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dc.contributor.author | Irie, Kazuhiro | en |
dc.contributor.author | Kikumori, Masayuki | en |
dc.contributor.author | Kamachi, Hiroaki | en |
dc.contributor.author | Tanaka, Keisuke | en |
dc.contributor.author | Murakami, Akira | en |
dc.contributor.author | Yanagita, Ryo C. | en |
dc.contributor.author | Tokuda, Harukuni | en |
dc.contributor.author | Suzuki, Nobutaka | en |
dc.contributor.author | Nagai, Hiroshi | en |
dc.contributor.author | Suenaga, Kiyotake | en |
dc.contributor.author | Nakagawa, Yu | en |
dc.contributor.alternative | 入江, 一浩 | ja |
dc.date.accessioned | 2012-07-05T02:32:36Z | - |
dc.date.available | 2012-07-05T02:32:36Z | - |
dc.date.issued | 2012 | - |
dc.identifier.issn | 0033-4545 | - |
dc.identifier.uri | http://hdl.handle.net/2433/157360 | - |
dc.description.abstract | Protein kinase C (PKC) isozymes are promising targets for anticancer therapy. Bryostatin-1 (bryo-1), a unique PKC activator with little tumor-promoting activity, is currently in clinical trials for the treatment of cancer. However, its limited availability from natural sources and its synthetic complexity have hampered studies of its mode of action and structural optimization as a therapeutic agent. The development of synthetically more accessible compounds with bryo-1-like activities is thus needed. Recently, we developed a simple and less lipophilic analogue of tumor-promoting aplysiatoxin (ATX) (aplog-1) as a promising lead for bryo-1-like anticancer drugs. Structure–activity studies suggested that local hydrophobicity around the spiroketal moiety of aplog-1 is a crucial determinant of its antiproliferative activity. The hydrophobic analogue (12,12-dimethyl-aplog-1) displayed more potent antiproliferative activity. Moreover, it showed little tumor-promoting activity and even suppressed the tumor promotion by 12-O-tetradecanoylphorbol 13-acetate (TPA) in vivo and in vitro. Aplog-1 and bryo-1 bound selectively to novel PKC isozymes (δ, η, and θ) while tumor promoters bound to both conventional and novel PKC isozymes. These results suggest that the unique biological activities of aplog-1 and bryo-1 are ascribable in part to the ability to bind to PKCδ, but weak binding to conventional PKC isozymes might also be important. | en |
dc.format.mimetype | application/pdf | - |
dc.language.iso | eng | - |
dc.publisher | International Union of Pure and Applied Chemistry | en |
dc.rights | © 2012 IUPAC. | en |
dc.subject | antiproliferative activity | en |
dc.subject | antitumor activity | en |
dc.subject | aplysiatoxin | en |
dc.subject | bioactive molecules | en |
dc.subject | biological activity | en |
dc.subject | bryostatin | en |
dc.subject | organic chemistry | en |
dc.subject | organic synthesis | en |
dc.subject | phorbol ester | en |
dc.subject | protein kinase C | en |
dc.subject | structure–activity | en |
dc.subject | tumor promoter | en |
dc.title | Synthesis and structure–activity studies of simplified analogues of aplysiatoxin with antiproliferative activity like bryostatin-1 | en |
dc.type | journal article | - |
dc.type.niitype | Journal Article | - |
dc.identifier.ncid | AA00797859 | - |
dc.identifier.jtitle | Pure and Applied Chemistry | en |
dc.identifier.volume | 84 | - |
dc.identifier.issue | 6 | - |
dc.identifier.spage | 1341 | - |
dc.identifier.epage | 1351 | - |
dc.relation.doi | 10.1351/PAC-CON-11-08-22 | - |
dc.textversion | publisher | - |
dcterms.accessRights | open access | - |
出現コレクション: | 学術雑誌掲載論文等 |
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