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Poxvirus interferon-resistance genes: Their evolutionary past and role in anti-cancer therapy.

机译:痘病毒干扰素抗性基因:它们的进化过去以及在抗癌治疗中的作用。

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摘要

The poxvirus E3L and K3L genes function as interferon (IFN)-resistance genes. This investigation examines their evolutionary past as well as their role in viral oncolysis. An evolutionary analysis demonstrates that these genes are highly conserved amongst the orthopoxviruses, with homologs present in the capripoxviruses, leporipoxviruses, suipoxviruses, and yatapoxviruses. E3L is present in the parapoxviruses but K3L is absent. Neither gene, however, is present in the avipoxviruses nor the molluscipoxviruses. Results from this study support a model for poxviral evolution that states avipoxviruses diverged at an early point in history. After this split, ancient parapoxviruses obtained an E3L-like sequence during a cellular capture event while molluscipoxviruses did not. A second capture event of a K3L-like protein resulted in parapoxviruses diverging from the remaining chordopoxviruses. Some lineages of chordopoxviruses have undergone partial deletions or point mutations of the E3L and K3L genes to form the modern group of E3L and K3L genes. These mutations suggest a varied necessity for the IFN-resistance genes likely altering pathogenesis or host-range.; Vaccinia virus (VV), a member of the orthopox genus, is known for its role as a smallpox vaccine. By creating mutations in VVE3L, we have developed several oncolytic viruses that preferentially replicate in and lyse ras-transformed cells. The mutant VVs constructed are PKR-sensitive and are thus dependent on the Ras-induced PKR inhibitor present in cells with an overactive Ras pathway or other IFN system dysregulation. When one of two tumors was treated, mutant VV induced regression of both local and distant breast cancer xenografts in SCID/bg mice. The anti-cancer regimen was not toxic, causing no significant weight loss or pathogenesis in treated mice. Given the recombination properties of VV and the varied genes encoded by VV that affect cell division and PKR activation, this system offers the potential of multiple therapeutic vectors. Targeted therapy, such as the PKR/IFN sensitive and ras-dependent VV, may be part of the future of individualized treatment for cancer patients.
机译:痘病毒E3L和K3L基因起干扰素(IFN)抵抗基因的作用。这项研究检查了它们的进化历史以及它们在病毒溶瘤中的作用。进化分析表明,这些基因在正痘病毒中是高度保守的,其同源物存在于capripoxviruses,leporipoxviruses,suipoxviruses和yatapoxviruses中。副痘病毒中存在E3L,但不存在K3L。但是,禽痘病毒和软体流感病毒都没有基因。这项研究的结果支持了一种痘病毒进化模型,该模型表明禽痘病毒在历史的早期就发散了。分裂之后,古代的副痘病毒在细胞捕获事件中获得了类似E3L的序列,而软体神经病毒则没有。 K3L样蛋白的第二次捕获事件导致副痘病毒与其余的脊索病毒不同。某些腱索病毒谱系已发生E3L和K3L基因的部分缺失或点突变,从而形成了E3L和K3L基因的现代群体。这些突变表明可能改变发病机理或宿主范围的IFN抗性基因的多样性。痘苗病毒(VV)是正痘属的一员,以天花疫苗的作用而闻名。通过在VVE3L中创建突变,我们开发了几种溶瘤病毒,它们优先在ras转化的细胞中复制并裂解它们。构建的突变型VV对PKR敏感,因此依赖于Ras通路过度活跃或其他IFN系统失调的细胞中存在的Ras诱导的PKR抑制剂。当治疗两个肿瘤之一时,突变型VV诱导了SCID / bg小鼠局部和远处乳腺癌异种移植的消退。该抗癌方案无毒,在治疗的小鼠中不会引起明显的体重减轻或发病机理。考虑到VV的重组特性以及VV编码的影响细胞分裂和PKR激活的各种基因,该系统提供了多种治疗载体的潜力。靶向治疗,例如PKR / IFN敏感和ras依赖型VV,可能是癌症患者个体化治疗未来的一部分。

著录项

  • 作者

    Mitnik, Chandra Rose.;

  • 作者单位

    Arizona State University.;

  • 授予单位 Arizona State University.;
  • 学科 Biology Microbiology.; Biology Molecular.; Health Sciences Oncology.
  • 学位 Ph.D.
  • 年度 2004
  • 页码 160 p.
  • 总页数 160
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 微生物学;分子遗传学;肿瘤学;
  • 关键词

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