TRANSLATIONAL CORRELATES OF AN EPOTHILONE B ANALOG

埃坡霉素 B 类似物的翻译相关性

• 批准号: 6377952
• 负责人: SUSAN BAND HORWITZ
• 金额: $ 8.38万
• 依托单位: ALBERT EINSTEIN COLLEGE OF MEDICINE
• 依托单位国家: 美国
• 财政年份: 2000
• 资助国家: 美国
• 起止时间: 2000-04-01 至 2002-03-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/6377952
• 关键词: BCL2 gene /protein; HeLa cells; analog; antineoplastics; apoptosis; biological signal transduction; clinical research; clinical trial phase I; drug metabolism; drug resistance; female; gene induction /repression; gene mutation; human subject; human therapy evaluation; membrane transport proteins; multidrug resistance; neoplasm /cancer chemotherapy; ovary neoplasms; p53 gene /protein; paclitaxel; pharmacokinetics; phosphoproteins; tubulin

The optimum dose, clinical toxicity and antitumor activity of BMS-247550 will be determined in a dose-escalation phase I clinical trial of patients with advanced Taxol-refractory ovarian cancer. We will evaluate the effects of BMS-24755 on its molecular target, the microtubule, specifically beta- tubulin and investigate its role in modulating the expression and function of defined biological markers that regulate drug transport, cytoskeletal integrity and cell death. All results will be correlated with pharmacokinetics, clinicopathology and patient response using univariate and multivariate analyses, and the findings from this pilot study applied to a large-scale study. Tumor biopsies will be harvested from pre- and post- treatment patients, together with malignant fluid, when available. Total RNA, DNA and protein will be isolated from all specimens and stored at 70 centigrade. Correlates of BMS-247550 dose pharmacokinetics with microtubule bundle and aster formation in peripheral blood mononuclear cells (PBMC's ) will be determined. The primary aims of this scientific exploratory study are: 1. To evaluate the relationship between tumor response and (a) the occurrence of mutation in the class I isotype of beta-tubulin and (b) beta- tubulin isotype distribution. Mutations in beta-tubulin have been isolated in Taxol-resistant cancer cell lines, and mutations in the GTP-binding regions of beta-tubulin have been associated with poor response/survival to Taxol monotherapy in NSCLC patients. 2. To investigate MDR1, MRP and cMOAT mRNA and protein expression as prognosticators of tumor response to BMS-247550. 3. To correlate the effects of BMS-247550 on the expression of proteins which regulate apoptosis, such as bcl-2 family members and IAP (inhitors of apoptosis) members, e.g. survivin and p53. Changes in mitochondrial membrane potential, an early indicator of apoptosis, will be evaluated by flow cytometry and compared in pre-and post-treatment tumor samples and correlated with response. 4. To determine the relationship between stathmin expression and phosphorylation status as a function of response.

BMS-247550 的最佳剂量、临床毒性和抗肿瘤活性将在晚期紫杉醇难治性卵巢癌患者的剂量递增 I 期临床试验中确定。我们将评估 BMS-24755 对其分子靶标微管（特别是 β-微管蛋白）的影响，并研究其在调节特定生物标志物的表达和功能中的作用，这些生物标志物调节药物转运、细胞骨架完整性和细胞死亡。所有结果将通过单变量和多变量分析与药代动力学、临床病理学和患者反应相关，并将该试点研究的结果应用于大规模研究。肿瘤活检将从治疗前和治疗后的患者身上采集，如果有的话，还会采集恶性液体。将从所有样本中分离出总RNA、DNA和蛋白质，并在70摄氏度下保存。将确定 BMS-247550 剂量药代动力学与外周血单核细胞 (PBMC) 中微管束和 aster 形成的相关性。这项科学探索性研究的主要目的是： 1. 评估肿瘤反应与 (a) β-微管蛋白 I 类同种型突变的发生和 (b) β-微管蛋白同种型分布之间的关系。 β-微管蛋白突变已在紫杉醇耐药癌细胞系中分离出来，β-微管蛋白 GTP 结合区的突变与 NSCLC 患者对紫杉醇单药治疗的不良反应/生存相关。 2. 研究 MDR1、MRP 和 cMOAT mRNA 和蛋白表达作为肿瘤对 BMS-247550 反应的预测因子。 3. 关联 BMS-247550 对调节细胞凋亡的蛋白质表达的影响，例如 bcl-2 家族成员和 IAP（细胞凋亡抑制剂）成员，例如生存素和p53。线粒体膜电位的变化是细胞凋亡的早期指标，将通过流式细胞术进行评估，并在治疗前后的肿瘤样本中进行比较，并与反应相关。 4.确定stathmin表达和磷酸化状态之间作为反应函数的关系。