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著作: Taneichi Maiko/Ishida Hideaki/Kajino Kiichi/Ogasawara Kazumasa/Tanaka Yuriko/[笠井 道之]/Mori Masahito/Nishida Mitsuhiro/Yamamura Hiroyuki/Mizuguchi Junichiro/Uchida Tetsuya/Antigen chemically coupled to the surface of liposomes are cross-presented to CD8+ T cells and induce potent antitumor immunity./[The Journal of Immunology]

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LastModified
2013年6月13日(木) 15:21:45
Operator
三木 ちひろ
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[センター長]/[徳島大学.疾患プロテオゲノム研究センター]
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種別 必須 学術論文(審査論文)
言語 必須 英語
招待 推奨
審査 推奨 Peer Review
カテゴリ 推奨
共著種別 推奨
学究種別 推奨
組織 推奨
著者 必須
  1. (英) Taneichi Maiko
    役割 任意
    貢献度 任意
    学籍番号 推奨
  2. (英) Ishida Hideaki
    役割 任意
    貢献度 任意
    学籍番号 推奨
  3. (英) Kajino Kiichi
    役割 任意
    貢献度 任意
    学籍番号 推奨
  4. (英) Ogasawara Kazumasa
    役割 任意
    貢献度 任意
    学籍番号 推奨
  5. (英) Tanaka Yuriko
    役割 任意
    貢献度 任意
    学籍番号 推奨
  6. 笠井 道之
    役割 任意
    貢献度 任意
    学籍番号 推奨
  7. (英) Mori Masahito
    役割 任意
    貢献度 任意
    学籍番号 推奨
  8. (英) Nishida Mitsuhiro
    役割 任意
    貢献度 任意
    学籍番号 推奨
  9. (英) Yamamura Hiroyuki
    役割 任意
    貢献度 任意
    学籍番号 推奨
  10. (英) Mizuguchi Junichiro
    役割 任意
    貢献度 任意
    学籍番号 推奨
  11. (英) Uchida Tetsuya
    役割 任意
    貢献度 任意
    学籍番号 推奨
題名 必須

(英) Antigen chemically coupled to the surface of liposomes are cross-presented to CD8+ T cells and induce potent antitumor immunity.

副題 任意
要約 任意

(英) We have previously demonstrated that liposomes with differential lipid components display differential adjuvant effects when Ags are chemically coupled to their surfaces. In the present study, Ag presentation of liposome-coupled OVA was investigated in vitro, and it was found that OVA coupled to liposomes made using unsaturated fatty acid was presented to both CD4+ and CD8+ T cells, whereas OVA coupled to liposomes made using saturated fatty acid was presented only to CD4+ T cells. Confocal laser scanning microscopic analysis demonstrated that a portion of the OVA coupled to liposomes made using unsaturated, but not saturated fatty acid, received processing beyond the MHC class II compartment, suggesting that the degradation of OVA might occur in the cytosol, and that the peptides generated in this manner would be presented to CD8+ T cells via MHC class I. The ability to induce cross-presentation of an Ag coupled to liposomes consisting of unsaturated fatty acid was further confirmed by in vivo induction of CTL and by the induction of tumor eradication in mice; E.G7 tumors in mice that received combined inoculation with OVA(257-264)-liposome conjugates, CpG, and anti-IL-10 mAbs were completely eradicated. In those mice, the frequency of CD8+ T cells reactive with OVA(257-264) peptides in the context of H-2K(b) was significantly increased. These results suggested that, by choosing lipid components for liposomes, surface-coupled liposomal Ags might be applicable for the development of tumor vaccines to present tumor Ags to APCs and induce antitumor responses.

キーワード 推奨
  1. (英) Animals
  2. (英) Antigens
  3. (英) CD4-Positive T-Lymphocytes
  4. (英) CD8-Positive T-Lymphocytes
  5. (英) Cells, Cultured
  6. (英) Cross-Priming
  7. 細胞質分裂(cytokinesis)
  8. (英) Female
  9. (英) Intracellular Membranes
  10. リポソーム(liposomes)
  11. (英) Mice
  12. (英) Mice, Inbred BALB C
  13. (英) Mice, Inbred C57BL
  14. (英) Neoplasms, Experimental
  15. (英) Ovalbumin
発行所 推奨
誌名 必須 The Journal of Immunology([The American Association of Immunologists])
(pISSN: 0022-1767, eISSN: 1550-6606)
ISSN 任意 0022-1767
ISSN: 0022-1767 (pISSN: 0022-1767, eISSN: 1550-6606)
Title: Journal of immunology (Baltimore, Md. : 1950)
Title(ISO): J Immunol
Publisher: American Association of Immunologists
 (NLM Catalog  (Scopus  (CrossRef (Scopus information is found. [need login])
必須 177
必須 4
必須 2324 2330
都市 任意
年月日 必須 2006年 8月 15日
URL 任意
DOI 任意
PMID 任意 16887993    (→Scopusで検索)
CRID 任意
WOS 任意 000239745300040
Scopus 任意
評価値 任意
被引用数 任意
指導教員 推奨
備考 任意
  1. (英) Affiliation: Department of Safety Research on Blood and Biological Products, National Institute of Infectious Diseases, 4-7-1 Gakuen, Musashimurayama-city, Tokyo, Japan.

  2. (英) PublicationType: Journal Article

  3. (英) PublicationType: Research Support, Non-U.S. Gov't