&lt;p&gt;Lipid-Based Gliclazide Nanoparticles for Treatment of Diabetes: Formulation, Pharmacokinetics, Pharmacodynamics and Subacute Toxicity Study&lt;/p&gt;

Nazief, Alaa M.; Hassaan, Passainte S.; Khalifa, Hoda; Sokar, Magda; El-Kamel, Amal H.

doi:10.2147/ijn.s235290

Cited by 28 publications

(16 citation statements)

References 48 publications

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“…Moreover, upon increasing the surfactant content, the dispersion became slightly viscous, which prevented the partition of SUL in the external aqueous phase. Contrary to the early reported attempt, 42 we did not detect any significant decrease in the % EE upon emulsifier content elevation, which might be due to the difference of either surfactant or drug nature, as well as the range of surfactant concentration chosen. Nevertheless, our findings were supported by previous reports in the literature.…”

Section: Resultscontrasting

confidence: 99%

“…These are crucial parameters that mainly allow efficient uptake in the intestine, especially in the lymphoid tissue, thus achieving an improvement of drug oral bioavailability. 42 Figure 2 demonstrated the particle and PdI values of several batches of SUL-LPS (F 1 -F 20 ). The particle size of the investigated LPS was in the nanometric range of 49.33 ± 6.46 to 396.9 ± 17.57 nm, along with low PdI values of less than 1, indicating an acceptable dispersion homogeneity.…”

Section: Resultsmentioning

confidence: 99%

“…Their nanoscale dimensions combined with improved surface area could strongly enhance encapsulated drug diffusion and absorption through the GIT tract. 42 Moreover, their surface decoration with the phospholipid (LS75), one of the cell membrane components, could stimulate SUL integration within the cells. Phospholipid could interact with mucous leading to a slight modulation of the mucosal membrane, an increase in the fluidity of the lipid bilayers and eventually promoting drug penetration along the GIT tract.…”

Section: Resultsmentioning

confidence: 99%

“… 73 Recently, in vivo subacute toxicity studies, ranging from 14 to 21 days, were reported to initially assess the toxicity of different nanoplatforms. 19 , 42 , 74 …”

Section: Resultsmentioning

confidence: 99%

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Precisely Fabricated Sulpiride-Loaded Nanolipospheres with Ameliorated Oral Bioavailability and Antidepressant Activity

Mohyeldin¹,

Samy²,

Ragab³

et al. 2021

IJN

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Background Sulpiride (SUL), is a selective antidopaminergic drug that had extensive biological activities. However, its sparingly aqueous solubility and limited gastrointestinal permeability lead to scanty oral bioavailability which hinders its clinical efficacy. Objective SUL-loaded lipospheres (SUL-LPS) were designed to serve as an oral biocompatible nanovector for improving SUL permeability as well as conquering its low oral absorption and then in turn enhancing its antidepressant action. Methods SUL-LPS were fabricated via two processing techniques namely, melt emulsification and solvent evaporation. The impact of different lipid cores, phospholipid shells together with various surfactant concentrations and types on the lipospheres properties were screened. Detailed physicochemical elucidations were performed followed by ex vivo permeation appraisal using the non-everted intestine model. The pharmacokinetic parameters of SUL-LPS, free SUL and marketed product were assessed following oral administration to healthy rats. Reserpine-induced depression rat model was used to assess the antidepressant action of SUL-LPS on which full behavioural and biochemical analysis was conducted. Safety attributes of nanoencapsulated SUL on the brain and other internal organs were evaluated. Results The optimum LPS revealed an excellent nanosize with a narrow PdI, negative zeta potential and acceptable entrapment efficiency of 68.62 nm, 0.242, −30.4 mV and 84.12%, respectively. SUL-LPS showed a sustained release pattern and 2.1-fold enhancement in the intestinal permeation parameters with low mucin interaction. Oral pharmacokinetic appraisal exhibited that LPS provided 3.4-fold improvement in SUL oral bioavailability together with long-circulating properties, relative to the free drug. Pharmacodynamic study confirmed the superior antidepressant action of SUL-LPS as evident by 1.6 and 1.25-fold elevation in the serotonin and dopamine expressions, respectively. Meanwhile, nanotoxicological appraisal proved the biocompatibility of SUL-LPS upon repetitive oral administration. Conclusion Rationally designed lipospheres hold promising in vitro and in vivo characteristics for efficient delivery of SUL with high oral bioavailability, antidepressant activity together with a good safety profile.

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Section: Resultscontrasting

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

“… 73 Recently, in vivo subacute toxicity studies, ranging from 14 to 21 days, were reported to initially assess the toxicity of different nanoplatforms. 19 , 42 , 74 …”

Section: Resultsmentioning

confidence: 99%

See 2 more Smart Citations

Precisely Fabricated Sulpiride-Loaded Nanolipospheres with Ameliorated Oral Bioavailability and Antidepressant Activity

Mohyeldin¹,

Samy²,

Ragab³

et al. 2021

IJN

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“…In order to assure SLN stability, cryoprotectants are typically added to SLN dispersions at concentrations of 10–15% (of the total formulation) prior to lyophilization to reduce particle aggregation and effect reconstitution [ 20 ]. Trehalose is an efficient cryoprotectant for SLN formulations [ 21 , 22 , 23 ]; it was therefore used at a concentration of 10% in the present study.…”

Section: Resultsmentioning

confidence: 99%

Lyophilized Drug-Loaded Solid Lipid Nanoparticles Formulated with Beeswax and Theobroma Oil

Amekyeh

Billa

2021

Molecules

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Solid lipid nanoparticles (SLNs) have the potential to enhance the systemic availability of an active pharmaceutical ingredient (API) or reduce its toxicity through uptake of the SLNs from the gastrointestinal tract or controlled release of the API, respectively. In both aspects, the responses of the lipid matrix to external challenges is crucial. Here, we evaluate the effects of lyophilization on key responses of 1:1 beeswax–theobroma oil matrix SLNs using three model drugs: amphotericin B (AMB), paracetamol (PAR), and sulfasalazine (SSZ). Fresh SLNs were stable with sizes ranging between 206.5–236.9 nm. Lyophilization and storage for 24 months (4–8 °C) caused a 1.6- and 1.5-fold increase in size, respectively, in all three SLNs. Zeta potential was >60 mV in fresh, stored, and lyophilized SLNs, indicating good colloidal stability. Drug release was not significantly affected by lyophilization up to 8 h. Drug release percentages at end time were 11.8 ± 0.4, 65.9 ± 0.04, and 31.4 ± 1.95% from fresh AMB-SLNs, PAR-SLNs, and SSZ-SLNs, respectively, and 11.4 ± 0.4, 76.04 ± 0.21, and 31.6 ± 0.33% from lyophilized SLNs, respectively. Thus, rate of release is dependent on API solubility (AMB < SSZ < PAR). Drug release from each matrix followed the Higuchi model and was not affected by lyophilization. The above SLNs show potential for use in delivering hydrophilic and lipophilic drugs.

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Potential Nanomaterials for the Treatment and Management of Diabetes Mellitus

Tiwari

Wadher

2023

Nanomaterials for Sustainable Development

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<p>Lipid-Based Gliclazide Nanoparticles for Treatment of Diabetes: Formulation, Pharmacokinetics, Pharmacodynamics and Subacute Toxicity Study</p>

Cited by 28 publications

References 48 publications

Precisely Fabricated Sulpiride-Loaded Nanolipospheres with Ameliorated Oral Bioavailability and Antidepressant Activity

Precisely Fabricated Sulpiride-Loaded Nanolipospheres with Ameliorated Oral Bioavailability and Antidepressant Activity

Lyophilized Drug-Loaded Solid Lipid Nanoparticles Formulated with Beeswax and Theobroma Oil

Potential Nanomaterials for the Treatment and Management of Diabetes Mellitus

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