Yuhei Iwata scite author profile

Yuhei Iwata

5Publications

79Citation Statements Received

3Citation Statements Given

How they've been cited

116

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Affiliations

Shiseido Group (Japan)

Publications

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Evaluation of antitumor activities of hyaluronate binding antitumor drugs: synthesis, characterization and antitumor activity

Akima

Itô

Iwata

et al. 1996

Journal of Drug Targeting

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To enhance the selective delivery of antitumor drugs into regional lymph nodes and cancerous tissues via a hyaluronate (HA) receptor (CD44), we synthesized HA-mitomycin C complex and HA-epirubicin complex. To investigate the specific distribution of HA into regional lymph nodes and to evaluate the HA receptor on lewis lung carcinoma cells, we also synthesized 14C-labelled HA and fluorescent HA (FR-HA). The metabolic studies of 14C-HA and HA-epirubicin complex were performed in rats. The specific distribution of both compounds to the lymph nodes were observed after sc treatment. Internalization mechanisms of HA into carcinoma cells (lewis lung carcinoma) via HA receptor was investigated using fluorescent HA (FR-HA) in vitro. Internalization of FR-HA following binding to the cell surfaces was observed. HA-Mitomycin C (MMC) exhibited potent anti-metastatic effects against lewis lung carcinoma implanted in mice at an extremely low dose (0.01 mg/kg) whereas free MMC had no effects.

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Effect of 2-Hydroxypropyl-β-cyclodextrin on Percutaneous Absorption of Methyl Paraben

Tanaka

Iwata

Kouzuki

et al. 1995

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A potential use of 2-hydroxypropyl-beta-cyclodextrin (HP-beta-CyD) to solubilize methyl paraben and to suppress its percutaneous absorption was examined, and compared with nonionic surfactant HCO-60. HP-beta-CyD significantly increased the solubility of methyl paraben in water, where the apparent 1:1 stability constant of the soluble complex was determined to be 2150 M-1. The in-vitro cutaneous permeability of methyl paraben through an isolated skin of hairless mouse was suppressed by HP-beta-CyD, thus promoting the bioconversion of methyl paraben to the less toxic metabolite, p-hydroxybenzoic acid (p-HBA) in the epidermis. These effects of HP-beta-CyD were greater than those of HCO-60. HP-beta-CyD (2% w/v) reduced the in-vivo percutaneous absorption of methyl paraben by 66% 24 h after the topical application of a solution containing [14C]methyl paraben to hairless mouse skin. Additionally, the percutaneous absorption of [14C]HP-beta-CyD was confirmed to be extremely low. These results suggest that HP-beta-CyD is useful in liquid preparations of methyl paraben for topical application.

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Investigation on improving percutaneous absorption of amino acid.

Kouzuki¹,

Iwata²,

Kobayashi³

1995

DDS

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Percutaneous absorption of amino acids. (2).

Kouzuki¹,

Nomura²,

Iwata³

1996

DDS

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Studies on the Metabolic Fate of Sodium Hyaluronate (SL-1010) after Intra-articular Administration. (I). Distribution, Metabolism and Excretion after Intra-articular Injection into Rabbit Knee.

Akima

Sato

Hasegawa

et al. 1993

Drug Metabolism and Pharmacokinetics

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Yuhei Iwata

Evaluation of antitumor activities of hyaluronate binding antitumor drugs: synthesis, characterization and antitumor activity

Effect of 2-Hydroxypropyl-β-cyclodextrin on Percutaneous Absorption of Methyl Paraben

Investigation on improving percutaneous absorption of amino acid.

Percutaneous absorption of amino acids. (2).

Studies on the Metabolic Fate of Sodium Hyaluronate (SL-1010) after Intra-articular Administration. (I). Distribution, Metabolism and Excretion after Intra-articular Injection into Rabbit Knee.

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