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Comparative and molecular approaches to improve identification, classification, and therapeutic approaches to cancer.

机译:比较和分子方法,可改善对癌症的识别,分类和治疗方法。

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摘要

A major area of contemporary research in cancer is focused on improving tumor classification into clinically relevant subgroups of disease. To achieve this, it is important to understand the molecular events that driver tumor heterogeneity both at the cellular level and at the tissue level. I initially tested the hypothesis that canine lymphoma is composed of a group of molecularly distinct entities with prognostic significance. The results show that canine lymphoma can be stratified into molecular subgroups that have prognostic value and can assist to guide therapy. Next, I tested the hypothesis that canine hemangiosarcoma (HSA) is organized hierarchically with a cancer stem cell (CSC)-like population of cells at the apex. The data show that variable numbers of CSC-like cells are invariably present in HSA. These CSC-like cells retain the capacity to differentiate into vascular, inflammatory, or adipogenic tissue, suggesting that their multipotency is a contributing factor to the observed heterogeneity in this disease. Finally, I tested the hypothesis that CSCs, or CSC-like cells from three histologically distinct types of canine cancer (HSA, osteosarcoma, and glioblastoma) share molecular and functional properties. Using a system that allowed me to eliminate tumor-specific culture conditions, I showed that despite extensive heterogeneity in CSC-like cells from these tumors, they all showed reduced activity of pathways associated with proliferation and development. In summary, my results confirm that cellular heterogeneity exists both within and among tumors. A better understanding of the mechanisms that drive this will improve patient stratification and guide efforts to develop rational, more effective therapies.
机译:当代癌症研究的主要领域集中在改善将肿瘤分类为疾病的临床相关亚组。为此,了解在细胞水平和组织水平上驱动肿瘤异质性的分子事件很重要。我最初测试了犬淋巴瘤由一组具有预后意义的分子不同的实体组成的假说。结果表明,犬淋巴瘤可分为具有预后价值并有助于指导治疗的分子亚组。接下来,我测试了这样的假设,即犬血管瘤肉瘤(HSA)在顶点处与癌干细胞(CSC)样细胞群分层组织。数据显示,HSA中始终存在可变数量的CSC样细胞。这些CSC样细胞保留了分化为血管,炎症或脂肪形成组织的能力,这表明它们的多能性是该疾病中观察到的异质性的一个促成因素。最后,我检验了以下假设:来自三种组织学不同类型的犬癌(HSA,骨肉瘤和成胶质细胞瘤)的CSC或类CSC细胞具有分子和功能特性。使用可以消除肿瘤特异性培养条件的系统,我发现尽管这些肿瘤的CSC样细胞具有广泛的异质性,但它们均显示出与增殖和发育相关的途径活性降低。总之,我的结果证实了细胞内异质性同时存在于肿瘤内部和肿瘤之间。更好地理解引起这种情况的机制将改善患者分层并指导努力开发合理,更有效的疗法。

著录项

  • 作者

    Frantz, Aric M.;

  • 作者单位

    University of Minnesota.;

  • 授予单位 University of Minnesota.;
  • 学科 Biology Molecular.;Health Sciences Oncology.;Biology Veterinary Science.;Biology Bioinformatics.
  • 学位 Ph.D.
  • 年度 2013
  • 页码 216 p.
  • 总页数 216
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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