A blood RNA transcriptome signature for COVID-19

A blood RNA transcriptome signature for COVID-19

Background COVID-19 is a respiratory viral infection with unique features including a more chronic course and systemic disease manifestations including multiple organ involvement; and there are differences in disease severity between ethnic groups. The immunological basis for disease has not been fu...

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Veröffentlicht in:BMC medical genomics 2021-06, Vol.14 (1), p.1-8, Article 155
Hauptverfasser: Kwan, Philip Kam Weng, Cross, Gail B., Naftalin, Claire M., Ahidjo, Bintou A., Mok, Chee Keng, Fanusi, Felic, Permata Sari, Intan, Chia, Siok Ching, Kumar, Shoban Krishna, Alagha, Rawan, Tham, Sai Meng, Archuleta, Sophia, Sessions, October M., Hibberd, Martin L., Paton, Nicholas I.
Format: Artikel
Sprache:eng
Schlagworte:
Apoptosis
Biomarkers
Blood
Carcinogenesis
Chronic infection
Coronaviruses
COVID-19
Ethnicity
Gene expression
Genetics & Heredity
Genomes
Genomics
Illnesses
Infections
Infectious diseases
Influenza
Life Sciences & Biomedicine
Medical examination
Medical research
Medicine, Experimental
Minority & ethnic groups
p53 Protein
Respiratory syncytial virus
Ribonucleic acid
RNA
RNA sequencing
SARS-CoV-2
Science & Technology
Severe acute respiratory syndrome coronavirus 2
Software
Transcriptomes
Viral infections
Whole blood
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Zusammenfassung:Background COVID-19 is a respiratory viral infection with unique features including a more chronic course and systemic disease manifestations including multiple organ involvement; and there are differences in disease severity between ethnic groups. The immunological basis for disease has not been fully characterised. Analysis of whole-blood RNA expression may provide valuable information on disease pathogenesis. Methods We studied 45 patients with confirmed COVID-19 infection within 10 days from onset of illness and a control group of 19 asymptomatic healthy volunteers with no known exposure to COVID-19 in the previous 14 days. Relevant demographic and clinical information was collected and a blood sample was drawn from all participants for whole-blood RNA sequencing. We evaluated differentially-expressed genes in COVID-19 patients (log2 fold change >= 1 versus healthy controls; false-discovery rate < 0.05) and associated protein pathways and compared these to published whole-blood signatures for respiratory syncytial virus (RSV) and influenza. We developed a disease score reflecting the overall magnitude of expression of internally-validated genes and assessed the relationship between the disease score and clinical disease parameters. Results We found 135 differentially-expressed genes in the patients with COVID-19 (median age 35 years; 82% male; 36% Chinese, 53% South Asian ethnicity). Of the 117 induced genes, 14 were found in datasets from RSV and 40 from influenza; 95 genes were unique to COVID-19. Protein pathways were mostly generic responses to viral infections, including apoptosis by P53-associated pathway, but also included some unique pathways such as viral carcinogenesis. There were no major qualitative differences in pathways between ethnic groups. The composite gene-expression score was correlated with the time from onset of symptoms and nasal swab qPCR CT values (both p < 0.01) but was not related to participant age, gender, ethnicity or the presence or absence of chest X-ray abnormalities (all p > 0.05). Conclusions The whole-blood transcriptome of COVID-19 has overall similarity with other respiratory infections but there are some unique pathways that merit further exploration to determine clinical relevance. The approach to a disease score may be of value, but needs further validation in a population with a greater range of disease severity.
ISSN:1755-8794
1755-8794
DOI:10.1186/s12920-021-01006-w