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在原代人鼻腔培养物中比较关注的 SARS-CoV-2 变异株,表明德尔塔变异株具有最高的细胞病变效应,而奥密克戎变异株复制速度最快。

Comparison of SARS-CoV-2 variants of concern in primary human nasal cultures demonstrates Delta as most cytopathic and Omicron as fastest replicating.

机构信息

Department of Microbiology, University of Pennsylvania Perelman School of Medicine, Philadelphia, Pennsylvania, USA.

Department of Otorhinolaryngology- Head and Neck Surgery, Perelman School of Medicine, University of Pennsylvania, Philadelphia, Pennsylvania, USA.

出版信息

mBio. 2024 Apr 10;15(4):e0312923. doi: 10.1128/mbio.03129-23. Epub 2024 Mar 13.

Abstract

UNLABELLED

The SARS-CoV-2 pandemic was marked with emerging viral variants, some of which were designated as variants of concern (VOCs) due to selection and rapid circulation in the human population. Here, we elucidate functional features of each VOC linked to variations in replication rate. Patient-derived primary nasal cultures grown at air-liquid interface were used to model upper respiratory infection and compared to cell lines derived from human lung epithelia. All VOCs replicated to higher titers than the ancestral virus, suggesting a selection for replication efficiency. In primary nasal cultures, Omicron replicated to the highest titers at early time points, followed by Delta, paralleling comparative studies of population sampling. All SARS-CoV-2 viruses entered the cell primarily via a transmembrane serine protease 2 (TMPRSS2)-dependent pathway, and Omicron was more likely to use an endosomal route of entry. All VOCs activated and overcame dsRNA-induced cellular responses, including interferon (IFN) signaling, oligoadenylate ribonuclease L degradation, and protein kinase R activation. Among the VOCs, Omicron infection induced expression of the most IFN and IFN-stimulated genes. Infections in nasal cultures resulted in cellular damage, including a compromise of cell barrier integrity and loss of nasal cilia and ciliary beating function, especially during Delta infection. Overall, Omicron was optimized for replication in the upper respiratory tract and least favorable in the lower respiratory cell line, and Delta was the most cytopathic for both upper and lower respiratory cells. Our findings highlight the functional differences among VOCs at the cellular level and imply distinct mechanisms of pathogenesis in infected individuals.

IMPORTANCE

Comparative analysis of infections by SARS-CoV-2 ancestral virus and variants of concern, including Alpha, Beta, Delta, and Omicron, indicated that variants were selected for efficiency in replication. In infections of patient-derived primary nasal cultures grown at air-liquid interface to model upper respiratory infection, Omicron reached the highest titers at early time points, a finding that was confirmed by parallel population sampling studies. While all infections overcame dsRNA-mediated host responses, infections with Omicron induced the strongest interferon and interferon-stimulated gene response. In both primary nasal cultures and lower respiratory cell line, infections by Delta were most damaging to the cells as indicated by syncytia formation, loss of cell barrier integrity, and nasal ciliary function.

摘要

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SARS-CoV-2 大流行的特点是出现了新的病毒变体,其中一些由于在人类群体中的选择和快速传播而被指定为关注变体(VOC)。在这里,我们阐明了与复制率变化相关的每个 VOC 的功能特征。使用在气液界面培养的患者来源的原代鼻腔培养物来模拟上呼吸道感染,并与源自人肺上皮的细胞系进行比较。所有 VOC 的复制滴度均高于原始病毒,表明选择了复制效率。在原代鼻腔培养物中,Omicron 在早期时间点的复制滴度最高,其次是 Delta,与人群采样的比较研究一致。所有 SARS-CoV-2 病毒主要通过跨膜丝氨酸蛋白酶 2(TMPRSS2)依赖性途径进入细胞,而 Omicron 更可能通过内体途径进入细胞。所有 VOC 均激活并克服了双链 RNA 诱导的细胞反应,包括干扰素(IFN)信号转导、寡聚腺苷酸核糖核酸酶 L 降解和蛋白激酶 R 激活。在 VOC 中,Omicron 感染诱导了最多的 IFN 和 IFN 刺激基因的表达。在鼻腔培养物中的感染导致细胞损伤,包括细胞屏障完整性受损以及鼻纤毛和纤毛摆动功能丧失,尤其是在 Delta 感染期间。总体而言,Omicron 在呼吸道上部的复制得到了优化,在下部呼吸道细胞系中最不利,而 Delta 对上下呼吸道细胞的细胞病变作用最大。我们的研究结果强调了 VOC 在细胞水平上的功能差异,并暗示了感染个体中不同的发病机制。

重要性

对 SARS-CoV-2 原始病毒和关注变体(包括 Alpha、Beta、Delta 和 Omicron)的感染进行比较分析表明,变体是为复制效率而选择的。在使用在气液界面培养的患者来源的原代鼻腔培养物进行的上呼吸道感染模型感染中,Omicron 在早期时间点达到了最高滴度,这一发现得到了平行人群采样研究的证实。虽然所有感染均克服了双链 RNA 介导的宿主反应,但 Omicron 感染诱导了最强的干扰素和干扰素刺激基因反应。在原代鼻腔培养物和下部呼吸道细胞系中,Delta 感染对细胞的损伤最大,表现为合胞体形成、细胞屏障完整性丧失和鼻纤毛功能丧失。

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