Spanlastics as a Potential Approach for Enhancing the Nose-To-Brain Delivery of Piperine: In Vitro Prospect and In Vivo Therapeutic Efficacy for the Management of Epilepsy

Gupta, Isha; Adin, Syeda Nashvia; Rashid, Md Abdur; Alhamhoom, Yahya; Aqil, Mohd.; Mujeeb, Mohd.

doi:10.3390/pharmaceutics15020641

Cited by 21 publications

(7 citation statements)

References 27 publications

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“…The RBF was placed in a desicator for 24 h. The dried film was hydrated in a water–PRG solution for 1 h before being stored in the refrigerator to achieve adequate swelling. The obtained dispersion was probe sonicated for 4 min with a titanium probe ultra sonicator (UP 100 H, Hielscher Ultrasonics GmbH, Berlin) and then characterized for polydispersity index (PDI), entrapment efficiency and vesicle size (Adin, Gupta, Rashid, et al, 2023; Gupta, Adin, Aqil, Mujeeb, & Sultana, 2022a; Gupta, Adin, Rashid, et al, 2023).…”

Section: Methodsmentioning

confidence: 99%

“…The RBF was placed in a desicator for 24 h. The dried film was hydrated in a water-PRG solution for 1 h before being stored in the refrigerator to achieve adequate swelling. The obtained dispersion was probe sonicated for 4 min with a titanium probe ultra sonicator (UP 100 H, Hielscher Ultrasonics GmbH, Berlin) and then characterized for polydispersity index (PDI), entrapment efficiency and vesicle size(Adin, Gupta, Rashid, et al, 2023;Gupta, Adin, Aqil, Mujeeb, & Sultana, 2022a;Gupta, Adin, Rashid, et al, 2023).2.8.2 | Characterization of prepared PRG-NRN nanoliposomesThe vesicle size and PDI of the developed PRG-NRN liposomes were estimated using a Zetasizer (Malvern Instruments, Worcestershire, UK) after diluting the sample with Mill-Q water (50 times) at 25 ± 1 C in triplicate at a scattering angle of 90 C(Gupta, Adin, Aqil, Mujeeb, & Sultana, 2022a).2.8.3 | Percentage drug entrapment efficiency and percentage drug loading The entrapment efficiency of liposomes was evaluated using ultracentrifugation. The samples were stored at 40 C overnight before being centrifuged at 20,000 rpm for 1 h at 40 C (REMI, cooling centrifuge, Mumbai, India).…”

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confidence: 99%

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Application of QbD‐based approach to the development and validation of an RP‐HPLC method for simultaneous estimation of pregabalin and naringin in dual‐drug loaded liposomes

Gupta

Adin

Aqil

et al. 2023

Biomedical Chromatography

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The current work delineates the development of a novel, rugged and sensitive stability‐indicating risk‐based HPLC method based on an analytical quality‐by‐design (QbD) approach for the concurrent estimation of naringin and pregabalin in dual‐drug‐loaded nanopharmaceuticals. Preliminary screening trials were conducted, along with systemic risk analysis, in order to identify the critical method attributes, namely injection volume, pH and acetonitrile content, that influence critical quality attributes. The Box–Behnken design was used to optimize the tailing factor as a response to pregabalin and naringin in a short run time. The chromatographic conditions were improved by running 17 experimental runs generated by design expert software. After analysing the optimized zone within the confines of the design space, the following chromatographic conditions were chosen: mobile phase water–acetonitrile adjusted to pH 6.9 with phosphate buffer (80:20, %v/v), at flow rate of 1.0 ml/min using a C18 analytical column at an isobestic wavelength of 212 nm. Furthermore, the optimized method was validated in accordance with International Conference on Harmonization guidelines and was found to be within the prescribed limits. The developed RP‐HPLC method has a high degree of practical utility in in vivo and in vitro studies for the synchronous detection of pregabalin and naringin in pharmaceutical nanodosage forms such as protein‐based nanoparticles, nanocrystals, polymeric nanoparticles and metallic nanoparticles.

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Section: Methodsmentioning

confidence: 99%

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confidence: 99%

Application of QbD‐based approach to the development and validation of an RP‐HPLC method for simultaneous estimation of pregabalin and naringin in dual‐drug loaded liposomes

Gupta

Adin

Aqil

et al. 2023

Biomedical Chromatography

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“…Exosome, as a nano-delivery platform, could be loaded with nucleic acids for targeted delivery into the body for gene expression, which overcomes the limitations of current gene therapy delivery technology. 158 PTT and PDT are two effective cancer treatment modalities, which have attracted widespread attention because of their high selectivity and noninvasiveness. 159 However, it is difficult to completely eradicate solid tumors with PTT/PDT alone.…”

Section: Exosomes As Drug Delivery Vehicles In Therapeutic Applicationsmentioning

confidence: 99%

Application of exosomes as nanocarriers in cancer therapy

Hu,

Zhu,

Chai

et al. 2023

J. Mater. Chem. B

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“…The observed increment in % EE as the concentration of phospholipid increases might be attributed to the increase in domain size of the bilayer ensuing from the formation of a higher quantity of TE vesicles. This, in turn, allows for a greater capacity for HSD entrapment within the TE vesicles [33]. The efficiency of the transethosomal system is significantly impacted by ethanol as well; raising the concentration of ethanol will enhance entrapment efficiency.…”

Section: Response (Y 3 ): Impact Of Independent Variable On %Eementioning

confidence: 99%

Formulation and Characterization of Hesperidin-Loaded Transethosomal Gel for Dermal Delivery to Enhance Antibacterial Activity: Comprehension of In Vitro, Ex Vivo, and Dermatokinetic Analysis

Alam,

Imran,

Jahan

et al. 2023

Gels

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In this study, hesperidin was loaded into a transethosome and was developed employing the rotary evaporator method. The formulation was optimized using the Box–Behnken design (BBD). The optimized HSD-TE formulation has a spherical shape, vesicle size, polydispersity index, entrapment efficiency, and zeta potential within the range of 178.98 nm; the PDI was 0.259 with a zeta potential of −31.14 mV and % EE of 89.51%, respectively. The in vitro drug release shows that HSD-TE exhibited the release of 81.124 ± 3.45% in comparison to HSD suspension. The ex vivo skin permeation showed a 2-fold increase in HSD-TE gel permeation. The antioxidant activity of HSD-TE was found to be 79.20 ± 1.77% higher than that of the HSD solution. The formulation showed 2-fold deeper HSD-TE penetration across excised rat skin membranes in confocal laser microscopy scanning, indicating promising in vivo prospects. In a dermatokinetic study, HSD-TE gel was compared to HSD conventional gel where TE significantly boosted HSD transport in the epidermis and dermal layers. The formulation showed greater efficacy than free HSD in the inhibition of microbial growth, as evidenced by antibacterial activity on the Gram-negative and positive bacteria. These investigations found that the HSD-TE formulation could enhance the topical application in the management of cutaneous bacterial infections.

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Spanlastics as a Potential Approach for Enhancing the Nose-To-Brain Delivery of Piperine: In Vitro Prospect and In Vivo Therapeutic Efficacy for the Management of Epilepsy

Cited by 21 publications

References 27 publications

Application of QbD‐based approach to the development and validation of an RP‐HPLC method for simultaneous estimation of pregabalin and naringin in dual‐drug loaded liposomes

Application of QbD‐based approach to the development and validation of an RP‐HPLC method for simultaneous estimation of pregabalin and naringin in dual‐drug loaded liposomes

Application of exosomes as nanocarriers in cancer therapy

Formulation and Characterization of Hesperidin-Loaded Transethosomal Gel for Dermal Delivery to Enhance Antibacterial Activity: Comprehension of In Vitro, Ex Vivo, and Dermatokinetic Analysis

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