Modification of Drug Crystallization by Cyclodextrins in Pre-formulation Study

Iohara, Daisuke; Anraku, Makoto; Uekama, Kaneto; Hirayama, Fumitoshi

doi:10.1248/cpb.c18-00752

Cited by 8 publications

(5 citation statements)

References 40 publications

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“…Aprotinin (a small protein with a molecular weight of 6500 Da) is a competitive enzyme inhibitor of several serine proteases, such as trypsin and chymotrypsin [108]. It has been used as an enzyme inhibitor in various studies investigating protein and peptide drug absorption across Citric acid Insulin [96,97] Cyclodextrins Limaprost [98] Glycerides DuP 532 [99] Lauroyl carnitine chloride Insulin [100] Sodium lauryl sulfate (SLS/sodium dodecyl sulfate) Cefazolin [101] Sodium N-[8-(2-hydroxybenzoyl) aminocaprylate] Semaglutide [102] the intestinal membrane. One study has revealed that insulin-containing microemulsions concomitantly orally administered with aprotinin, compared with those without aprotinin, significantly decrease plasma glucose levels between 90-120 min after administration in both nondiabetic and diabetic rat models [109].…”

Section: Enzymatic Inhibitorsmentioning

confidence: 99%

Oral delivery of glutathione: antioxidant function, barriers and strategies

Wei

Thakur

Liu

et al. 2022

Acta Materia Medica

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Glutathione (GSH) is a tripeptide with potent antioxidant activity, which is involved in numerous basic biological processes and has been used for interventions in various degenerative diseases. However, oral delivery of GSH remains challenging, similarly to that of other protein and peptide drugs, because the physicochemical barriers in the gastrointestinal (GI) tract lead to low oral bioavailability. Although several approaches have been explored to improve delivery, such as co-administration with penetration enhancers and enzymatic inhibitors, or encapsulation into nanoparticles, microemulsions and liposomes, appropriate formulations with clinical therapeutic effects remain to be developed. This review discusses approaches explored to developing an oral GSH delivery system that could provide protection against proteolytic degradation in the GI tract and enhance molecular absorption across the epithelial membrane. This system may be beneficial for the design and development of an oral formulation of GSH in the future.

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Section: Enzymatic Inhibitorsmentioning

confidence: 99%

Oral delivery of glutathione: antioxidant function, barriers and strategies

Wei

Thakur

Liu

et al. 2022

Acta Materia Medica

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“…The polymorph control on drug crystals is a primary concern in pharmaceutics because the morphology differences lead to direct variances in drug efficacy. Therefore, the preceding reports on the polymorphism of CD-containing crystals are exclusively for their inclusion complexes, − while no polymorphism has hitherto been reported for uncomplexed native CDs. When native CDs spontaneously crystallize in aqueous solution, several water molecules are incorporated inside and outside the CD cavity. ,, For β-CD, the crystal structure with variable hydration water molecules ranging from 9.4 to 12.3, i.e ., β-CD·(9.4–12.3)H 2 O, has already been identified .…”

Section: Introductionmentioning

confidence: 99%

Optical Trapping-Induced New Polymorphism of β-Cyclodextrin in Unsaturated Solution

Shih

Hsu

Chen

et al. 2021

Crystal Growth & Design

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A new polymorph of β-cyclodextrin (β-CD) was produced by optical trapping with a 1064 nm continuous wave laser beam in D2O solution. Upon optical trapping of β-CD in unsaturated solutions, a single prism crystal or multiple plate crystals were formed at and near the laser focus. The resulting crystals differed in morphology and in the Raman spectrum. Furthermore, the solubility of the plate crystal in D2O was much lower than that of the prism crystal, implying that the former crystal is thermodynamically more stable than the latter. The single-crystal X-ray crystallographic analysis showed that the prism crystal has practically the same crystallographic parameters as the crystal reported for β-CD dodecahydrate and is thought to be the thermodynamically most stable phase. These results reveal that the plate crystal is a new polymorph characteristic of optical trapping. Crucially, this is the first success to produce a new polymorph via the laser-induced crystallization method. More interestingly, the generation probability of these two polymorphs turned out to be a critical function of the initial β-CD concentration, laser power, and laser polarization mode. In particular, the polymorphism could be entirely controlled by adjusting the initial concentration, which allowed us to obtain pure prism and plate crystals at high and low CD concentrations, respectively. The dynamics and mechanism of this unique optical trapping-induced polymorphism are discussed in terms of the pre-nucleation cluster size determined by the initial concentration, the trapping efficiency as a function of the cluster size and the laser power, and the molecular alignment in the pre-nucleation clusters steered by the laser polarization mode.

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“…Crystallization has been a topic of research due to its key role in geochemistry, biology, and synthetic materials, which are extensively applied in the chemical, pharmaceutical, and food sectors [1][2][3] . Especially in the pharmaceutical sector, 90% of the goods are crystalline organic compounds that require refinement through recrystallization procedures 4,5) .…”

Section: Introductionmentioning

confidence: 99%

A Facile Raman Spectroscopy Method for Online Monitoring of Crystal Plane Orientation of Favipiravir

Tang

Feng

Kang

et al. 2023

CHEMICAL & PHARMACEUTICAL BULLETIN

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The efficiency of pharmacotherapy is significantly influenced by the crystal habit and polymorphic form of the drugs. Especially due to the anisotropy of different facets in crystalline material, crystal habit impacts the physicochemical properties and behaviors of a drug, which has been rarely reported. This paper describes a facile method for online monitoring of crystal plane orientation of favipiravir(T-705) by Raman spectroscopy. Firstly, we investigated the synergy of multiple physicochemical fields (solvation, agitated flow fields, etc.), and then prepared favipiravir crystals with different orientations in a controllable manner. Secondly, to establish the connection between crystal planes and Raman spectra, the favipiravir crystals were theoretically analyzed at the molecular and structural levels using density functional theory (DFT) and 3D visualization tools. Finally, we based on standard samples and applied it to 12 actual samples to evaluate the crystal habit of favipiravir. The results are similar to the classical XRD method. Additionally, the XRD method is difficult to be monitored online, while the Raman method is non-contact, fast, and requires no sample preparation, showing a great application prospect in the pharmaceutical process.

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Modification of Drug Crystallization by Cyclodextrins in Pre-formulation Study

Cited by 8 publications

References 40 publications

Oral delivery of glutathione: antioxidant function, barriers and strategies

Oral delivery of glutathione: antioxidant function, barriers and strategies

Optical Trapping-Induced New Polymorphism of β-Cyclodextrin in Unsaturated Solution

A Facile Raman Spectroscopy Method for Online Monitoring of Crystal Plane Orientation of Favipiravir

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