Transcriptomic Studies Revealed Pathophysiological Impact of COVID-19 to Predominant Health Conditions

Overview

Journal Brief Bioinform

Publisher Oxford University Press

Specialty Biology

Date 2021 Jun 2

PMID 34076249

Citations 12

Authors

Zulkar Nain

Shital K Barman

Md Moinuddin Sheam

Shifath Bin Syed

Abdus Samad

Julian M W Quinn

Mohammad Minnatul Karim

Mahbubul Kabir Himel

Rajib Kanti Roy

Mohammad Ali Moni

Sudhangshu Kumar Biswas

Affiliations

Soon will be listed here.

Abstract

Despite the association of prevalent health conditions with coronavirus disease 2019 (COVID-19) severity, the disease-modifying biomolecules and their pathogenetic mechanisms remain unclear. This study aimed to understand the influences of COVID-19 on different comorbidities and vice versa through network-based gene expression analyses. Using the shared dysregulated genes, we identified key genetic determinants and signaling pathways that may involve in their shared pathogenesis. The COVID-19 showed significant upregulation of 93 genes and downregulation of 15 genes. Interestingly, it shares 28, 17, 6 and 7 genes with diabetes mellitus (DM), lung cancer (LC), myocardial infarction and hypertension, respectively. Importantly, COVID-19 shared three upregulated genes (i.e. MX2, IRF7 and ADAM8) with DM and LC. Conversely, downregulation of two genes (i.e. PPARGC1A and METTL7A) was found in COVID-19 and LC. Besides, most of the shared pathways were related to inflammatory responses. Furthermore, we identified six potential biomarkers and several important regulatory factors, e.g. transcription factors and microRNAs, while notable drug candidates included captopril, rilonacept and canakinumab. Moreover, prognostic analysis suggests concomitant COVID-19 may result in poor outcome of LC patients. This study provides the molecular basis and routes of the COVID-19 progression due to comorbidities. We believe these findings might be useful to further understand the intricate association of these diseases as well as for the therapeutic development.

Citing Articles

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