首页> 外文期刊>Japanese journal of clinical oncology. >Drug-induced apoptosis and p53, BCL-2 and BAX expression in breast cancer tissues in vivo and in fibroblast cells in vitro.
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Drug-induced apoptosis and p53, BCL-2 and BAX expression in breast cancer tissues in vivo and in fibroblast cells in vitro.

机译:药物诱导的细胞凋亡和P53,BCL-2和体内乳腺癌组织中的BAX表达和体外成纤维细胞。

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BACKGROUND: Chemotherapeutic management of breast cancers is a difficult task as they show significant differences in chemosensitivity. The present study was undertaken to determine the usefulness of the apoptosis-related factors as indicators of tumor sensitivity to 5'-deoxyfluorouridine (5'-DFUR) in breast cancers. METHODS: (1) Forty-six breast cancer patients were randomly assigned to a group in which oral 5'-DFUR (1200 mg/day) was administered for more than 5 days before operation (24 patients) and a control group who received no preoperative chemotherapy (22 patients). Surgical specimens were examined for the frequency of apoptotic cells [apoptotic index (AI)] by a terminal deoxynucleotidyl transferase-mediated deoxyuridine triphosphate nick end labeling method and for the expression of p53, BCL-2 and BAX by immunohistochemical staining. (2) Normal human diploid fetal lung fibroblast, IMR90 and SV40 transformed IMR90 were exposed to 5-FU. Apoptotic cells were detected by flow cytometry and BCL-2 and BAX mRNAs by real-time quantitative RT-PCR analysis. RESULTS: (1) No significant difference in the AIs or in BCL-2 and BAX scores was observed between the 5'-DFUR-treated and control groups. However, in the p53 negative subgroup (n = 36), AI and BAX scores were higher and BCL-2 scores lower in the 5'-DFUR group than in the control group (P = 0.006, 0.008 and 0.050, respectively). (2) The sensitivity of IMR90 was significantly decreased by SV40 transformation and the 5-FU-induced cytotoxicity was mainly due to induction of apoptosis. The BCL-2/BAX mRNA ratio was decreased in response to 5-FU in IMR90. These results correlated with our clinical data. CONCLUSIONS: Preoperative treatment with 5'-DFUR induced apoptosis and changes in BCL-2 and BAX expression in p53 negative breast cancers. p53 status, AI and the BCL-2/BAX ratio may be useful information for the choice of postoperative chemotherapy for breast cancer.
机译:背景:乳腺癌的化学治疗管理是一项艰巨的任务,因为它们表现出大量的化学敏感性差异。本研究旨在确定凋亡相关因素的有用性,作为乳腺癌中肿瘤敏感度(5'-DFUR)的肿瘤敏感性的指标。方法:(1)(1)将46例乳腺癌患者随机分配给其中口服5'-DFUR(1200mg /天)在手术前(24名患者)和收到没有术前化疗(22名患者)。通过末端脱氧核苷酸转移酶介导的脱氧核酸三磷酸碎片末端标记方法检查外科标本[凋亡指数(AI)]的偶溶瘤细胞频率[凋亡指数(AI)]。通过免疫组化染色表达P53,BCL-2和BAX的表达。 (2)正常人类二倍体胎儿肺成纤维细胞,IMR90和SV40转化的IMR90暴露于5-FU。通过流式细胞术和Bcl-2和Bax MRNA通过实时定量RT-PCR分析检测凋亡细胞。结果:(1)在5'-DFUR处理和对照组之间观察到AIS或BCL-2中没有显着差异和BCL-2和BAX评分。然而,在p53阴性亚组(n = 36)中,AI和Bax评分较高,并且在5'-dfur组中比对照组中的Bcl-2分别降低(P = 0.006,0.008和0.050)。 (2)SV40转化的IMR90的敏感性显着降低,5-FU诱导的细胞毒性主要是由于诱导细胞凋亡。响应于IMR90中的5-FU,BCL-2 / BAX mRNA比率降低。这些结果与我们的临床数据相关。结论:术前治疗5'-DFUR诱导凋亡和Bcl-2中Bcl-2的变化和P53阴性乳腺癌中的Bax表达。 P53状态,AI和BCL-2 / BAX比率可能是用于选择乳腺癌术后化疗的有用信息。

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