Virus-host interactome and proteomic survey of PMBCs from COVID-19 patients reveal potential virulence factors influencing SARS-CoV-2 pathogenesis

Li, Jingjiao; Guo, Mingquan; Tian, Xiaoxu; Liu, Chengrong; Wang, Xin; Yang, Xing; Wu, Ping; Xiao, Zixuan; Qu, Yafei; Yin, Yue; Fu, Joyce; Zhu, Zhaoqin; Liu, Zhenshan; Peng, Chao; Zhu, Tongyu; Liang, Qiming

doi:10.1101/2020.03.31.019216

Cited by 78 publications

(81 citation statements)

References 32 publications

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“…Finally, we found upregulated ZAP70 (29), a tyrosine kinase that regulates motility, adhesion and cytokine expression of mature T-cells, as well as thymocyte development. A recent study found the SARS-CoV-2 nsp9 and nsp10 interact with NKRF (66), that inhibits IL-8 and IL-6 induction by competing with NF-КB for promoter binding. This interaction would lead to IL8/IL6 induction, and, among other, inhibition of ZAP70.…”

Section: The Interferon Signaling Is Activated In Dsmentioning

confidence: 99%

Network analysis of Down syndrome and SARS-CoV-2 identifies risk and protective factors for COVID-19

Toma

Dierssen

2020

Preprint

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Background: SARS-CoV-2 has spread uncontrollably worldwide while we still ignore how particularly vulnerable populations, such as Down syndrome (DS) individuals are affected by the COVID-19 pandemic. Individuals with DS have more risk of infections with respiratory complications and present signs of auto-inflammation. They also suffer from multiple comorbidities that are associated with poorer COVID-19 prognosis in the general population. All this might place DS individuals at higher risk of SARS-CoV-2 infection or poorer clinical outcomes.Methods: In order to get insight into the interplay between DS genes and SARS-cov2 infection and pathogenesis we retrieved the genes belonging to the molecular pathways involved in COVID-19 and the host proteins interacting with viral proteins from SARS-CoV-2. We therefore analyzed the overlaps of these genes with HSA21 genes, HSA21 interactors and other genes consistently differentially expressed in DS (using public transcriptomic datasets) creating a DS-SARS-CoV-2 network.Results: We detected COVID-19 protective and risk factors that might affect the susceptibility of individuals with DS both at the infection stage and in the progression to acute respiratory distress syndrome.Conclusion: Our analysis suggests that at the infection stage DS individuals might be more susceptible to infection due to triplication of TMPRSS2, that primes the viral S protein for entry in the host cells, even though the anti-viral interferon I signaling is upregulated in DS and this might increase the initial anti-viral response. In the second pro-inflammatory immunopathogenic phase of the infection, the prognosis for DS patients might worsen due to upregulation of inflammatory genes that might favor the typical cytokine storm of COVID-19. We also detected strong downregulation of the NLRP3 gene, critical for maintenance of homeostasis against pathogenic infections, possibly leading to bacterial infection complications.

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Section: The Interferon Signaling Is Activated In Dsmentioning

confidence: 99%

Network analysis of Down syndrome and SARS-CoV-2 identifies risk and protective factors for COVID-19

Toma

Dierssen

2020

Preprint

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“…With careful sample treatment, -omics can be very well used for diagnostic chips and to unravel to exact roles of individual substances within these cells, their metabolism, their transcription during cell division, or all of the above. Proteomics has been massively employed to elucidate the host interactions of SARS-CoV-2, the causative agent of COVID-19 [27][28][29][30][31][32], the greatest pandemic in our millennium.…”

Section: Proteomics Metabolomics Transcriptomics and Polyomicsmentioning

confidence: 99%

“…One very prominent aspect of microfluidic research is diagnostics on the single-cell or even molecular level. The significance of recent research towards microfluidics-based single cell diagnostic chips is apparent in health care, in our homes, and also very prominently in the fight against the COVID 19 pandemic: The diagnostic targets range from circulating tumor cells (CTC) [1][2][3][4][5][6], over parasites in blood [7][8][9][10][11][12][13][14][15], male fertility [16][17][18][19][20], molecular markers for infections [11,15,[21][22][23], cells of a specific stage in their life cycle [24,25], plant pathogens [26] and the SARS-CoV-2 proteome [27][28][29][30][31][32]. Depending on the exact target (either the entire cell or sub-cellular markers) there are different approaches to on-chip detection, each with their own underlying fundamentals and set of limitations.…”

Section: Introductionmentioning

confidence: 99%

Lab-on-a-Chip Technologies for the Single Cell Level: Separation, Analysis, and Diagnostics

Hochstetter

2020

Micromachines

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In the last three decades, microfluidics and its applications have been on an exponential rise, including approaches to isolate rare cells and diagnose diseases on the single-cell level. The techniques mentioned herein have already had significant impacts in our lives, from in-the-field diagnosis of disease and parasitic infections, through home fertility tests, to uncovering the interactions between SARS-CoV-2 and their host cells. This review gives an overview of the field in general and the most notable developments of the last five years, in three parts: 1. What can we detect? 2. Which detection technologies are used in which setting? 3. How do these techniques work? Finally, this review discusses potentials, shortfalls, and an outlook on future developments, especially in respect to the funding landscape and the field-application of these chips.

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“…But viral entry into the host cell is a prerequisite for this to happen. In the case of Covid-19, viral entry was shown to be mediated by the ACE2 receptor and the TMPRSS2 protease 27 Two recent studies capturing viral-host interactome tagged viral proteins as baits followed by affinity-purification and mass-spectrometry to identify a set of 332 (set 1: Gordon et al 16 ) and another set of 224 high confidence human proteins (set 2: Li et al 14 ) in HEK293 cell-lines which interact and co-precipitate with proteins of the Covid-19 (Supplementary Table 2). To test our hypothesis, we estimated the percentage expression of 553 host proteins (combined set of protein from both studies, Figure 4) that interact with viral proteins (a.k.a the viral interatome) across various cell-types in the different human tissues that may come in contact with the virus.…”

Section: Non-ace2 Expressing Cells Highly Express Proteins Found In Tmentioning

confidence: 99%

“…Further, researchers have used affinity-purification mass spectrometry to quantify the protein-protein interactions between viral proteins and human host proteins. These studies found 553 human host proteins in a human kidney cell line (HEK293) that suggest the mechanism of how Covid-19 invokes host inflammatory response 14 and identified potential drug targets for therapy 16 .…”

Section: Introductionmentioning

confidence: 99%

Integrated analysis of bulk multi omic and single-cell sequencing data confirms the molecular origin of hemodynamic changes in Covid-19 infection explaining coagulopathy and higher geriatric mortality

Johri

Jain

Gupta

2020

Preprint

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Besides severe respiratory distress, recent reports in Covid-19 patients have found a strong association between platelet counts and patient survival. Along with hemodynamic changes such as prolonged clotting time, high fibrin degradation products and D-dimers, increased levels of monocytes with disturbed morphology have also been identified. In this study, through an integrated analysis of bulk RNA-sequencing data from Covid-19 patients with data from single-cell sequencing studies on lung tissues, we found that most of the cell-types that contributed to the altered gene expression were of hematopoietic origin. We also found that differentially expressed genes in Covid-19 patients formed a significant pool of the expressing genes in phagocytic cells such as Monocytes and platelets. Interestingly, while we observed a general enrichment for Monocytes in Covid-19 patients, we found that the signal for FCGRA3+ Monocytes was depleted. Further, we found evidence that age-associated gene expression changes in Monocytes and platelets, associated with inflammation, mirror gene expression changes in Covid-19 patients suggesting that pro-inflammatory signalling during aging may worsen the infection in older patients. We identified more than 20 genes that change in the same direction between Covid-19 infection and aging cells that may act as potential therapeutic targets. Of particular interest were IL2RG, GNLY and GMZA expressed in platelets, which facilitates cytokine signalling in Monocytes through an interaction with platelets. To understand whether infection can directly manipulate the biology of Monocytes and platelets, we hypothesize that these non-ACE2 expressing cells may be infected by the virus through the phagocytic route. We observed that phagocytic cells such as Monocytes, T-cells, and platelets have a significantly higher expression of genes that are a part of the Covid-19 viral interactome. Hence these cell-types may have an active rather than a reactive role in viral pathogenesis to manifest clinical symptoms such as coagulopathy. Therefore, our results present molecular evidence for pursuing both anti-inflammatory and anticoagulation therapy for better patient management especially in older patients.

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Virus-host interactome and proteomic survey of PMBCs from COVID-19 patients reveal potential virulence factors influencing SARS-CoV-2 pathogenesis

Cited by 78 publications

References 32 publications

Network analysis of Down syndrome and SARS-CoV-2 identifies risk and protective factors for COVID-19

Network analysis of Down syndrome and SARS-CoV-2 identifies risk and protective factors for COVID-19

Lab-on-a-Chip Technologies for the Single Cell Level: Separation, Analysis, and Diagnostics

Integrated analysis of bulk multi omic and single-cell sequencing data confirms the molecular origin of hemodynamic changes in Covid-19 infection explaining coagulopathy and higher geriatric mortality

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