Phylogenetic position and genetic features of HIV-1 in CNS

M. Piterskiy, O. A. Khodakov, Tatyana V. Mikheeva, Natalia V. Bilalova, Alena B. Konkova-Reidman, Yuliya A. Zakharova, A. V. Semenov
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The viral load of HIV-1 in blood plasma and cerebrospinal fluid (CSF) was measured using the \"AmpliSens HIV Monitor-FRT\" reagents kit. Sanger sequencing was performed using the AmpliSens HIV-Resist-Seq assay kit on an Applied Biosystems 3500 analyzer. Phylogenetic analysis of the pol gene fragments of HIV-1 strains (the site encoding the viral protease and part of the reverse transcriptase) was carried out using maximum likelihood method with the GTR+G nucleotide substitution model. Comparisons of the tertiary structure of viral proteins were performed according to three-dimensional models of the protease and p51 and p66 reverse transcriptase subunits obtained by homologous reconstruction using the SWISS-MODEL tools. \nResults. The viral load in the sample of patients with severe CNS lesions in blood plasma was 6.27 times higher than in CSF and amounted to 4.67 and 3.87 lg copies/ml respectively by median (p = 0,004). \nPhylogenetic analysis with the use of all available HIV-1 genomes from GenBank, which differed from the studied ones by less than 5% showed close genetic relations of viruses circulating in Chelyabinsk region, apart from strains circulating in Russian Federation, with viruses circulating in neighboring countries, in most abundance — from Ukraine and Kyrgyzstan, slightly less — from Belarus, Tajikistan, Kazakhstan and Armenia and also with strains from certain foreign countries: Poland and Germany. Phylogenetic analysis of 38 HIV-1 genomes revealed significant genetic distances between HIV isolates from blood plasma and CSF in 5 patients, 4 of whom were PWID, which may indicate an event of superinfection. \nThe amount of independent amino acid substitutions in protease in isolates from blood plasma ranged from 1 to 3, in isolates from CSF — from 1 to 2. An amount of such substitutions in a fragment of reverse transcriptase in isolates from blood plasma ranged from 1 to 6, while in isolates from CSF, it ranged from 1 to 7. HIV isolates from blood plasma and CSF from 5 patients had differences in the tertiary structure of HIV-1 reverse transcriptase p51 subunit in amino acid positions 16–20 and 210–235. Isolates from 3 other patients differed in the tertiary structure only in amino acid positons 210–235. Isolates from 3 patients differed in the structure of HIV-1 RT p66 subunit in a non-nucleoside reverse transcriptase inhibitor binding pocket (NNRTI) region. Fixed differences in the tertiary structure of p51 subunit required at minimum only 1 amino acid substitution to emerge. Alterations in the tertiary structure of p66 subunit required at least 3 amino acid substitutions. \nConclusion. Microevolution of HIV-1 proceeds in parallel within the same patient, in different compartments, which is reflected in the accumulation of amino acid substitutions different from another compartment in the conserved pol gene. There is a weak correlation between the viral load level in plasma and in CSF. The genetic heterogeneity of HIV strains from patients of the Chelyabinsk region indicates a high frequency of reintroduction of HIV infection in the region from other countries. Differences in the tertiary structure of HIV-1 reverse transcriptase between blood plasma and CSF isolates are regularly fixed in certain domens, which also confirms the presence of parallel HIV microevolution during virus persistence in tissues separated by the blood-brain barrier which allows a better understanding of the fixation trends of individual amino acid substitutions during HIV-induced damage to central nervous system.","PeriodicalId":508236,"journal":{"name":"Journal of microbiology, epidemiology and immunobiology","volume":"13 8","pages":""},"PeriodicalIF":0.0000,"publicationDate":"2024-03-13","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":null,"platform":"Semanticscholar","paperid":null,"PeriodicalName":"Journal of microbiology, epidemiology and immunobiology","FirstCategoryId":"1085","ListUrlMain":"https://doi.org/10.36233/0372-9311-442","RegionNum":0,"RegionCategory":null,"ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":null,"EPubDate":"","PubModel":"","JCR":"","JCRName":"","Score":null,"Total":0}
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Abstract

Background. Due to the wide coverage with antiretroviral therapy, the life expectancy of HIV infected people has significantly increased. Against the background of a decrease in mortality from HIV infection, HIV-associated neurocognitive disorders, which develop even during effective treatment, are of high importance. The overall prevalence of this pathology among HIV-infected people reaches 42.6%. The objective of the study was to research the genetic features and phylogenetic position of HIV-1 persisting in the central nervous system. Materials and methods. The clinical study group consisted of 38 patients with severe neurocognitive disorders against the background of HIV infection in stage 4B. The viral load of HIV-1 in blood plasma and cerebrospinal fluid (CSF) was measured using the "AmpliSens HIV Monitor-FRT" reagents kit. Sanger sequencing was performed using the AmpliSens HIV-Resist-Seq assay kit on an Applied Biosystems 3500 analyzer. Phylogenetic analysis of the pol gene fragments of HIV-1 strains (the site encoding the viral protease and part of the reverse transcriptase) was carried out using maximum likelihood method with the GTR+G nucleotide substitution model. Comparisons of the tertiary structure of viral proteins were performed according to three-dimensional models of the protease and p51 and p66 reverse transcriptase subunits obtained by homologous reconstruction using the SWISS-MODEL tools. Results. The viral load in the sample of patients with severe CNS lesions in blood plasma was 6.27 times higher than in CSF and amounted to 4.67 and 3.87 lg copies/ml respectively by median (p = 0,004). Phylogenetic analysis with the use of all available HIV-1 genomes from GenBank, which differed from the studied ones by less than 5% showed close genetic relations of viruses circulating in Chelyabinsk region, apart from strains circulating in Russian Federation, with viruses circulating in neighboring countries, in most abundance — from Ukraine and Kyrgyzstan, slightly less — from Belarus, Tajikistan, Kazakhstan and Armenia and also with strains from certain foreign countries: Poland and Germany. Phylogenetic analysis of 38 HIV-1 genomes revealed significant genetic distances between HIV isolates from blood plasma and CSF in 5 patients, 4 of whom were PWID, which may indicate an event of superinfection. The amount of independent amino acid substitutions in protease in isolates from blood plasma ranged from 1 to 3, in isolates from CSF — from 1 to 2. An amount of such substitutions in a fragment of reverse transcriptase in isolates from blood plasma ranged from 1 to 6, while in isolates from CSF, it ranged from 1 to 7. HIV isolates from blood plasma and CSF from 5 patients had differences in the tertiary structure of HIV-1 reverse transcriptase p51 subunit in amino acid positions 16–20 and 210–235. Isolates from 3 other patients differed in the tertiary structure only in amino acid positons 210–235. Isolates from 3 patients differed in the structure of HIV-1 RT p66 subunit in a non-nucleoside reverse transcriptase inhibitor binding pocket (NNRTI) region. Fixed differences in the tertiary structure of p51 subunit required at minimum only 1 amino acid substitution to emerge. Alterations in the tertiary structure of p66 subunit required at least 3 amino acid substitutions. Conclusion. Microevolution of HIV-1 proceeds in parallel within the same patient, in different compartments, which is reflected in the accumulation of amino acid substitutions different from another compartment in the conserved pol gene. There is a weak correlation between the viral load level in plasma and in CSF. The genetic heterogeneity of HIV strains from patients of the Chelyabinsk region indicates a high frequency of reintroduction of HIV infection in the region from other countries. Differences in the tertiary structure of HIV-1 reverse transcriptase between blood plasma and CSF isolates are regularly fixed in certain domens, which also confirms the presence of parallel HIV microevolution during virus persistence in tissues separated by the blood-brain barrier which allows a better understanding of the fixation trends of individual amino acid substitutions during HIV-induced damage to central nervous system.
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中枢神经系统中 HIV-1 的系统发育位置和遗传特征
背景。由于抗逆转录病毒疗法的广泛应用,艾滋病病毒感染者的预期寿命显著延长。在艾滋病病毒感染者死亡率下降的背景下,即使在有效治疗期间也会出现的艾滋病病毒相关神经认知障碍就显得尤为重要。在艾滋病病毒感染者中,这种病症的总发病率高达 42.6%。本研究的目的是研究持续存在于中枢神经系统中的 HIV-1 的遗传特征和系统发育位置。材料和方法。临床研究组由 38 名严重神经认知障碍患者组成,患者均为 4B 期 HIV 感染者。使用 "AmpliSens HIV Monitor-FRT "试剂盒检测血浆和脑脊液(CSF)中的 HIV-1 病毒载量。在 Applied Biosystems 3500 分析仪上使用 AmpliSens HIV-Resist-Seq 检测试剂盒进行了桑格测序。使用最大似然法和 GTR+G 核苷酸替换模型对 HIV-1 株系的 pol 基因片段(编码病毒蛋白酶和部分反转录酶的位点)进行了系统进化分析。根据使用 SWISS-MODEL 工具通过同源重建获得的蛋白酶、p51 和 p66 逆转录酶亚基的三维模型,对病毒蛋白的三级结构进行了比较。研究结果严重中枢神经系统病变患者血浆样本中的病毒载量是脑脊液样本的 6.27 倍,中位数分别为 4.67 和 3.87 lg copies/ml(p = 0,004)。利用 GenBank 中所有可用的 HIV-1 基因组进行的系统发育分析表明,车里雅宾斯克地区流行的病毒与周边国家流行的病毒之间有着密切的遗传关系,除了在俄罗斯联邦流行的毒株之外,还有来自乌克兰和吉尔吉斯斯坦的大量病毒,来自白俄罗斯、塔吉克斯坦、哈萨克斯坦和亚美尼亚的少量病毒,以及来自某些外国的毒株:波兰和德国。对 38 个 HIV-1 基因组进行的系统进化分析表明,在 5 名患者(其中 4 人是吸毒者)的血浆和 CSF 中分离出的 HIV 之间存在明显的遗传距离,这可能表明发生了超级感染事件。血浆中分离出的蛋白酶中独立氨基酸替换的数量为 1 至 3 个,而 CSF 中分离出的蛋白酶中独立氨基酸替换的数量为 1 至 2 个。血浆中分离出的逆转录酶片段中独立氨基酸替换的数量为 1 至 6 个,而 CSF 中分离出的逆转录酶片段中独立氨基酸替换的数量为 1 至 7 个。另外 3 名患者的分离物仅在 210-235 位氨基酸的三级结构上存在差异。3 名患者的分离物在 HIV-1 RT p66 亚基的非核苷类逆转录酶抑制剂结合袋(NNRTI)区域的结构上存在差异。p51 亚基三级结构的固定差异至少只需要 1 个氨基酸替换就会出现。p66 亚基三级结构的改变至少需要 3 个氨基酸的替换。结论在同一患者体内,HIV-1 的微进化在不同区段平行进行,这反映在保守的 pol 基因中不同于另一区段的氨基酸替代的积累上。血浆中的病毒载量水平与脑脊液中的病毒载量水平之间存在微弱的相关性。来自车里雅宾斯克地区病人的 HIV 株系的遗传异质性表明,该地区再次发生来自其他国家的 HIV 感染的频率很高。血浆和 CSF 分离物中 HIV-1 逆转录酶三级结构的差异在某些 domens 中固定不变,这也证实了病毒在被血脑屏障隔开的组织中存活期间存在并行的 HIV 微进化,从而可以更好地理解在 HIV 引起的中枢神经系统损害期间单个氨基酸替代的固定趋势。
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