0210 nano-technology, In vivo pharmacokinetics

Abstract

Aims: The aim was to improve the absorption and bioavailability of [6]-shogaol with β-cyclodextrin (β-CD) prior to in vitro and in vivo evaluation.Methods: [6]-Shogaol/β-CDs inclusion complexes (6-...

Published

2019

44. The effect of nanoparticle size on in vivo pharmacokinetics and cellular interaction.

Author

Hoshyar, Nazanin, Gray, Samantha, Han, Hongbin, and Bao, Gang

Abstract

Nanoparticle-based technologies offer exciting new approaches to disease diagnostics and therapeutics. To take advantage of unique properties of nanoscale materials and structures, the size, shape and/or surface chemistry of nanoparticles need to be optimized, allowing their functionalities to be tailored for different biomedical applications. Here we review the effects of nanoparticle size on cellular interaction and in vivo pharmacokinetics, including cellular uptake, biodistribution and circulation half-life of nanoparticles. Important features of nanoparticle probes for molecular imaging and modeling of nanoparticle size effects are also discussed. [ABSTRACT FROM AUTHOR]

Published

2016

45. Use of biorelevant media for assessment of a poorly soluble weakly basic drug in the form of liquisolid compacts: in vitro and in vivo study.

Author

Badawy, Mahmoud A., Kamel, Amany O., and Sammour, Omaima A.

Subjects

*DRUG delivery systems, *GASTROINTESTINAL system physiology, *PHARMACOKINETICS, *ACHLORHYDRIA, *TURBIDITY, *DISSOLUTION (Chemistry), *GASTROINTESTINAL motility, *DRUG tablets

Abstract

The purpose of this work is to use biorelevant media to evaluate the robustness of a poorly water soluble weakly basic drug to variations along the gastrointestinal tract (GIT) after incorporation in liquisolid compacts and to assess the success of these models in predicting thein vivoperformance. Liquisolid tablets were prepared using mosapride citrate as a model drug. A factorial design experiment was used to study the effect of three factors, namely: drug concentration at two levels (5% and 10%), carriers at three levels (avicel, mannitol and lactose) and powder excipients ratio (R) of the coating material at two levels (25 and 30). Thein vitrodissolution media utilized were 0.1 N HCl, hypoacidic stomach model and a transfer model simulating the transfer from the stomach to the intestine. All compacts released above 95% of drug after 10 min in 0.1 N HCl. In the hypoacidic model, the compacts with R 30 were superior compared to R 25, where they released >90% of drug after 10 min compared to 80% for R 25. After the transfer of the optimum compacts from Simulated gastric fluid fast (SGFfast) to fasted state simulated intestinal fluid, slight turbidity appeared after 30 min, and the amount of drug dissolved slightly decreased from 96.91% to 90.59%. However, after the transfer from SGFfast to fed state simulated intestinal fluid, no turbidity or precipitation occurred throughout time of the test (60 min).In vivopharmacokinetic study in human volunteers proved the success of thein vitromodels with enhancement of the oral bioavailability (121.20%) compared to the commercial product. [ABSTRACT FROM PUBLISHER]

Published

2016

46. Effects of Borneol on the Release of Compound Danshen Colon-Specific Osmotic Pump Capsule In Vitro and Pharmacokinetics Study in Beagle Dogs

Author

Shao, Liangyu, Sun, Chaojie, Lu, Wenjie, Chen, Jiayi, Su, Dan, Gao, Song, Chen, Shengqi, Fang, Wenyou, Liu, Yu, Wang, Bin, and Hu, Rongfeng

Published

2020

47. Preclinical drug metabolism and pharmacokinetics of salinomycin, a potential candidate for targeting human cancer stem cells.

Author

Resham, Kahkashan, Patel, Prinesh N., Thummuri, Dinesh, Guntuku, Lalita, Shah, Vanya, Bambal, Ramesh B., and Naidu, V.G.M.

Subjects

*SALINOMYCIN, *DRUG metabolism, *PHARMACOKINETICS, *ANTIPROTOZOAL agents, *STEM cells

Abstract

There has been a search for new anticancer agents to treat cancer resistance throughout the globe. Salinomycin (SAL), a broad spectrum antibiotic and a coccidiostat has been found to counter tumour resistance and kill cancer stem cells with better efficacy than the existing chemotherapeutic agents; paclitaxel and doxorubicin. This refocused its importance for treatment of human cancers. In this study, we studied the in vitro drug metabolism and pharmacokinetic parameters of SAL. SAL undergoes rapid metabolism in liver microsomes and has a high intrinsic clearance. SAL metabolism is mainly mediated by CYP enzymes; CYP3A4 the major enzyme metabolising SAL. The percent plasma protein binding of SAL in human was significantly lower as compared to mouse and rat plasma. CYP inhibition was carried out by chemical inhibition and recombinant enzyme studies. SAL was found to be a moderate inhibitor of CYP2D6 as well as CYP3A4. As CYP3A4 was the major enzyme responsible for metabolism of SAL, in vivo pharmacokinetic study in rats was done to check the effect of concomitant administration of Ketoconazole (KTC) on SAL pharmacokinetics. KTC, being a selective CYP3A4 inhibitor increased the systemic exposure of SAL significantly to 7-fold in AUC 0–α and 3-fold increase in C max of SAL in rats with concomitant KTC administration. [ABSTRACT FROM AUTHOR]

Published

2015

48. Preparation, Characterization, in vivo Pharmacokinetics and Tumor Inhibition Properties of PEGylated Liposomes Containing Etoposide.

Author

Jun, Shi, Yi, Cheng, Fangli, Ma, Weihong, Chen, and Xiaoyan, Wang

Abstract

Liposomal formulations of a potent antitumor drug, etoposide were prepared by ethanol injection method successfully. The characteristics of the etoposide liposomes, for particle size, encapsulation efficiency, leakage ratio, ? potential and physical stability, were evaluated. In vivo pharmacokinetics and tumor inhibition ratio of mice were also examined. The liposomes were characterized by high entrapment efficiency, uniform size distribution and moderate ? potential. In addition, the liposomes modified by PEG2000-DSPE could raise the AUC and prolonged the resident time of etoposide in the blood circulating system as compared to conventional liposomes containing etoposide and free etoposide solutions, and improve the tumor inhibition ratio demonstrated by anti-tumor activity experiments. [ABSTRACT FROM PUBLISHER]

Published

2012

49. Novel extended in vitro-in vivo correlation model for the development of extended-release formulations for baclofen: From formulation composition to in vivo pharmacokinetics

Author

Tae Hwan Kim, Beom Soo Shin, Jürgen B. Bulitta, Soyoung Shin, and Do Hyung Kim

Subjects

Baclofen, Chemistry, Pharmaceutical, Population, Pharmaceutical Science, 02 engineering and technology, Models, Biological, 030226 pharmacology & pharmacy, Excipients, 03 medical and health sciences, chemistry.chemical_compound, Dogs, Hypromellose Derivatives, 0302 clinical medicine, IVIVC, Pharmacokinetics, In vivo, Animals, education, Dissolution, education.field_of_study, Chromatography, Chemistry, 021001 nanoscience & nanotechnology, In vitro, body regions, Drug Liberation, Delayed-Action Preparations, 0210 nano-technology, In vivo pharmacokinetics, Tablets

Abstract

In vitro-in vivo correlation (IVIVC), a predictive mathematical model between the in vitro dissolution and the in vivo pharmacokinetics has been utilized for the development of new extended release (ER) formulations. The aim of the present study was to extend the IVIVC approach, which correlates among the formulation composition, the in vitro dissolution, and the plasma drug concentration, to predict plasma drug concentrations from a given composition of the formulation, and vice versa, using baclofen as a model drug. Baclofen ER tablets with different dissolution rates were prepared by varying the composition of hydroxypropyl methylcellulose (HPMC). First, the HPMC compositions and the corresponding in vitro dissolutions parameters were correlated, and then the in vitro dissolution parameters were correlated with the in vivo dissolution parameters extracted from the pharmacokinetic profiles of the baclofen ER formulations via population pharmacokinetic modeling. The final extended IVIVC model linked the composition of the formulation, the in vitro dissolution, and the in vivo plasma concentration profile and was successfully applied for the prediction of in vivo pharmacokinetics from the amount of HPMC in baclofen ER formulations. The present approach holds great promise for designing optimal compositions of ER formulations to present desired plasma concentration profile.

Published

2019

50. In Vivo Pharmacokinetics of Bromfenac Ophthalmic Solution 0.075%, Bromfenac Ophthalmic Solution 0.07%, and Nepafenac/Amfenac Ophthalmic Suspension 0.3% in Rabbits

Author

Mark C. Jasek, Angela Justice, Paul C. Cockrum, and John D. Sheppard

Subjects

0301 basic medicine, medicine.medical_specialty, PK, genetic structures, Aqueous humor, Nepafenac, Retina, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Bromfenac Ophthalmic Solution, Pharmacokinetics, Ophthalmic Suspension, Ophthalmology, Ocular, medicine, Original Research, Iris-ciliary body, business.industry, Choroid, Iris ciliary body, eye diseases, NSAID, 030104 developmental biology, chemistry, 030221 ophthalmology & optometry, sense organs, business, Amfenac, In vivo pharmacokinetics, Sclera, medicine.drug

Abstract

Introduction Little is known of the ocular distribution characteristics of currently branded non-steroidal anti-inflammatory drugs (NSAIDs) in the United States. This study was designed to predict the ocular bioavailability characteristics in humans using Dutch Belted rabbits as a surrogate. Commercially available, topically-applied NSAIDs containing bromfenac or nepafenac/amfenac were evaluated. Methods 126 healthy adult Dutch Belted rabbits were randomly assigned to three treatment cohorts (BromSite® twice daily [BID] in the right eye, BromSite® once daily [QD] in the right eye, Prolensa® QD in the right eye and Ilevro™ QD in the left eye) and 7 post-dosing time points (0.5, 1, 2, 4, 8, 12, 24 h after final instillation). The study eyes received 40 µL of the assigned drug for a consecutive 9 days. Samples of aqueous humor, iris-ciliary body, choroid, sclera, and retina were harvested from the study eyes at the assigned time point after the last dose on the 9th day. NSAID content in ocular tissues was analyzed using high-performance liquid chromatography (HPLC), and area under the curve (AUC0.5–24h), maximum concentration (Cmax), and time to maximum concentration (Tmax) were determined. Results Peak NSAID concentrations were reached within 1–3 h in the anterior segment and within 1–3 h in the posterior segment after last dose. Throughout the ocular tissues, both AUC and Cmax for BromSite® (BID and QD) were consistently higher than respective NSAID concentrations of Prolensa® QD and Ilevro® QD. When comparing BromSite® BID to QD, the BID regimen produced generally higher but statistically similar bromfenac concentrations throughout the ocular tissues except in the aqueous humor and iris-ciliary body, where the AUC BID was statistically significantly higher with BromSite® BID. Conclusion As a surrogate to human ocular bioavailability, BromSite® demonstrated significantly greater NSAID compared to Prolensa® QD and Ilevro® QD. The DuraSite® component of BromSite® appears to enhance ocular penetration throughout both anterior and posterior tissues. Funding Sun Pharmaceutical Industries Ltd.

Published

2018