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HIV Evolution: Fast or Slow?

机译:HIV演变:快还是慢?

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Summary form only given. It is known that in the human immunodeficiency virus (HIV) genome regions responsible for interactions with the host's immune system, namely, cytotoxic T-lymphocyte (CTL) epitopes, tend to be clustered together, sometimes found in more conserved parts of genome. On the other hand, more variable regions tend to have lower density of CTL epitopes. Furthermore, high recombination rate, coupled with high mutation rate, results in overall high diversity of HIV sequences, which is expected to result in little if any association between different regions of a genome. Or is it not? Employing data mining technique, we show that indeed some rather strong associations between different regions of HIV genome can be detected, even when circulating recombinant forms are considered. This can partly be attributed to strong functional constraints acting on protein sequences and certain CTL epitopes regions in particular.
机译:仅提供摘要表格。众所周知,在人类免疫缺陷病毒(HIV)基因组区域中,负责与宿主免疫系统相互作用的区域,即细胞毒性T淋巴细胞(CTL)表位,倾向于聚集在一起,有时在基因组中更保守的部分发现。另一方面,更多的可变区倾向于具有较低密度的CTL表位。此外,高重组率和高突变率导致HIV序列总体多样性高,这有望导致基因组不同区域之间几乎没有关联。还是不是?利用数据挖掘技术,我们证明,即使考虑到循环重组形式,确实可以检测到HIV基因组不同区域之间的某些相当强的关联。这部分可以归因于作用于蛋白质序列特别是某些CTL表位区域的强大功能限制。

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