Preparation, pharmacokinetics and biodistribution of baicalin-loaded liposomes

Wei, Yumeng; Guo, Jianmin; Zheng, Xiaoli; Wu, Jun; Zhou, Yang; Yu, Yu; Ye, Yun; Zhang, Liangke; Zhao, Ling

doi:10.2147/ijn.s66312

Cited by 34 publications

(14 citation statements)

References 35 publications

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“…This function was and still remains most frequently applied to the analysis of dissolution and release studies involving nanoparticulate drug systems: nano- and micro-capsules [137,138], nanosuspensions [139], nanosized zeolits [140], PLGA nanoparticles [141], inorganic nanoparticles [142,143], solid lipid nanoparticles (SLN), and nano-structured lipid carrier (NLC) [144], as well as different liposomal formulations [145,146,147,148].…”

Section: Release Models Based On Fick’s First Lawmentioning

confidence: 99%

Mathematical Modeling of Release Kinetics from Supramolecular Drug Delivery Systems

et al. 2019

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Embedding of active substances in supramolecular systems has as the main goal to ensure the controlled release of the active ingredients. Whatever the final architecture or entrapment mechanism, modeling of release is challenging due to the moving boundary conditions and complex initial conditions. Despite huge diversity of formulations, diffusion phenomena are involved in practically all release processes. The approach in this paper starts, therefore, from mathematical methods for solving the diffusion equation in initial and boundary conditions, which are further connected with phenomenological conditions, simplified and idealized in order to lead to problems which can be analytically solved. Consequently, the release models are classified starting from the geometry of diffusion domain, initial conditions, and conditions on frontiers. Taking into account that practically all solutions of the models use the separation of variables method and integral transformation method, two specific applications of these methods are included. This paper suggests that “good modeling practice” of release kinetics consists essentially of identifying the most appropriate mathematical conditions corresponding to implied physicochemical phenomena. However, in most of the cases, models can be written but analytical solutions for these models cannot be obtained. Consequently, empiric models remain the first choice, and they receive an important place in the review.

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Section: Release Models Based On Fick’s First Lawmentioning

confidence: 99%

Mathematical Modeling of Release Kinetics from Supramolecular Drug Delivery Systems

et al. 2019

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“…Among them, the zero-order model was the best fit found to describe the curves of RVC release from donor and acceptor liposomes, as shown in S2 Table . As for the combined liposomes, the best fit was achieved with the Weibull model ( S2 Table ), which has been previously used to describe the kinetic curves of other liposomal formulations [ 35 , 36 ]. In that case, the release exponent from Eq 4 (b value, S2 Table ) was greater than unity (sigmoid curve), indicating a complex release mechanism [ 37 ].…”

Section: Resultsmentioning

confidence: 99%

Encapsulation of ropivacaine in a combined (donor-acceptor, ionic-gradient) liposomal system promotes extended anesthesia time

et al. 2017

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Ropivacaine is a local anesthetic with similar potency but lower systemic toxicity than bupivacaine, the most commonly used spinal anesthetic. The present study concerns the development of a combined drug delivery system for ropivacaine, comprised of two types of liposomes: donor multivesicular vesicles containing 250 mM (NH4)2SO4 plus the anesthetic, and acceptor large unilamellar vesicles with internal pH of 5.5. Both kinds of liposomes were composed of hydrogenated soy-phosphatidylcholine:cholesterol (2:1 mol%) and were prepared at pH 7.4. Dynamic light scattering, transmission electron microscopy and electron paramagnetic resonance techniques were used to characterize the average particle size, polydispersity, zeta potential, morphology and fluidity of the liposomes. In vitro dialysis experiments showed that the combined liposomal system provided significantly longer (72 h) release of ropivacaine, compared to conventional liposomes (~45 h), or plain ropivacaine (~4 h) (p <0.05). The pre-formulations tested were significantly less toxic to 3T3 cells, with toxicity increasing in the order: combined system < ropivacaine in donor or acceptor liposomes < ropivacaine in conventional liposomes < plain ropivacaine. The combined formulation, containing 2% ropivacaine, increased the anesthesia duration up to 9 h after subcutaneous infiltration in mice. In conclusion, a promising drug delivery system for ropivacaine was described, which can be loaded with large amounts of the anesthetic (2%), with reduced in vitro cytotoxicity and extended anesthesia time.

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“…For example, the baicalin liposomes modified with folic acid and polyethylene glycol (PEG) can improve the cellular uptake rate and tumor targeting, as well as extend the retention time in the body (Chen et al, 2016). Baicalin liposomes are also known to strengthen oral bioavailability and tissue distribution (Wei et al, 2014). Nonetheless, to date, limited information is available relative to baicalin drug delivery systems for AS therapy.…”

Section: Drug Delivery Systemsmentioning

confidence: 99%

Regulatory Mechanisms of Baicalin in Cardiovascular Diseases: A Review

et al. 2020

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Cardiovascular diseases (CVDs) is the leading cause of high morbidity and mortality worldwide, which emphasizes the urgent necessity to develop new pharmacotherapies. In eastern countries, traditional Chinese medicine Scutellaria baicalensis Georgi has been used clinically for thousands of years. Baicalin is one of the main active ingredients extracted from Chinese herbal medicine S. baicalensis. Emerging evidence has established that baicalin improves chronic inflammation, immune imbalance, disturbances in lipid metabolism, apoptosis and oxidative stress. Thereby it offers beneficial roles against the initiation and progression of CVDs such as atherosclerosis, hypertension, myocardial infarction and reperfusion, and heart failure. In this review, we summarize the pharmacological features and relevant mechanisms by which baicalin regulates CVDs in the hope to reveal its application for CVDs prevention and/or therapy.

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Preparation, pharmacokinetics and biodistribution of baicalin-loaded liposomes

Cited by 34 publications

References 35 publications

Mathematical Modeling of Release Kinetics from Supramolecular Drug Delivery Systems

Mathematical Modeling of Release Kinetics from Supramolecular Drug Delivery Systems

Encapsulation of ropivacaine in a combined (donor-acceptor, ionic-gradient) liposomal system promotes extended anesthesia time

Regulatory Mechanisms of Baicalin in Cardiovascular Diseases: A Review

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