The Requirement for Trib2 in the Maintenance of Acute Myeloid Leukemia

Trib2 在维持急性髓系白血病中的需要

• 批准号: 8256131
• 负责人: Will H. Bailis
• 金额: $ 4.22万
• 依托单位: UNIVERSITY OF PENNSYLVANIA
• 依托单位国家: 美国
• 财政年份: 2012
• 资助国家: 美国
• 起止时间: 2012-07-06 至 2015-07-05
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/8256131
• 关键词: Acute Myelocytic Leukemia; Alleles; Apoptosis; Biological Assay; CCAAT-Enhancer-Binding Proteins; Cell Differentiation process; Cell Line; Cells; Collection; Data; Differentiation Therapy; Down-Regulation; Event; Exhibits; Gene Expression Regulation; Goals; Growth; Hematopoietic; Homologous Gene; Human; In Vitro; Laboratories; Lead; Maintenance; Malignant Neoplasms; Malignant neoplasm of lung; Metabolism; Modeling; Mus; Myelogenous; Oncogenes; Oncogenic; Pathogenesis; Patients; Phenotype; Play; Publishing; Role; Sampling; Signal Transduction; Technology; Testing; Tissues; Work; cancer cell; cancer therapy; cancer type; design; inhibitor/antagonist; leukemia; malignant phenotype; melanoma; mouse model; neoplastic cell; self-renewal; small hairpin RNA; therapeutic development; tumor

DESCRIPTION (provided by applicant): Tribbles homologue 2 (Trib2) was first shown to be an oncogene in AML and subsequently has been identified as an oncogene in melanoma and lung cancer. Although Trib2 is able to induce AML in a mouse model, it is not know if persistent Trib2 expression is necessary to maintain the transformed phenotype. My goal is to identify the function of Trib2 in maintaining the transformed phenotype of AML. Our published and preliminary data show that Tribbles inhibits differentiation of AML cell lines and promotes leukemia, in part, by blocking C/EBP¿. Thus, targeting Trib2 in Trib2-dependent AMLs will promote tumor cell differentiation, which has proven a successful strategy in treating AML, and a long-term goal of this study to inform the design of Trib2 inhibitors for the treatment of cancer The proposed studies seek to understand Trib2 in the context of abnormal gene regulation in cancer and will identify its role in regulating self-renewal, proliferation, survival, differentiaton, and cancer cell metabolism. We will test the requirement for Trib2 in maintaining AML identity by creating a murine model of Trib2-induced AML in which Trib2 expression can be conditionally regulated. We will extend our studies to human cells by employing knockdown of Trib2 by shRNA to determine whether human AML cell lines and primary AML samples that express high levels of Trib2 are sensitive to Trib2 inhibition. By demonstrating that Trib-associated AMLs require persistent Trib2 activity, our studies will validate Trib2 as a target for therapy, a findig that will likely extend to multiple other types of cancers that exhibit Trib2 dysregulation. PUBLIC HEALTH RELEVANCE: Tribbles homologue 2 (Trib2) has been implicated in malignant melanoma, lung cancer, and acute myeloid leukemia (AML). We propose to study the requirements for Trib2 in AML and its mechanism of action. We believe these studies will further our understanding of the role Trib2 plays in cancer and inform the development of therapeutic Trib2 inhibitors.

描述（由申请人提供）：tribles同源物2 （Trib2）首先被证明是AML的致癌基因，随后被确定为黑色素瘤和肺癌的致癌基因。虽然Trib2能够在小鼠模型中诱导AML，但尚不清楚是否需要持续的Trib2表达来维持转化的表型。我的目标是确定Trib2在维持AML转化表型中的功能。我们发表的初步数据表明，Tribbles抑制AML细胞系的分化并促进白血病，部分原因是通过阻断C/EBP¿。因此，在Trib2依赖性AMLs中靶向Trib2将促进肿瘤细胞分化，这已被证明是治疗AML的成功策略，也是本研究的长期目标，为设计用于治疗癌症的Trib2抑制剂提供信息。所提出的研究旨在了解Trib2在癌症异常基因调控背景下的作用，并将确定其在调节自我更新、增殖、存活、分化和癌细胞代谢中的作用。我们将通过创建Trib2诱导的AML小鼠模型来测试Trib2在维持AML特性中的要求，其中Trib2的表达可以有条件地调节。我们将把我们的研究扩展到人类细胞，通过shRNA敲低Trib2来确定表达高水平Trib2的人类AML细胞系和原发AML样本是否对Trib2抑制敏感。通过证明tribe相关的aml需要持续的Trib2活性，我们的研究将验证Trib2作为治疗靶点，这一发现可能会扩展到表现出Trib2失调的多种其他类型的癌症。