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对新冠肺炎重症监护病房患者的自身免疫蛋白质组学分析显示,与男性生殖系统相关的自身抗体水平升高。

Auto-immunoproteomics analysis of COVID-19 ICU patients revealed increased levels of autoantibodies related to the male reproductive system.

作者信息

Schmidt Frank, Abdesselem Houari B, Suhre Karsten, Vaikath Nishant N, Sohail Muhammad U, Al-Nesf Maryam, Bensmail Ilham, Mashod Fathima, Sarwath Hina, Bernhardt Joerg, Schaefer-Ramadan Stephanie, Tan Ti-Myen, Morris Priscilla E, Schenck Edward J, Price David, Mohamed-Ali Vidya, Al-Maadheed Mohammed, Arredouani Abdelilah, Decock Julie, Blackburn Jonathan M, Choi Augustine M K, El-Agnaf Omar M

机构信息

Proteomics Core, Weill Cornell Medicine-Qatar, Doha, Qatar.

Proteomics Core Facility, Qatar Biomedical Research Institute (QBRI), Qatar Foundation, Hamad Bin Khalifa University (HBKU), Doha, Qatar.

出版信息

Front Physiol. 2023 Jul 14;14:1203723. doi: 10.3389/fphys.2023.1203723. eCollection 2023.

Abstract

Coronavirus disease (COVID-19) manifests many clinical symptoms, including an exacerbated immune response and cytokine storm. Autoantibodies in COVID-19 may have severe prodromal effects that are poorly understood. The interaction between these autoantibodies and self-antigens can result in systemic inflammation and organ dysfunction. However, the role of autoantibodies in COVID-19 complications has yet to be fully understood. The current investigation screened two independent cohorts of 97 COVID-19 patients [discovery (Disc) cohort from Qatar (case = 49 vs. control = 48) and replication (Rep) cohort from New York (case = 48 vs. control = 28)] utilizing high-throughput KoRectly Expressed (KREX) Immunome protein-array technology. Total IgG autoantibody responses were evaluated against 1,318 correctly folded and full-length human proteins. Samples were randomly applied on the precoated microarray slides for 2 h. Cy3-labeled secondary antibodies were used to detect IgG autoantibody response. Slides were scanned at a fixed gain setting using the Agilent fluorescence microarray scanner, generating a 16-bit TIFF file. Group comparisons were performed using a linear model and Fisher's exact test. Differentially expressed proteins were used for KEGG and WIKIpathway annotation to determine pathways in which the proteins of interest were significantly over-represented. Autoantibody responses to 57 proteins were significantly altered in the COVID-19 Disc cohort compared to healthy controls ( ≤ 0.05). The Rep cohort had altered autoantibody responses against 26 proteins compared to non-COVID-19 ICU patients who served as controls. Both cohorts showed substantial similarities ( = 0.73) and exhibited higher autoantibody responses to numerous transcription factors, immunomodulatory proteins, and human disease markers. Analysis of the combined cohorts revealed elevated autoantibody responses against SPANXN4, STK25, ATF4, PRKD2, and CHMP3 proteins in COVID-19 patients. The sequences for SPANXN4 and STK25 were cross-validated using sequence alignment tools. ELISA and Western blot further verified the autoantigen-autoantibody response of SPANXN4. SPANXN4 is essential for spermiogenesis and male fertility, which may predict a potential role for this protein in COVID-19-associated male reproductive tract complications, and warrants further research.

摘要

冠状病毒病(COVID-19)表现出许多临床症状,包括加剧的免疫反应和细胞因子风暴。COVID-19中的自身抗体可能具有严重的前驱效应,但人们对此了解甚少。这些自身抗体与自身抗原之间的相互作用可导致全身炎症和器官功能障碍。然而,自身抗体在COVID-19并发症中的作用尚未完全明确。本研究使用高通量正确表达(KREX)免疫组蛋白阵列技术,对两个独立队列的97例COVID-19患者进行了筛查[来自卡塔尔的发现(Disc)队列(病例=49例,对照=48例)和来自纽约的重复(Rep)队列(病例=48例,对照=28例)]。评估了针对1318种正确折叠的全长人类蛋白质的总IgG自身抗体反应。将样品随机施加到预包被的微阵列载玻片上2小时。使用Cy3标记的二抗检测IgG自身抗体反应。使用安捷伦荧光微阵列扫描仪在固定增益设置下扫描载玻片,生成16位TIFF文件。使用线性模型和Fisher精确检验进行组间比较。对差异表达的蛋白质进行KEGG和维基通路注释,以确定感兴趣的蛋白质显著富集的通路。与健康对照相比,COVID-19 Disc队列中对57种蛋白质的自身抗体反应显著改变(≤0.05)。与作为对照的非COVID-19重症监护病房患者相比,Rep队列中对26种蛋白质的自身抗体反应发生了改变。两个队列显示出高度相似性(=0.73),并且对多种转录因子、免疫调节蛋白和人类疾病标志物表现出更高的自身抗体反应。对合并队列的分析显示,COVID-19患者中针对SPANXN4、STK25、ATF4、PRKD2和CHMP3蛋白的自身抗体反应升高。使用序列比对工具对SPANXN4和STK25的序列进行了交叉验证。ELISA和蛋白质印迹进一步验证了SPANXN4的自身抗原-自身抗体反应。SPANXN4对精子发生和男性生育至关重要,这可能预示该蛋白在COVID-19相关男性生殖道并发症中具有潜在作用,值得进一步研究。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4663/10374950/5c27a301f685/fphys-14-1203723-g001.jpg

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