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Lack of Molecular Mimicry between Nonhuman Primates and Infectious Pathogens: The Possible Genetic Bases

机译:非人类灵长类动物和传染病之间缺乏分子模拟:可能的遗传基础

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摘要

Recently, it was found that proteomes from poliovirus, measles virus, dengue virus, and severe acute respiratory syndrome-related Coronavirus 2 (SARS-CoV-2) have high molecular mimicry at the heptapeptide level with the human proteome, while heptapeptide commonality is minimal or absent with proteomes from nonhuman primates, that is, gorilla, chimpanzee, and rhesus macaque. To acquire more data on the issue, analyses here have been expanded to Ebola virus,Francisella tularensis, human immunodeficiency virus-1 (HIV-1),Toxoplasma gondii, Variola virus, andYersinia pestis. Results confirm that heptapeptide overlap is high between pathogens andHomo sapiens, but not between pathogens and primates. Data are discussed in light of the possible genetic bases that differently model primate phenomes, thus possibly underlying the zero/low level of molecular mimicry between infectious agents and primates. Notably, this study might help address preclinical vaccine tests that currently utilize primates as animal models, since autoimmune cross-reactions and the consequent adverse events cannot occurin absentiaof shared sequences.
机译:最近,发现来自Poliovirus,麻疹病毒,登革热病毒和严重急性呼吸综合征相关的冠状病毒2(SARS-COV-2)的蛋白质组在七肽水平与人蛋白质中具有高分子模拟,而七肽共性最小或者缺乏来自非人的灵长类动物,即大猩猩,黑猩猩和恒河猴。要获取更多问题的数据,这里的分析已经扩展到埃博拉病毒,Francisella Tularensis.,人类免疫缺陷病毒-1(HIV-1),Toxoplasma Gondii.,variola病毒,和yersinia pestis.。结果证实,病原体和病原体之间的七肽重叠高HOMO SAPIENS.,但在病原体和灵长类动物之间没有。鉴于可能的遗传基础讨论了数据,这些基础不同地模拟灵长类动物的碱基,因此可能在感染剂和灵长脂酸酯之间的零/低水平的分子模拟物。值得注意的是,本研究可能有助于解决当前利用灵长类动物作为动物模型的临床前疫苗测试,因为自身免疫交叉反应和随之而来的不良事件无法发生缺席共享序列。

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