Understanding the Molecular Determinants of Reassortment in Orthobunyaviruses and Phleboviruses.

了解正布尼亚病毒和白蛉病毒重配的分子决定因素。

基本信息

项目摘要

Project Summary/Abstract Genome reassortment drives the diversity we see in segmented RNA viruses. Unlike recombination, intact genes are readily exchanged between two co-infecting viruses, resulting in their rapid evolution. Reassortment amongst influenza viruses is a well-established driver of host range and virulence. Though reassortment occurs frequently amongst bunyaviruses and can result in highly virulent reassortants such as Ngari virus, the underlying mechanisms are unknown. Understanding how these viruses reassort and modify virulence will allow us to predict potential virus emergence or modulations in host range allowing potential species jumps. The goal of this project is to investigate the molecular determinants of reassortment and virulence amongst orthobunyaviruses and phleboviruses. These are tri-segmented negative sense RNA viruses with Small (S), Medium (M) and Large (L) segments encoding the nucleocapsid protein, glycoproteins GnGc and a viral polymerase (L protein), respectively. Some viruses also encode nonstructural proteins on the S and/or M segments. Aim 1, will investigate segment compatibility amongst the priority pathogens Severe fever with thrombocytopenia syndrome virus and Heartland virus, using a forward and reverse genetics approach. Aim 2, will investigate homologous and heterologous segment dynamics within infected cells. Aim 3, will investigate the virulence of natural reassortants of Oropouche virus and potential reassortants of SFTSV and HRTV. These studies are of significant importance, as only by understanding the fundamental aspects of the biology of these viruses will we be able to understand the molecular determinants of their reassortment. This proposal will support my long-term career goal of understanding novel virus emergence and evolution. My mentorship team consists of Professor Paul Duprex, an expert in paramyxoviruses and cross-species viral transmission, Dr. Anita McElroy, an expert in Rift Valley fever virus (RVFV) transmission and immunology, Dr. Amy Hartman, an expert in RVFV pathogenesis in rats and monkeys and Dr. Seema Lakdawala, an expert in influenza virus biology and reassortment. With the support of strong mentors and collaborators I will receive training in the skills required to complete the proposed aims. Upon completion of the K99 phase I will be in a strong position to pursue an independent and successful research position contributing to the bunyavirus field.
项目摘要/摘要 基因组重组推动了我们在分段RNA病毒中看到的多样性。与重组不同, 完整的基因很容易在两个共同感染的病毒之间交换,导致它们快速进化。 流感病毒之间的重新分类是宿主范围和毒力的一个公认的驱动因素。尽管 重组经常发生在布尼亚病毒中,并可能导致剧毒的重组,如 阿里病毒的潜在机制尚不清楚。了解这些病毒如何重新组合和修改 毒力将使我们能够预测潜在的病毒出现或宿主范围内的调节,从而允许潜在的物种 跳跃。这个项目的目标是研究重组和毒力的分子决定因素。 在正野病毒和细小病毒中。这些病毒是三节段负义RNA病毒,具有小的 (S)、中(M)和大(L)片段编码核衣壳蛋白、糖蛋白GnGc和一种病毒 聚合酶(L蛋白)。一些病毒还在S和/或M蛋白上编码非结构蛋白 细分市场。目标1,将调查优先病原体与重症发热之间的区段兼容性 使用正向和反向遗传学方法的血小板减少综合征病毒和哈特兰病毒。目标2, 将研究感染细胞内的同源和异源片段动力学。目标3,将调查 Oropouche病毒天然重组体和SFTSV和HRTV潜在重组体的毒力。这些 研究是非常重要的,因为只有通过了解这些生物的生物学基本方面 我们将能够理解病毒重新分类的分子决定因素。这项建议将支持 我的长期职业目标是了解新奇病毒的出现和进化。我的导师团队由 副粘病毒和跨物种病毒传播专家保罗·杜普雷克斯教授安妮塔·麦克尔罗伊博士, 裂谷热病毒(RVFV)传播和免疫学专家艾米·哈特曼博士,RVFV专家 大鼠和猴子的致病机制以及流感病毒生物学和 重新编排。在强大的导师和合作者的支持下,我将接受所需技能的培训 完成提议的目标。在K99阶段完成后,我将处于有利的地位,可以继续 对布尼亚病毒领域做出贡献的独立和成功的研究职位。

项目成果

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Natasha Louise Tilston-Lunel其他文献

Natasha Louise Tilston-Lunel的其他文献

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{{ truncateString('Natasha Louise Tilston-Lunel', 18)}}的其他基金

Understanding the Molecular Determinants of Reassortment in Orthobunyaviruses and Phleboviruses.
了解正布尼亚病毒和白蛉病毒重配的分子决定因素。
  • 批准号:
    10039167
  • 财政年份:
    2020
  • 资助金额:
    $ 24.9万
  • 项目类别:
Understanding the Molecular Determinants of Reassortment in Orthobunyaviruses and Phleboviruses.
了解正布尼亚病毒和白蛉病毒重配的分子决定因素。
  • 批准号:
    10674269
  • 财政年份:
    2020
  • 资助金额:
    $ 24.9万
  • 项目类别:
Understanding the Molecular Determinants of Reassortment in Orthobunyaviruses and Phleboviruses.
了解正布尼亚病毒和白蛉病毒重配的分子决定因素。
  • 批准号:
    10251993
  • 财政年份:
    2020
  • 资助金额:
    $ 24.9万
  • 项目类别:

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