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Investigating the role of Sox2 in stomach tissue homeostasis and cancer.

机译:研究Sox2在胃组织动态平衡和癌症中的作用。

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摘要

The transcription factor Sox2 is essential for the establishment and maintenance of multiple stem cell populations and its coding region is amplified in certain carcinomas. However, Sox2's role in stomach homeostasis and cancer is poorly understood. In this thesis, I used mouse genetics to investigate the expression pattern and function of Sox2 in the adult stomach during normal tissue homeostasis and tumorigenesis. Using a genetic lineage tracing system, I found that Sox2 expression marks a gastric stem cell population capable of self renewal and differentiation throughout the lifetime of a mouse, raising the key question of whether Sox2 itself is required for adult stomach function. Using a combination of novel mouse models, I examined the consequences of Sox2 loss of function on stomach regeneration as well as the susceptibility of Sox2+ cells to transformation. Surprisingly, I found that Sox2 itself is dispensable during stomach homeostasis, although Sox2-expressing cells readily give rise to Wnt-driven adenomas. To gain insight into the molecular function of Sox2, I performed ChIP-Seq analysis which revealed that the majority of Sox2 targets in mouse gastric stem and progenitor cells are related to tissue-specific functions such as endoderm development, Wnt signaling and gastric cancer while only a small set of genes overlaps with targets occupied by Sox2 in other stem cell populations.;SOX2 has been described as an amplified oncogene in several types of human cancers derived from the foregut endoderm including lung and esophageal squamous cell carcinomas. Unexpectedly, I found that Sox2 loss enhances stomach tumor formation and organoid growth in an Apc/Wnt depdendent adenoma mouse model. Using a reporter assay, I further showed that altered Sox2 levels modulate Tcf/Lef-dependent transcription, providing a molecular explanation for the observed proliferation phenotypes. In summary, my genetic and molecular studies offer insight into how Sox2 regulates stomach tissue homeostasis and cancer and evidence that Sox2's mode of action is context and tissue specific.
机译:转录因子Sox2对于多个干细胞群体的建立和维持至关重要,其编码区在某些癌症中被扩增。但是,人们对Sox2在胃稳态和癌症中的作用知之甚少。在本文中,我利用小鼠遗传学研究了正常组织稳态和肿瘤发生过程中成年胃中Sox2的表达模式和功能。使用遗传谱系追踪系统,我发现Sox2表达标志着能够在小鼠的整个生命周期中自我更新和分化的胃干细胞群体,从而提出了一个关键问题,即成年的胃功能是否需要Sox2本身。使用新颖的小鼠模型的组合,我检查了Sox2功能丧失对胃再生的影响以及Sox2 +细胞转化的敏感性。出乎意料的是,我发现Sox2本身在胃稳态过程中是可有可无的,尽管表达Sox2的细胞很容易引起Wnt驱动的腺瘤。为了深入了解Sox2的分子功能,我进行了ChIP-Seq分析,结果表明,小鼠胃干和祖细胞中的大多数Sox2靶标与组织特异性功能有关,例如内胚层发育,Wnt信号传导和胃癌,而只有一小组基因与其他干细胞群体中Sox2占据的靶标重叠。SOX2已被描述为几种起源于前肠内胚层的人类癌症中的扩增癌基因,包括肺癌和食道鳞状细胞癌。出乎意料的是,我发现在Apc / Wnt依赖性腺瘤小鼠模型中,Sox2的丢失会增强胃肿瘤的形成和类器官的生长。使用记者测定法,我进一步表明改变的Sox2水平可调节Tcf / Lef依赖性转录,为观察到的增殖表型提供了分子解释。总而言之,我的基因和分子研究提供了关于Sox2如何调节胃组织稳态和癌症的见识,并证明了Sox2的作用方式是背景和组织特异性的。

著录项

  • 作者

    Sarkar, Abby Joya.;

  • 作者单位

    Harvard University.;

  • 授予单位 Harvard University.;
  • 学科 Cellular biology.;Oncology.
  • 学位 Ph.D.
  • 年度 2015
  • 页码 116 p.
  • 总页数 116
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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