Genetic Analysis of Breast Cancer Progression in Mice Using Inducible Transposition

使用诱导转座对小鼠乳腺癌进展进行遗传分析

• 批准号: 10155442
• 负责人: EDWARD J GUNTHER
• 金额: $ 35.16万
• 依托单位: PENNSYLVANIA STATE UNIV HERSHEY MED CTR
• 依托单位国家: 美国
• 财政年份: 2017
• 资助国家: 美国
• 起止时间: 2017-06-16 至 2022-05-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/10155442
• 关键词: 3-Dimensional; Address; Advanced Malignant Neoplasm; Animal Model; Apoptosis; Automobile Driving; Benign; Breast; Breast Cancer Genetics; Breast Cancer Model; Candidate Disease Gene; Catalogs; Cell Proliferation; Cells; Clinical; Complement; Complex; Disease; Disease Progression; Disease Resistance; Disease remission; Doxycycline; Drug Targeting; Drug resistance; ERBB2 gene; Engineering; Enterobacteria phage P1 Cre recombinase; Estrogen Receptors; Event; Evolution; Fostering; Genes; Genetic; Genetic Screening; Genome; Goals; Growth; Hormonal; Human; Hyperplasia; Jumping Genes; Knowledge; Malignant - descriptor; Malignant Neoplasms; Mammary Neoplasms; Mammary Tumorigenesis; Modeling; Monitor; Mouse Mammary Tumor Virus; Mus; Mutagenesis; Mutation; Oncogenes; Oncogenic; Organoids; Outcome; Pathway interactions; Pharmaceutical Preparations; Phenotype; Publishing; Recurrence; Refractory Disease; Relapse; Reporting; Resistance; Scoring Method; Signal Transduction; Sleeping Beauty; Somatic Mutation; Sum; System; Testing; Tissues; Validation; WNT Signaling Pathway; Withdrawal; Work; advanced breast cancer; aggressive therapy; base; bioinformatics pipeline; breast cancer genomics; breast cancer progression; cancer genome; candidate validation; design; driver mutation; gene discovery; gene interaction; genetic analysis; genome database; genome-wide; imaging modality; imaging platform; in vivo; innovation; integration site; lapatinib; live cell imaging; malignant breast neoplasm; mammary; mouse model; neoplastic cell; novel; novel strategies; prospective; quantitative imaging; rare cancer; refractory cancer; resistance gene; screening; targeted treatment; three dimensional cell culture; trait; tumor progression; validation studies

Project Summary Despite the impressive catalog of mutations amassed from sequencing human breast cancer genomes, most genomes decoded so far derive from early-stage disease, which likely leaves many genetic events driving disease progression undiscovered. Ongoing efforts to decode the more complex genomes from more advanced and drug-resistant breast cancers hold great promise, but the higher mutation burden in these cancers complicates the difficult task of distinguishing causative driver events from innocuous passengers events. Animal models that offer a genome-wide view of the mutations acquired during breast cancer progression can provide cross-species validation crucial for validating candidate driver genes. Drawing on the breast cancer genomics landscape and our own mouse modeling work, we formulated the hypothesis that breast cancer progression depends on driver mutations acquired in a disease stage- specific manner, obscured by continuously accruing passenger mutations. Based on this hypothesis, we developed the following long-term goal: discover novel drivers of breast cancer progression by performing genetic screens in mouse breast cancer models using timed mobilization of transposons (so-called “jumping genes”) at discrete disease stages. In unpublished preliminary studies, we engineered new mouse models for discovering and validating candidate mammary oncogenes. To enable oncogene discovery, we generated an inducible version of the Sleeping Beauty (SB) transposition system, which enables timed transposon mobilization in the mouse breast. We confirmed that this system provides an efficient cancer gene discovery platform by identifying known and novel oncogenes that cooperate with Wnt pathway activation to drive mammary tumorigenesis in vivo. To complement this high-throughput cancer gene discovery platform, we designed a novel strategy for efficiently validating candidate oncogenes and probing their mechanisms of action by monitoring the growth of mammary tissue fragments (organoids) grown in 3D culture. This strategy employs live-cell imaging for quantitative scoring of the oncogene-driven events that culminate in mammary cell overgrowth. We will address our hypothesis by completing three Specific Aims. In Aim 1, transposon-based gene discovery will be employed in the context of mouse models engineered to express known breast cancer- relevant oncogenes. Our goal is to identify novel candidate genes that drive the transition from mammary hyperplasia to focal mammary cancer. In Aim 2, delayed transposon mobilization will be initiated within established mammary cancers arising in the classic MMTV-Neu breast cancer model. Our goal is to identify candidate genes that drive resistance to Lapatinib, a clinically important drug that blocks Her2/Neu signaling. In Aim 3, we will optimize our live-cell imaging platform and apply it to test whether and how candidate cancer genes confer malignant capabilities to mammary cells grown in 3D culture.

项目总结

项目成果

Evolution of Relapse-Proficient Subclones Constrained by Collateral Sensitivity to Oncogene Overdose in Wnt-Driven Mammary Cancer.

Wnt 驱动的乳腺癌中对癌基因过量的附带敏感性限制了复发性亚克隆的进化。

• DOI: 10.1016/j.celrep.2018.12.096
• 发表时间: 2019
• 期刊: Cell reports
• 影响因子: 8.8
• 作者: Keller,RossR;Gunther,EdwardJ
• 通讯作者: Gunther,EdwardJ

A Multistage Murine Breast Cancer Model Reveals Long-Lived Premalignant Clones Refractory to Parity-Induced Protection.

多阶段小鼠乳腺癌模型揭示了对奇偶诱导保护无效的长寿命癌前克隆。

• DOI: 10.1158/1940-6207.capr-19-0322
• 发表时间: 2020
• 期刊: Cancer prevention research (Philadelphia, Pa.)
• 作者: Li,Shuo;Gestl,ShelleyA;Gunther,EdwardJ
• 通讯作者: Gunther,EdwardJ