Genotechnologic Analysis of Control System of Proliferation and Metastasis by Gangliosides in Melanoma

• Project/Area Number: 10670793
• Research Category: Grant-in-Aid for Scientific Research (C)
• Allocation Type: Single-year Grants
• Section: 一般
• Research Field: Dermatology
• Research Institution: Yamaguchi University
• Principal Investigator: SHIMIZU Takahiro Yamaguchi University School of Medicine, Assistant, 医学部, 助手 (10263774)
• Co-Investigator(Kenkyū-buntansha): YASUI Hiroo Yamaguchi University Hospital, Assistant, 医学部・附属病院, 助手 (70304483) ; HAMAMOTO Yoshiaki Yamaguchi University School of Medicine, Assistant Professor, 医学部, 講師 (90238080) ; MUTO Masahiko Yamaguchi University School of Medicine, Professor, 医学部, 教授 (40175625)
• Project Period (FY): 1998 – 1999
• Project Status: Completed (Fiscal Year 1999)
• Budget Amount: ¥700,000 (Direct Cost: ¥700,000); Fiscal Year 1999: ¥700,000 (Direct Cost: ¥700,000)
• Keywords: Malignant melanoma / Ganglioside / SK-MEL-28 / GD3-positive cell / GD3-deficient melanomma cell line / Cell proliferation / Extracellular matrix protein / Cell attachment / GD3欠損ヒト黒色腫変異細胞株N2 / GD3合成酵素cDNA / トランスフェクト

Research Abstract

We investigated biological functions of gangliosides in melanoma using cell lines and tissue specimens obtained from the patients. SK-MEL-28 (GD3- and GM3-positive cell line) had higher activity of cell proliferation than its GD3-defecient mutant clone. Metastatic melanoma patients with the new ganglioside expression (GM3-predominant) seemed to survive longer than the ones with increased levels of both GM3 and GD3. GD3 was considered to have pivotal parts in concering tumor progression and prognosis. The GD3-deficient cell line, however, showed increased expression of α2β1 and α3β1 integrin receptors and significantly higher ability to adhere to extracellular matrix proteins including type I and IV collagens and laminin than the parent clone (SK-MEL-28). The treatment with monoclonal antibodies against GDs in SK-MEL-28 inhibited the cell attachment to the matrix proteins. Our findings suggest that gangliosides GM3 (by influencing integrin receptor levels) and GD3 (by interacting directly with matrix proteins) might play different biological roles in the progression of melanoma.

Research Products

• [Publications] Nakano J: "Lack of Induction of Anti-Gangrioside GM_3 antibody in the Patients with Maignant Melanoma in Japanese"Pigment Cell Research. 11. 213-215 (1998)
  • Description: 「研究成果報告書概要(和文)」より
• [Publications] Nakano J: "Biologic Roles of Gangrioside GM_3 and GD_3 in the Attachment of human Melanoma Cells to Extramatrix Proteins"Journal of Investigative Dermatology Symposium Proceedings. 4. 173-176 (1999)
  • Description: 「研究成果報告書概要(和文)」より
• [Publications] 武藤正彦: "ヒトメラノーマの分子疫学"腫瘍マーカー研究会誌(電子ジャーナル). (掲載予定). (2000)
  • Description: 「研究成果報告書概要(和文)」より
• [Publications] Nakano, J., et al: "Lack of Induction of Anti-Gangrioside GMィイD23ィエD2 antibody in the Patients with Malignant Melanoma in Japanese"Pigment Cell Research. 11. 213-215 (1998)
  • Description: 「研究成果報告書概要(欧文)」より
• [Publications] Nakano, J., et al: "Biologic Roles of Gangrioside GMィイD23ィエD2 and GDィイD23ィエD2 in the Attachment of Human Melanoma Cells to Extramatrix Proteins"Journal of Investigative Dermatology Symposium Proceedings. 4. 173-176 (1999)
  • Description: 「研究成果報告書概要(欧文)」より
• [Publications] Muto, M., et al: "Molecular Epidemiology of Human Melanoma"Journal of Tumor Marker research (an electronic journal). in press. (2000)
  • Description: 「研究成果報告書概要(欧文)」より
• [Publications] Nakano J: "Lack of Induction of Anti-Gangrioside GM_3 antibody in the Patients with Malignant Melanoma in Japanese"Pigment Cell Research. 11. 213-215 (1998)
• [Publications] Nakano J: "Biologic Roles of Gangrioside GM_3 and GD_3 in the Attachment of Human Melanoma Cells to Extramatrix Proteins"Journal of Investigative Dermatology Symposium Proceedings. 4. 173-176 (1999)
• [Publications] 武藤正彦: "ヒトメラノーマの分子疫学"腫瘍マーカー研究会誌(電子ジャーナル). (掲載予定). (2000)
• [Publications] Nakano J: "Lack of Induction of Anti-Gangrioside GM3 Antibody in the Patients with Malignant Melanoma in Japanese" Pigment Cell Research. 11. 213-215 (1998)