Design, optimization and characterization of coenzyme Q10- and D-panthenyl triacetate-loaded liposomes

Çelik, Burak; Sagiroglu, Ali Asram; Özdemir, Samet

doi:10.2147/ijn.s140835

Cited by 28 publications

(15 citation statements)

References 38 publications

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“…0.20 ± 0.001 indicated homogeneous population of liposomes (Table 2). This was in accordance with the studies of other authors who also achieved to develop Q 10 -loaded liposomes of particle size less than 200 nm and of satisfactory homogeneity [29,30]. The storage of liposomes LD1 at different temperatures (4 °C, RT and 40 °C) for 6 months revealed that their particle size did not change significantly when they were stored at 4 °C and RT, compared to their initial values.…”

Section: Characterization and Stability Evaluation Of The Q 10 -Loaded Liposome Dispersionssupporting

confidence: 92%

Development of hydrophilic gels containing coenzyme Q₁₀-loaded liposomes: characterization, stability and rheology measurements

Dragićević¹,

Krajišnik

Milić

et al. 2018

Drug Development and Industrial Pharmacy

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Section: Characterization and Stability Evaluation Of The Q 10 -Loaded Liposome Dispersionssupporting

confidence: 92%

Development of hydrophilic gels containing coenzyme Q₁₀-loaded liposomes: characterization, stability and rheology measurements

Dragićević¹,

Krajišnik

Milić

et al. 2018

Drug Development and Industrial Pharmacy

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“…S4 ). The aqueous solubility of CoQ 10 by itself is reported to be around 0.7 ng/ml [ 66 ]. Therefore, a CoQ 10 concentration of >2 mM indicates an >2.4 × 10 6 fold increase of solubility.…”

Section: Resultsmentioning

confidence: 99%

Micellization of coenzyme Q by the fungicide caspofungin allows for safe intravenous administration to reach extreme supraphysiological concentrations

Wang¹,

Hekimi²

2020

Redox Biology

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Coenzyme Q 10 (CoQ 10 ; also known as ubiquinone) is a vital, redox-active membrane component that functions as obligate electron transporter in the mitochondrial respiratory chain, as cofactor in other enzymatic processes and as antioxidant. CoQ 10 supplementation has been widely investigated for treating a variety of acute and chronic conditions in which mitochondrial function or oxidative stress play a role. In addition, it is used as replacement therapy in patients with CoQ deficiency including inborn primary CoQ 10 deficiency due to mutations in CoQ 10 -biosynthetic genes as well as secondary CoQ 10 deficiency, which is frequently observed in patients with mitochondrial disease syndrome and in other conditions. However, despite many tests and some promising results, whether CoQ 10 treatment is beneficial in any indication has remained inconclusive. Because CoQ 10 is highly insoluble, it is only available in oral formulations, despite its very poor oral bioavailability. Using a novel model of CoQ-deficient cells, we screened a library of FDA-approved drugs for an activity that could increase the uptake of exogenous CoQ 10 by the cell. We identified the fungicide caspofungin as capable of increasing the aqueous solubility of CoQ 10 by several orders of magnitude. Caspofungin is a mild surfactant that solubilizes CoQ 10 by forming nano-micelles with unique properties favoring stability and cellular uptake. Intravenous administration of the formulation in mice achieves unprecedented increases in CoQ 10 plasma levels and in tissue uptake, with no observable toxicity. As it contains only two safe components (caspofungin and CoQ 10 ), this injectable formulation presents a high potential for clinical safety and efficacy.

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“…Response was predicted by the following quadratic polynomial equation ( Equation 4 ):

where Y represents the predicted response, A and B indicate the independent variables, β 0 is the intercept value, β 1 and β 2 are linear coefficients of the model, β 12 is interaction coefficient, while β 11 and β 22 are quadratic coefficients. 28 , 29 …”

Section: Methodsmentioning

confidence: 99%

Risperidone mucoadhesive buccal tablets: formulation design, optimization and evaluation

Çelik

2017

DDDT

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The aim of this study was to design and optimize risperidone (RIS) mucoadhesive buccal tablets for systemic delivery as an alternative route. Direct compression method was used for the preparation of buccal tablets, and screening studies were conducted with different polymers to determine their effects on tablet characteristics. Carbopol® (CP) and sodium alginate (SA) were selected as two polymer types for further optimization studies by applying response surface methodology. Tablet hardness (TH), ex vivo residence time (RT), and peak detachment force (DF) from buccal mucosa were selected as three important responses. Physicochemical compatibility of formulation excipients and RIS was evaluated by using Fourier transform infrared (FT-IR) spectroscopy and differential scanning calorimetry (DSC) analysis. In vitro drug release profiles and release kinetics were investigated; swelling index and matrix erosion studies were conducted. Optimum formulation consisted of 16.4% CP and 20.3% SA, which provided 7.67±0.29 hour ex vivo RT, 45.52±4.85 N TH, and 2.12±0.17 N DF. FT-IR spectroscopy and DSC analysis revealed that there was no chemical interaction present between tablet ingredients. Cumulative RIS release of >90% was achieved after 8 hours of in vitro dissolution studies, which was supported by swelling and matrix erosion analysis. Mechanism of RIS release was fitted best to zero-order model, while release exponent (n) value of 0.77 demonstrated an anomalous (non-Fickian) release, indicating combined erosion and swelling mechanism. The results suggested that optimized buccal tablets of RIS would be a promising and alternative delivery system for the treatment of schizophrenia.

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Design, optimization and characterization of coenzyme Q10- and D-panthenyl triacetate-loaded liposomes

Cited by 28 publications

References 38 publications

Development of hydrophilic gels containing coenzyme Q₁₀-loaded liposomes: characterization, stability and rheology measurements

Development of hydrophilic gels containing coenzyme Q₁₀-loaded liposomes: characterization, stability and rheology measurements

Micellization of coenzyme Q by the fungicide caspofungin allows for safe intravenous administration to reach extreme supraphysiological concentrations

Risperidone mucoadhesive buccal tablets: formulation design, optimization and evaluation

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Design, optimization and characterization of coenzyme Q10- and D-panthenyl triacetate-loaded liposomes

Cited by 28 publications

References 38 publications

Development of hydrophilic gels containing coenzyme Q10-loaded liposomes: characterization, stability and rheology measurements

Development of hydrophilic gels containing coenzyme Q10-loaded liposomes: characterization, stability and rheology measurements

Micellization of coenzyme Q by the fungicide caspofungin allows for safe intravenous administration to reach extreme supraphysiological concentrations

Risperidone mucoadhesive buccal tablets: formulation design, optimization and evaluation

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Development of hydrophilic gels containing coenzyme Q₁₀-loaded liposomes: characterization, stability and rheology measurements

Development of hydrophilic gels containing coenzyme Q₁₀-loaded liposomes: characterization, stability and rheology measurements