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4D-DIA蛋白质组学揭示了新冠病毒奥密克戎变异株感染后宿主唾液反应的新见解。

4D-DIA Proteomics Uncovers New Insights into Host Salivary Response Following SARS-CoV-2 Omicron Infection.

作者信息

de Lima Iasmim Lopes, Cataldi Thais Regiani, Brites Carlos, Labate Mônica Teresa Veneziano, Vaz Sara Nunes, Deminco Felice, da Cunha Gustavo Santana, Labate Carlos Alberto, Eberlin Marcos Nogueira

机构信息

PPGEMN, School of Engineering, Mackenzie Presbyterian University & MackGraphe - Mackenzie Institute for Research in Graphene and Nanotechnologies, Mackenzie Presbyterian Institute, São Paulo, São Paulo 01302-907, Brazil.

Department of Genetics, "Luiz de Queiroz" College of Agriculture, University of São Paulo/ESALQ, Piracicaba, São Paulo 13418-900, Brazil.

出版信息

J Proteome Res. 2025 Feb 7;24(2):499-514. doi: 10.1021/acs.jproteome.4c00630. Epub 2025 Jan 13.

Abstract

Since late 2021, Omicron variants have dominated the epidemiological scenario as the most successful severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) sublineages, driving new and breakthrough infections globally over the past two years. In this study, we investigated for the first time the host salivary response of COVID-19 patients infected with Omicron variants (BA.1, BA.2, and BA.4/5) by using an untargeted four-dimensional data-independent acquisition (4D-DIA)-based proteomics approach. We identified 137 proteins whose abundance levels differed between the COVID-19 positive and negative groups. Salivary signatures were mainly enriched in ribosomal proteins, linked to mRNAviral translation, protein synthesis and processing, immune innate, and antiapoptotic signaling. The higher abundance of 14-3-3 proteins (YWHAG, YWHAQ, YWHAE, and SFN) in saliva, first reported here, may be associated with increased infectivity and improved viral replicative fitness. We also identified seven proteins (ACTN1, H2AC2, GSN, NDKA, CD109, GGH, and PCYOX) that yielded comprehension into Omicron infection and performed outstandingly in screening patients with COVID-19 in a hospital setting. This panel also presented an enhanced anti-COVID-19 and anti-inflammatory signature, providing insights into disease severity, supported by comparisons with other proteome data sets. The salivary signature provided valuable insights into the host's response to SARS-CoV-2 Omicron infection, shedding light on the pathophysiology of COVID-19, particularly in cases associated with mild disease. It also underscores the potential clinical applications of saliva for disease screening in hospital settings. Data are available via ProteomeXchange with the identifier PXD054133.

摘要

自2021年末以来,奥密克戎变体作为最成功的严重急性呼吸综合征冠状病毒2(SARS-CoV-2)亚谱系主导了流行病学态势,在过去两年中引发了全球范围内的新感染和突破性感染。在本研究中,我们首次使用基于非靶向四维数据非依赖采集(4D-DIA)的蛋白质组学方法,调查了感染奥密克戎变体(BA.1、BA.2和BA.4/5)的COVID-19患者的宿主唾液反应。我们鉴定出137种蛋白质,其丰度水平在COVID-19阳性和阴性组之间存在差异。唾液特征主要富集在核糖体蛋白中,与mRNA病毒翻译、蛋白质合成与加工、先天免疫和抗凋亡信号传导有关。本文首次报道唾液中14-3-3蛋白(YWHAG、YWHAQ、YWHAE和SFN)丰度较高,这可能与传染性增加和病毒复制适应性改善有关。我们还鉴定出七种蛋白质(ACTN1、H2AC2、GSN、NDKA、CD109、GGH和PCYOX),这些蛋白质有助于理解奥密克戎感染情况,并且在医院环境中对COVID-19患者进行筛查时表现出色。该蛋白组还呈现出增强的抗COVID-19和抗炎特征,通过与其他蛋白质组数据集比较,为疾病严重程度提供了见解。唾液特征为宿主对SARS-CoV-2奥密克戎感染的反应提供了有价值的见解,揭示了COVID-19的病理生理学,特别是在与轻症相关的病例中。它还强调了唾液在医院环境中进行疾病筛查的潜在临床应用。数据可通过ProteomeXchange获得,标识符为PXD054133。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/368f/11812090/81d97bfee00b/pr4c00630_0001.jpg

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