High-Density Blood Transcriptomics Reveals Precision Immune Signatures of SARS-CoV-2 Infection in Hospitalized Individuals

Prokop, Jeremy W.; Hartog, Nicholas; Chesla, Dave; Faber, William E.; Love, Chanise P; Karam, Rachid; Abualkheir, Nelly; Feldmann, Benjamin; McBride, Tamara; Leimanis, Mara L.; English, B. Keith; Holsworth, Amanda; Frisch, Austin; Bauss, Jacob; Kalpage, Nathisha; Derbedrossian, Aram; Pinti, Ryan M; Hale, Nicole; Mills, Joshua; Eby, Alexandra; VanSickle, Elizabeth; Pageau, Spencer C; Shankar, Rama; Chen, Bin; Carcillo, Joseph A.; Sanfilippo, Dominic; Olivero, Rosemary; Bupp, Caleb; Rajasekaran, Surender

doi:10.3389/fimmu.2021.694243

Cited by 28 publications

(32 citation statements)

References 69 publications

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“…Transcriptome wide analyses of blood from severe COVID-19 patients reveals a series of activated immune system genes including those associated with neutrophils, secretory granules, neutrophil extracellular traps (NETS) along with clonal expansion of adaptive immune response and diminished lymphocyte gene expression [ 188 ]. The following sections provide an overview of the exuberant innate and poor adaptive immune responses and subsequent cytokine storm and tissue damage sequalae observed in severe cases of COVID-19.…”

Section: The Potential Implications and Clinical Translation Of Senescence And Aging In Covid-19mentioning

confidence: 99%

Role of Senescence and Aging in SARS-CoV-2 Infection and COVID-19 Disease

Lynch

Guo

Gibson

et al. 2021

Cells

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Coronavirus disease 2019 (COVID-19), caused by severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), has resulted in a global pandemic associated with substantial morbidity and mortality worldwide, with particular risk for severe disease and mortality in the elderly population. SARS-CoV-2 infection is driven by a pathological hyperinflammatory response which results in a dysregulated immune response. Current advancements in aging research indicates that aging pathways have fundamental roles in dictating healthspan in addition to lifespan. Our review discusses the aging immune system and highlights that senescence and aging together, play a central role in COVID-19 pathogenesis. In our review, we primarily focus on the immune system response to SARS-CoV-2 infection, the interconnection between severe COVID-19, immunosenescence, aging, vaccination, and the emerging problem of Long-COVID. We hope to highlight the importance of identifying specific senescent endotypes (or “sendotypes”), which can used as determinants of COVID-19 severity and mortality. Indeed, identified sendotypes could be therapeutically exploited for therapeutic intervention. We highlight that senolytics, which eliminate senescent cells, can target aging-associated pathways and therefore are proving attractive as potential therapeutic options to alleviate symptoms, prevent severe infection, and reduce mortality burden in COVID-19 and thus ultimately enhance healthspan.

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Section: The Potential Implications and Clinical Translation Of Senescence And Aging In Covid-19mentioning

confidence: 99%

Role of Senescence and Aging in SARS-CoV-2 Infection and COVID-19 Disease

Lynch

Guo

Gibson

et al. 2021

Cells

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“…The phenotypes seen in the Geno2MP data suggested a broader analysis of CCR5 in disease pathologies. With the robust expression of CCR5 in blood and our history in studying the blood of immune challenged individuals, we selected to process CCR5 biology for blood-based RNAseq of 7,280 samples from 62 different BioProjects and three of our studies where we have patient-to-transcriptome insights ( 74 – 76 ) ( Figure 7 ). All these samples were blood collected into RNA PAXgene tubes to standardize sample collection.…”

Section: Resultsmentioning

confidence: 99%

“…Therefore, we focused analysis on three cohorts our team collected blood PAXgene tube RNAseq in hospitalized patients with MODS, RSV, or COVID-19 in an age range from weeks of life to elderly. The adult hospitalized COVID-19 cohort shows highest CCR5 expression in the male Hispanic control patient 21 age 50-59 ( Figure 7C ), who had the highest interferon response, was noted to have a unique transcriptome, was the furthest outlier of the control samples, had markers of multiple organ damage, and generally seemed to be a highly divergent sample from the cohort ( 74 ). The second highest was a 50-59 yo European ancestry male who had a lethal case of COVID-19 marked by a SAPSII score of 61, suggesting multiple organ complications, had a robust interferon response, elevated cytokine expression profile, the highest cell markers of peripheral monocytes, and a weak clonal expansion of the immune repertoire.…”

Section: Resultsmentioning

confidence: 99%

“…Open Targets Genetics ( 73 ) was used for the understanding of GWAS and pheWAS associations. Samples from our previous RNAseq work and details of methods used can be found in the three publications for MODS, RSV, or COVID-19 ( 74 – 76 ). All PAXgene tube blood RNAseq datasets within the NCBI SRA were downloaded with the SRA toolkit ( ) and processed for abundance using Salmon_0.14.1 ( 77 ) and the Gencode38 transcriptome ( 78 ).…”

Section: Methodsmentioning

confidence: 99%

“…All PAXgene tube blood RNAseq datasets within the NCBI SRA were downloaded with the SRA toolkit ( ) and processed for abundance using Salmon_0.14.1 ( 77 ) and the Gencode38 transcriptome ( 78 ). Microglia datasets were extracted from BioProjects PRJNA649597, PRJNA662330, PRJNA665286, PRJNA667596, PRJNA688478, PRJNA689841, PRJNA387182, PRJNA483247 and the blood RNAseq datasets from BioProjects PRJEB14743, PRJEB20731, PRJEB23048, PRJEB27958, PRJEB27965, PRJEB33892, PRJEB36928, PRJEB41073, PRJEB44660, PRJNA201433, PRJNA230906, PRJNA232593, PRJNA251404, PRJNA277352, PRJNA305001, PRJNA315611, PRJNA327986, PRJNA329148, PRJNA352062, PRJNA354367, PRJNA357628, PRJNA358580, PRJNA369684, PRJNA378794, PRJNA380820, PRJNA384259, PRJNA390289, PRJNA397222, PRJNA398240, PRJNA401870, PRJNA427575, PRJNA437114, PRJNA454694, PRJNA476781, PRJNA493832, PRJNA494155, PRJNA504827, PRJNA511891, PRJNA526259, PRJNA526839, PRJNA533086, PRJNA552286, PRJNA562305, PRJNA588242, PRJNA591657, PRJNA600846, PRJNA601661, PRJNA607120, PRJNA630674, PRJNA632871, PRJNA634938, PRJNA638653, PRJNA639278, PRJNA647880, PRJNA664368, PRJNA679264, PRJNA679331, PRJNA680771, PRJNA683803, PRJNA686397, PRJNA702558, PRJNA728070 in addition to our groups studies on MODS, RSV, and COVID-19 ( 74 – 76 ). All Gencode38 mapped reads for these samples can be found at .…”

Section: Methodsmentioning

confidence: 99%

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CCR5 and Biological Complexity: The Need for Data Integration and Educational Materials to Address Genetic/Biological Reductionism at the Interface of Ethical, Legal, and Social Implications

et al. 2021

Self Cite

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In the age of genomics, public understanding of complex scientific knowledge is critical. To combat reductionistic views, it is necessary to generate and organize educational material and data that keep pace with advances in genomics. The view that CCR5 is solely the receptor for HIV gave rise to demand to remove the gene in patients to create host HIV resistance, underestimating the broader roles and complex genetic inheritance of CCR5. A program aimed at providing research projects to undergraduates, known as CODE, has been expanded to build educational material for genes such as CCR5 in a rapid approach, exposing students and trainees to large bioinformatics databases and previous experiments for broader data to challenge commitment to biological reductionism. Our students organize expression databases, query environmental responses, assess genetic factors, generate protein models/dynamics, and profile evolutionary insights into a protein such as CCR5. The knowledgebase generated in the initiative opens the door for public educational information and tools (molecular videos, 3D printed models, and handouts), classroom materials, and strategy for future genetic ideas that can be distributed in formal, semiformal, and informal educational environments. This work highlights that many factors are missing from the reductionist view of CCR5, including the role of missense variants or expression of CCR5 with neurological phenotypes and the role of CCR5 and the delta32 variant in complex critical care patients with sepsis. When connected to genomic stories in the news, these tools offer critically needed Ethical, Legal, and Social Implication (ELSI) education to combat biological reductionism.

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