Transcriptome-wide association study reveals candidate causal genes for lumbar spinal stenosis

Jiawen Xu; Haibo Si; Yi Zeng; Yuangang Wu; Shaoyun Zhang; Bin Shen

doi:10.1302/2046-3758.126.BJR-2022-0160.R1

Bone & Joint Research (Jun 2023)

Transcriptome-wide association study reveals candidate causal genes for lumbar spinal stenosis

Jiawen Xu,
Haibo Si,
Yi Zeng,
Yuangang Wu,
Shaoyun Zhang,
Bin Shen

Affiliations

Jiawen Xu: Orthopedic Research Institute, Department of Orthopedics, Sichuan University West China Hospital, Chengdu, China
Haibo Si: Orthopedic Research Institute, Department of Orthopedics, Sichuan University West China Hospital, Chengdu, China
Yi Zeng: Orthopedic Research Institute, Department of Orthopedics, Sichuan University West China Hospital, Chengdu, China
Yuangang Wu: Orthopedic Research Institute, Department of Orthopedics, Sichuan University West China Hospital, Chengdu, China
Shaoyun Zhang: Orthopedic Research Institute, Department of Orthopedics, Sichuan University West China Hospital, Chengdu, China
Bin Shen: Orthopedic Research Institute, Department of Orthopedics, Sichuan University West China Hospital, Chengdu, China

DOI: https://doi.org/10.1302/2046-3758.126.BJR-2022-0160.R1
Journal volume & issue: Vol. 12, no. 6
pp. 387 – 396

Abstract

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Aims: Lumbar spinal stenosis (LSS) is a common skeletal system disease that has been partly attributed to genetic variation. However, the correlation between genetic variation and pathological changes in LSS is insufficient, and it is difficult to provide a reference for the early diagnosis and treatment of the disease. Methods: We conducted a transcriptome-wide association study (TWAS) of spinal canal stenosis by integrating genome-wide association study summary statistics (including 661 cases and 178,065 controls) derived from Biobank Japan, and pre-computed gene expression weights of skeletal muscle and whole blood implemented in FUSION software. To verify the TWAS results, the candidate genes were furthered compared with messenger RNA (mRNA) expression profiles of LSS to screen for common genes. Finally, Metascape software was used to perform enrichment analysis of the candidate genes and common genes. Results: TWAS identified 295 genes with permutation p-values < 0.05 for skeletal muscle and 79 genes associated for the whole blood, such as RCHY1 (PTWAS = 0.001). Those genes were enriched in 112 gene ontology (GO) terms and five Kyoto Encyclopedia of Genes and Genomes pathways, such as ‘chemical carcinogenesis - reactive oxygen species’ (LogP value = −2.139). Further comparing the TWAS significant genes with the differentially expressed genes identified by mRNA expression profiles of LSS found 18 overlapped genes, such as interleukin 15 receptor subunit alpha (IL15RA) (PTWAS = 0.040, PmRNA = 0.010). Moreover, 71 common GO terms were detected for the enrichment results of TWAS and mRNA expression profiles, such as negative regulation of cell differentiation (LogP value = −2.811). Conclusion: This study revealed the genetic mechanism behind the pathological changes in LSS, and may provide novel insights for the early diagnosis and intervention of LSS. Cite this article: Bone Joint Res 2023;12(6):387–396.

Published in Bone & Joint Research

ISSN: 2046-3758 (Online)
Publisher: The British Editorial Society of Bone & Joint Surgery
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Specialties of internal medicine: Diseases of the musculoskeletal system
Website: https://online.boneandjoint.org.uk/journal/bjr

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