Tatsuki Shinoda scite author profile

Electron trapping sites in titanium(IV) oxide photocatalyst powders were investigated by photoacoustic (PA) Fourier transform near-infrared spectroscopy (FT-NIR) and mid-infrared spectroscopy (FT-MIR). PA measurements using FT-NIR and FT-MIR enabled in situ observation of the energy levels of electron trapping sites in wide energy levels (0.1−1.9 eV) below the bottom of the conduction band. During ultraviolet (UV) irradiation, PA intensity increased depending on the wavenumber, and changes in the PA spectra were observed as a result of the trivalent titanium species generated by accumulation of electrons at trapping sites. Moreover, the PA spectral shape during UV irradiation was essentially different between the crystal structures, and it greatly depended on the crystal structure rather than other properties such as specific surface area and particle size. The results for various samples suggest that anatase has shallower energy levels of electron trapping sites than those of rutile and brookite, with the main energy level of the trapping sites being deep in the order of brookite > rutile > anatase. Thus, the PA technique using FT-NIR and FT-MIR is an effective method for measurements of energy levels of electron trapping sites in semiconductor photocatalysts.

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Electroresponsive Pulsatile Depot Delivery of Insulin from Poly(dimethylaminopropylacrylamide) Gel in Rats

KagataniX¹,

Shinoda²,

Konno³

et al. 1997

Journal of Pharmaceutical Sciences

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We describe a model for pulsatile drug delivery with an electroresponsive polymer that is stimulated by an externally applied electrical field. Insulin loaded in an electroresponsive poly(dimethylaminopropylacrylamide) (PDMAPAA) gel was administered as a subcutaneous depot in rats. The gel induced a pulsatile plasma glucose decrease in correspondence to stimulation with a constant current of 1.0 mA (0.36 mA/cm2). The first drop occurred at 0.5 h after a 1-min application of current at 0 h and the second drop occurred at 3 h after a 10-min application of current at 2 h. Calculation of pharmacological bioavailability showed that the gel released 0.12% of the loaded insulin after these two stimuli. This in vivo study demonstrates the feasibility of this pulsatile delivery system. The mechanism of insulin release from the electroresponsive PDMAPAA gel is associated with electrokinetic flow of solvated insulin with water; that is, transportation process of counterions (electrophoresis) and water molecules (electroosmosis) in the crosslinked polyelectrolyte gel network.

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Lactose-carrying polystyrene as a drug carrier: investigation of body distributions to parenchymal liver cells using 125I-labelled lactose-carrying polystyrene

Goto

Yura

Chang

et al. 1994

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In vivo fate of folate–BSA in non‐tumor‐ and tumor‐bearing mice

Shinoda¹,

Takagi²,

Maeda³

et al. 1998

Journal of Pharmaceutical Sciences

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KB tumor cells exhibit an increased number of folate receptors on their membrane. This receptor has been proposed as a promising target for tumor drug targeting. Therefore, the disposition of folate-conjugated bovine serum albumin (folate-BSA) was examined as a model system for drug targeting. Nude mice which had received KB tumor cell transplants were given bolus intravenous administration of either 111In-labeled folate-BSA (111In-folate-BSA; 1 mg/kg) or unmodified 111In-BSA (111In-BSA; 1 mg/kg). The disposition characteristics and pharmacokinetics of 111In-folate-BSA were compared with those of the 111In-BSA as a control. The half-life of the beta-phase of 111ln-folate-BSA in plasma was 140 min. The tumor uptake rate index for 111In-folate-BSA was 0.46 microL/min/g, and that for 111In-BSA was 0.32 microL/min/g. This index of 111In-folate-BSA was slightly higher than that of 111In-BSA in vivo, by a factor of 1.4. In vivo experiments showed folate-BSA has a relatively long plasma duration. 111In-folate-BSA also showed selective distribution to tumors, but not as great as recent results from in vitro experiments. Therefore, the low vascular permeability of BSA into solid tumor tissue and inhibition of folate-mediated 111In-folate-BSA uptake by tumor cells from the blood may be the rate-limiting factor of distribution.

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Characteristics of the gastric pH profiles of unfed and fed cynomolgus monkeys as pharmaceutical product development subjects

Kondo¹,

Shinoda²,

Nakashima³

et al. 2002

Biopharm & Drug Disp

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Gastric pH is an important factor which significantly affects the dissolution of drugs, and therefore their bioavailability. In this study, the gastric pHs were measured directly with a miniature pH electrode inserted through the nostril into the body of the stomach of cynomolgus monkeys. Results from three separate sets of measurements using the same male monkeys indicated that the median gastric pH profiles of unfed monkeys were low, fluctuating between pH 1 and pH 3. However, the median gastric pHs in fed monkeys given about 108 g of a biscuit-type solid food, which are commonly provided, shifted toward a more neutral range between pH 5 and pH 7, and remained in this range for about 9 h. This result contrasted with reported results for humans after eating a standard meal, which showed a neutral range between pH 5 and pH 7 for a brief period. Consequently, these results indicate that although the gastric pH of unfed cynomolgus monkeys is similar to that of fasting humans, there is a great difference in the gastric pH profiles between humans and monkeys after eating, which suggests that further studies are needed to establish optimal feeding conditions for bioavailability studies in monkeys.

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Tatsuki Shinoda

Photoacoustic Fourier Transform Near- and Mid-Infrared Spectroscopy for Measurement of Energy Levels of Electron Trapping Sites in Titanium(IV) Oxide Photocatalyst Powders

Electroresponsive Pulsatile Depot Delivery of Insulin from Poly(dimethylaminopropylacrylamide) Gel in Rats

Lactose-carrying polystyrene as a drug carrier: investigation of body distributions to parenchymal liver cells using 125I-labelled lactose-carrying polystyrene

In vivo fate of folate–BSA in non‐tumor‐ and tumor‐bearing mice

Characteristics of the gastric pH profiles of unfed and fed cynomolgus monkeys as pharmaceutical product development subjects

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