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Methods to Generate Genetically Engineered Mouse Models of Soft Tissue Sarcoma

机译：产生软组织肉瘤基因工程小鼠模型的方法

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摘要

We discuss the generation of primary soft tissue sarcomas in mice using the Cre-loxP system to activate conditional mutations in oncogenic Kras and the tumor suppressor p53 (LSL-Kras^G12D/+; p53^flox/flox). Sarcomas can be generated either by adenoviral delivery of Cre recombinase, activation of transgenic Cre recombinase with tamoxifen, or through transplantation of isolated satellite cells with Cre activation in vitro. Various applications of these models are discussed, including anticancer therapies, metastasis, in vivo imaging, and genetic requirements for tumorigenesis.

机译：我们讨论了使用Cre-loxP系统激活致癌性Kras和肿瘤抑制因子p53（LSL-Kras ^{G12D / + ; p53 ^{flox / flox ）。肉瘤可通过腺病毒递送Cre重组酶，用他莫昔芬激活转基因Cre重组酶或通过体外分离的带有Cre激活的卫星细胞移植而产生。讨论了这些模型的各种应用，包括抗癌治疗，转移，体内成像以及肿瘤发生的遗传要求。}}

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期刊名称 other
作者
Rebecca D. Dodd; Leonor Añó; Jordan M. Blum; Zhizhong Li; David Van Mater; David G. Kirsch;
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年(卷),期 -1(1267),-1
年度 -1
页码 283–295
总页数 14
原文格式 PDF
正文语种
中图分类
关键词
Sarcoma Mouse models Cancer Transgenic mice Satellite cells Genetically engineered mouse models;

机译：肉瘤;小鼠模型;癌症;转基因小鼠;卫星细胞;基因工程小鼠模型;

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专利

1. Efficacy of sunitinib and radiotherapy in genetically engineered mouse model of soft-tissue sarcoma. [J] . Yoon SS, Stangenberg L, Lee YJ International Journal of Radiation Oncology, Biology, Physics . 2009,第4期

机译：舒尼替尼和放疗在软组织肉瘤基因工程小鼠模型中的功效。
2. Xenograft and genetically engineered mouse model systems of osteosarcoma and Ewing's sarcoma: Tumor models for cancer drug discovery [J] . SampsonV.B., KamaraD.F., KolbE.A. Expert opinion on drug discovery . 2013,第10期

机译：骨肉瘤和尤因氏肉瘤的异种移植和基因工程小鼠模型系统：用于癌症药物发现的肿瘤模型
3. Epigenetic Regulation of SMARCB1 By miR-206,-381 and-671-5p Is Evident in a Variety of SMARCB1 Immunonegative Soft Tissue Sarcomas, While miR-765 Appears Specific for Epithelioid Sarcoma. A miRNA Study of 223 Soft Tissue Sarcomas [J] . Sapi Zoltan, Papp Gergo, Szendroi Miklos, Genes, Chromosomes and Cancer . 2016,第10期

机译：在各种类型的SMARCB1免疫阴性软组织肉瘤中，显然可以通过miR-206，-381和-671-5p对SMARCB1进行表观遗传调控，而miR-765似乎对上皮样肉瘤具有特异性。 223个软组织肉瘤的miRNA研究
4. GENE EXPRESSION PROFILING UNCOVERS A ROLE FOR GENETIC MAKE-UP IN SUSCEPTIBILITY AND PROGRESSION OF SOFT TISSUE SARCOMAS [C] . Beth A Tamburini, Susan Trapp, Tzu Lip Phang, Annual conference of the Veterinary Cancer Society . 2008

机译：基因表达分析揭示了遗传构成在易感性和软组织肉瘤的进展中的作用
5. Characterization of a Mouse Model of Soft Tissue Sarcoma: Intraoperative Molecular Imaging and miRNA Regulation of Metastasis [D] . Mito, Jeffrey. 2013

机译：小鼠软组织肉瘤模型的表征：术中分子成像和转移的miRNA调节。
6. Efficacy of Sunitinib and Radiotherapy in Genetically Engineered Mouse Model of Soft-tissue Sarcoma [O] . Sam S. Yoon, Lars Stangenberg, Yoon-Jin Lee, -1

机译：Sunitinib和放疗在遗传工程肉瘤的转基因小鼠模型中的功效
7. Methods to Generate Genetically Engineered Mouse Models of Soft Tissue Sarcoma [O] . Rebecca D. Dodd, Leonor Añó, Jordan M. Blum, 2015

机译：生成遗传工程鼠尾草型肉瘤的方法

Methods to Generate Genetically Engineered Mouse Models of Soft Tissue Sarcoma

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