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Narrowing the field: cancer-specific promoters for mitochondrially-targeted p53-BH3 fusion gene therapy in ovarian cancer

机译：缩小领域：线粒体靶向p53-BH3融合基因治疗卵巢癌的癌症特异性启动子

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BackgroundDespite years of research, the treatment options and mortality rate for ovarian cancer remain relatively stagnant. Resistance to chemotherapy and high heterogeneity in mutations contribute to ovarian cancer’s lethality, including many mutations in tumor suppressor p53. Though wild type p53 gene therapy clinical trials failed in ovarian cancer, mitochondrially-targeted p53 fusion constructs, including a fusion with pro-apoptotic protein Bad, have shown much higher apoptotic potential than wild type p53 in vitro. Due to the inherent toxicities of mitochondrial apoptosis, cancer-specificity for the p53 fusion constructs must be developed. Cancer-specific promoters such as hTERT, hTC, Brms1, and Ran have shown promise in ovarian cancer.

机译：背景尽管进行了多年的研究，但卵巢癌的治疗选择和死亡率仍然相对停滞。对化学疗法的抵抗力和突变的高度异质性导致卵巢癌的致死性，其中包括肿瘤抑制因子p53的许多突变。尽管野生型p53基因疗法的临床试验在卵巢癌中失败了，但线粒体靶向的p53融合构建体（包括与促凋亡蛋白Bad的融合体）在体外的凋亡潜力远高于野生型p53。由于线粒体凋亡的内在毒性，必须开发针对p53融合构建体的癌症特异性。癌特异性启动子如hTERT，hTC，Brms1和Ran在卵巢癌中显示出希望。

著录项

期刊名称 Journal of Ovarian Research
作者
Katherine Redd Bowman; Ji Hoon Kim; Carol S. Lim;
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作者单位

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年(卷),期 2019(12),-1
年度 2019
页码 38
总页数 12
原文格式 PDF
正文语种
中图分类生理学;
关键词
Ovarian cancer p53 Gene therapy Cancer-specific promoters Mitochondrial targeting hTERT Ran Brms1;

机译：卵巢癌;p53;基因治疗;癌症特异性启动子;线粒体靶向;hTERT;Ran;Brms1;

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专利

1. Narrowing the field: cancer-specific promoters for mitochondrially-targeted p53-BH3 fusion gene therapy in ovarian cancer [J] . Katherine Redd Bowman, Ji Hoon Kim, Carol S. Lim Journal of Ovarian Research . 2019,第1期

机译：缩小现场：卵巢癌的线粒体靶向P53-BH3融合基因治疗的癌症特异性启动子
2. Cancer-specific promoters for expression-targeted gene therapy: ran, brms1 and mcm5 [J] . Chen Xuguang, Scapa Jacqueline E., Liu David X., The journal of gene medicine . 2016,第7期

机译：用于表达靶向基因治疗的癌症特异性启动子：ran，brms1和mcm5
3. The Evaluation and Comparison of Transcriptionally Targeted Noxa and Puma Killer Genes to Initiate Apoptosis Under Cancer-Specific Promoter CXCR1 in Hepatocarcinoma Gene Therapy [J] . Shahryar Khoshtinat Nikkhoi, Hedieh Heydarzadeh, Saeed Ranjbar, Hepatitis Monthly . 2016,第10期

机译：肝癌基因治疗中癌症特异性启动子CXCR1诱导转录靶向的Noxa和Puma杀手基因启动细胞凋亡的评估和比较
4. Tensor decomposition-based unsupervised feature extraction for integrated analysis of TCGA data on microRNA expression and promoter methylation of genes in ovarian cancer [C] . Y-h. Taguchi, Ka-Lok Ng IEEE International Conference on Bioinformatics and Bioengineering . 2018

机译：基于张量分解的无预测特征提取，用于卵巢癌中基因TCGA数据综合分析及卵巢癌基因的促进剂甲基化
5. Breast cancer-specific activation of topoisomerase IIalpha and its application in the tumor-targeting gene therapy. [D] . Day, Chi-Ping. 2005

机译：拓扑异构酶IIalpha的乳腺癌特异性激活及其在肿瘤靶向基因治疗中的应用。
6. CDKN2D-WDFY2 Is a Cancer-Specific Fusion Gene Recurrent in High-Grade Serous Ovarian Carcinoma [O] . Kalpana Kannan, Cristian Coarfa, Kimal Rajapakshe, 2014

机译：CDKN2D-WDFY2是高级别浆液性卵巢癌中常见的癌症特异性融合基因。
7. Novel, chimeric, cancer-specific, and radiation-inducible gene promoters for suicide gene therapy of cancer [O] . Jie Xiong, Wen-jie Sun, Wei-feng Wang, 2011

机译：用于癌症的自杀基因治疗的新型，嵌合，癌症特异性和辐射诱导基因启动子

Narrowing the field: cancer-specific promoters for mitochondrially-targeted p53-BH3 fusion gene therapy in ovarian cancer

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