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Investigation of host and viral genetic factors influencing HIV-1 evolution across North America: implications for vaccine design

机译:影响整个北美HIV-1进化的宿主和病毒遗传因素的调查:对疫苗设计的影响

摘要

Human leukocyte antigen (HLA) class I restricted cytotoxic T-lymphocyte (CTL) responses drive HIV-1 evolution through the selection of immune escape mutations, however, the extent to which population-level patterns of immune escape have changed over the course of the HIV-1 epidemic in North America remains incompletely known. The objective of this thesis was to explore how immune selection pressures mediated through host HLA-restricted CTL responses have shaped the genomic and functional evolution of the HIV-1 gag gene over the course of the epidemic in North America. Results support the continued dynamic adaptation of HIV-1 as it passes through human hosts rather than the substantial accumulation of escape mutations over the course of the epidemic in North America. Additionally, only modest increases in gag-mediated replication capacity between pre- and post-1985 sequences were observed. Although the mechanism(s) behind these increases remain unknown, they may be attributable to factors other than CTL-driven immune responses.
机译:人类白细胞抗原(HLA)I类限制性细胞毒性T淋巴细胞(CTL)反应通过选择免疫逃逸突变来驱动HIV-1进化,但是,在整个免疫过程中,人群水平的免疫逃逸模式已改变的程度在北美,HIV-1流行病仍不完全清楚。本文的目的是探讨在北美流行期间,通过宿主HLA限制性CTL反应介导的免疫选择压力如何影响HIV-1 gag基因的基因组和功能进化。结果支持HIV-1在通过人类宿主时继续动态适应,而不是在北美流行期间逃脱突变的大量积累。此外,在1985年前后的序列中,gag介导的复制能力仅适度增加。尽管这些增加背后的机制仍然未知,但它们可能归因于CTL驱动的免疫反应以外的因素。

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    Cotton Laura Anne;

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  • 年度 2012
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