Association between the physical stability of flurbiprofen suspension and the interaction of HPMC/SDS

The anionic surfactant sodium dodecylsulfate (SDS) has improved the physical stability of flurbiprofen (FBP) suspension, which was suspended by 0.2% (w/v) hydroxypropylmethyl cellulose (HPMC, K4M). Therefore, the physical stability of FBP suspensions and the interaction of HPMC/SDS were studied, and a certain association between them was revealed. The anti-solvent precipitation method was used to prepare suspensions. The apparent drug concentration from different sites was evaluated to get the dispersion of drug actually. The process of flocculation and deflocculation with the addition of SDS was caught by analyzing the morphology of the suspended particles. The physical stability of the FBP suspensions was characterized mainly by measuring the re-dispersion time, the zeta potential and particle size. Meanwhile, conductivity measurements were carried out to obtain the characteristic concentrations of SDS in HPMC/SDS system. The viscosities, the abilities for improving the solubility and wettability of FBP in the separate and mixed HPMC/SDS solutions were also contrasted respectively. The suspensions prepared with HPMC/SDS possessed better physical stability. The suspensions were uniform when the concentration of SDS was between the critical adsorption concentration (CAC) and the polymer saturation point (PSP). After PSP, the uniformity became worse and worse until the SDS was enough to form a deflocculation state. Besides, the re-dispersion time of FBP suspensions was longest when the concentration of SDS around CAC and shorter by shorter after the critical micelle concentration (CMC). The article provided a new sight on the relation between the interaction of excipient matrix and pharmaceutical preparations.     

Novel montelukast sodium-loaded stable oral suspension bioequivalent to the commercial granules in rats

To develop a montelukast sodium–loaded stable oral suspension bioequivalent to the commercial granules in rats, several montelukast sodium-loaded suspensions were prepared with a suspending agent, stabilizers and anti-aggregation agents, and their stabilities were investigated by visually observing the sedimentation phenomenon and determining the concentration of the degradation product. Moreover, dissolution and pharmacokinetic studies of the optimized formulation were examined in rats compared to commercial montelukast sodium-loaded granules. Avicel RC-591 (Avicel), a suspending agent, prevented the sedimentation of these suspensions at >2.496 (w/v) per cent composition. Amongst the stabilizers tested, fumaric acid provided the lowest concentration of montelukast sulphoxide (a degradation product) in these suspensions at 40 °C, demonstrating its excellent stabilizing activity. Furthermore, as an anti-aggregation agent, glycerin gave lower amounts of degradation product than those with poloxamer 407 and Tween 80. In particular, montelukast-loaded oral suspension, an aqueous suspension containing montelukast sodium/Avicel/fumaric acid/glycerin at a concentration of 312/2496/15.6/62.4 (mg/100 ml), and the commercial granules exhibited similar dissolution profiles in 0.5 % (w/v) aqueous solution of sodium lauryl sulphate. Moreover, the pharmacokinetics in rats provided by this suspension was comparable to that of the commercial granules, suggesting that they were bioequivalent. In addition, it was physically and chemically stable at 40 °C for at least 6 months. Thus, this montelukast sodium-loaded oral suspension, with bioequivalence to the commercial granules and excellent stability, could be a prospective dosage form for the treatment of asthma.     

萘丁美酮干混悬剂的制备及其初步稳定性研究

目的　制备萘丁美酮干混悬剂。方法　考察常用的羟丙基甲基纤维素、羧甲基纤维素钠、聚维酮、黄原胶、甲基纤维素等辅料对干混悬剂的影响。通过对其沉降体积比、再分散性指标的考察 ,筛选了 2 %HPMC助悬剂 ,并从流变学、混悬剂黏度及显微形态等方面对其稳定性进行了研究。同时考察了药物加速实验下粒子形态的稳定性。结果　所制干混悬剂工艺简单、稳定性良好 ,形成的混悬液符合干混悬剂的各项质量指标。结论　所制备的萘丁美酮干混悬剂可达到干混悬剂要求 ,制剂质量稳定。     

富马酸氯马斯汀干混悬剂的制备及稳定性研究

目的：制备富马酸氯马斯汀干混悬剂。方法：考察常用的羟丙基甲基纤维素(HPMC)、羧甲基纤维素钠(CMC-Na)、聚维酮(PVPK90)、黄原胶、甲基纤维素(MC)等辅料对干混悬剂的影响。通过对其沉降体积比、再分散性指标的考察，筛选了2％HPMC作为助悬剂，从流变学、混悬剂黏度及显微形态的观察对其稳定性进行研究。同时考察了药物在加速试验下粒子形态的稳定性。结果：所制干混悬剂工艺简单、稳定性良好，形成混悬液，符合干混悬剂的各项质量标准。结论：本品达到干混悬剂要求，制剂质量稳定。     

消旋卡多曲干混悬液的制备与稳定性考察

目的 制备消旋卡多曲干混悬液. 方法 考察常用的羟丙基甲基纤维素（HPMC）、羧甲基纤维素钠、聚维酮、黄原胶、甲基纤维素等辅料对干混悬液的影响.通过对其沉降体积比、再分散性指标的考察,筛选了2%HPMC助悬剂,并从流变学、混悬液黏度及显微形态等方面对其稳定性进行了研究. 同时考察药物加速实验下粒子形态的稳定性.结果 所制干混悬液工艺简单、稳定性良好,形成的混悬液符合干混悬液的各项质量指标. 结论 该法所制备的消旋卡多曲干混悬液可达到干混悬液要求,制剂质量稳定.     

Formulation and evaluation of reconstitutable suspensions containing ibuprofen-loaded Eudragit microspheres

The objective of this work was to develop and evaluate reconstitutable suspensions of ibuprofen-loaded microspheres prepared with an acrylic polymer (Eudragit RS-PM). The microspheres were prepared by the quasi-emulsion solvent diffusion technique. To prepare reconstitutable suspension formulation, the microspheres used had a mean particle size of 316.6 microm and 99.8% loading efficiency. Xanthan gum was chosen as the suspending agent for the suspension formulations. D-sorbitol was used to impart palatability of suspensions. The amount of D-sorbitol affected sedimentation volume and redispersibility properties of suspensions. The highest improving effect was shown with 20.0% and 25.0% of D-sorbitol concentrations. It was observed that dispersion media of suspensions showed non-Newtonian flow characteristics. To ensure minimum drug leakage from the microspheres into the suspension, the pH was buffered at 3.60 using citrate buffer. The ibuprofen content calculated from the suspended microspheres was consistent with that from microspheres alone. This result indicated that no leakage of drug occurred from the microspheres in the suspension on storage. Moreover, the same release rate of ibuprofen from the microspheres suspension and microspheres alone indicated that the suspension medium studied did not affect the property of drug release. This study suggested that stable suspensions of ibuprofen-loaded microspheres could be formulated with 0.6% w/v xanthan gum by the addition of 20% w/v D-sorbitol.     

Assessment of the precorneal residence of an ophthalmic ointment in healthy subjects.

1. The precorneal residence of an ophthalmic ointment radiolabelled by inclusion of technetium-99m tin colloid was assessed in seven volunteer subjects using the technique of gamma scintigraphy and compared with a solution of 0.3% w/v hydroxypropylmethylcellulose, (HPMC) radiolabelled by inclusion of technetium-99m diethylenetriaminepentaacetic acid in the same subjects. 2. The mean half-times (+/- s.d.) of corneal residence were 6490 +/- 5404 s (108 min) for the ointment and 13 +/- 24 s for the 0.3% w/v HPMC solution (P < 0.01). 3. The area-under-curve value (AUC(0,540 s)), which reflects the total residence time of the preparation on the ocular surface, was calculated for each vehicle in each subject. The mean (+/- s.d.) AUC(0,540 s) value for the ointment was 42170 (+/- 5032)% s and for the 0.3% w/v HPMC solution it was 8394 (+/- 4641)% s (P < 0.01).     

Effect of cyclodextrins on the complexation and nasal permeation of melatonin

The inclusion complexation of melatonin (MT) with modified cyclodextrins (CDs) was studied with an objective of improving the solubility and nasal absorption of MT. The formation of inclusion complex of MT with Hydroxypropyl beta CD (HPbeta CD) and randomly methylated beta CD (RMbeta CD) was characterized in solution and solid states by phase solubility and differential scanning calorimetry analyses. The phase solubility data indicate a linear increase in the solubility of MT with CDs demonstrating Higuchi's A(L)-type phase solubility profiles. The effect of CDs on the permeation of MT across EpiAirway(TM)-100 cultures was studied using a modified nonstatic diffusion setup. CDs were employed at different concentrations with 1% w/v micronized MT suspension in hydroxypropyl methyl cellulose (HPMC) vehicle. At low CD concentrations (1% w/v), the permeation of MT from HPMC formulation was significantly increased (125%,p < .001). However, the permeation was significantly reduced when CDs were used at relatively high concentrations (5 to 10% w/v concentration for HPbetaCD and 10% w/v concentration for RMbetaCD,p < .001). All the tissues were viable with good tissue integrity at the end of permeation experiments, as measured by methylthiazoletetrazolium assay and transepithelial electrical resistance measurements. In conclusion, formation of inclusion complex of MT with HPbetaCD and RMbetaCD was demonstrated in solution and solid state. Both HPbetaCD and RM betaCD at 1% w/v concentration were found to improve the nasal permeability of MT from HPMC gel formulations.     

水飞蓟素混悬剂的制备及稳定性和溶出度考察

目的:制备和初步筛选水飞蓟素混悬剂并对其物理稳定性和溶出度进行评价。方法:采用研磨法制备水飞蓟素混悬剂,并考察了处方因素对混悬剂稳定性以及释放度等的影响。结果:当水飞蓟素混悬剂中甘油用量为4%、羧甲基纤维素钠为1%和聚乙烯吡咯烷酮为12%时,沉降容积比、黏度和再分散性分别为90%,48mPa·s和100%。甘油和聚乙烯吡咯烷的加入使水飞蓟素在2min内累积释放量迅速达到20%以上。结论:初步确立水飞蓟素混悬剂的处方,其物理稳定性良好,且体外释放与同类水飞蓟素制剂比较有明显提高。     

New surface-active polymers for ophthalmic formulations: evaluation of ocular tolerance.

Two n-octenylsuccinate starch (AS) types of unknown molecular weights were assessed for ocular tolerance. Irritation potential of different solutions (containing 2 and 15% (w/w) AS) and AS stabilized emulsions (containing 15% (w/w) AS) was evaluated in vivo in rabbit eyes, using a confocal laser scanning microscope, and in vitro on treated excised pig corneas by light microscopy of histological cross sections. Both AS types were previously characterized by viscosity, osmolality and surface tension measurements. All tested solutions and emulsions showed good eye tolerance regardless of concentration and emulsifying properties suggesting AS to be a good alternative to commonly used solubilizing or emulsifying agents in ophthalmic formulations.     

The relation between narrow-dispersed microcapsules and surfactants

Electric ink display is one of the prospect technologies in paper-like display. In this paper, electric ink microcapsules are prepared by means of an in situ polymerization and complex coacervation. In order to obtain the microcapsules in a uniform size distribution, this study focused on the inter-facial tension between tetrachloroethylene and water solution, the dispersion of the core droplets and the microencapsulation with different kind of surfactants. By measuring the inter-facial tensions between water and tetrachloroethylene, it is found that urea-formaldehyde (UF) pre-polymer presents certain surface activity due to the inter-facial tension descending from 43 mN m(-1) to 35 mN m(-1). Because the surface activity of pre-polymer is not valid, the water-soluble emulsifiers can occupy on the surface of the droplets and prevent the UF resin depositing there. The analysis of the size distribution shows that the UF microcapsules are multi-dispersed. Furthermore, the influence of anionic surfactant of SDS on the size distribution of the core droplets is also investigated. The average diameters of the core droplets prepared with 0.005 wt% and 0.012 wt% SDS are approximately 50 microm and 28 microm, respectively. That reveals the existence of SDS not only decreases the droplet diameters, but also makes the size distribution centralized. Because the surface of the core droplets is charged due to the absorption of SDS anionic, the Gelatin and Gum Arabic (GA) coacervating layer is easy to form there. The size of the GA microcapsules prepared with 0.003 wt% SDS is approximately 65 microm. Finally; the responsive behaviour of the microcapsules to electric field is also investigated.     

The relation between narrow-dispersed microcapsules and surfactants

Electric ink display is one of the prospect technologies in paper-like display. In this paper, electric ink microcapsules are prepared by means of an in situ polymerization and complex coacervation. In order to obtain the microcapsules in a uniform size distribution, this study focused on the inter-facial tension between tetrachloroethylene and water solution, the dispersion of the core droplets and the microencapsulation with different kind of surfactants. By measuring the inter-facial tensions between water and tetrachloroethylene, it is found that urea-formaldehyde (UF) pre-polymer presents certain surface activity due to the inter-facial tension descending from 43?mN?m^?1 to 35?mN?m^?1. Because the surface activity of pre-polymer is not valid, the water-soluble emulsifiers can occupy on the surface of the droplets and prevent the UF resin depositing there. The analysis of the size distribution shows that the UF microcapsules are multi-dispersed. Furthermore, the influence of anionic surfactant of SDS on the size distribution of the core droplets is also investigated. The average diameters of the core droplets prepared with 0.005?wt% and 0.012?wt% SDS are?～50?µm and 28?µm, respectively. That reveals the existence of SDS not only decreases the droplet diameters, but also makes the size distribution centralized. Because the surface of the core droplets is charged due to the absorption of SDS anionic, the Gelatin and Gum Arabic (GA) coacervating layer is easy to form there. The size of the GA microcapsules prepared with 0.003?wt% SDS is?～65?µm. Finally; the responsive behaviour of the microcapsules to electric field is also investigated.     

Effect of polymer molecular weight on the production of drug nanoparticles

Stable, polymer-coated nanoparticles of two hydrophobic drugs, namely nabumetone and halofantrine, have been prepared by a wet-bead milling process performed in the presence of a stabilizing homopolymer, either hydroxypropylmethylcellulose (HPMC) or polyvinylpyrrolidone (PVP), of differing molecular weights and concentrations. Although nabumetone nanoparticles could only be produced when HPMC was used as stabilizing polymer, halofantrine nanoparticles could be prepared using either HPMC or PVP. Stable nanoparticles of nabumetone could be produced using a HPMC solution of viscosity average molecular weight, M(v), of 5 kg/mol over an approximate four fold polymer concentration range (0.63-2.5% w/w) when a drug loading of 20% w/w was used. Increasing the molecular weight of HPMC up to a limiting M(v) of 89 kg/mol did not result in the formation of nanoparticles at any of the polymer concentrations examined. The amount of polymer absorbed onto the nanoparticles was determined by measuring the depletion of polymer from solution based on either an ultra-violet (PVP) or optical rotatory dispersion (ORD) (HPMC) assay. The slightly lower concentration of HMPC found to be present on the surface of the halofantrine nanoparticles compared with the nabumetone nanoparticles suggested a differing affinity of the polymer for the surface of the two drugs.     

Stability of allopurinol and of five antineoplastics in suspension

The stability of allopurinol, azathioprine, chlorambucil, melphalan, mercaptopurine, and thioguanine each in an extemporaneously prepared suspension was studied. Tablets of each drug were crushed, mixed with a suspending agent, and brought to a final volume of 10, 15, or 20 ml with a 2:1 mixture of simple syrup and wild cherry syrup. Suspensions were prepared in the following concentrations: allopurinol (20 mg/ml), azathioprine (50 mg/ml), chlorambucil (2 mg/ml), melphalan (2 mg/ml), mercaptopurine (50 mg/ml), and thioguanine (40 mg/ml). Using high-performance liquid chromatography or ultraviolet scans, duplicate assays were performed on each suspension periodically during storage for up to 84 days at ambient room temperature or 5 degrees C. The time required for the suspensions to drop below 90% of labeled strength was used as an indicator of drug stability. Allopurinol and azathioprine were stable for at least 56 days at room temperature and at 5 degrees C. Chlorambucil decomposed rapidly at room temperature but was stable for seven days when stored at 5 degrees C. Melphalan suspensions did not meet the stated criteria for stability even at the time of initial assay. Mercaptopurine and thioguanine were stable for 14 and 84 days, respectively, at room temperature; at 5 degrees C, assay values dropped below those obtained at room temperature. In the suspension formulation tested, allopurinol, azathioprine, mercaptopurine, and thioguanine are stable for at least 14 days at room temperature; chlorambucil suspensions should be refrigerated and discarded after seven days. Melphalan decomposes too rapidly to make this suspension formulation feasible for extemporaneous compounding.     

Considerations in the use of hydroxypropyl-beta-cyclodextrin in the formulation of aqueous ophthalmic solutions of hydrocortisone.

The in vivo ocular bioavailability of hydrocortisone (HC) in the NZW rabbit was determined following topical administration of solutions containing HC (1%) with hydroxypropyl-beta-cyclodextrin (HP-beta-CD) alone, or containing the mucoadhesive, viscosity enhancing polymers sodium hyaluronate (0.2 and 0.5% w/v) or Carbopol 934P (0.1% w/v). A 1% HC suspension was used as control. Formulation of HC as a solution with HP-beta-CD in the absence of polymer increased the bioavailability of HC in the aqueous humour by approximately 55% and cornea by 75% when compared to suspension. Inclusion of either polymer did not result in any further increase in ocular bioavailability over that noted for the polymer-free solution. The in vitro corneal permeability of HC was also evaluated. A linear relationship (r(2)=0.999) was noted between corneal permeability and the concentration of free (uncomplexed) HC in solution. Permeability was greatest when formulated either as a suspension, or as an HP-beta-CD solution in which the concentration of free (uncomplexed) HC is equivalent to that of a saturated solution. Thus, when using cyclodextrins in the reformulation of ophthalmic suspensions as solutions, consideration must be given to the concentration of cyclodextrin used and to the benefits of including viscosity enhancing polymers.     

Effect of Formulation on the Rheology of Theophylline Compound Suspensions in Gelucires

The theophylline derivatives, etofylline, diprophylline and proxyphylline, which exhibit increasing aqueous solubitity, were used to prepare suspensions in seven saturated polyglycolysed glycerides (Gelucires) characterized by their rising hydrophilic-lipophilic balance (HLB). Drug concentration was set at 25% w/w and the production temperature was set at the Gelucire melting point plus 30°C in order to obtain suitable suspensions. Various formulation factors were studied. Ostwald flow indices revealed that the suspensions had a thixotropic shear-thinning behaviour and a relative viscosity which increased as drug aqueous solubility rose and Gelucire HLB decreased. These rheological properties could be explained by the chemical composition of Gelucires and drugs used. A microstructure was proposed for the liquid suspension such that colloidal particles and aggregates formed in these suspensions directly influenced the observed rheological properties. Observation of solidified suspensions by scanning electron microscopy confirmed this hypothesis. Moreover, a correlation between the relative viscosity of drug suspensions on the one hand and drug concentration, drug solubility and Gelucire HLB on the other allowed for the calculation of the required concentration of each theophylline derivative in each Gelucire to obtain a given viscosity.     

Oral delivery of diclofenac sodium using a novel solid-in-oil suspension

The present work reports on a new pharmaceutical formulation for oral delivery of diclofenac sodium (DFNa), a non-steroidal anti-inflammatory drug (NSAID). Although DFNa itself is water-soluble at neutral pH, it was readily suspended in soybean oil via complex formation with an edible lipophilic surfactant and a matrix protein. The resulting solid-in-oil (S/O) suspension containing stably encapsulated DFNa in an oil phase markedly reduced the risks for gastrointestinal ulcers upon oral administration even at the LD(50) level in rats (ca. 50 mg/kg DFNa). In addition, plasma concentration of DFNa upon administration of an S/O suspension was comparable with that of the aqueous counterpart at the same DFNa dose. These results indicate the potential use of S/O suspensions as novel oil-based pharmaceutical formulations for oral delivery of water-soluble drugs without causing severe mucitis.     

A predictive model for the release of slightly water-soluble drugs from HPMC matrices

A model to predict the fraction of slightly water-soluble drug released as a function of release time (t, h), HPMC concentration (C(H), w/w), drug solubility in distilled water at 37 degrees C (C(s), g/100 mL), and volume of drug molecule (V, nm3) was derived when theophyline, tinidazole, and propylthiouracil were selected as model drugs. The model is log (M(t)/M(infinity)) = 0.8683 logt-0.1930C(s) logt + 0.5406V logt-1.227C(H) + 0.1594C(s) + 0.4423C(H)C(s) - 0.8655 (n = 130, r = 0.9969), where Mt is the amount of drug released at time t, Minfinity is the amount of drug released over a very long time, which corresponds in principle to the initial loading, n is the number of samples, and r is the correlation coefficient. The model was validated using sulfamethoxazole and satisfactory results were obtained. The model can be used to predict the release fraction of variousslightly water-soluble drugs from HPMC matrices having different polymer levels.     

Solubilization of tropicamide by hydroxypropyl-beta-cyclodextrin and water-soluble polymers: in vitro/in vivo studies

1% (w/v) aqueous solutions of tropicamide (TR), a poorly water-soluble mydriatic-cycloplegic drug, are usually obtained by adjusting the pH to approximately 5.0, at the expense, however, of ocular tolerance and bioavailability. The capacity of hydroxypropyl-beta-cyclodextrin (HP-beta-CD) to solubilize TR in pH 7.4 0.02 M phosphate buffer was investigated in the absence and presence of hydrophilic polymers (PVP, CMC and HPMC). Approximately 3.5% (w/v) HP-beta-CD was required to solubilize 1% (w/v) TR in pH 7.4 buffer at room temperature. The required amount was reduced to 0.9% (w/v) by heating at 120 degrees C in the presence of 0.1% (w/v) HPMC. Mydriatic activity tests in rabbits showed an improved bioavailability and maximal mydriatic response for two CD formulations, with and without HPMC, when compared to standard 1% (w/v) TR eyedrops, buffered at pH 5.0. The improved in vivo behaviour of the CD formulations are likely due to their physiological pH, resulting in a reduced irritant effect, although an effect of HP-beta-CD on corneal permeability cannot be dismissed a priori.