Effect of particle size on oral absorption of carvedilol nanosuspensions: in vitro and in&amp;nbsp;vivo&amp;nbsp;evaluation

Liu, Dandan; Pan, Hao; He, Fengwei; Wang, Xiaoyu; Li, Jinyu; Yang, Xinggang; Pan, Weisan

doi:10.2147/ijn.s87143

Cited by 40 publications

(19 citation statements)

References 30 publications

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“…The results obtained from DSC and PXRD combined, show that carvedilol lyophillized formulations were in the amorphous state. Numerous diffraction peaks of carvedilol were observed at 2θ of 12.4°, 24.4° and 26.1°, and this reveals the crystalline nature of carvedilol [1,18,19].…”

Section: Characteristics Of CLmentioning

confidence: 86%

“…Usually, a small value of PDI indicates a homogenous population, while a larger PDI means a high heterogeneity in particle size [21]. Pure carvedilol had an irregular shape, while the lipid Dynasan shape was cluster-like, and the CL-SLN (F3) exhibited a flaky shape [18].…”

Section: Discussionmentioning

confidence: 99%

“…The results showed that the particles were flakes with a narrow size distribution, and had smooth surfaces. Particle size results and SEM images pointed out that particles were different not only in size, but also in shape., Carvedilol pure powders had a non-uniform shape, while SLN formulations had a flaky shape [18,19].…”

Section: Physicochemical Characteristics Of Slnsmentioning

confidence: 99%

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Preparation and evaluation of carvedilol-loaded solid lipid nanoparticles for targeted drug delivery

Kipriye¹,

Şenel²,

Yenilmez³

2017

Trop. J. Pharm Res

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Section: Characteristics Of CLmentioning

confidence: 86%

Section: Discussionmentioning

confidence: 99%

Section: Physicochemical Characteristics Of Slnsmentioning

confidence: 99%

See 1 more Smart Citation

Preparation and evaluation of carvedilol-loaded solid lipid nanoparticles for targeted drug delivery

Kipriye¹,

Şenel²,

Yenilmez³

2017

Trop. J. Pharm Res

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“…Solubility and PAMPA assay in agreement with in vivo kinetic studies.103pMMA coated thiolated chitosan nanoparticleRadical polymerizationDocetaxelIITenfold increase in oral bioavailability of nanoparticle formulation may be attributed to mucoadhesion, P-gp efflux inhibition and permeability enhancement effect of thiolated chitosan.104PEG- b -PLA nanoparticleFlash nanoprecipitationDoxorubicinIIIOverexpression of P-gp in MDR cell contribute low cellular accumulation. Self-assembled PEG- b -PLA nanoparticle demonstrated higher retention in MDR cell and passive targeting to tumor cell.105NanocrystalCombination technology (antisolvent precipitation and microfluidization)BexaroteneIINanocrystal formulation optimized using L9 orthogonal array stabilized using lecithin and poloxamer 188 for oral and parenteral delivery.106NanocrystalAntisolvent precipitationCarvedilolIISDS stabilized nanosuspension demonstrated increased C max and AUC while decrease in T max when compared with coarse suspension.107NanocrystalWet media MillingFebuxostatIIHPMC and vitamin E TPGS stabilized system with 221.6% increase in relative bioavailability.108NanocrystalPrecipitation-high pressure homogenization methodNitrendipineIISurface modified chitosan nanocrystal stabilized with polyvinyl alcohol (PVA) has better stability and bioavailability compared with unmodified crystals.109NanocrystalWet-milling technologyTranilastIIHydroxy propyl cellulose-SL and SDS stabilized redispersible system exhibited improvement in the dissolution behavior under acidic conditions and enhancing the therapeutic potential of tranilast to treat liver dysfunction.110Solid nanodispersionDry media millingIngliforib, celecoxib furosemideII, IVNovel formulation approach combining two technologies, i.e .,solid dispersion and nanocrystal, and stabilized with PVP K12 and SDS.111Solid dispersionSpray drying techniqueTacrolimusIIThe formulation containing drug–Eudragit E exhibited higher drug solubility as it inhibits reprecipitation in neutral pH condition.112Solid dispersionLyophillization techniqueAtorvastatinIISolid dispersion formulation containing skimmed milk as a carrier in varying ratio has shown 33 fold increase in sol...…”

Section: Formulation Approaches For Manipulating Solubility and Permementioning

confidence: 99%

Understanding peroral absorption: regulatory aspects and contemporary approaches to tackling solubility and permeability hurdles

Shekhawat

Pokharkar

2017

Acta Pharmaceutica Sinica B

133

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Oral drug absorption is a process influenced by the physicochemical and biopharmaceutical properties of the drug and its inter-relationship with the gastrointestinal tract. Drug solubility, dissolution and permeability across intestinal barrier are the key parameters controlling absorption. This review provides an overview of the factors that affect drug absorption and the classification of a drug on the basis of solubility and permeability. The biopharmaceutical classification system (BCS) was introduced in early 90׳s and is a regulatory tool used to predict bioavailability problems associated with a new entity, thereby helping in the development of a drug product. Strategies to combat solubility and permeability issues are also discussed.

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“…Particle Size Distribution and Zeta potential Analysis: 33 Particle size, size distribution and zeta potential of diacerein nanosuspension were determined using Zetatrac (Microtrac Inc., USA). Zetatrac utilizes a high-frequency AC electric field to oscillate the charged particles.…”

Section: Differential Scanning Calorimetry (Dsc)mentioning

confidence: 99%

Untitled

2017

IJPSR

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ABSTRACT:Diacerein is an Osteoarthritic drug that exhibited suboptimal oral bioavailability upon oral administration of conventional dosage form. Nanosuspension gaining more attention for improving oral bioavailability of such drugs. This study was aimed to enhance the solubility and dissolution of diacerein by preparing Nanosuspension. Diacerein Nanosuspension was prepared using combination of High Speed Homogenization (HSH) and Media Milling (MM), Poloxamer 407 (stabilizer) and ZrO 2 beads (milling media). Various formulation and processing parameters were optimized in preliminary studies. Concentration of stabilizer and milling media were optimized for Cumulative percentage release (%CPR), saturation solubility (SS) and mean particle size (MPS) using 3 2 full factorial design. Optimized batch was derived statistically using desirability function of Minitab17. Model was validated by formulating checkpoint batch. Accelerated stability study was carried out for optimized batch. Identification and compatibility study of drug and stabilizers were carried out using FTIR and DSC studies. Preliminary parameters were optimized by varying one parameter at a time, while keeping other constant by trial and error method. Optimized batch has 100%w/v milling media and 1%w/v of Poloxamer407. %CPR, SS and MPS were found to be 97.74%, 1.245mg/ml and 221.5nm respectively. Four hundred times enhancement in SS that of bulk drug and 97.74%CPR at 2min was observed after nanonization. It was concluded that Combination of HSH and MM technique can be successfully used for preparation of Diacerein Nanosuspension. Prepared nanosuspension significantly enhances solubility and in-vitro dissolution of Diacerein.

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Effect of particle size on oral absorption of carvedilol nanosuspensions: in vitro and in vivo evaluation

Cited by 40 publications

References 30 publications

Preparation and evaluation of carvedilol-loaded solid lipid nanoparticles for targeted drug delivery

Preparation and evaluation of carvedilol-loaded solid lipid nanoparticles for targeted drug delivery

Understanding peroral absorption: regulatory aspects and contemporary approaches to tackling solubility and permeability hurdles

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