ABCB5 P-Glycoprotein in Cancer Multidrug Resistance

ABCB5 P-糖蛋白在癌症多药耐药性中的作用

• 批准号: 7034755
• 负责人: Markus H. Frank
• 金额: $ 30万
• 依托单位: BOSTON CHILDREN'S HOSPITAL
• 依托单位国家: 美国
• 财政年份: 2006
• 资助国家: 美国
• 起止时间: 2006-04-14 至 2011-02-28
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/7034755
• 关键词: P glycoprotein; clinical research; multidrug resistance; neoplasm /cancer

DESCRIPTION (provided by applicant): Multidrug resistance (MDR) mediated by MDR1 (ABCB1) P-glycoprotein and related ATP-binding cassette (ABC) transporters is an impediment to successful cancer therapy. ABCB5 P-glycoprotein is a novel ABC transporter, which mediates drug efflux in cancer cells and regulates cell fusion and resultant differentiation of progenitor cells in physiological tissues. It is hypothesized that ABCB5 mediates dual functions in cancer, conferring MDR via its function as a drug efflux transporter, and regulating tumor renewal as a determinant of cell fusion involving tumor stem cells. This study aims to (1) identify systematically ABCB5 drug efflux substrates and examine the role of ABCB5 in the chemoresistance to such compounds, (2) determine whether ABCB5-expressing cancer cells function as tumor stem cells, and (3) investigate the role of ABCB5 in cancer MDR and tumor formation in vivo and examine whether ABCB5 can be specifically targeted for tumor eradication. First, ABCB5 gene and protein expression will be assayed across the NCI-60 cancer cell lines with resistance profiles for >100,000 compounds and drug resistance correlations will be established by. COMPARE analysis. Candidate ABCB5 transport substrates will be validated experimentally using competitive drug efflux analysis in ABCB5 gene-transfected cell lines, and chemosensitivity assays performed in ABCB5-blocked human cancer cell lines and murine ABCB5 -/- knockout cells. Second, the capacity of ABCB5-positive tumor cells vis-a-vis ABCB5-negative tumor bulk populations for self-renewal and the mechanistic contribution of ABCB5-positive progenitor cells to tumor culture growth and differentiation will be examined in vitro using tumor clonogenicity and cell fusion assays. Third, the in vivo role of ABCB5 in chemoresistance to identified drug substrates and the in vivo relevance of ABCB5-positive tumor cells for tumor formation and growth will be studied in human to mouse tumor xenograft models. The results will define the role of ABCB5 in cancer MDR and will establish whether chemoresistant ABCB5- positive cells function as tumor stem cells in expressing cancers. Thus, the findings will identify whether ABCB5 represents a novel therapeutic target in clinical oncology.

描述（由申请人提供）：由MDR1 (ABCB1) p -糖蛋白和相关的atp结合盒（ABC）转运体介导的多药耐药（MDR）是成功治疗癌症的障碍。ABCB5 p -糖蛋白是一种新型的ABC转运蛋白，它介导肿瘤细胞内的药物外排，并调节生理组织中祖细胞的细胞融合和分化。据推测，ABCB5在癌症中具有双重功能，通过其作为药物外排转运体的功能赋予耐多药，并作为肿瘤干细胞细胞融合的决定因素调节肿瘤更新。本研究旨在(1)系统鉴定ABCB5药物外排底物，并研究ABCB5在这些化合物的化疗耐药中的作用；(2)确定表达ABCB5的癌细胞是否具有肿瘤干细胞功能；(3)研究ABCB5在体内癌症MDR和肿瘤形成中的作用，并研究ABCB5是否可以特异性靶向根除肿瘤。首先，ABCB5基因和蛋白的表达将在NCI-60癌细胞系中进行检测，并对bb10万种化合物进行耐药分析，建立耐药相关性。比较分析。候选ABCB5转运底物将在ABCB5基因转染细胞系中通过竞争性药物外排分析进行实验验证，并在ABCB5阻断的人类癌细胞系和小鼠ABCB5- /-敲除细胞中进行化学敏感性试验。其次，abcb5阳性肿瘤细胞相对于abcb5阴性肿瘤群体的自我更新能力，以及abcb5阳性祖细胞对肿瘤培养生长和分化的机制贡献将在体外通过肿瘤克隆性和细胞融合实验进行检测。第三，将在人-小鼠肿瘤异种移植模型中研究ABCB5在体内对已鉴定药物底物的化疗耐药中的作用，以及ABCB5阳性肿瘤细胞在体内与肿瘤形成和生长的相关性。该结果将确定ABCB5在癌症耐多药中的作用，并将确定化疗耐药ABCB5阳性细胞是否在表达癌症中作为肿瘤干细胞发挥作用。因此，研究结果将确定ABCB5是否代表临床肿瘤学的新治疗靶点。