Voloch Carolina M, da Silva Francisco Ronaldo, de Almeida Luiz G P, Brustolini Otavio J, Cardoso Cynthia C, Gerber Alexandra L, Guimarães Ana Paula de C, Leitão Isabela de Carvalho, Mariani Diana, Ota Victor Akira, Lima Cristiano X, Teixeira Mauro M, Dias Ana Carolina F, Galliez Rafael Mello, Faffe Débora Souza, Pôrto Luís Cristóvão, Aguiar Renato S, Castiñeira Terezinha M P P, Ferreira Orlando C, Tanuri Amilcar, de Vasconcelos Ana Tereza R
Departamento de Genética, Instituto de Biologia, Universidade Federal do Rio de Janeiro, Av. Carlos Chagas Filho, 373 - Cidade Universitária da Universidade Federal do Rio de Janeiro - Ilha do Fundão, Rio de Janeiro 21941-902, Brazil.
Laboratório de Bioinformática, Laboratório Nacional de Computação Científica, Av. Getúlio Vargas, 333 - Quitandinha, Petrópolis 25651-076, Brazil.
Virus Evol. 2021 Sep 29;7(2):veab078. doi: 10.1093/ve/veab078.
Long-term infection of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) represents a challenge to virus dispersion and the control of coronavirus disease 2019 (COVID-19) pandemic. The reason why some people have prolonged infection and how the virus persists for so long are still not fully understood. Recent studies suggested that the accumulation of intra-host single nucleotide variants (iSNVs) over the course of the infection might play an important role in persistence as well as emergence of mutations of concern. For this reason, we aimed to investigate the intra-host evolution of SARS-CoV-2 during prolonged infection. Thirty-three patients who remained reverse transcription polymerase chain reaction (RT-PCR) positive in the nasopharynx for on average 18 days from the symptoms onset were included in this study. Whole-genome sequences were obtained for each patient at two different time points. Phylogenetic, populational, and computational analyses of viral sequences were consistent with prolonged infection without evidence of coinfection in our cohort. We observed an elevated within-host genomic diversity at the second time point samples positively correlated with cycle threshold (Ct) values (lower viral load). Direct transmission was also confirmed in a small cluster of healthcare professionals that shared the same workplace by the presence of common iSNVs. A differential accumulation of missense variants between the time points was detected targeting crucial structural and non-structural proteins such as Spike and helicase. Interestingly, longitudinal acquisition of iSNVs in Spike protein coincided in many cases with SARS-CoV-2 reactive and predicted T cell epitopes. We observed a distinguishing pattern of mutations over the course of the infection mainly driven by increasing A→U and decreasing G→A signatures. G→A mutations may be associated with RNA-editing enzyme activities; therefore, the mutational profiles observed in our analysis were suggestive of innate immune mechanisms of the host cell defense. Therefore, we unveiled a dynamic and complex landscape of host and pathogen interaction during prolonged infection of SARS-CoV-2, suggesting that the host's innate immunity shapes the increase of intra-host diversity. Our findings may also shed light on possible mechanisms underlying the emergence and spread of new variants resistant to the host immune response as recently observed in COVID-19 pandemic.
严重急性呼吸综合征冠状病毒2(SARS-CoV-2)的长期感染对病毒传播以及2019冠状病毒病(COVID-19)大流行的控制构成挑战。一些人感染时间延长的原因以及病毒如何持续如此长时间仍未完全清楚。最近的研究表明,感染过程中宿主内单核苷酸变异(iSNV)的积累可能在持续性以及关注突变的出现中起重要作用。因此,我们旨在研究SARS-CoV-2在长期感染期间的宿主内进化。本研究纳入了33例从症状出现起平均18天鼻咽部逆转录聚合酶链反应(RT-PCR)仍呈阳性的患者。在两个不同时间点获取了每位患者的全基因组序列。病毒序列的系统发育、群体和计算分析与长期感染一致,且我们的队列中没有合并感染的证据。我们在第二个时间点的样本中观察到宿主内基因组多样性增加,且与循环阈值(Ct)值(较低病毒载量)呈正相关。通过共同iSNV的存在,在一小群共用同一工作场所的医护人员中也证实了直接传播。在针对关键结构和非结构蛋白(如刺突蛋白和螺旋酶)的时间点之间检测到错义变异的差异积累。有趣的是,刺突蛋白中iSNV的纵向获得在许多情况下与SARS-CoV-2反应性和预测的T细胞表位一致。我们在感染过程中观察到一种独特的突变模式,主要由A→U增加和G→A减少的特征驱动。G→A突变可能与RNA编辑酶活性有关;因此,我们分析中观察到的突变谱提示了宿主细胞防御的先天免疫机制。因此,我们揭示了SARS-CoV-2长期感染期间宿主与病原体相互作用的动态和复杂图景,表明宿主的先天免疫塑造了宿主内多样性的增加。我们的发现也可能为最近在COVID-19大流行中观察到的对宿主免疫反应具有抗性的新变体的出现和传播的潜在机制提供线索。
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