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タイトル: Clonogenic assayを用いた腎細胞癌に対するインターフェロンの抗腫瘍効果の検討 --単独ならびに制癌剤との併用効果について--
その他のタイトル: Antiproliferative effect of interferon-alpha on human renal cell carcinoma in clonogenic assay--single and combination effect with cancer chemotherapeutic agent
著者: 大村, 清隆  KAKEN_name
塚本, 泰司  KAKEN_name
著者名の別形: Ohmura, Kiyotaka
Tsukamoto, Taiji
キーワード: Adult
Aged
Antineoplastic Agents/administration & dosage
Antineoplastic Combined Chemotherapy Protocols/pharmacology
Carcinoma, Renal Cell/pathology
Cell Division/drug effects
Dose-Response Relationship, Drug
Drug Synergism
Female
Humans
Interferon Type I, Recombinant/administration & dosage/pharmacology
Kidney Neoplasms/pathology
Male
Middle Aged
Tumor Cells, Cultured/drug effects/pathology
Tumor Stem Cell Assay
発行日: May-1989
出版者: 泌尿器科紀要刊行会
誌名: 泌尿器科紀要
巻: 35
号: 5
開始ページ: 737
終了ページ: 747
抄録: Clonogenic assayを用いて, 腎細胞癌に対するインターフェロン(IFN)の抗腫瘍効果を検討した所, 濃度依存性がみられ, 手術時採取した標本15例に就て, コロニー形成率が低下する群(10例)と, 高濃度でもコロニー形成率の低下しない群(5例)がみられた.rIFN-αA 1, 000 IU/ml濃度での15例の感受性は3例に止まった.IFNの抗腫瘍効果には限界があり, 株化腎細胞癌, 株化培養細胞を用いての制癌剤併用効果は, VBL, ADM, MTX, 5-FU何れとも効果があった
With human tumor clonogenic assay, the direct antiproliferative activity of recombinant human leukocyte interferon alpha (IFN-alpha) was investigated on human renal cell carcinomas (RCCs), which consisted of a human RCC cell line (ACHN), two human RCC xenografts and fifteen primary RCCs. The combination effect of IFN-alpha with a cancer chemotherapeutic agent was studied, as well, with the assay system. IFN-alpha showed a dose-dependent antiproliferative activity against the human RCCs. The clonal growth of ACHN cell line was inhibited by less than 50% at the concentration of 1, 000 IU/ml. Two xenografts had a different sensitivity to IFN-alpha, in which the percent colony formation was less than 20% in RCC-3 at the concentration of 100-100, 000 IU/ml, while in RCC-4 more than 50% even at the high concentration of 10, 000 IU/ml. In 15 primary tumors obtained at surgery, two types of response to IFN-alpha were demonstrated. One was the response in which the colony formation was inhibited in a dose-dependent manner as an increment of IFN-alpha concentration, and the other in which the colony formation was not sufficiently inhibited even at the high concentration of IFN-alpha. The dose-dependent inhibition of colony formation was demonstrated in 10 out of 15 specimens (66.7%). When the colony formation suppressed to less than 50% of control was considered to be sensitive to IFN-alpha, 6.7% of these 15 primary tumors were sensitive to IFN-alpha at 100 IU/ml, 20.0% at 1, 000 IU/ml and 20.0% at 10, 000 IU/ml. Combination effects of IFN-alpha and with each of four different cancer chemotherapeutic agents (vinblastine, adriamycin, methotrexate, 5-fluorouracil) were investigated on the ACHN cell line. Every combination type produced a subadditive or synergistic combination effect. In particular, the combination of IFN-alpha with vinblastine of more than 0.1 microgram/ml concentration yielded a combination effect of statistical significance (p less than 0.001). Even against premary tumors, the combination of IFN-alpha with vinblastine showed a synergistic effect in one out of every three tumors. These results suggested that the combination of IFN-alpha with a cancer chemotherapeutic agent would enhance the clinical effect of IFN-alpha alone in only a certain situation.
URI: http://hdl.handle.net/2433/116545
PubMed ID: 2801371
出現コレクション:Vol.35 No.5

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