Your search keyword '"Ketoprofen chemistry"' showing total 635 results

1. Modulation of chondroprotective hyaluronic acid and poloxamer gel with Ketoprofen loaded transethosomes: Quality by design-based optimization, characterization, and preclinical investigations in osteoarthritis.

Author

Mammella A, Bhavana V, Chary PS, Anuradha U, and Mehra NK

Subjects

Animals, Rats, Male, Rats, Wistar, Hyaluronic Acid chemistry, Hyaluronic Acid pharmacology, Ketoprofen pharmacology, Ketoprofen chemistry, Osteoarthritis drug therapy, Osteoarthritis pathology, Poloxamer chemistry, Poloxamer pharmacology, Gels chemistry

Abstract

Osteoarthritis (OA) is a chronic joint disease that results in biomechanical and morphological changes that contribute to cartilage degradation. Ketoprofen (KP), used in the treatment of OA, is a selective inhibitor of cyclooxygenase-2 (COX-2). Topical administration of KP bypasses gastric irritation as well as first-pass metabolism and increases localized delivery. The research intricates fabrication and optimization of KP-loaded transethosomes (KP-TEs) via Taguchi orthogonal array design and Central composite design (CCD). The optimized KP-TEs depicted an average vesicle size of 110.0 ± 1.70 nm, poly dispersibility index (PDI) of 0.103 ± 0.01, zeta potential -6.08 ± 0.27 mV, and conductivity of 0.049 ± 0.0001 mS/cm. The optimized KP-TEs were loaded in composite hyaluronic acid (HA) and poloxamer 407 (Px407) for an improvement of osteotrophic and chondroprotective transethosomal gel. The drug content of KP-TEs-HA/Px407 gel was found to be 90.08 ± 1.25 %. Preclinical research has been carried out by using the monosodium iodoacetate to develop model for osteoarthritis in male wistar rats. The X-ray imaging of KP-TEs-HA/Px407 gel treated group showed intact meniscus, healthy articular joint, and normal synovial lining same as the healthy control group. The IL - 1β IL-6, IL-22, TNF-α, and IL-10, levels, X-ray imaging, and studies on histopathology demonstrated the effectiveness of transethosomal gel in reducing pain and inflammation., Competing Interests: Declaration of competing interest Regarding this article, the authors disclosed no conflicts of interest., (Copyright © 2024 Elsevier B.V. All rights reserved.)

Published

2024

2. Surfactant-Assisted Wet Granulation-Based Matrix Tablets without Exceptional Additives: Prolonging Systemic Exposure of Model BCS Class II Ketoprofen.

Author

Shamim R, Shafique S, Hussain K, Abbas N, Ijaz S, and Bukhari NI

Subjects

Humans, Male, Adult, Anti-Inflammatory Agents, Non-Steroidal pharmacokinetics, Anti-Inflammatory Agents, Non-Steroidal administration & dosage, Anti-Inflammatory Agents, Non-Steroidal chemistry, Chemistry, Pharmaceutical methods, Young Adult, Polyethylene Glycols chemistry, Polyvinyls chemistry, Drug Compounding methods, Drug Liberation, Area Under Curve, Excipients chemistry, Ketoprofen administration & dosage, Ketoprofen pharmacokinetics, Ketoprofen chemistry, Tablets, Surface-Active Agents chemistry, Delayed-Action Preparations pharmacokinetics, Delayed-Action Preparations administration & dosage, Solubility, Biological Availability

Abstract

The present study was aimed to ameliorate the issue of solubility and thereby, bioavailability of ketoprofen, a BCS Class II drug. The sustained release matrix tablets (MT) were prepared using surfactant-assisted wet granulation (SAWG) with 1-5% of different surfactants. The tablet characteristics were within the compendial limits. The selected sustained release-compliant matrix tablet formulation containing granules prepared using 3% Soluplus® (MT2) released the drug by swelling-erosion. In human volunteers, MT2 attained the maximum plasma concentration (C max ) of 5.72µg /ml ± 0.30 h, time to C max (T max ) of 5.56 ± 0.30 h and maintained the plasma concentration above its minimum effective concentration (MEC), 0.7 µg.ml -1 till 24h. A control formulation, prepared from granules without surfactant (MT16), promptly attained C max of 9.62 ± 0.76 µg/ml within 1h but rapidly declined to below MEC in 8h. Area under the curve from initial point to infinity (AUC 0-∞ ) of MT2 (78.65 ± 7.64 µg.h.ml -1 ) was 2.29 folds higher than 34.39 ± 3.06 µg.h.ml -1 of MT16. With decreased C max , increased AUC 0-∞ , delayed T max and retained ketoprofen concentration above MEC for longer time, MT2 corresponded with the in-vitro sustained drug release characteristic. There is a likelihood of administration of once-a-day single dose of MT2 without plasma fluctuations, expected from two doses of MT16. SAWG helped developing a swellable-erodible sustained release matrix tablet formulation of ketoprofen with the desired biopharmaceutical and pharmacokinetics properties, merely by addition of Soluplus® in granules and without incorporation of any special ingredients or the major manipulation of the formulative ingredients in the formulation., (© 2024. The Author(s), under exclusive licence to American Association of Pharmaceutical Scientists.)

Published

2024

3. Multiresponsive 4D Printable Hydrogels with Anti-Inflammatory Properties.

Author

Regato-Herbella M, Mantione D, Blachman A, Gallastegui A, Calabrese GC, Moya SE, Mecerreyes D, and Criado-Gonzalez M

Subjects

Mice, Animals, RAW 264.7 Cells, Ketoprofen chemistry, Ketoprofen pharmacology, Hydrogen-Ion Concentration, Methacrylates chemistry, Methacrylates pharmacology, Acrylamides chemistry, Acrylamides pharmacology, Reactive Oxygen Species metabolism, Temperature, Biocompatible Materials chemistry, Biocompatible Materials pharmacology, Printing, Three-Dimensional, Hydrogels chemistry, Hydrogels pharmacology, Anti-Inflammatory Agents pharmacology, Anti-Inflammatory Agents chemistry

Abstract

Multiresponsive hydrogels are valuable as biomaterials due to their ability to respond to multiple biologically relevant stimuli, i.e., temperature, pH, or reactive oxygen species (ROS), which can be present simultaneously in the body. In this work, we synthesize triple-responsive hydrogels through UV light photopolymerization of selected monomer compositions that encompass thermoresponsive N -isopropylacrylamide (NIPAM), pH-responsive methacrylic acid (MAA), and a tailor-made ROS-responsive diacrylate thioether monomer (EG 3 SA). As a result, smart P[NIPAM x - co -MAA y - co -(EG 3 SA) z ] hydrogels capable of being manufactured by digital light processing (DLP) 4D printing are obtained. The thermo-, pH-, and ROS-response of the hydrogels are studied by swelling tests and rheological measurements at different temperatures (25 and 37 °C), pHs (3, 5, 7.4, and 11), and in the absence or presence of ROS (H 2 O 2 ). The hydrogels are employed as matrixes for the encapsulation of ketoprofen (KET), an anti-inflammatory drug that shows a tunable release, depending on the hydrogel composition and stimuli applied. The cytotoxicity properties of the hydrogels are tested in vitro with mouse embryonic fibroblasts (NIH 3T3) and RAW 264.7 murine macrophage (RAW) cells. Finally, the anti-inflammatory properties are assessed, and the results exhibit a ≈70% nitric oxide reduction up to base values of pro-inflammatory RAW cells, which highlights the anti-inflammatory capacity of P[NIPAM 80 - co -MAA 15 - co -(EG 3 SA) 5 ] hydrogels, per se , without being necessary to encapsulate an anti-inflammatory drug within their network. It opens the route for the fabrication of customizable 4D printable scaffolds for the effective treatment of inflammatory pathologies.

Published

2024

4. Enhancing ketoprofen's solubility and anti-inflammatory efficacy with safe methyl-β-cyclodextrin complexation.

Author

Rajamohan R, Kamaraj E, Muthuraja P, Murugavel K, Govindasamy C, Prabakaran DS, Malik T, and Lee YR

Subjects

Animals, Spectroscopy, Fourier Transform Infrared, Rats, Ketoprofen chemistry, Ketoprofen pharmacology, beta-Cyclodextrins chemistry, Solubility, Anti-Inflammatory Agents, Non-Steroidal chemistry, Anti-Inflammatory Agents, Non-Steroidal pharmacology

Abstract

Improved solubility and anti-inflammatory (AI) properties are imperative for enhancing the effectiveness of poorly water-soluble drugs, particularly non-steroidal anti-inflammatory drugs (NSAIDs). To address these critical issues, our focus is on obtaining NSAID materials in the form of inclusion complexes (IC) with methyl-beta-cyclodextrin (MCD). Ketoprofen (KTP) is selected as the NSAID for this study due to its potency in treating various types of pain, inflammation, and arthritis. Our objective is to tackle the solubility challenge followed by enhancing the AI activity. Confirmation of complexation is achieved through observing changes in the absorbance and fluorescence intensities of KTP upon the addition of MCD, indicating a 1:1 stoichiometric ratio. Phase solubility studies demonstrated improved dissolution rates after the formation of ICs. Further analysis of the optimized IC is conducted using FT-IR, NMR, FE-SEM, and TG/DTA techniques. Notable shifts in chemical shift values and morphological alterations on the surface of the ICs are observed compared to their free form. Most significantly, the IC exhibited superior AI and anti-arthritic (AA) activity compared to KTP alone. These findings highlight the potential of ICs in expanding the application of KTP, particularly in pharmaceuticals, where enhanced stability and efficacy of natural AIs and AAs are paramount., (© 2024. The Author(s).)

Published

2024

5. Templated Nucleation of Clotrimazole and Ketoprofen on Polymer Substrates.

Author

Bellucci MA, Yuan L, Woollam GR, Wang B, Fang L, Zhou Y, Greenwell C, Sekharan S, Ling X, and Sun G

Subjects

Hydrogen Bonding, Kinetics, Machine Learning, Clotrimazole chemistry, Crystallization, Ketoprofen chemistry, Polymers chemistry, Molecular Dynamics Simulation

Abstract

The use of different template surfaces in crystallization experiments can directly influence the nucleation kinetics, crystal growth, and morphology of active pharmaceutical ingredients (APIs). Consequently, templated nucleation is an attractive approach to enhance crystal nucleation kinetics and preferentially nucleate desired crystal polymorphs for solid-form drug molecules, particularly large and flexible molecules that are difficult to crystallize. Herein, we investigate the effect of polymer templates on the crystal nucleation of clotrimazole and ketoprofen with both experiments and computational methods. Crystallization was carried out in toluene solvent for both APIs with a template library consisting of 12 different polymers. In complement to the experimental studies, we developed a computational workflow based on molecular dynamics (MD) and derived descriptors from the simulations to score and rank API-polymer interactions. The descriptors were used to measure the energy of interaction (EOI), hydrogen bonding, and rugosity (surface roughness) similarity between the APIs and polymer templates. We used a variety of machine learning models (14 in total) along with these descriptors to predict the crystallization outcome of the polymer templates. We found that simply rank-ordering the polymers by their API-polymer interaction energy descriptors yielded 92% accuracy in predicting the experimental outcome for clotrimazole and ketoprofen. The most accurate machine learning model for both APIs was found to be a random forest model. Using these models, we were able to predict the crystallization outcomes for all polymers. Additionally, we have performed a feature importance analysis using the trained models and found that the most predictive features are the energy descriptors. These results demonstrate that API-polymer interaction energies are correlated with heterogeneous crystallization outcomes.

Published

2024

6. A facile colorimetric sensor for ketoprofen detection in milk: Integrating molecularly imprinted polymers with Cu-doped Fe 3 O 4 nanozymes.

Author

Su Y, Yin X, Wei X, Xu R, Wei L, Chen Y, Ding L, and Song D

Subjects

Animals, Limit of Detection, Molecular Imprinting, Polymers chemistry, Milk chemistry, Colorimetry methods, Copper chemistry, Ketoprofen chemistry, Ketoprofen analysis, Food Contamination analysis, Molecularly Imprinted Polymers chemistry

Abstract

A facile and efficient detection method is required to address the potential health risks of ketoprofen (KP) in animal-derived foods. Herein, we integrated molecularly imprinted polymers (MIPs) with Cu-doped Fe 3 O 4 nanozymes (Fe 3 O 4 -Cu) to develop a selective colorimetric sensor for KP detection. Chitosan and glutaraldehyde were used as functional monomers and cross-linkers to fabricate proposed the MIPs@Fe 3 O 4 -Cu. On KP addition, it was specifically captured by the imprinted cavities, thereby blocking the channels between chromogenic substrates and Fe 3 O 4 -Cu. Based on this rationale, a selective colorimetric sensor utilizing MIPs@Fe 3 O 4 -Cu was established, exhibiting a linear range of 0.25-100 μM and a detection limit of 0.073 μM. The developed method was validated through its application in milk samples, yielding satisfactory recoveries with low relative standard deviations. This efficient and selective colorimetric sensor holds immense significance for KP detection in complex samples., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper. Acknowledgements This work was supported by the Natural Science Foundation of Jilin Province of China (No. 20220101061JC) and Jilin Provincial Science and Technology Development Plan Project (20230402022GH)., (Copyright © 2024. Published by Elsevier Ltd.)

Published

2025

7. Ozonolysis of ketoprofen in polluted water: Reaction pathways, kinetics, removal efficiency, and health effects.

Author

Mei Q, Qiu Z, Jiang J, Li M, Wang Q, and He M

Subjects

Kinetics, Anti-Inflammatory Agents, Non-Steroidal chemistry, Models, Chemical, Water Purification methods, Ketoprofen chemistry, Ozone chemistry, Water Pollutants, Chemical chemistry

Abstract

Ketoprofen (KET), as a non-steroidal anti-inflammatory drug frequently detected in aqueous environments, is a threat to human health due to its accumulation and low biodegradability, which requires the transformation and degradation of KET in aqueous environments. In this paper, the reaction process of ozone-initiated KET degradation in water was investigated using density functional theory (DFT) method at the M06-2X/6-311++g(3df,2p)//M06-2X/6-31+g(d,p) level. The detailed reaction path of KET ozonation is proposed. The thermodynamic results show that ozone-initiated KET degradation is feasible. Under ultraviolet irradiation, the reaction of ozone with water can also produce OH radicals (HO · ) that can react with KET. The degradation reaction of KET caused by HO · was further studied. The kinetic calculation illustrates that the reaction rate (1.99 × 10 -1 (mol/L) -1 sec -1 ) of KET ozonation is relatively slow, but the reaction rate of HO · reaction is relatively high, which can further improve the degradation efficiency. On this basis, the effects of pollutant concentration, ozone concentration, natural organic matter, and pH value on degradation efficiency under UV/O 3 process were analyzed. The ozonolysis reaction of KET is not sensitive to pH and is basically unaffected. Finally, the toxicity prediction of oxidation compounds produced by degradation reaction indicates that most of the degradation products are harmless, and a few products containing benzene rings are still toxic and have to be concerned. This study serves as a theoretical basis for analyzing the migration and transformation process of anti-inflammatory compounds in the water environment., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2023. Published by Elsevier B.V.)

Published

2025

8. Abietic acid antagonizes the anti-inflammatory effects of celecoxib and ketoprofen: Preclinical assessment and molecular dynamic simulations.

Author

Hasan R, Bhuia MS, Chowdhury R, Saha S, Khan MA, Afroz M, Ansari SA, Ansari IA, Melo Coutinho HD, and Islam MT

Subjects

Animals, Humans, Chickens, Anti-Inflammatory Agents chemistry, Anti-Inflammatory Agents pharmacology, Anti-Inflammatory Agents pharmacokinetics, Inflammation drug therapy, Inflammation metabolism, Erythrocytes drug effects, Erythrocytes metabolism, Celecoxib pharmacology, Celecoxib chemistry, Celecoxib pharmacokinetics, Molecular Dynamics Simulation, Ketoprofen pharmacology, Ketoprofen chemistry, Ketoprofen pharmacokinetics

Abstract

The present work is designed to explore the anti-inflammatory properties of AA and its modulatory effects on celecoxib (CEL) and ketoprofen (KET) through in vitro, ex vivo, in vivo, and in silico approaches. Different concentrations of AA were utilized to evaluate the membrane-stabilizing potential via egg albumin and the Human Red Blood Cell (HRBC) denaturation model. In the animal model, formalin (50 μL) was injected into the right hind paw of young chicks to induce inflammation. AA was administered at 20 and 40 mg/kg (p.o.) to the experimental animals. We used CEL and KET as positive controls. The vehicle was provided as a control group. Two combinations of AA with CEL and KET were also investigated in all tests to assess the modulatory activity of AA. In addition, in silico investigation was used for predictions about drug-likeness, pharmacokinetics, and toxicity of the selected chemical compounds, and the study also evaluated the binding affinity, visualization, and stability of ligand-receptor interactions through molecular dynamic (MD) simulation. Results manifested that AA concentration-dependently significantly inhibited the egg albumin denaturation (IC 50 : 27.53 ± 0.88 μg/ml) and breakdown of HRBC (IC 50 : 15.69 ± 0.75 μg/ml), indicating the membrane stabilizing potential compared to the control group. AA also significantly (p < 0.05) lessened the frequency of licking and alleviated the paw edema in a dose-dependent manner in an in vivo test. However, AA reduced the activity of CEL and KET in combination treatment. AA showed good pharmacokinetic characteristics to be considered as a therapeutic candidate. Additionally, the in silico study displayed that AA demonstrated a relatively higher docking score of -9.1 kcal/mol with the cyclooxygenase-2 (COX-2) enzyme and stable binding in MD simulation. Whereas the standard ligand (CEL) expressed the highest binding value of -9.2 kcal/mol to the COX-2., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financialinterestsor personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 Elsevier Ltd. All rights reserved.)

Published

2024

9. Computational exploration of novel ketoprofen derivatives: Molecular dynamics simulations and MM-PBSA calculations for COX-2 inhibition as promising anti-inflammatory drugs.

Author

Bettadj FZY, Benchouk W, and Guendouzi A

Subjects

Humans, Anti-Inflammatory Agents, Non-Steroidal chemistry, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Ketoprofen chemistry, Cyclooxygenase 2 metabolism, Cyclooxygenase 2 chemistry, Molecular Dynamics Simulation, Cyclooxygenase 2 Inhibitors chemistry, Cyclooxygenase 2 Inhibitors pharmacology

Abstract

Computer-aided drug design is widely employed to identify novel compounds for therapeutic applications. Ketoprofen (KTP), a commonly used and marketed nonsteroidal anti-inflammatory drug (NSAID), is effective in treating pain, fever, inflammation, and some cancers. In this research, we explored the behavior of six analogues designed by structurally modifying the KTP molecule. Specifically, KTP-A and KTP-B contain a -CN group at the ortho position, KTP-C and KTP-D have a -CN group at the meta position, and KTP-E and KTP-F feature a -CF 3 group at the meta position. To assess these analogues, we conducted molecular dynamics simulations (MD) to study their inhibitory effects on human cyclooxygenase 2 (COX-2), providing detailed insights into the structure and dynamics of the protein both with and without ligands. MD simulation, enhanced by technological advances, has proven to be a powerful tool for new drug discovery. We further quantified the binding affinity of these drug molecules toward COX-2 using molecular mechanics Poisson-Boltzmann surface area (MM-PBSA) binding free energy calculations. The dynamic properties were evaluated through analyses of root mean square deviations (RMSD), root mean square fluctuations (RMSF), radius of gyration (Rg), solvent-accessible surface area (SASA), covariance matrix, principal component analysis (PCA), and Gibbs free energy landscapes (FEL). Ultimately, this study confirms that the six KTP derivatives are promising candidates for the treatment of inflammation, with KTP-B standing out as particularly effective., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 Elsevier Ltd. All rights reserved.)

Published

2024

10. Modeling the Structure of Ketoprofen-Poly(vinylpyrrolidone) Amorphous Solid Dispersions with Empirical Potential Structure Refinements of X-ray Scattering Data.

Author

Wilke SK, Al-Rubkhi A, Benmore CJ, Byrn SR, and Weber R

Subjects

Crystallization, Chemistry, Pharmaceutical methods, Drug Compounding methods, Models, Molecular, Drug Stability, Ketoprofen chemistry, Povidone chemistry, X-Ray Diffraction methods

Abstract

The metastability of amorphous formulations poses barriers to their safe and widespread commercialization. The propensity of amorphous solid dispersions (ASDs) to crystallize is directly linked to their molecular structure. Amorphous structures are inherently complex and thus difficult to fully characterize by experiments, which makes structural simulations an attractive route for investigating which structural characteristics correlate with ASD stability. In this study, we use empirical potential structure refinement (EPSR) to create molecular models of ketoprofen-poly(vinylpyrrolidone) (KTP/PVP) ASDs with 0-75 wt % drug loading. The EPSR technique uses X-ray total scattering measurements as constraints, yielding models that are consistent with the X-ray data. We perform several simulations to assess the sensitivity of the EPSR approach to input parameters such as intramolecular bond rotations, PVP molecule length, and PVP tacticity. Even at low drug loading (25 wt %), ∼40% of KTP molecules participate in KTP-KTP hydrogen bonding. The extent of KTP-PVP hydrogen bonding does not decrease significantly at higher drug loadings. However, the models' relative uncertainties are too large to conclude whether ASDs' lower stabilities at high drug loadings are due to changes in drug-excipient hydrogen bonding or a decrease in steric hindrance of KTP molecules. This study illustrates how EPSR, combined with total scattering measurements, can be a powerful tool for investigating structural characteristics in amorphous formulations and developing ASDs with improved stability.

Published

2024

11. Revisiting and Updating the Interaction between Human Serum Albumin and the Non-Steroidal Anti-Inflammatory Drugs Ketoprofen and Ketorolac.

Author

Cunha RS, Cruz PF, Costa T, Almeida ZL, Lima MEF, Serpa C, and Chaves OA

Subjects

Humans, Circular Dichroism, Thermodynamics, Spectrometry, Fluorescence, Binding Sites, Ketoprofen chemistry, Ketoprofen metabolism, Ketoprofen pharmacokinetics, Anti-Inflammatory Agents, Non-Steroidal chemistry, Anti-Inflammatory Agents, Non-Steroidal metabolism, Anti-Inflammatory Agents, Non-Steroidal pharmacokinetics, Protein Binding, Ketorolac chemistry, Ketorolac metabolism, Ketorolac pharmacokinetics, Serum Albumin, Human chemistry, Serum Albumin, Human metabolism

Abstract

Ketoprofen (KTF) and ketorolac (KTL) are among the most primarily used non-steroidal anti-inflammatory drugs (NSAIDs) in humans to alleviate moderate pain and to treat inflammation. Their binding affinity with albumin (the main globular protein responsible for the biodistribution of drugs in the bloodstream) was previously determined by spectroscopy without considering some conventional pitfalls. Thus, the present work updates the biophysical characterization of the interactions of HSA:KTF and HSA:KTL by 1 H saturation-transfer difference nuclear magnetic resonance ( 1 H STD-NMR), ultraviolet (UV) absorption, circular dichroism (CD), steady-state, and time-resolved fluorescence spectroscopies combined with in silico calculations. The binding of HSA:NSAIDs is spontaneous, endothermic, and entropically driven, leading to a conformational rearrangement of HSA with a slight decrease in the α-helix content (7.1% to 7.6%). The predominance of the static quenching mechanism (ground-state association) was identified. Thus, both Stern-Volmer quenching constant ( K SV ) and binding constant ( K b ) values enabled the determination of the binding affinity. In this sense, the K SV and K b values were found in the order of 10 4 M -1 at human body temperature, indicating moderate binding affinity with differences in the range of 0.7- and 3.4-fold between KTF and KTL, which agree with the previously reported experimental pharmacokinetic profile. According to 1 H STD-NMR data combined with in silico calculations, the aromatic groups in relation to the aliphatic moiety of the drugs interact preferentially with HSA into subdomain IIIA (site II) and are stabilized by interactions via hydrogen bonding and hydrophobic forces. In general, the data obtained in this study have been revised and updated in comparison to those previously reported by other authors who did not account for inner filter corrections, spectral backgrounds, or the identification of the primary mathematical approach for determining the binding affinity of HSA:KTF and HSA:KTL.

Published

2024

12. Modified Release 3D-Printed Capsules Containing a Ketoprofen Self-Nanoemulsifying System for Personalized Medical Application.

Author

Shaqour B, Natsheh H, Kittana N, Jaradat N, Abualhasan M, Eid AM, Moqady R, AbuHijleh A, Abu Alsaleem S, Ratrout S, De Wever L, Vervaet C, and Vanhoorne V

Subjects

Humans, Polyethylene Glycols chemistry, Drug Delivery Systems methods, Delayed-Action Preparations, Methylcellulose chemistry, Methylcellulose analogs & derivatives, Polyvinyl Alcohol chemistry, Ketoprofen chemistry, Printing, Three-Dimensional, Precision Medicine methods, Capsules, Emulsions chemistry, Drug Liberation

Abstract

This study explores the realm of personalized medicine by investigating the utilization of 3D-printed dosage forms, specifically focusing on patient-specific enteric capsules designed for the modified release of ketoprofen, serving as a model drug. The research investigates two distinct scenarios: the modification of drug release from 3D-printed capsules crafted from hydroxypropyl methylcellulose phthalate:polyethylene glycol (HPMCP:PEG) and poly(vinyl alcohol) (PVA), tailored for pH sensitivity and delayed release modes, respectively. Additionally, a novel ketoprofen-loaded self-nanoemulsifying drug delivery system (SNEDDS) based on pomegranate seed oil (PSO) was developed, characterized, and employed as a fill material for the capsules. Through the preparation and characterization of the HPMCP:PEG based filament via the hot-melt extrusion method, the study thoroughly investigated its thermal and mechanical properties. Notably, the in vitro drug release analysis unveiled the intricate interplay between ketoprofen release, polymer type, and capsule thickness. Furthermore, the incorporation of ketoprofen into the SNEDDS exhibited an enhancement in its in vitro cylooxygenase-2 (COX-2) inhibitory activity. These findings collectively underscore the potential of 3D printing in shaping tailored drug delivery systems, thereby contributing significantly to the advancement of personalized medicine.

Published

2024

13. A new biphenol-dipicolylamine based ligand and its dinuclear Zn 2+ complex as fluorescent sensors for ibuprofen and ketoprofen in aqueous solution.

Author

Paderni D, Macedi E, Giacomazzo GE, Formica M, Giorgi L, Valtancoli B, Rossi P, Paoli P, Conti L, Fusi V, and Giorgi C

Subjects

Ligands, Water chemistry, Density Functional Theory, Phenols chemistry, Spectrometry, Fluorescence, Molecular Structure, Models, Molecular, Solutions, Zinc chemistry, Fluorescent Dyes chemistry, Fluorescent Dyes chemical synthesis, Coordination Complexes chemistry, Coordination Complexes chemical synthesis, Amines chemistry, Picolinic Acids chemistry, Ketoprofen chemistry, Ibuprofen chemistry

Abstract

In this work, the study of the new ligand 3,3'-bis[ N , N -bis(pyridine-2-ylmethyl)aminomethyl]-2,2'-dihydroxybiphenyl (L) is reported, where a central 2,2'-biphenol (BPH) fluorophore was functionalized at 3,3'-positions with two dipicolylamine (DPA) side arms as receptor units. Following the synthesis and full chemical-physical characterization, the acid-base and Zn 2+ -coordination abilities of L were investigated through a combination of potentiometric, UV-Vis, fluorescence, NMR, XRD and DFT measurements. The optical properties of the ligand turned out to be strongly dependent on the pH, being straightforwardly associated with the protonation state of the BPH moiety, whereas its peculiar design allowed to form stable mono and dinuclear Zn 2+ complexes. In the latter species, the presence of two Zn 2+ ions coordinatively unsaturated and placed at close distance to each other, prompted us to test their usefulness as metallo-receptors for two environmental pollutants of great relevance, ibuprofen and ketoprofen. Potentiometric and fluorescence investigations evidenced that these important non-steroidal anti-inflammatory drugs (NSAIDs) are effectively coordinated by the metallo-receptors and, of relevance, both the stability and the fluorescence properties of the resulting ternary adducts are markedly affected by the different chemical architectures of the two substrates. This study aims at highlighting the promising perspectives arising from the use of polyamino phenolic ligands as chemosensors for H + /Zn 2+ and other additional anionic targets in their metal-complexed forms.

Published

2024

14. Experimental and Machine-Learning-Assisted Design of Pharmaceutically Acceptable Deep Eutectic Solvents for the Solubility Improvement of Non-Selective COX Inhibitors Ibuprofen and Ketoprofen.

Author

Cysewski P, Jeliński T, Przybyłek M, Mai A, and Kułak J

Subjects

Cyclooxygenase Inhibitors chemistry, Hydrogen Bonding, Solvents chemistry, Ketoprofen chemistry, Ibuprofen chemistry, Solubility, Machine Learning, Deep Eutectic Solvents chemistry

Abstract

Deep eutectic solvents (DESs) are commonly used in pharmaceutical applications as excellent solubilizers of active substances. This study investigated the tuning of ibuprofen and ketoprofen solubility utilizing DESs containing choline chloride or betaine as hydrogen bond acceptors and various polyols (ethylene glycol, diethylene glycol, triethylene glycol, glycerol, 1,2-propanediol, 1,3-butanediol) as hydrogen bond donors. Experimental solubility data were collected for all DES systems. A machine learning model was developed using COSMO-RS molecular descriptors to predict solubility. All studied DESs exhibited a cosolvency effect, increasing drug solubility at modest concentrations of water. The model accurately predicted solubility for ibuprofen, ketoprofen, and related analogs (flurbiprofen, felbinac, phenylacetic acid, diphenylacetic acid). A machine learning approach utilizing COSMO-RS descriptors enables the rational design and solubility prediction of DES formulations for improved pharmaceutical applications.

Published

2024

15. Role for Carboxylic Acid Moiety in NSAIDs: Favoring the Binding at Site II of Bovine Serum Albumin.

Author

de Carvalho Bertozo L, Tadeu HC, Sebastian A, Maszota-Zieleniak M, Samsonov SA, and Ximenes VF

Subjects

Animals, Cattle, Humans, Binding Sites, Diflunisal chemistry, Ibuprofen chemistry, Ketoprofen chemistry, Ligands, Naproxen chemistry, Protein Binding, Anti-Inflammatory Agents, Non-Steroidal chemistry, Carboxylic Acids chemistry, Molecular Docking Simulation, Serum Albumin, Bovine chemistry, Serum Albumin, Bovine metabolism

Abstract

The molecular structures of nonsteroidal anti-inflammatory drugs (NSAIDs) vary, but most contain a carboxylic acid functional group (RCOOH). This functional group is known to be related to the mechanism of cyclooxygenase inhibition and also causes side effects, such as gastrointestinal bleeding. This study proposes a new role for RCOOH in NSAIDs: facilitating the interaction at the binding site II of serum albumins. We used bovine serum albumin (BSA) as a model to investigate the interactions with ligands at site II. Using dansyl-proline (DP) as a fluorescent site II marker, we demonstrated that only negatively charged NSAIDs such as ibuprofen (IBP), naproxen (NPX), diflunisal (DFS), and ketoprofen (KTP) can efficiently displace DP from the albumin binding site. We confirmed the importance of RCOO by neutralizing IBP and NPX through esterification, which reduced the displacement of DP. The competition was also monitored by stopped-flow experiments. While IBP and NPX displaced DP in less than 1 s, the ester derivatives were ineffective. We also observed a higher affinity of negatively charged NSAIDs using DFS as a probe and ultrafiltration experiments. Molecular docking simulations showed an essential salt bridge between the positively charged residues Arg409 and Lys413 with RCOO-, consistent with the experimental findings. We performed a ligand dissociation pathway and corresponding energy analysis by applying molecular dynamics. The dissociation of NPX showed a higher free energy barrier than its ester. Apart from BSA, we conducted some experimental studies with human serum albumin, and similar results were obtained, suggesting a general effect for other mammalian serum albumins. Our findings support that the RCOOH moiety affects not only the mechanism of action and side effects but also the pharmacokinetics of NSAIDs.

Published

2024

16. Carrageenan-xanthan nanocomposite film with improved bioadhesion and permeation profile in human skin: A cutaneous-friendly platform for ketoprofen local delivery.

Author

Sari MHM, Saccol CP, Custódio VN, da Rosa LS, da Costa JS, Fajardo AR, Ferreira LM, and Cruz L

Subjects

Humans, Carrageenan chemistry, Skin, Ketoprofen pharmacology, Ketoprofen chemistry, Nanocomposites chemistry, Polysaccharides, Bacterial

Abstract

Ketoprofen (KET), commonly used for inflammation in clinical settings, leads to systemic adverse effects with prolonged use, mitigated by topical administration. Nanotechnology-based cutaneous forms, like films, may enhance KET efficacy. Therefore, this study aimed to prepare and characterize films containing KET nanoemulsions (F-NK) regarding mechanical properties, chemical composition and interactions, occlusive potential, bioadhesion, drug permeation in human skin, and safety. The films were prepared using a κ-carrageenan and xanthan gum blend (2 % w/w, ratio 3: 1) plasticized with glycerol through the solvent casting method. Non-nanoemulsioned KET films (F-K) were prepared for comparative purposes. F-NK was flexible and hydrophilic, exhibited higher drug content and better uniformity (94.40 ± 3.61 %), maintained the NK droplet size (157 ± 12 nm), and was thinner and lighter than the F-K. This film also showed increased tensile strength and Young's modulus values, enhanced bioadhesion and occlusive potential, and resulted in more of the drug in the human skin layers. Data also suggested that nano-based formulations are homogeneous and more stable than F-KET. Hemolysis and chorioallantoic membrane tests suggested the formulations' safety. Thus, the nano-based film is suitable for cutaneous KET delivery, which may improve the drug's efficacy in managing inflammatory conditions., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 Elsevier B.V. All rights reserved.)

Published

2024

17. Evaluation of the in vitro human skin percutaneous absorption of ketoprofen in topical anhydrous and aqueous gels.

Author

Ip K, Song G, Banov D, Bassani AS, Liu Y, Song H, and Valdez BC

Subjects

Humans, Skin Absorption, Skin metabolism, Anti-Inflammatory Agents, Non-Steroidal, Administration, Cutaneous, Gels, Water metabolism, Ketoprofen chemistry, Ketoprofen metabolism

Abstract

Background: Ketoprofen is a nonsteroidal anti-inflammatory drug used for the treatment of acute and chronic pain associated with inflammatory conditions. This study aims to evaluate the in vitro percutaneous absorption of ketoprofen 10% formulated in proprietary anhydrous and aqueous gels using the Franz skin finite dose model., Materials and Methods: The anhydrous gel was initially characterized for cytotoxicity using EpiDerm skin tissue model by cell proliferation assay and Western blot analysis. The Ultra Performance Liquid Chromatography method for measuring ketoprofen was validated and the stability of ketoprofen 10% in the anhydrous gel formulation was evaluated at 5°C and 25°C for 181 days. The percutaneous absorption of ketoprofen was determined using donated human skin. The tissue sections were mounted within Franz diffusion cells. A variable finite dose of each ketoprofen formulation in either anhydrous or aqueous gel was applied to the skin sections and receptor solutions were collected at various time points., Results: Cell proliferation assay showed minimal cell death when EpiDerm skin tissue was exposed to the anhydrous gel for 24 h; the levels of protein markers of cell proliferation were not affected after 17-h exposure. Ketoprofen was stable in the anhydrous gel when stored at 5°C and 25°C. When compounded in the anhydrous and aqueous gels, ketoprofen had mean flux rate of 2.22 and 2.50 μg/cm 2 /h, respectively, after 48 h. The drug was distributed to the epidermis and dermis sections of the skin. Both the anhydrous and aqueous gels facilitated the percutaneous absorption of ketoprofen without statistically significant differences., Conclusion: The anhydrous gel can be used as a base to facilitate the transdermal delivery of ketoprofen. Although the anhydrous and aqueous gels can deliver a similar amount of ketoprofen, the anhydrous gel (water activity below 0.6) allows for extended default beyond-use-date of compounding preparations., (© 2024 Professional Compounding Centers of America. Skin Research and Technology published by John Wiley & Sons Ltd.)

Published

2024

18. Eutectic phase transition during tablet manufacture: effect of melting point of eutectic forming drug.

Author

Marei HF, El Maghraby GM, and Arafa MF

Subjects

Anti-Inflammatory Agents, Non-Steroidal chemistry, Tablets, Lidocaine, Solubility, Ketoprofen chemistry, Diclofenac analogs & derivatives

Abstract

The aim was to investigate eutectic transition during tableting and storage. Mixtures of lidocaine and series of NSAIDs with increasing melting point were used as model systems to guide formulators to scaleup eutectic forming materials gaining enhanced dissolution while avoiding deleterious physical changes. Physical mixtures of NSAIDs with lidocaine were prepared at eutectic forming ratio. These were directly compressed, dry co-ground before compression, or compressed after wet granulation. Dissolution of tablets was compared to corresponding dry co-ground mixture. Thermograms of direct compressed tablet were compared to co-ground mixture and pure compound. Stability of direct compressed tablets was assessed. Tableting initiated eutexia which enhanced dissolution of NSAIDs. Eutexia was associated with tablet softening in case of low melting point ketoprofen and aceclofenac. Wet granulation hastened eutexia developing unacceptable tablet in case ketoprofen and aceclofenac. Tablets prepared by direct compression of physical mixtures underwent gradual eutectic transition upon storage with the magnitude of eutectic transition reducing with increased melting point of NSAIDs. Ketoprofen was physically unstable but aceclofenac degraded chemically as well. Tenoxicam and meloxicam tablets were physically and chemically stable. Direct compression after physical mixing is the best tableting technique, but low melting point drugs should consider different strategy before compression.

Published

2023

19. Interpreting permeability as a function of free drug fraction: The case studies of cyclodextrins and liposomes.

Author

Tzanova MM, Nguyen L, Moretti F, Grassi M, Magnano GC, Voinovich D, Stein PC, Hiorth M, and di Cagno MP

Subjects

Liposomes chemistry, 2-Hydroxypropyl-beta-cyclodextrin, Hydrocortisone chemistry, Permeability, Cyclodextrins chemistry, beta-Cyclodextrins chemistry, Ketoprofen chemistry

Abstract

In order to solubilize poorly soluble active pharmaceutical ingredients, various strategies have been implemented over the years, including the use of nanocarriers, such as cyclodextrins and liposomes. However, improving a drug's apparent solubility does not always translate to enhanced bioavailability. This work aimed to investigate to which extent complexation with cyclodextrins and incorporation into liposomes influence drug in vitro permeability and to find a mechanistic description of the permeation process. For this purpose, we investigated hydroxypropyl-β-cyclodextrin (HP-β-CD) and phosphatidylcholine liposomes formulations of three chemically diverse compounds (atenolol, ketoprofen and hydrocortisone). We studied drug diffusion of the formulations by UV-localized spectroscopy and advanced data fitting to extract parameters such as diffusivity and bound-/free drug fractions. We then correlated this information with in vitro drug permeability obtained with the novel PermeaPad Ⓡ barrier. The results showed that increased concentration of HP-β-CD leads to increased solubilization of the poorly soluble unionized ketoprofen, as well as hydrocortisone. However, this net increment of apparent solubility was not proportional to the increased flux measured. On the other hand, normalising the flux over the empirical free drug concentration, i.e., the free fraction, gave a meaningful absolute permeability coefficient. The results achieved for the liposomal formulation were consistent with the finding on cyclodextrins. In conclusion, we proved the adequacy and usefulness of our method for calculating free drug fractions in the examined enabling formulations, supporting the validity of the established drug diffusion/permeation theory that the unbounded drug fraction is the main driver for drug permeation across a membrane., Competing Interests: Declaration of Competing Interest Massimiliano Pio di Cagno, the corresponding and leading author of this article, is Scientific Consultant for Phabioc GmbH, the producer of the PermeaPad(Ⓡ)., (Copyright © 2023 The Author(s). Published by Elsevier B.V. All rights reserved.)

Published

2023

20. LC-MS/MS approach for simultaneous assessment of hyoscine N-butyl bromide and ketoprofen in biological fluids and pharmaceuticals.

Author

Ali HM, Alsohaimi IH, Hasanin THA, Batubara AS, Bukhary DM, Mostafa EM, and Gamal M

Subjects

Humans, Butylscopolammonium Bromide, Scopolamine, Chromatography, Liquid, Tandem Mass Spectrometry, Pharmaceutical Preparations, Ketoprofen chemistry

Abstract

The mixture of hyoscine N-butyl bromide (HBB) and ketoprofen (KTP) is commonly used for the handling of abdominal spasms and pain relief. There are two challenges that restrict the simultaneous assessment of HBB and KTP in biological fluids and pharmaceuticals. The first issue is the difficulty of elution of HBB and the second one is the presence of KTP as a racemic mixture in all pharmaceutical formulations, which obscures its appearance as a single peak. An ultrasensitive and highly efficient liquid chromatography-mass/mass spectrometric (LC-MS/MS) method is designed and validated for the first concurrent assessment of HBB and KTP in spiked human serum and urine, and pharmaceutical formulations. The estimated linearity ranges for HBB and KTP were respectively, 0.5-500 and 0.05-500 ng/ml, with excellent correlation coefficients. Validation results showed that the value of relative standard deviations were <2% for HBB and KTP. The mean extraction recoveries for HBB and KTP were, respectively, 91.04 and 97.83% in Spasmofen® ampoules; 95.89 and 97.00% in spiked serum; and 97.31 and 95.63% in spiked urine. The presented innovative chromatographic approach was utilized for the measurement of trace amounts of coexisting pharmaceuticals in pharmacokinetics studies and routine therapeutic medication monitoring., (© 2023 John Wiley & Sons Ltd.)

Published

2023

21. Design and Development of Functionalized Single-walled Carbon Nanotube-ethosomes for Transdermal Delivery of Ketoprofen.

Author

Xiaowei J, Lijuan Y, Yanling L, Qiuxiao L, and Bohong G

Subjects

Administration, Cutaneous, Skin metabolism, Skin Absorption, Ketoprofen chemistry, Ketoprofen pharmacokinetics, Nanotubes, Carbon chemistry

Abstract

The purpose of this study was to combine carbon nanotube with ethosomes in order to obtain hybrid nanocarriers for transdermal delivery of ketoprofen (KP). KP-loaded functionalized single-walled carbon nanotube (f-SWCNTs) composite ethosomes (f-SWCNTs-KP-ES) were designed and were verified by a series of characterizations. The particle size of the preparation is less than 400 nm. DSC and XRD experiments showed that KP existed in an amorphous state after it was adsorbed and loaded on f-SWCNTs. TEM experiments showed that the structure of SWCNTs remained intact after oxidation and modification by PEI. FTIR results showed that PEI were successfully modified on the surface of SWCNT-COOH, and KP was successfully loaded on f-SWCNTs. In vitro release characteristics showed that the preparation had sustained release behavior and conformed to the first-order kinetic equation model. In addition, f-SWCNTs-KP-ES gel were prepared and in vitro skin permeation and in vivo pharmacokinetics were studied. The results showed that f-SWCNTs-KP-ES gel could enhance the skin permeation rate of KP and increase the drug retention of drugs in the skin. The characterization results consistently showed f-SWCNTs is a promising drug carrier. The hybrid nanocarrier prepared by the combination of f-SWCNTs and ethosomes can enhance the transdermal absorption of drugs and improve the bioavailability of drugs, which has a certain significance for the development of advanced hybrid nano-preparations.

Published

2023

22. Fluorescent sensing of non-steroidal anti-inflammatory drugs naproxen and ketoprofen by dansylated squaramide-based receptors.

Author

Picci G, Aragoni MC, Arca M, Caltagirone C, Formica M, Fusi V, Giorgi L, Ingargiola F, Lippolis V, Macedi E, Mancini L, Mummolo L, and Prodi L

Subjects

Dimethyl Sulfoxide, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Anti-Inflammatory Agents, Non-Steroidal chemistry, Naproxen pharmacology, Naproxen chemistry, Ketoprofen pharmacology, Ketoprofen chemistry

Abstract

Bis-squaramide receptors L1-L4 bearing a dansyl moiety were synthesised and their potential applications as fluorescent probes towards non steroidal anti-inflammatory drugs naproxen and ketoprofen was investigated. A detailed photophysical characterization in CH 3 CN/DMSO solution (9 : 1 v/v) was conducted and demonstrated that the two macrocyclic receptors L1 and L2 show good sensitivity towards ketoprofen with an ON-OFF fluorescent response, while the two open chain receptors L3 and L4 behave similarly with the three guests considered. DFT theoretical calculations carried out on L2 and L4 as model receptors allowed to propose a possible coordination mode towards the guests. Finally, 1 H-NMR spectroscopy in DMSO- d 6 /0.5% water solution demonstrated that the four receptors interact with the considered guests via H-bonds.

Published

2023

23. New look at the metabolism of nonsteroidal anti-inflammatory drugs: influence on human serum albumin antioxidant activity.

Author

Rogóż W, Pożycka J, Kulig K, Owczarzy A, Szkudlarek A, and Maciążek-Jurczyk M

Subjects

Humans, Naproxen pharmacology, Naproxen chemistry, Naproxen metabolism, Antioxidants pharmacology, Serum Albumin, Human, Diclofenac pharmacology, Diclofenac chemistry, Serum Albumin chemistry, Anti-Inflammatory Agents, Non-Steroidal chemistry, Binding Sites, Ketoprofen chemistry

Abstract

Body's homeostasis is dependent on many factors, such as maintaining balance between free radicals formation and degradation. Human serum albumin (HSA) also plays an important role in homeostasis. The aim of this study was thermodynamic analysis of the interaction between ketoprofen (KET), naproxen (NPX), diclofenac (DIC) and HSA, as well as the effect of drug-albumin binding on HSA antioxidant activity using calorimetric and spectrophotometric techniques. Based on the calorimetric analysis it has been shown that accompanied by hydrophobic interaction drugs-albumin binding is an exoenergetic reaction. All analyzed drugs and HSA showed the ability to react with free radicals such as a radical cation, formed as a result of the reaction between 2,2'-Azino-bis(3-ethylbenzothiazoline-6-sulfonic acid) diammonium salt (ABTS) and potassium persulfate (K 2 S 2 O 8 ). Using ABTS assay a synergistic effect of ketoprofen (KET) and naproxen (NPX) on HSA antioxidant activity was observed while the effect of diclofenac (DIC) binding with albumin was probably additive. Because some medications including KET, NPX and DIC belong to over the counter (OTC) non-steroidal anti-inflammatory drugs (NSAIDs), it is necessary to understand their influence on HSA antioxidant activity.Communicated by Ramaswamy H. Sarma.

Published

2023

24. Synthesis, In Vitro Anti-Inflammatory Activity, and HRMS Analysis of New Amphetamine Derivatives.

Author

Manolov S, Ivanov I, Bojilov D, and Nedialkov P

Subjects

Amphetamine pharmacology, Ibuprofen chemistry, Naproxen chemistry, Anti-Inflammatory Agents pharmacology, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Anti-Inflammatory Agents, Non-Steroidal chemistry, Ketoprofen chemistry

Abstract

Herein, we report the obtaining of new hybrid molecules of amphetamine with different profens (amfens). The obtained amfens are characterized by their melting points, UV, 1 H-, 13 C-NMR, and HRMS spectra. A complete and detailed mass spectral analysis of the newly obtained derivatives of amphetamine with ibuprofen, flurbiprofen, ketoprofen, naproxen, and carprofen was performed. In vitro inhibition of albumin denaturation of each new compound was assessed, and they showed significant activity. The IC 50 values of the obtained amphetamine-profen derivatives ranged from 92.81 to 159.87 µg/mL. This indicates that the new hybrids inherit the anti-inflammatory properties of profens. Using in silico method, the toxicity was also calculated. The obtained results are given in LD 50 values. Depending on the route of administration, the amfens are less toxic compared to the standard amphetamine.

Published

2022

25. Removal of Non-Steroidal Anti-Inflammatory Drugs from Drinking Water Sources by GO-SWCNT Buckypapers.

Author

Baratta M, Tursi A, Curcio M, Cirillo G, Nezhdanov AV, Mashin AI, Nicoletta FP, and De Filpo G

Subjects

Diclofenac chemistry, Naproxen chemistry, Anti-Inflammatory Agents, Non-Steroidal chemistry, Drinking Water, Ketoprofen chemistry, Environmental Pollutants

Abstract

Pharmaceutical products such as antibiotics, analgesics, steroids, and non-steroidal anti-inflammatory drugs (NSAIDs) are new emerging pollutants, often present in wastewater, potentially able to contaminate drinking water resources. Adsorption is considered the cheapest and most effective technique for the removal of pollutants from water, and, recently, membranes obtained by wet filtration method of SWCNT aqueous solutions (SWCNT buckypapers, SWCNT BPs) have been proposed as self-standing porous adsorbents. In this paper, the ability of graphene oxide/single-walled carbon nanotube composite membranes (GO-SWCNT BPs) to remove some important NSAIDs, namely Diclofenac, Ketoprofen, and Naproxen, was investigated at different pH conditions (pH 4, 6, and 8), graphene oxide amount (0, 20, 40, 60, and 75 wt.%), and initial NSAIDs concentration (1, 10, and 50 ppm). For the same experimental conditions, the adsorption capacities were found to strongly depend on the graphene oxide content. The best results were obtained for 75 wt.% graphene oxide with an adsorption capacity of 118 ± 2 mg g -1 for Diclofenac, 116 ± 2 mg g -1 for Ketoprofen, and 126 ± 3 mg g -1 for Naproxen at pH 4. Overall, the reported data suggest that GO-SWCNT BPs can represent a promising tool for a cheap and fast removal of NSAIDs from drinking water resources, with easy recovery and reusability features.

Published

2022

26. One Hundred Carboxylate Receptors.

Author

Rüütel A, Tshepelevitsh S, and Leito I

Subjects

Anions, Carboxylic Acids, Ibuprofen chemistry, Naproxen chemistry, Ketoprofen chemistry

Abstract

This work presents a compilation of binding constant (log K ass ) values in DMSO-d 6 /H 2 O (0.5% m/m) for a variety of receptors with 12 carboxylate anions (formate, acetate, lactate, pivalate, sorbate, hexanoate, benzoate, glyphosate, glucuronate, ibuprofen, naproxen, and ketoprofen). A total of 489 log K ass values are listed for 100 anion receptor molecules. Most log K ass values originate from previously published articles, along with some values for previously unpublished receptor molecules, spanning a workflow of 8 years. The purpose of this study is to serve as a comprehensive information source for selecting suitable receptor candidates to be used in practical carboxylate sensing applications, such as constructing ion-selective electrodes (ISE-s). To support such decision making, all receptors are presented together with lipophilicity (log P o/w ) data.

Published

2022

27. Ketoprofen-induced Photoallergic Reaction.

Author

Rosan T and Ljubojević Hadžavdić S

Subjects

Female, Humans, Middle Aged, Sunscreening Agents, Anti-Inflammatory Agents, Non-Steroidal, Ultraviolet Rays adverse effects, Patch Tests adverse effects, Ketoprofen adverse effects, Ketoprofen chemistry, Dermatitis, Photoallergic etiology, Dermatitis, Photoallergic pathology

Abstract

Dear Editor, Photoallergic reactions are classic T-cell-mediated or delayed-type hypersensitivity reactions of the skin in response to a photoallergen (or a cross-reacting chemical) to which a subject was sensitized in the past (1). The immune system recognizes the changes caused by ultraviolet (UV) radiation; it produces antibodies and causes inflammation of the skin in the exposed areas (2). Common photoallergic drugs and ingredients are included in some sunscreens, aftershave lotions, antimicrobials (especially sulfonamides), non-steroidal anti-inflammatory drugs (NSAIDs), diuretics, anticonvulsants, chemotherapy drugs, fragrances, and other hygiene products (1,3,4). A 64-year-old female patient was admitted to the Department of Dermatology and Venereology with erythema and underlining edema on her left foot (Figure 1). A few weeks earlier, the patient had had a fracture of the metatarsal bones and since then she had been taking NSAIDs systemically every day to suppress pain. Five days before being admitted to our Department, the patient started applying 2.5% ketoprofen gel to her left foot twice daily and was frequently exposed to the sun. For the last twenty years, the patient had been struggling with chronic back pain and was frequently taking different NSAIDs (ibuprofen, diclofenac, etc.). The patient also suffered from essential hypertension and was regularly taking ramipril. She was advised to discontinue ketoprofen application, avoid sunlight, and apply betamethasone cream twice daily for 7 days, which lead to complete resolution of the skin lesions in a few weeks. Two months later, we performed patch and photopatch tests to baseline series and topical ketoprofen. Only the irradiated side of the body where ketoprofen-containing gel was applied showed positive reaction to ketoprofen. Photoallergic reactions manifest as eczematous, pruritic lesions, which may spread to involve other areas of the skin that were not previously exposed to the sun (4). Ketoprofen is a nonsteroidal anti-inflammatory drug composed of a benzoylphenyl propionic acid that is commonly used both topically and systemically for the treatment of musculoskeletal diseases because of its analgesic and anti-inflammatory effects and low toxicity, but it is one of the most frequent photoallergens (1,5,6). Ketoprofen-induced photosensitivity reactions usually present as photoallergic dermatitis characterized as acute dermatitis with edema, erythema, papulovesicles, blisters, or erythema exsudativum multiforme-like lesions at the application site 1 week to 1 month after the initiation of use (7). Depending on the frequency and intensity of sun exposure, ketoprofen photodermatitis may continue or reoccur up to 1 to 14 years after discontinuing the medication (6,8). Moreover, ketoprofen contaminates clothing, shoes, and bandages, and some cases of photoallergy relapses have been reported that were induced by ketoprofen-contaminated objects after they were used again in the presence of UV radiation (5,6). Due to their similar biochemical structure, patients with ketoprofen photoallergy should avoid using some drugs such as some NSAIDs (suprofen, tiaprofenic acid), antilipidemic agent (fenofibrate) and sunscreens based on benzophenones (6,9). Physicians and pharmacists should advise patients of the potential risks when topical NSAIDs are applied on the photoexposed skin.

Published

2022

28. An Evolving Role of Aqueous Piperazine to Improve the Solubility of Non-Steroidal Anti-Inflammatory Drugs.

Author

Fang Z, Zhang B, Xing W, Yu H, Xing C, Gong N, Lu Y, and Du G

Subjects

Anti-Inflammatory Agents, Non-Steroidal chemistry, Calorimetry, Differential Scanning, Ibuprofen chemistry, Indomethacin chemistry, Phenylbutazone, Piperazine, Powders, Salts, Solubility, Spectroscopy, Fourier Transform Infrared, Sulindac, Water chemistry, X-Ray Diffraction, Flurbiprofen, Ketoprofen chemistry

Abstract

Piperazine (PIP) is a pharmaceutically acceptable molecule and a good co-conformer in crystallographic engineering. Most of the non-steroidal anti-inflammatory drugs (NSAIDs) have poor aqueous solubility, which hinders their clinical application. The reports show that the solubility of many insoluble drugs can be significantly improved through salt formation with the PIP. In this work, we obtained a series of NSAIDs-PIP salts, such as ibuprofen-piperazine (IBU-0.5PIP) salt, indomethacin-piperazine (IND-0.5PIP) salt, sulindac-piperazine (SUL-0.5PIP) salt, phenylbutazone-piperazine (PBZ-0.5PIP) salt, ketoprofen-piperazine (KPF-0.5PIP) salt and flurbiprofen-piperazine (FLB-0.5PIP) salt. The spatial structure, arrangement, interaction and associations were expatiated by single crystal X-ray diffraction. Powder X-ray diffraction, Fourier transform infrared, differential scanning calorimetry, and thermogravimetric analysis were used to characterize the novel salts. The six new salts had more than 10 folds of solubility and a faster dissolution rate improved corresponding to the bulk drugs in pure water, and the significant improvement of solubility is closely related to the structure of salts., Competing Interests: Declaration of Competing Interest The authors declare no competing financial interest., (Copyright © 2022 American Pharmacists Association. All rights reserved.)

Published

2022

29. Disposable stochastic sensors for fast analysis of ibuprofen, ketoprofen, and flurbiprofen in their topical pharmaceutical formulations.

Author

Ţuchiu BM, Stefan-van Staden RI, Bădulescu M, and van Staden JF

Subjects

Anti-Inflammatory Agents, Non-Steroidal, Carbon, Copper, Drug Compounding, Ibuprofen chemistry, Flurbiprofen, Ketoprofen chemistry

Abstract

Three disposable stochastic sensors based on maltodextrin (dextrose equivalent = 4-7) and nanostructures (copper monolayer, carbon monolayer and carbon-copper composite layer) deposited using cold plasma on copy paper were proposed for the fast analysis of ibuprofen, ketoprofen and flurbiprofen in pharmaceutical formulation samples. The widest linear concentration ranges recorded were: for ibuprofen 1 fmol/L - 1 mmol/L when the disposable stochastic sensor based on carbon monolayer was used, for ketoprofen 1 fmol/L - 1 mmol/L when the disposable stochastic sensors based on copper monolayer and carbon-copper composite layer were used, and for flurbiprofen 1 fmol/L - 10 mmol/L when the disposable stochastic sensor based on carbon-copper composite layer was used. The lowest limit of detection recorded for each non-steroidal anti-inflammatory drug was 1 fmol/L., (Copyright © 2022 Elsevier B.V. All rights reserved.)

Published

2022

30. Ionic liquid of ketoprofen-piperine modulates the pharmaceutical and therapeutic characters of ketoprofen.

Author

Hassan SA, Gad SF, Abdu-Allah HHM, Qayed WS, AbouElmagd SA, and Ibrahim EA

Subjects

Alkaloids, Animals, Anti-Inflammatory Agents, Non-Steroidal chemistry, Benzodioxoles, Pharmaceutical Preparations, Piperidines, Polyunsaturated Alkamides, Rats, Ionic Liquids, Ketoprofen chemistry

Abstract

Efficiency of drug delivery is product of drug properties and formulation design. Modulating drug's unfavorable properties such as poor solubility or permeation is the first step towards optimum delivery. By combining a drug with a selected bulky counter ion, it can be transformed into a low-melting point salt, i.e., an ionic liquid (IL), with favorable physicochemical properties. In this study, we prepared a novel IL of anti-inflammatory drug, ketoprofen (KP), to enable its transdermal administration. KP was paired with piperine (PI) forming equimolar KP-PI IL, via solvent evaporation. KP-PI IL showed extended stability. Thermal analysis and X-ray diffractometry proved that KP was transformed into a low-melting point amorphous form, while spectroscopic analysis and computational studies demonstrated that KP-PI interaction was mediated by hydrogen bonding. In the IL form, KP's solubility increased due to IL formation by 71 to 83%, while 218% more KP was permeated through rat skin in the IL form, than in a KP/PI mixture. Importantly, upon transdermal administration to rats with induced paw edema; KP-PI IL resulted in a 68% less paw swelling than KP/PI mixture. These findings demonstrate the utility of IL as an economic, simple and efficient strategy for improving the therapeutic application of drugs/drug combinations., (Copyright © 2022 Elsevier B.V. All rights reserved.)

Published

2022

31. A new case of photoallergic contact dermatitis caused by benzophenones in magazine covers.

Author

Samaran Q, Raison-Peyron N, Clark E, Svedman C, Dahlin J, Dereure O, Bruze M, and Bourrain JL

Subjects

Anti-Inflammatory Agents, Non-Steroidal, Benzophenones adverse effects, Gas Chromatography-Mass Spectrometry, Humans, Patch Tests, Dermatitis, Allergic Contact complications, Dermatitis, Allergic Contact etiology, Dermatitis, Photoallergic diagnosis, Dermatitis, Photoallergic etiology, Ketoprofen adverse effects, Ketoprofen chemistry

Abstract

Background: Allergic contact dermatitis (ACD) and photoallergic contact dermatitis (PACD) to benzophenone present in printing ink have been reported. However, precise chemical analyses and extended photo-patch tests have not been performed in these cases., Objectives: To determine which components present in a magazine cover are responsible for a patient's skin reaction, to determine the primary sensitizer, and precisely diagnose ACD and PACD., Methods: After initial photo-patch tests were performed on a patient with a history of reaction to magazine covers after sun exposure, gas chromatography-mass spectrometry and high-performance liquid chromatography analyses of the magazine covers, and additional photo-patch tests were performed., Results: The first photo-patch test results confirmed PACD to ketoprofen and fenofibrate and evoked PACD to the magazine covers. 4-methyl benzophenone (4-MBP) and 1-hydroxy-cyclohexyl-phenyl-ketone (1-HCPK) were found in the magazine cover. Additional photo-patch tests confirmed PACD to 1-HCPK and to benzophenone, and photo-aggravated ACD to 4-MBP. The primary sensitizer was ketoprofen., Conclusions: Benzophenones are present in a wide variety of products, without always being listed on the packaging. Patients previously sensitized to other ketones, such as ketoprofen, may react to benzophenones without being able to avoid contact with these molecules. New regulations may be needed for more efficient eviction advice., (© 2022 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2022

32. Photochemical Reaction of Ketoprofen with Proteinogenic Amino Acids.

Author

Kashihara W, Shinoda M, Tsuchiya K, Isozaki T, Mijiddorj B, Ueda K, and Suzuki T

Subjects

Amino Acids, Anions, Anti-Inflammatory Agents, Non-Steroidal chemistry, Humans, Photochemistry, Protons, Ketoprofen chemistry

Abstract

Ketoprofen (KP) is one of the most popular nonsteroidal anti-inflammatory drugs; however, drug-induced photosensitivity of KP has been reported as a serious adverse effect. KP incorporated into a protein can produce an allergen under UV irradiation, which causes drug-induced photosensitivity. The photochemistry of KP with 20 kinds of proteinogenic amino acids in phosphate buffer solutions at pH 7.4 was studied by transient absorption spectroscopy. The KP carboxylate anion (KP - ) gave rise to a carbanion via a decarboxylation within a laser pulse, and the carbanion yielded 3-ethylbenzophenone ketyl biradical (3-EBPH) through a proton transfer reaction. Twelve kinds of proteinogenic amino acids obviously accelerated the reaction. Structural information on the complexes of KP docked in the binding sites of human serum albumin (HSA) was obtained by molecular mechanics (MM) and molecular dynamics (MD) calculations. The photochemical reaction of KP - with amino acid residues in HSA was discussed on the basis of the experimental and calculational results. The information on the reactivity of KP with the amino acids and the stable structures of the KP-HSA complexes should be essential for understanding of the initial step for drug-induced photosensitivity.

Published

2022

33. Enantioselective chitosan-based racemic ketoprofen imprinted polymer: Chiral recognition and resolution study.

Author

Mabrouk M, Hammad SF, Abdella AA, and Mansour FR

Subjects

Stereoisomerism, Molecularly Imprinted Polymers chemistry, Polymers chemistry, Solvents chemistry, Ketoprofen chemistry, Chitosan chemistry, Molecular Imprinting methods

Abstract

This work presented a novel racemic imprinting process employing the chiral properties of chitosan monomer. The preparation of racemic ketoprofen (RS-KTP) imprinted polymer (RS-MIP) was conducted using glutaraldehyde as a crosslinker. The nature of elution solvent affected the % desorption ratio suggesting a heterogenous nature of the formed binding sites. Good imprinting was indicated by an imprinting factor of 3.50 for S-KTP. The enantioselectivity of the RS-MIP was indicated by enantioselectivity coefficient of 2.31 and % enantiomeric excess (%ee) of 28.55%. A SPE cartridge packed with RS-MIP enabled resolution of RS-KTP using gradient elution solvent system. Scatchard plot revealed two binding sites types of different affinity towards S-KTP and density observed for the RS-MIP. The binding capacity of RS-MIP showed observed dependence on the % ee of S-KTP indicating its enantioselectivity. The success of using racemic template for the preparation of enantioselective MIP brings a new possibility to achieve enantioseparation of racemic mixtures having very expensive or unavailable pure enantiomers., (Copyright © 2022 Elsevier B.V. All rights reserved.)

Published

2022

34. Modeling of Adhesion in Tablet Compression at the Molecular Level Using Thermal Analysis and Molecular Simulations.

Author

Chaturvedi K, Shah HS, Morris KR, and Dave RH

Subjects

Adhesiveness, Calorimetry, Differential Scanning, Compressive Strength, Flurbiprofen chemistry, Ibuprofen chemistry, Ketoprofen chemistry, Models, Molecular, Tablets chemistry

Abstract

The molecular basis of adhesion leading to sticking was investigated by exploring the correlation between thermal analysis and molecular simulations. It is hypothesized that intermolecular interactions between a drug molecule and a punch face are the first step in the adhesion process and the rank order of adhesion during tablet compression should correspond to the rank order of the energies of these interactions. In the present study, the sticking propensity was investigated using ibuprofen, flurbiprofen, and ketoprofen as model substances. At the intermolecular level, a thermal analysis model was proposed as an experimental technique to estimate the work of adhesion between ibuprofen, flurbiprofen, and ketoprofen in a DSC aluminum pan. The linear relationship was established between the enthalpy of vaporization and sample mass to demonstrate the accuracy of the instruments used. The threshold mass for ibuprofen, flurbiprofen, and ketoprofen was determined to be 107, 112, and 222 μg, respectively, after three replicate measurements consistent with the experimental results. Ketoprofen showed a 2-fold higher threshold mass compared to ibuprofen and flurbiprofen, which predicts that ketoprofen should have the highest sticking propensity. Computationally, the rank order of the work of adhesion between ibuprofen, flurbiprofen, and ketoprofen with the metal surface was simulated to be -75.91, 44.75, and -96.91 kcal/mol, respectively, using Materials Studio. The rank order of the interaction between the drug molecule and the iron superlattice decreases in the order ketoprofen > ibuprofen > flurbiprofen. The results indicate that the thermal model can be successfully implemented to assess the sticking propensity of a drug at the molecular level. Also, a new molecular simulation script was successfully applied to determine the interaction energy of the drug molecule upon contact with iron.

Published

2022

35. Ketoprofen and Loxoprofen Platinum(IV) Complexes Displaying Antimetastatic Activities by Inducing DNA Damage, Inflammation Suppression, and Enhanced Immune Response.

Author

Li Z, Wang Q, Li L, Chen Y, Cui J, Liu M, Zhang N, Liu Z, Han J, and Wang Z

Subjects

Animals, Cell Line, Tumor, Coordination Complexes chemistry, Drug Screening Assays, Antitumor, Humans, Lymphocytes, Tumor-Infiltrating immunology, Coordination Complexes pharmacology, DNA Damage, Inflammation chemically induced, Ketoprofen chemistry, Lymphocytes, Tumor-Infiltrating drug effects, Neoplasm Metastasis prevention & control, Phenylpropionates chemistry, Platinum chemistry

Abstract

Metastasis is a major contributor of death in cancer patients, and there is an urgent need for effective treatments of metastatic malignancies. Herein, ketoprofen (KP) and loxoprofen (LP) platinum(IV) complexes with antiproliferative and antimetastatic properties were designed and prepared by integrating chemotherapy and immunotherapy targeting cyclooxygenase-2 (COX-2), matrix metalloproteinase-9 (MMP-9), and programmed death ligand 1 (PD-L1), besides DNA. A mono-KP platinum(IV) complex with a cisplatin core is screened out as a candidate possessing potent anti-proliferative and anti-metastasis activities both in vitro and in vivo. It induces serious DNA damage and further leads to high expression of γ-H2AX and p53. Moreover, it promotes apoptosis of tumor cells through mitochondrial apoptotic pathway Bcl-2/Bax/caspase3. Then, COX-2, MMP-9, NLRP3, and caspase1 as pivotal enzymes igniting inflammation and metastasis are obviously inhibited. Notably, it significantly improves immune response through restraining the expression of PD-L1 to increase CD3 + and CD8 + T infiltrating cells in tumor tissues.

Published

2021

36. Comprehensive Characterisation of the Ketoprofen-β-Cyclodextrin Inclusion Complex Using X-ray Techniques and NMR Spectroscopy.

Author

Betlejewska-Kielak K, Bednarek E, Budzianowski A, Michalska K, and Maurin JK

Subjects

Molecular Structure, Ketoprofen chemistry, Magnetic Resonance Spectroscopy methods, X-Ray Diffraction methods, beta-Cyclodextrins chemistry

Abstract

Racemic ketoprofen (KP) and β-cyclodextrin (β-CD) powder samples from co-precipitation ( 1 ), evaporation ( 2 ), and heating-under-reflux ( 3 ) were analysed using X-ray techniques and nuclear magnetic resonance (NMR) spectroscopy. On the basis of NMR studies carried out in an aqueous solution, it was found that in the samples obtained by methods 1 and 2, there were large excesses of β-CD in relation to KP, 10 and 75 times, respectively, while the sample obtained by method 3 contained equimolar amounts of β-CD and KP. NMR results indicated that KP/β-CD inclusion complexes were formed and the estimated binding constants were approximately 2400 M -1 , showing that KP is quite strongly associated with β-CD. On the other hand, the X-ray single-crystal technique in the solid state revealed that the ( S )-KP/β-CD inclusion complex with a stoichiometry of 2:2 was obtained as a result of heating-under-reflux, for which the crystal and molecular structure were examined. Among the methods used for the preparation of the KP/β-CD complex, only method 3 is suitable.

Published

2021

37. Role of Chiral Configuration in the Photoinduced Interaction of D- and L-Tryptophan with Optical Isomers of Ketoprofen in Linked Systems.

Author

Ageeva AA, Magin IM, Doktorov AB, Plyusnin VF, Kuznetsova PS, Stepanov AA, Alekseev AA, Polyakov NE, and Leshina TV

Subjects

Molecular Structure, Stereoisomerism, Energy Transfer, Ketoprofen chemistry, Photochemistry, Tryptophan chemistry

Abstract

The study of the L- and D-amino acid properties in proteins and peptides has attracted considerable attention in recent years, as the replacement of even one L-amino acid by its D-analogue due to aging of the body is resulted in a number of pathological conditions, including Alzheimer's and Parkinson's diseases. A recent trend is using short model systems to study the peculiarities of proteins with D-amino acids. In this report, the comparison of the excited states quenching of L- and D-tryptophan (Trp) in a model donor-acceptor dyad with ( R )- and ( S )-ketoprofen (KP-Trp) was carried out by photochemically induced dynamic nuclear polarization (CIDNP) and fluorescence spectroscopy. Quenching of the Trp excited states, which occurs via two mechanisms: prevailing resonance energy transfer (RET) and electron transfer (ET), indeed demonstrates some peculiarities for all three studied configurations of the dyad: ( R,S )-, ( S,R )-, and ( S,S )-. Thus, the ET efficiency is identical for ( S,R )- and ( R,S )-enantiomers, while RET differs by 1.6 times. For ( S,S )-, the CIDNP coefficient is almost an order of magnitude greater than for ( R,S )- and ( S,R )-. To understand the source of this difference, hyperpolarization of ( S,S )-and ( R,S )- has been calculated using theory involving the electron dipole-dipole interaction in the secular equation.

Published

2021

38. How to Obtain the Maximum Properties Flexibility of 3D Printed Ketoprofen Tablets Using Only One Drug-Loaded Filament?

Author

Pyteraf J, Jamróz W, Kurek M, Szafraniec-Szczęsny J, Kramarczyk D, Jurkiewicz K, Knapik-Kowalczuk J, Tarasiuk J, Wroński S, Paluch M, and Jachowicz R

Subjects

Calorimetry, Differential Scanning, Delayed-Action Preparations, Drug Compounding methods, Drug Design, Drug Liberation, Elasticity, Excipients chemistry, Polyvinyl Alcohol, Precision Medicine, Reproducibility of Results, Solubility, Spectroscopy, Fourier Transform Infrared, Temperature, X-Ray Diffraction, X-Ray Microtomography, Chemistry, Pharmaceutical methods, Ketoprofen chemical synthesis, Ketoprofen chemistry, Printing, Three-Dimensional, Tablets

Abstract

The flexibility of dose and dosage forms makes 3D printing a very interesting tool for personalized medicine, with fused deposition modeling being the most promising and intensively developed method. In our research, we analyzed how various types of disintegrants and drug loading in poly(vinyl alcohol)-based filaments affect their mechanical properties and printability. We also assessed the effect of drug dosage and tablet spatial structure on the dissolution profiles. Given that the development of a method that allows the production of dosage forms with different properties from a single drug-loaded filament is desirable, we developed a method of printing ketoprofen tablets with different dose and dissolution profiles from a single feedstock filament. We optimized the filament preparation by hot-melt extrusion and characterized them. Then, we printed single, bi-, and tri-layer tablets varying with dose, infill density, internal structure, and composition. We analyzed the reproducibility of a spatial structure, phase, and degree of molecular order of ketoprofen in the tablets, and the dissolution profiles. We have printed tablets with immediate- and sustained-release characteristics using one drug-loaded filament, which demonstrates that a single filament can serve as a versatile source for the manufacturing of tablets exhibiting various release characteristics.

Published

2021

39. Synthesis of a PVA drug delivery system for controlled release of a Tramadol-Dexketoprofen combination.

Author

Flores-Arriaga JC, Chavarría-Bolaños D, Pozos-Guillén AJ, Escobar-Barrios VA, and Cerda-Cristerna BI

Subjects

Adult, Analgesics, Opioid administration & dosage, Anti-Inflammatory Agents, Non-Steroidal administration & dosage, Delayed-Action Preparations, Drug Combinations, Drug Liberation, Humans, Ketoprofen administration & dosage, Male, Membranes, Artificial, Partial Thromboplastin Time, Prothrombin Time, Spectroscopy, Fourier Transform Infrared, Tramadol administration & dosage, Analgesics, Opioid chemistry, Anti-Inflammatory Agents, Non-Steroidal chemistry, Drug Delivery Systems, Ketoprofen chemistry, Polyvinyl Alcohol, Tramadol chemistry

Abstract

The local administration of analgesic combinations by means of degradable polymeric drug delivery systems is an alternative for the management of postoperative pain. We formulated a Tramadol-Dexketoprofen combination (TDC) loaded in poly(vinyl alcohol) (PVA) film. Films were prepared by the solvent casting method using three different molecular weights of PVA and crosslinking those films with citric acid, with the objective of controlling the drug release rate, which was evaluated by UV-vis spectrometry. Non-crosslinked PVA films were also evaluated in the experiments. Differential scanning calorimetry (DSC) analysis of samples corroborated the crosslinking of PVA by the citric acid. Blank and loaded PVA films were tested in vitro for its impact on blood coagulation prothrombin time (PT) and partial thromboplastin time (PTT). The swelling capacity was also evaluated. Crosslinked PVA films of higher-molecular weight showed a prolonged release rate compared with that of the lower-molecular-weight films tested. Non-crosslinked PVA films released 11-14% of TDC. Crosslinked PVA films released 80% of the TDC loaded (p < 0.05). This suggests that crosslinking films can modify the drug release rate. The blank and loaded PVA films induced PT and PTT in the normal range. The results showed that the polymeric films evaluated here have the appropriate properties to allow films to be placed directly on surgical wounds and have the capacity for controlled drug release to promote local analgesia for the control of postoperative pain.

Published

2021

40. Core-shell MOF@COFs used as an adsorbent and matrix for the detection of nonsteroidal anti-inflammatory drugs by MALDI-TOF MS.

Author

Zheng R, Yang Y, Yang C, and Xia Y

Subjects

Adsorption, Anti-Inflammatory Agents, Non-Steroidal chemistry, Aspirin chemistry, Drinking Water analysis, Ketoprofen chemistry, Lakes analysis, Limit of Detection, Naproxen chemistry, Saliva chemistry, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization methods, Water Pollutants, Chemical analysis, Water Pollutants, Chemical chemistry, Anti-Inflammatory Agents, Non-Steroidal analysis, Aspirin analysis, Ketoprofen analysis, Metal-Organic Frameworks chemistry, Naproxen analysis

Abstract

A core-shell material (UiO@TapbTp) has been developed as an adsorbent and matrix to detect nonsteroidal anti-inflammatory drugs (NSAIDS) by matrix laser desorption/ionization time-of-flight mass spectrometry (MALDI-TOF MS) in complex samples. The hybrid material is prepared by growing covalent organic framework (COF, TapbTp) layers in situ on an amino-modified metal-organic framework (MOF, UiO-66-NH 2 ). The combination of the MOF and COF overcomes their individual shortcomings and integrates both of their advantages. Compared with the bare COF and MOF, the core-shell composite exhibits improved enrichment ability and matrix performance. With the help of pre-enrichment under optimized conditions, the limits of detection (LODs) for ketoprofen, naproxen, and aspirin are reduced by nearly 1000 times, with values of 0.001 mg L -1 , 0.010 mg L -1 , and 0.001 mg L -1 , respectively, and the relative standard deviations (RSDs) are all below 12.35%. The good recoveries (84.8-118%) in (spiked) saliva and environmental water sample further verify the applicability of the method in complex samples.

Published

2021

41. Electrospun Janus Beads-On-A-String Structures for Different Types of Controlled Release Profiles of Double Drugs.

Author

Li D, Wang M, Song WL, Yu DG, and Bligh SWA

Subjects

Cellulose analogs & derivatives, Cellulose chemistry, Delayed-Action Preparations pharmacology, Drug Carriers chemistry, Drug Liberation, Ketoprofen chemistry, Ketoprofen pharmacology, Methylene Blue chemistry, Methylene Blue pharmacology, Multifunctional Nanoparticles chemistry, Nanofibers chemistry, Polymers chemistry, X-Ray Diffraction methods, Delayed-Action Preparations chemistry, Drug Delivery Systems instrumentation, Drug Delivery Systems methods

Abstract

A side-by-side electrospinning process characterized by a home-made eccentric spinneret was established to produce the Janus beads-on-a-string products. In this study, ketoprofen (KET) and methylene blue (MB) were used as model drugs, which loaded in Janus beads-on-a-string products, in which polyvinylpyrrolidone K90 (PVP K90) and ethyl cellulose (EC) were exploited as the polymer matrices. From SEM images, distinct nanofibers and microparticles in the Janus beads-on-a-string structures could be observed clearly. X-ray diffraction demonstrated that all crystalline drugs loaded in Janus beads-on-a-string products were transferred into the amorphous state. ATR-FTIR revealed that the components of prepared Janus nanostructures were compatibility. In vitro dissolution tests showed that Janus beads-on-a-string products could provide typical double drugs controlled-release profiles, which provided a faster immediate release of MB and a slower sustained release of KET than the electrospun Janus nanofibers. Drug releases from the Janus beads-on-a-string products were controlled through a combination of erosion mechanism (linear MB-PVP sides) and a typical Fickian diffusion mechanism (bead KET-EC sides). This work developed a brand-new approach for the preparation of the Janus beads-on-a-string nanostructures using side-by-side electrospinning, and also provided a fresh idea for double drugs controlled release and the potential combined therapy.

Published

2021

42. Triplet stabilization for enhanced drug photorelease from sunscreen-based photocages.

Author

Lineros-Rosa M, Cuquerella MC, Francés-Monerris A, Monari A, Miranda MA, and Lhiaubet-Vallet V

Subjects

Anti-Inflammatory Agents, Non-Steroidal radiation effects, Ethanol chemistry, Hexanes chemistry, Ketoprofen radiation effects, Models, Chemical, Photolysis radiation effects, Photosensitizing Agents radiation effects, Prodrugs radiation effects, Propiophenones radiation effects, Solvents chemistry, Sunscreening Agents radiation effects, Ultraviolet Rays, Anti-Inflammatory Agents, Non-Steroidal chemistry, Ketoprofen chemistry, Photosensitizing Agents chemistry, Prodrugs chemistry, Propiophenones chemistry, Sunscreening Agents chemistry

Abstract

Recently, sunscreen-based drug photocages have been introduced to provide UV protection to photoactive drugs, thus increasing their photosafety. Here, combined experimental and theoretical studies performed on a photocage based on the commercial UVA filter avobenzone (AB) and on the photosensitizing non-steroidal anti-inflammatory drug ketoprofen (KP) are presented unveiling the photophysical processes responsible for the light-triggered release. Particular attention is paid to solvent stabilization of the drug and UV filter excited states, respectively, which leads to a switching between the triplet excited state energies of the AB and KP units. Most notably, we show that the stabilization of the AB triplet excited state in ethanol solution is the key requirement for an efficient photouncaging. By contrast, in apolar solvents, in particular hexane, KP has the lowest triplet excited state, hence acting as an energy acceptor quenching the AB triplet manifold, thus inhibiting the desired photoreaction.

Published

2021

43. The Effects of Prodrug Size and a Carbonyl Linker on l-Type Amino Acid Transporter 1-Targeted Cellular and Brain Uptake.

Author

Venteicher B, Merklin K, Ngo HX, Chien HC, Hutchinson K, Campbell J, Way H, Griffith J, Alvarado C, Chandra S, Hill E, Schlessinger A, and Thomas AA

Subjects

Anti-Inflammatory Agents, Non-Steroidal chemistry, Brain metabolism, Dose-Response Relationship, Drug, Humans, Ketoprofen chemistry, Molecular Structure, Particle Size, Prodrugs chemistry, Structure-Activity Relationship, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Brain drug effects, Ketoprofen pharmacology, Large Neutral Amino Acid-Transporter 1 metabolism, Prodrugs pharmacology

Abstract

The l-type amino acid transporter 1 (LAT1, SLC7A5) imports dietary amino acids and amino acid drugs (e. g., l-DOPA) into the brain, and plays a role in cancer metabolism. Though there have been numerous reports of LAT1-targeted amino acid-drug conjugates (prodrugs), identifying the structural determinants to enhance substrate activity has been challenging. In this work, we investigated the position and orientation of a carbonyl group in linking hydrophobic moieties including the anti-inflammatory drug ketoprofen to l-tyrosine and l-phenylalanine. We found that esters of meta-carboxyl l-phenylalanine had better LAT1 transport rates than the corresponding acylated l-tyrosine analogues. However, as the size of the hydrophobic moiety increased, we observed a decrease in LAT1 transport rate with a concomitant increase in potency of inhibition. Our results have important implications for designing amino acid prodrugs that target LAT1 at the blood-brain barrier or on cancer cells., (© 2020 Wiley-VCH GmbH.)

Published

2021

44. Anti-Breast Cancer Activities of Ketoprofen-RGD Conjugate by Targeting Breast Cancer Stem-Like Cells and Parental Cells.

Author

Noori S, Rajabi S, Tavirani MR, Shokri B, and Zarghi A

Subjects

Amino Acid Sequence, Antibodies pharmacology, Antineoplastic Agents pharmacology, Apoptosis drug effects, Cell Line, Tumor, Cell Proliferation drug effects, Fas Ligand Protein pharmacology, Female, Humans, Janus Kinase 2 metabolism, Ketoprofen pharmacology, Molecular Targeted Therapy, Neoplastic Stem Cells, Reactive Oxygen Species metabolism, STAT3 Transcription Factor metabolism, Signal Transduction, Antineoplastic Agents chemistry, Breast Neoplasms drug therapy, Integrins antagonists & inhibitors, Ketoprofen chemistry, Oligopeptides chemistry

Abstract

Background: Cancer Stem Cells (CSCs) play an important role in various stages of cancer development, advancement, and therapy resistance. Ketoprofen-RGD has been revealed to act as an anti-cancer agent against some tumors., Objective: We aimed to explore the effects of a novel Ketoprofen-RGD compound on the suppression of Breast Cancer Stem-like Cells (BCSCs) and their parental cells., Methods: Mammospheres were developed from MCF-7 cells and assessed by CSC surface markers through flowcytometry. The anti-proliferative and pro-apoptotic activities of Ketoprofen-RGD were measured by MTS assay and flowcytometry. The expression levels of stemness markers and JAK2/STAT proteins were measured by quantitative Real Time-PCR (qRT-PCR) and western blotting, respectively. Intracellular Reactive Oxygen Species (ROS) was measured using a cell permeable, oxidant-sensitive fluorescence probe (carboxy-H2DCFDA)., Results: Ketoprofen-RGD significantly reduced the mammosphere formation rate and the expression of three out of six stemness markers and remarkably decreased viability and induced apoptosis of spheroidal and parental cells compared to controls. Further experiments using CD95L, as a death ligand, and ZB4 antibody, as an extrinsic apoptotic pathway blocker, showed that Ketoprofen-RGD induced intrinsic pathway, suggesting a mechanism by which Ketoprofen-RGD triggers apoptosis. ROS production was also another way to induce apoptosis. Results of western blot analysis also revealed a marked diminish in the phosphorylation of JAK2 and STAT proteins., Conclusion: Our study, for the first time, elucidated an anti-BCSC activity for Ketoprofen-RGD via declining stemness markers, inducing toxicity, and apoptosis in these cells and parental cells. These findings may suggest this compound as a promising anti-breast cancer., (Copyright© Bentham Science Publishers; For any queries, please email at epub@benthamscience.net.)

Published

2021

45. Stability of Ketoprofen Methylester in Plasma of Different Species.

Author

Hu SX, Ernst K, Benner CP, and Feenstra KL

Subjects

Animals, Cats, Cattle, Chemistry, Pharmaceutical, Dogs, Drug Evaluation, Preclinical methods, Drug Stability, Female, Horses, Hydrolysis, Ketoprofen administration & dosage, Ketoprofen chemistry, Ketoprofen pharmacokinetics, Male, Mice, Prodrugs administration & dosage, Prodrugs chemistry, Prodrugs pharmacokinetics, Rats, Sheep, Species Specificity, Swine, Ketoprofen analogs & derivatives

Abstract

Background: Pharmacokinetic and pharmacodynamic assessment of ester-containing drugs can be impacted by hydrolysis of the drugs in plasma samples post blood collection. The impact is different in the plasma of different species., Objective: This study evaluated the stability of a prodrug, ketoprofen methylester (KME), in commercially purchased and freshly collected plasma of mouse, rat, dog, cat, pig, sheep, cattle and horse., Methods: KME hydrolysis was determined following its incubation in commercially purchased and freshly collected plasma of those species. Different esterase inhibitors were evaluated for prevention of the hydrolysis in rat, dog and pig plasma., Results: KME was rapidly hydrolyzed in both commercially purchased and freshly collected plasma of mouse, rat, and horse. The hydrolysis was initially quick and then limited in cat plasma. KME hydrolysis was minimum in commercially purchased plasma of dog, pig, sheep and cattle but substantial in freshly collected plasma of those species. Different esterase inhibitors showed different effects on the stability of KME in rat, dog and pig plasma., Conclusion: These results indicate that plasma of different species has different hydrolytic activities to estercontaining drugs. The activities in commercially purchased and freshly collected plasma may be different and species-dependent. Esterase inhibitors have different effects on preventing hydrolysis of the ester-containing drugs in the plasma of different species., (Copyright© Bentham Science Publishers; For any queries, please email at epub@benthamscience.net.)

Published

2021

46. Radical reactions induced by ketoprofen in phospholipid membranes under ultraviolet light irradiation.

Author

Okazaki S, Hirata A, Shogomori Y, Takemoto M, Nagata T, Hayashida E, and Takeshita K

Subjects

1,2-Dipalmitoylphosphatidylcholine chemistry, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Cyclic N-Oxides chemistry, Egg Yolk chemistry, Free Radicals chemistry, Humans, Hydroxyl Radical chemistry, Ketoprofen adverse effects, Ketoprofen radiation effects, Pyridines chemistry, Superoxide Dismutase chemistry, Superoxides chemistry, Ultraviolet Rays, Anti-Inflammatory Agents, Non-Steroidal chemistry, Ketoprofen chemistry, Phosphatidylcholines chemistry

Abstract

2-(3-Benzoylphenyl)propanoic acid (ketoprofen), one of the nonsteroidal anti-inflammatory drugs, causes photocontact dermatitis by ultraviolet (UV) light as a side effect. In this study, we examined radical reactions induced by ketoprofen in the lipid membranes under UV irradiation using egg yolk phosphatidylcholine (egg-PC) liposomal membranes containing 5- or 16-doxyl stearic acid (5- or 16-DSA), which carry nitroxyl radical at the 5- or 16-position of the fatty acid chain, respectively. When the suspension of liposomal membrane was mixed with ketoprofen and irradiated with UV, electron spin resonance signal of 5- and 16-DSA in the membrane decreased. The decay consisted of fast decay and subsequent slow decay. The overall decay for 5-DSA was faster than that for 16-DSA. The rate of slower decay of 16-DSA increased with ketoprofen concentration. The bulk lipid in the membrane affected the rate of slower decay of 5-DSA; the rate increased with the amount of egg-PC and decreased in the rigid membrane composed of dipalmitoylphosphatidylcholine. When spin trapping studies with α-(4-pyridyl 1-oxide)-N-tert-butylnitrone (POBN) and 5,5-dimetyl-1-pyrroline-N-oxide (DMPO) were performed in ketoprofen solution, C-centered radical adducts of POBN and superoxide anion radical adducts of DMPO were detected after UV irradiation. POBN suppressed the signal decay of 5-DSA in the liposomal membrane, whereas superoxide dismutase accelerated it. These results support that ketoprofen penetrates the lipid membrane and induces a radical reaction near the polar region in the membrane, and that ketoprofen-related C-centered radical is involved in the radical reaction., (Copyright © 2020 Elsevier B.V. All rights reserved.)

Published

2021

47. Adsorption of ibuprofen, ketoprofen, and paracetamol onto activated carbon prepared from effluent treatment plant sludge of the beverage industry.

Author

Streit AFM, Collazzo GC, Druzian SP, Verdi RS, Foletto EL, Oliveira LFS, and Dotto GL

Subjects

Adsorption, Charcoal chemistry, Humans, Ibuprofen chemistry, Ketoprofen chemistry, Kinetics, Sewage, Wastewater, Water, Water Pollutants, Chemical analysis, Acetaminophen chemistry, Anti-Inflammatory Agents, Non-Steroidal chemistry, Beverages, Waste Disposal, Fluid methods, Water Pollutants, Chemical chemistry

Abstract

The presence of emerging contaminants such as pharmaceuticals in aquatic means presents as a serious threat, since their real consequences for the environment and human health are not well known. Therefore, this work consisted of preparing and characterize sludge-derived activated carbons (beverage sludge activated carbon - BSAC and acid-treated beverage sludge activated carbon - ABSAC) to investigate their use in the pharmaceuticals adsorption in aqueous media. The morphology study has demonstrated that ABSAC, unlike BSAC, exhibited an abundant porous structure, with smaller particles and bigger roughness. Adsorption results indicated that the ABSAC was more effective that BSAC, since it presented superior surface area (642 m 2  g -1 ) and total pore volume (0.485 cm 3  g -1 ) values. Pseudo-second-order kinetic model was more suitable to predict experimental data. Sips model best described the equilibrium data, with maximum adsorption capacities of 145, 105, and 57 mg g -1 for paracetamol, ibuprofen, and ketoprofen, respectively. Besides, the sludge-derived adsorbent was highly efficient in the treatment of a simulated drug effluent, removing 85.16% of the pharmaceutical compounds. Therefore, the material prepared in this work possesses intrinsic characteristics that make it a remarkable adsorbent to be applied in the treatment of pharmaceutical contaminants contained in industrial wastewater., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2020 Elsevier Ltd. All rights reserved.)

Published

2021

48. The Effect of Enantiomer Elution Order on the Determination of Minor Enantiomeric Impurity in Ketoprofen and Enantiomeric Purity Evaluation of Commercially Available Dexketoprofen Formulations.

Author

Tok KC, Gumustas M, Jibuti G, Suzen HS, Ozkan SA, and Chankvetadze B

Subjects

Calibration, Chemistry Techniques, Analytical, Chemistry, Pharmaceutical, Chromatography, Drug Compounding, Drug Contamination, Ketoprofen chemistry, Limit of Detection, Reproducibility of Results, Stereoisomerism, Amylose chemistry, Chromatography, High Pressure Liquid methods, Ketoprofen analogs & derivatives, Phenylcarbamates chemistry, Tromethamine chemistry

Abstract

In a recent study, opposite enantiomer elution order was observed for ketoprofen enantiomers on two amylose-phenylcarbamate-based chiral columns with the same chemical composition of the chiral selector but in one case with coated while in the other with an immobilized chiral selector. In the present study, the influence of this uncommon effect on method validation parameters for the determination of minor enantiomeric impurity in dexketoprofen was studied. The validated methods with two alternative elution orders for enantiomers were applied for the evaluation of enantiomeric impurity in six marketed dexketoprofen formulations from various vendors. In most of these formulations except one the content of enantiomeric impurity exceeded 0.1% ( w / w ).

Published

2020

49. Continuous Manufacturing of Ketoprofen Delayed Release Pellets Using Melt Extrusion Technology: Application of QbD Design Space, Inline Near Infrared, and Inline Pellet Size Analysis.

Author

Vo AQ, Kutz G, He H, Narala S, Bandari S, and Repka MA

Subjects

Drug Compounding, Drug Implants, Hot Melt Extrusion Technology, Particle Size, Solubility, Drug Liberation, Ketoprofen chemistry

Abstract

Delayed-release dosage forms are mainly manufactured as batch processes and include coated tablets, pellets, or particles with gastric resistant polymers. Authors propose a novel approach using the hot-melt extrusion technique to prepare delayed release dosage forms via a continuous manufacturing process, a new trend in the pharmaceutical industry. A full factorial design was employed to correlate input variables, including stearic acid (SA) content, drug content, and pellet size with drug release properties of the pellets. PLS fit method suitably elaborated the relationship between input and output variables with reasonably good fit and goodness of prediction. All three input factors influenced drug release in enzyme-free simulated gastric fluid (SGF) after 120 min; however, SA content did not significantly affect drug dissolution in the enzyme-free simulated intestinal fluid (SIF). An optimized formulation and design space were determined by overlaying multiple contours established from regression equations. The continuous manufacturing process was successfully monitored using inline near-infrared (NIR) and inline particle size analysis, with drug load and pellet size being well-controlled within the design space. The obtained pellets released less than 5% after 120 min in SGF and more than 85% and 95% after 30 min and 45 min, respectively, after switching to SIF., (Copyright © 2020 American Pharmacists Association®. Published by Elsevier Inc. All rights reserved.)

Published

2020

50. Novel organ-specific effects of Ketoprofen and its enantiomer, dexketoprofen on toxicological response transcripts and their functional products in salmon.

Author

Mennillo E, Pretti C, Cappelli F, Luci G, Intorre L, Meucci V, and Arukwe A

Subjects

Animals, Antioxidants pharmacology, Biomarkers metabolism, Biotransformation drug effects, Gills drug effects, Gills metabolism, Ketoprofen pharmacology, Liver drug effects, Liver metabolism, Organ Specificity drug effects, Oxidative Stress drug effects, Principal Component Analysis, RNA, Messenger genetics, RNA, Messenger metabolism, Stereoisomerism, Transcription, Genetic drug effects, Water Pollutants, Chemical toxicity, Ketoprofen analogs & derivatives, Ketoprofen chemistry, Ketoprofen toxicity, Organ Specificity genetics, Salmo salar genetics, Tromethamine toxicity

Abstract

Racemic ketoprofen (RS-KP) and its enantiomer, dexketoprofen (S(+)-KP) are widely used non-steroidal anti-inflammatory drugs (NSAIDs), and commonly detected in the aquatic environment. The present study has evaluated the toxicological effects of RS-KP and S(+)-KP on biotransformation and oxidative stress responses in gills and liver of Atlantic salmon. Fish were exposed for 10 days using different concentrations of RS-KP (1, 10 and 100 μg/L) and S(+)-KP (0.5, 5 and 50 μg/L). Biotransformation and oxidative stress responses were analysed at both transcript and functional levels. In the gills, significant inhibitory effect at transcriptional and enzymatic levels were observed for biotransformation and oxidative stress responses. On the contrary, biotransformation responses were significantly increased at transcriptional and translational levels in the liver, while the associated enzymatic activities did not parallel this trend and were inhibited and further demonstrated by principal component analysis (PCA). Our findings showed that both compounds produced comparable toxicological effects, by producing organ-specific effect differences. RS-KP and S(+)-KP did not bioaccumulate in fish muscle, either due to rapid metabolism or excretion as a result of their hydrophobic properties. Interestingly, the inhibitory effects observed in the gills suggest that these drugs may not undergo first pass metabolism, that might result to downstream differences in toxicological outcomes., (Copyright © 2020 The Authors. Published by Elsevier B.V. All rights reserved.)

Published

2020