Development of Diphenyl carbonate-Crosslinked Cyclodextrin Based Nanosponges for Oral Delivery of Baricitinib: Formulation, Characterization and Pharmacokinetic Studies

Aldawsari, Mohammed F.; Alhowail, Ahmad; Anwer, Md. Khalid; Ahmed, Mohammed Muqtader

doi:10.2147/ijn.s405534

Cited by 6 publications

(14 citation statements)

References 47 publications

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“…The relationship between EE and 1:n shows four different natures: Increase in EE with 1:n —observed for β-CD:CDI complexes with bortezomib ( 1 ) [ 79 ], flutamide ( 2 ) [ 80 ], piroxicam ( 3 ) [ 81 ], and sulfamethoxazole ( 4 ) [ 82 ], β-CD:DPC complexes with baricitinib ( 5 ) [ 83 ] and febuxostat ( 6 ) [ 84 ], naproxen-loaded β-CD:TDI ( 7 ) [ 85 ], and clotrimazole-loaded 2-HP-β-CD:DMC ( 8 ) [ 86 ]; Maximum EE for specific 1:n —observed for β-CD:DPC complexes with nifedipine (1:4) ( 9 ) [ 87 ] and rilpivirine (1:4) ( 10 ) [ 88 ], and for β-CD:PMDA complexes with acetylsalicylic acid (1:4) ( 11 ) [ 89 ], diclofenac sodium (1:2) ( 12 ) [ 90 ], and rosuvastatin calcium (1:6) ( 13 ) [ 91 ]; Decrease in EE with 1:n —observed for l -DOPA-loaded β-CD:CDI ( 14 ) [ 92 ] and 5-fluorouracil-loaded β-CD:DPC ( 15 ) [ 93 ]; No influence of 1:n on EE —observed for paliperidone-loaded β-CD:CDI ( 16 ) [ 94 ] and ciprofloxacin-loaded 2-HP-β-CD:DPC ( 17 ) [ 95 ]. …”

Section: Revision Of Cdnss’ Physicochemical Properties and Their Mutu...mentioning

confidence: 99%

“…Increase in EE with 1:n —observed for β-CD:CDI complexes with bortezomib ( 1 ) [ 79 ], flutamide ( 2 ) [ 80 ], piroxicam ( 3 ) [ 81 ], and sulfamethoxazole ( 4 ) [ 82 ], β-CD:DPC complexes with baricitinib ( 5 ) [ 83 ] and febuxostat ( 6 ) [ 84 ], naproxen-loaded β-CD:TDI ( 7 ) [ 85 ], and clotrimazole-loaded 2-HP-β-CD:DMC ( 8 ) [ 86 ];…”

Section: Revision Of Cdnss’ Physicochemical Properties and Their Mutu...mentioning

confidence: 99%

“…Lastly, the Brunauer–Emmett–Teller (BET) theory enables the evaluation of the surface area of CDNS particles. This method is implemented via evaluation of the pore volume of CDNS by adsorption of gas molecules, e.g., liquid nitrogen, which can then be used to calculate the pore diameter and, subsequently, the surface area [ 83 , 91 ].…”

Section: Revision Of Cdnss’ Physicochemical Properties and Their Mutu...mentioning

confidence: 99%

“…This phenomenon can be explained depending on the polymerization degree—for lower 1 :n , the CDNS network is uncompleted, resulting in poor drug complexation and poor ability to form dense, organized structures, whereas for higher 1 :n , polymer steric hindrances could lead to branching of the polymer structure. Particle size could also increase with the growth of 1 :n , as shown by the principles of β-CD:CDI complexes with bortezomib ( 1 ) [ 79 ], piroxicam ( 3 ) [ 81 ], and l -DOPA ( 14 ) [ 92 ], and of β-CD:DPC complexes with baricitinib ( 5 ) [ 83 ] and nifedipine ( 9 ) [ 87 ], which are the result of destabilization of the polymer network, as mentioned previously.…”

Section: Revision Of Cdnss’ Physicochemical Properties and Their Mutu...mentioning

confidence: 99%

“…The incorporation of drugs into CDNSs alone can lead to changes in the cumulative drug release observed at the same time, which translates into accelerating or slowing down the drug release rate ( Table 7 ). An increase in cumulative drug release as compared with the pure drug was observed for β-CD:CDI complexes with bortezomib ( 1 ) [ 79 ], flutamide ( 2 ) [ 80 ], atorvastatin calcium ( 23 ) [ 99 ], and rilpivirine ( 34 ) [ 107 ], β-CD:DPC complexes with baricitinib ( 5 ) [ 83 ], rilpivirine ( 10 ) [ 88 ], irbesartan ( 20 ) [ 97 ], dexamethasone ( 24 and 42 ) [ 100 , 113 ], efavirenz ( 31 ) [ 105 ], erlotinib ( 32 ) [ 106 ], and domperidone ( 39 ) [ 110 ], β-CD:PMDA complexes with rosuvastatin calcium ( 13 ) [ 91 ], irbesartan ( 21 ) [ 97 ], rilpivirine ( 35 ) [ 107 ], and imiquimod ( 46 ) [ 117 ], and 2-HP-β-CD:DPC complexes with ibuprofen ( 28 ) [ 102 ], due to increased wettability and improvement of the water solubility of the drug [ 80 , 88 , 97 , 99 , 107 ], reductions in drug crystallinity [ 88 , 97 ] and particle size [ 88 , 97 , 100 , 117 ], and increases in the surface area [ 83 , 88 ] resulting from encapsulation into CDNSs. On the other hand, a decrease in the amount of drug released was observed for β-CD:CDI complexes with paliperidone ( 16 ) [ 94 ], econazole nitrate ( 43 ) [ 114 ], and dexamethasone ( 44 ) [ 115 ], β-CD:DPC complexes with febuxostat ( 6 ) [ 84 ], clobetasol propionate ( 19 ) [ 96 ...…”

Section: Revision Of Cdnss’ Physicochemical Properties and Their Mutu...mentioning

confidence: 99%

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Exploring Cyclodextrin-Based Nanosponges as Drug Delivery Systems: Understanding the Physicochemical Factors Influencing Drug Loading and Release Kinetics

Pyrak,

Rogacka-Pyrak,

Gubica

et al. 2024

IJMS

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Cyclodextrin-based nanosponges (CDNSs) are complex macromolecular structures composed of individual cyclodextrins (CDs) and nanochannels created between cross-linked CD units and cross-linkers. Due to their unique structural and physicochemical properties, CDNSs can possess even more beneficial pharmaceutical features than single CDs. In this comprehensive review, various aspects related to CDNSs are summarized. Particular attention was paid to overviewing structural properties, methods of synthesis, and physicochemical analysis of CDNSs using various analytical methods, such as DLS, PXRD, TGA, DSC, FT-IR, NMR, and phase solubility studies. Also, due to the significant role of CDNSs in pharmaceutical research and industry, aspects such as drug loading, drug release studies, and kinetics profile evaluation of drug–CDNS complexes were carefully reviewed. The aim of this paper is to find the relationships between the physicochemical features and to identify crucial characteristics that are influential for using CDNSs as convenient drug delivery systems.

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Section: Revision Of Cdnss’ Physicochemical Properties and Their Mutu...mentioning

confidence: 99%

Section: Revision Of Cdnss’ Physicochemical Properties and Their Mutu...mentioning

confidence: 99%

Section: Revision Of Cdnss’ Physicochemical Properties and Their Mutu...mentioning

confidence: 99%

Section: Revision Of Cdnss’ Physicochemical Properties and Their Mutu...mentioning

confidence: 99%

Section: Revision Of Cdnss’ Physicochemical Properties and Their Mutu...mentioning

confidence: 99%

See 3 more Smart Citations

Exploring Cyclodextrin-Based Nanosponges as Drug Delivery Systems: Understanding the Physicochemical Factors Influencing Drug Loading and Release Kinetics

Pyrak,

Rogacka-Pyrak,

Gubica

et al. 2024

IJMS

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Advancements in application of chitosan and cyclodextrins in biomedicine and pharmaceutics: recent progress and future trends

Bahavarnia,

Hasanzadeh,

Bahavarnia

et al. 2024

RSC Adv.

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Design and optimization of DPC-crosslinked HPβCD nanosponges for entrectinib oral delivery: formulation, characterization, and pharmacokinetic studies

Reddy,

Bhikshapathi

2024

Futur J Pharm Sci

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Background In advanced or metastatic cancers characterized by specific genetic alterations, heightened growth and resistance to conventional therapies are common. Targeted treatments like entrectinib (ENT) precisely inhibit aberrant signaling pathways, potentially enhancing outcomes. The objective of this research is to develop and enhance the effectiveness of entrectinib-loaded nanosponge formulations by utilizing hydroxypropyl-β-cyclodextrin (HPβCD) to improve its oral bioavailability. Results The study employed surface response methodology and Design-Expert® software to optimize key formulation variables such as the molar concentration ratio of the polymer and cross-linker, as well as process variables such as stirring speed and duration. Optimization focused on particle size, polydispersity index, and percentage entrapment efficiency. Validation methods encompassed Fourier transform spectroscopy (FTIR), differential scanning calorimetry (DSC), scanning electron microscopy (SEM), in vitro release studies, and in vivo studies. After optimization, ENT-loaded HPβCD NSPs were formulated with a molar ratio (P:CL) of 0.800 mg, stirred at 3000 rpm for 420 min, achieving a desirability of 0.926. Predicted values for PS (particle size), PdI (polydispersity index), and EE % (entrapment efficiency) were 146.98 nm, 0.263, and 88.29%, respectively. The optimized formulation showed a mean size of 151.8 ± 5.6 nm, PDI of 0.233 ± 0.049, and EE of 87.36 ± 1.61%. Further validation through various analyses confirmed the optimization's efficacy, with notable improvements demonstrated in AUC0-t (6.30-fold) and Cmax (4.10 times) compared to the free drug. Conclusion The findings of the study indicated that nanosponges exhibit promise as an effective carrier for delivering entrectinib, addressing for advance tumor effectively by enhancing release and bioavailability in the treatment of cancer.

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Development of Diphenyl carbonate-Crosslinked Cyclodextrin Based Nanosponges for Oral Delivery of Baricitinib: Formulation, Characterization and Pharmacokinetic Studies

Cited by 6 publications

References 47 publications

Exploring Cyclodextrin-Based Nanosponges as Drug Delivery Systems: Understanding the Physicochemical Factors Influencing Drug Loading and Release Kinetics

Exploring Cyclodextrin-Based Nanosponges as Drug Delivery Systems: Understanding the Physicochemical Factors Influencing Drug Loading and Release Kinetics

Advancements in application of chitosan and cyclodextrins in biomedicine and pharmaceutics: recent progress and future trends

Design and optimization of DPC-crosslinked HPβCD nanosponges for entrectinib oral delivery: formulation, characterization, and pharmacokinetic studies

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