Genetic overlap and causality between COVID-19 and multi-site chronic pain: the importance of immunity

Yanjing Chen; Ping Liu; Zhiyi Zhang; Yingling Ye; Sijie Yi; Chunhua Fan; Wei Zhao; Jun Liu

doi:10.3389/fimmu.2024.1277720

Genetic overlap and causality between COVID-19 and multi-site chronic pain: the importance of immunity

Front Immunol. 2024 Mar 18:15:1277720. doi: 10.3389/fimmu.2024.1277720. eCollection 2024.

Authors

Yanjing Chen^#¹, Ping Liu^#¹, Zhiyi Zhang², Yingling Ye², Sijie Yi¹, Chunhua Fan¹, Wei Zhao³, Jun Liu³

Affiliations

¹ Department of Radiology, Second Xiangya Hospital, Central South University, Changsha, China.
² Fujian University of Traditional Chinese Medicine, Fuzhou, China.
³ Clinical Research Center for Medical Imaging in Hunan Province, Changsha, Hunan, China.

^# Contributed equally.

Abstract

Background: The existence of chronic pain increases susceptibility to virus and is now widely acknowledged as a prominent feature recognized as a major manifestation of long-term coronavirus disease 2019 (COVID-19) infection. Given the ongoing COVID-19 pandemic, it is imperative to explore the genetic associations between chronic pain and predisposition to COVID-19.

Methods: We conducted genetic analysis at the single nucleotide polymorphism (SNP), gene, and molecular levels using summary statistics of genome-wide association study (GWAS) and analyzed the drug targets by summary data-based Mendelian randomization analysis (SMR) to alleviate the multi-site chronic pain in COVID-19. Additionally, we performed a latent causal variable (LCV) method to investigate the causal relationship between chronic pain and susceptibility to COVID-19.

Results: The cross-trait meta-analysis identified 19 significant SNPs shared between COVID-19 and chronic pain. Coloc analysis indicated that the posterior probability of association (PPH4) for three loci was above 70% in both critical COVID-19 and COVID-19, with the corresponding top three SNPs being rs13135092, rs7588831, and rs13135092. A total of 482 significant overlapped genes were detected from MAGMA and CPASSOC results. Additionally, the gene ANAPC4 was identified as a potential drug target for treating chronic pain (P=7.66E-05) in COVID-19 (P=8.23E-03). Tissue enrichment analysis highlighted that the amygdala (P=7.81E-04) and prefrontal cortex (P=8.19E-05) as pivotal in regulating chronic pain of critical COVID-19. KEGG pathway enrichment further revealed the enrichment of pleiotropic genes in both COVID-19 (P=3.20E-03,Padjust=4.77E-02,hsa05171) and neurotrophic pathways (P=9.03E-04,Padjust =2.55E-02,hsa04621). Finally, the latent causal variable (LCV) model was applied to find the genetic component of critical COVID-19 was causal for multi-site chronic pain (P=0.015), with a genetic causality proportion (GCP) of was 0.60.

Conclusions: In this study, we identified several functional genes and underscored the pivotal role of the inflammatory system in the correlation between the paired traits. Notably, heat shock proteins emerged as potential objective biomarkers for chronic pain symptoms in individuals with COVID-19. Additionally, the ubiquitin system might play a role in mediating the impact of COVID-19 on chronic pain. These findings contribute to a more comprehensive understanding of the pleiotropy between COVID-19 and chronic pain, offering insights for therapeutic trials.

Keywords: COVID-19; GWAS; chronic multi-site pain; genetic overlap; inflammation; pleiotropy.

Publication types

Meta-Analysis

MeSH terms

COVID-19*
Chronic Pain*
Genetic Predisposition to Disease
Genome-Wide Association Study / methods
Humans
Pandemics

Grants and funding

The author(s) declare that no financial support was received for the research, authorship, and/or publication of this article.