Identification and Characterization of a Endogenous EGFR Regulatory Locus in Xiphophorus Genome
剑尾鱼基因组中内源 EGFR 调节位点的鉴定和表征
基本信息
- 批准号:10296895
- 负责人:
- 金额:$ 45.14万
- 依托单位:
- 依托单位国家:美国
- 项目类别:
- 财政年份:2021
- 资助国家:美国
- 起止时间:2021-09-01 至 2024-08-31
- 项目状态:已结题
- 来源:
- 关键词:Automobile DrivingBackcrossingsBenignBiological ModelsBook ChaptersCancer Cell GrowthCancer EtiologyCandidate Disease GeneCell DeathCell ProliferationCell SurvivalCetuximabChromosome 5Chromosome MappingCodeDevelopmentDoctor of PhilosophyEGFR Protein OverexpressionEGFR geneElementsEnrollmentEpidermal Growth Factor ReceptorExhibitsFc ReceptorFishesGenesGenetic ModelsGenomeGoalsHumanHybridsImpairmentInterviewJournalsKnock-outKnowledgeLeadLigand BindingMalignant NeoplasmsMedicineMembraneMethodsMolecularMolecular TargetMonoclonal AntibodiesMusMutationNamesOncogenesOncogenicOryziinaePathway interactionsPatientsPeer ReviewPenetrancePharmaceutical PreparationsPhenotypePhosphotransferasesPlatyfishPublishingReceptor Protein-Tyrosine KinasesRegulationRegulator GenesRelapseResearchResistanceResistance developmentSignal PathwaySignal TransductionStudentsTherapeuticTransgenic OrganismsTyrosine Kinase InhibitorUniversitiesXiphophoruscancer cellcancer therapycancer typecarcinogenesiscell typeclinical applicationdesigndimerdisorder controlgenetic analysisgenetic elementgenomic locusinhibitor/antagonistmelanomagenesismutantnext generationnovelnovel therapeutic interventionoverexpressionpostersprogramsresponsesegregationsmall moleculetreatment strategytumortumorigenesis
项目摘要
Project Summary:
The epidermal growth factor receptor (EGFR) is a leading oncogene firmly
associated with many types of cancer. Both anti-EGFR small molecules and
monoclonal antibodies have been developed to block its kinase activity for cancer
treatment. However, innate and acquired resistance are frequently observed in
clinical application. Such observations significantly limit anti-EGFR medicines
usage, and also challenge current knowledge of EGFR-driver cancer. Therefore,
it is necessary to study the relationship between EGFR and cancer from a
different angle, with different research strategy.
Xiphophorus maculatus encodes a mutant, autonomous, dysregulated and
oncogenic EGFR, named xmrk. However, carcinogenesis is only observed in
backcross interspecies hybrid between xmrk positive and xmrk-null Xiphophorus
species, or when xmrk is ectopically expressed in non-Xiphophorus model system
(e.g., medaka, murine). These suggest that X. maculatus genome also encode a
regulator gene that may co-evolved with xmrk and is able to suppressing its
oncogenic activity. Therefore, characterizing how the regulator, termed R(Diff)
inhibit xmrk, may lead to novel therapeutic strategy in controlling EGFR.
Our recent study has defined the R(Diff) tumor regulatory locus to a 101.7 kbp
locus on chromosome 5. This small candidate size and low candidate gene
number enables functional and mechanistic studies are impractical. Therefore,
this proposal is designed to final determine the R(Diff) locus by examining the
following aims:
Aim 1: We will characterize all expressed but unannotated genetic elements, in
addition to the known coding genes, within the newly identified candidate R(Diff)
locus, to fully annotate the R(Diff) locus.
Aim 2: We will determine the gene/element(s) carrying R(Diff) activity by
performing gene knock-out in non-tumor-bearing Xiphophorus fish, tumor-bearing
hybrids, and tumor-bearing transgenic medaka.
Aim 3: We will profile xmrk and R(Diff) candidates, as well as phenotypes of
several Xiphophorus hybrids, to define R(Diff) by association of candidate
sequence with varied phenotypes.
项目概要:
表皮生长因子受体 (EGFR) 是公认的主要致癌基因
与多种癌症有关。抗 EGFR 小分子和
单克隆抗体已被开发来阻断其激酶活性以治疗癌症
治疗。然而,先天性和获得性抵抗经常在
临床应用。这些观察结果极大地限制了抗 EGFR 药物
的使用,也挑战了当前对 EGFR 驱动癌症的认识。所以,
有必要从一个角度来研究EGFR与癌症的关系
不同的角度,有不同的研究策略。
斑剑鱼编码一种突变体、自主性、失调性和
致癌EGFR,命名为xmrk。然而,仅在以下情况下观察到致癌作用:
xmrk 阳性和 xmrk 无效剑尾鱼之间的回交种间杂交
种,或当 xmrk 在非剑尾鱼模型系统中异位表达时
(例如,青鳉、鼠科动物)。这些表明 X. maculatus 基因组还编码
可能与 xmrk 共同进化的调节基因,能够抑制其
致癌活性。因此,描述调节器的特性,称为 R(Diff)
抑制xmrk,可能会导致控制EGFR的新治疗策略。
我们最近的研究将 R(Diff) 肿瘤调控位点定义为 101.7 kbp
基因座位于 5 号染色体上。候选基因尺寸较小且候选基因较低
数量使得功能和机制研究是不切实际的。所以,
该提案旨在通过检查
以下目标:
目标 1:我们将表征所有已表达但未注释的遗传元件,
除了已知的编码基因外,在新确定的候选 R(Diff) 内
轨迹,完整注释 R(Diff) 轨迹。
目标 2:我们将通过以下方式确定携带 R(Diff) 活性的基因/元件:
对非荷瘤剑鱼、荷瘤鱼进行基因敲除
杂交种和携带肿瘤的转基因青鳉。
目标 3:我们将分析 xmrk 和 R(Diff) 候选者,以及表型
几个Xiphophorus杂种,通过候选者的关联来定义R(Diff)
具有不同表型的序列。
项目成果
期刊论文数量(2)
专著数量(0)
科研奖励数量(0)
会议论文数量(0)
专利数量(0)
Global assessment of organ specific basal gene expression over a diurnal cycle with analyses of gene copies exhibiting cyclic expression patterns.
通过对表现出循环表达模式的基因拷贝进行分析,对昼夜周期内器官特异性基础基因表达进行全面评估。
- DOI:
- 发表时间:2020-11-11
- 期刊:
- 影响因子:4.4
- 作者:Lu, Yuan;Boswell, Mikki;Boswell, William;Salinas, Raquel Ybanez;Savage, Markita;Reyes, Jose;Walter, Sean;Marks, Rebecca;Gonzalez, Trevor;Medrano, Geraldo;Warren, Wesley C;Schartl, Manfred;Walter, Ronald B
- 通讯作者:Walter, Ronald B
Validity of Xiphophorus fish as models for human disease.
剑鱼作为人类疾病模型的有效性。
- DOI:
- 发表时间:2024-01-01
- 期刊:
- 影响因子:4.3
- 作者:Schartl, Manfred;Lu, Yuan
- 通讯作者:Lu, Yuan
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- 批准号:
10718670 - 财政年份:2023
- 资助金额:
$ 45.14万 - 项目类别:
Advancement of the Xiphophorus Model for Studying Disease
研究疾病的剑尾动物模型的进展
- 批准号:
10805701 - 财政年份:2023
- 资助金额:
$ 45.14万 - 项目类别:
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