Huuskonen Sini, Liu Xiaonan, Pöhner Ina, Redchuk Taras, Salokas Kari, Lundberg Rickard, Maljanen Sari, Belik Milja, Reinholm Arttu, Kolehmainen Pekka, Tuhkala Antti, Tripathi Garima, Laine Pia, Belanov Sergei, Auvinen Petri, Vartiainen Maria, Keskitalo Salla, Österlund Pamela, Laine Larissa, Poso Antti, Julkunen Ilkka, Kakkola Laura, Varjosalo Markku
Institute of Biotechnology, Helsinki Institute of Life Science HiLIFE, University of Helsinki, Helsinki, Finland.
School of Pharmacy, University of Eastern Finland, Kuopio, Finland.
Cell Discov. 2024 Dec 9;10(1):125. doi: 10.1038/s41421-024-00748-y.
The continuous evolution of SARS-CoV-2 has led to the emergence of several variants of concern (VOCs) that significantly affect global health. This study aims to investigate how these VOCs affect host cells at proteome level to better understand the mechanisms of disease. To achieve this, we first analyzed the (phospho)proteome changes of host cells infected with Alpha, Beta, Delta, and Omicron BA.1 and BA.5 variants over time frames extending from 1 to 36 h post infection. Our results revealed distinct temporal patterns of protein expression across the VOCs, with notable differences in the (phospho)proteome dynamics that suggest variant-specific adaptations. Specifically, we observed enhanced expression and activation of key components within crucial cellular pathways such as the RHO GTPase cycle, RNA splicing, and endoplasmic reticulum-associated degradation (ERAD)-related processes. We further utilized proximity biotinylation mass spectrometry (BioID-MS) to investigate how specific mutation of these VOCs influence viral-host protein interactions. Our comprehensive interactomics dataset uncovers distinct interaction profiles for each variant, illustrating how specific mutations can change viral protein functionality. Overall, our extensive analysis provides a detailed proteomic profile of host cells for each variant, offering valuable insights into how specific mutations may influence viral protein functionality and impact therapeutic target identification. These insights are crucial for the potential use and design of new antiviral substances, aiming to enhance the efficacy of treatments against evolving SARS-CoV-2 variants.
严重急性呼吸综合征冠状病毒2(SARS-CoV-2)的持续进化导致了几种值得关注的变异株(VOC)的出现,这些变异株对全球健康产生了重大影响。本研究旨在探讨这些变异株如何在蛋白质组水平上影响宿主细胞,以更好地理解疾病机制。为实现这一目标,我们首先分析了感染α、β、δ以及奥密克戎BA.1和BA.5变异株的宿主细胞在感染后1至36小时内的(磷酸化)蛋白质组变化。我们的结果揭示了不同变异株之间蛋白质表达的独特时间模式,(磷酸化)蛋白质组动力学存在显著差异,表明存在变异株特异性适应。具体而言,我们观察到关键细胞途径(如RHO GTP酶循环、RNA剪接和内质网相关降解(ERAD)相关过程)中的关键成分表达增强并被激活。我们进一步利用邻近生物素化质谱法(BioID-MS)研究这些变异株的特定突变如何影响病毒与宿主蛋白的相互作用。我们全面的相互作用组学数据集揭示了每个变异株独特的相互作用谱,阐明了特定突变如何改变病毒蛋白功能。总体而言,我们的广泛分析提供了每个变异株宿主细胞的详细蛋白质组概况,为特定突变如何影响病毒蛋白功能以及影响治疗靶点识别提供了有价值的见解。这些见解对于新型抗病毒物质的潜在应用和设计至关重要,旨在提高针对不断进化的SARS-CoV-2变异株的治疗效果。
