Molecular Basis of Carcinogenesis of Aguired Cystic Disease of the Kidney

• Project/Area Number: 04670982
• Research Category: Grant-in-Aid for General Scientific Research (C)
• Allocation Type: Single-year Grants
• Research Field: Urology
• Research Institution: Tokyo Women's Medical College
• Principal Investigator: TOMA Hiroshi Tokyo Women's Medical College. Department of Urology. Professor, 医学部, 教授 (90075549)
• Co-Investigator(Kenkyū-buntansha): 山崎 雄一郎 東京女子医科大学, 医学部 (40200670) ; ITO Fumio Tokyo Women's Medical College. Department of Urology. Clinical Fellow., 医学部, 助手 (20211683) ; NAKAZAWA Hayakazu Tokyo Women's Medical College. Department of Urology. Assistant Professor, 医学部, 助教授 (00147381)
• Project Period (FY): 1992 – 1994
• Project Status: Completed(Fiscal Year 1994)
• Budget Amount: ¥2,100,000 (Direct Cost : ¥2,100,000); Fiscal Year 1994 : ¥600,000 (Direct Cost : ¥600,000); Fiscal Year 1993 : ¥600,000 (Direct Cost : ¥600,000); Fiscal Year 1992 : ¥900,000 (Direct Cost : ¥900,000)
• Keywords: RENAL CELL CARCINOMA / AQUIRED CYSTIC DISEASE OF KIDNEY / DIPHENYL THIAZOLE / N-NITROSOMORPHOLINE / N-nitrosomorpholin / 後天性多嚢胞化腎(ACDK) / diphenylthiazole(DPT) / introsomorpholine(NNM) / 異型嚢胞 / 癌抑制遺伝子 / 癌遺伝子 / dipheny thiazole(DPT) / nitrosomorpholine(NNM) / 異形嚢胞

Research Abstract

Recently, it is becoming a serious problem that patients with long term hemodialysis frequently develop aquired cystic disease of the kidney (ACDK), which presents a high rate of complication with renal cell carcinoma. In order to elucidate the mechamism by which renal cell cancer occurs in ACDK,we tried to establish a model of renal cell tumor derived from diphenyl thiazole (DPT) -induced polycystic kidney disease (PKD) in rats. In addition, we tried to analyze the early changes at molecular level during DPT-induced renal cyst formation to reveal the gene expressions specific to DPT-induction. For the former purpose, we administered N-nitrosomorpholine (NNM) known as a powerful carcinogenic substance to the rats with DPT-induced PKD and observed the neoplastic lesions derived from epithelium of cysts in two of 10 kidneys. For the latter purpose, we examined the structural change of extracellular matrix by immunohistochemical analysis of laminin, collagen type III and IV and chased the genes expressing specifically to the early phase of DPT-induced cyst formation by the run-on transcription and the RNA differential display analysis. As a result, we observed the expression of several genes including c-myc, c-fos and c-erbB_2 decreased the early days after administration of DPT.In addition, we obtained four candidates of those genes and determined the partial cDNA sequences of two candidates, which were not identical to any cDNA sequence already determined. From now on, we are goning to identify other genes expressing specifically to DPT-induction and next to search NNM-specific genes.

Research Products

• [Publications] 東間 紘: "腎細胞癌の多発性と腎機能温存手術" KARKINOS. 5(5). 531-538 (1992)
• [Publications] 中沢 速和: "透析患者の腎癌とACDK" 現代医療. 25(1). 491-496 (1993)
• [Publications] 東間 紘: "嚢胞腎の臨床的検討" 腎と透析. 32(1). 105-108 (1992)
• [Publications] 東間 紘: "ラット嚢胞腎の進展に及ぼすthromboxane synthesis inhibitorの効果" 医学のあゆみ. 157(8). 487 (1991)
• [Publications] H. Nakazawa: "DNA ploidy and proliferating cell nuclear antigens in renal cell carcinoma." UROLOGY 1992, a cura di LUCIANO GIULIANI PAOLO PUPPO. 331-334 (1992)