Prevalence, Patterns, and Genetic Association Analysis of Modic Vertebral Endplate Changes.
10.4184/asj.2017.11.4.594
- Author:
Rishi Mugesh KANNA
1
;
Rajasekaran SHANMUGANATHAN
;
Veera Ranjani RAJAGOPALAN
;
Senthil NATESAN
;
Raveendran MUTHURAJA
;
Kenneth Man Chee CHEUNG
;
Danny CHAN
;
Patrick Yu Ping KAO
;
Anita YEE
;
Ajoy Prasad SHETTY
Author Information
1. Department of Orthopaedics and Spine Surgery, Ganga Hospital, Coimbatore, India. sr@gangahospital.com
- Publication Type:Original Article
- Keywords:
Prevalence;
Modic changes;
Genetic association studies;
Single nucleotide polymorphism
- MeSH:
Cohort Studies;
Genetic Association Studies;
Humans;
Intervertebral Disc Degeneration;
Low Back Pain;
Magnetic Resonance Imaging;
Phenotype;
Polymorphism, Genetic;
Polymorphism, Single Nucleotide;
Prevalence*;
Prospective Studies;
Spine
- From:Asian Spine Journal
2017;11(4):594-600
- CountryRepublic of Korea
- Language:English
-
Abstract:
STUDY DESIGN: A prospective genetic association study. PURPOSE: The etiology of Modic changes (MCs) is unclear. Recently, the role of genetic factors in the etiology of MCs has been evaluated. However, studies with a larger patient subset are lacking, and candidate genes involved in other disc degeneration phenotypes have not been evaluated. We studied the prevalence of MCs and genetic association of 41 candidate genes in a large Indian cohort. OVERVIEW OF LITERATURE: MCs are vertebral endplate signal changes predominantly observed in the lumbar spine. A significant association between MCs and lumbar disc degeneration and nonspecific low back pain has been described, with the etiopathogenesis implicating various mechanical, infective, and biochemical factors. METHODS: We studied 809 patients using 1.5-T magnetic resonance imaging to determine the prevalence, patterns, distribution, and type of lumbar MCs. Genetic association analysis of 71 single nucleotide polymorphisms (SNPs) of 41 candidate genes was performed based on the presence or absence of MCs. SNPs were genotyped using the Sequenome platform, and an association test was performed using PLINK software. RESULTS: The mean age of the study population (n=809) was 36.7±10.8 years. Based on the presence of MCs, the cohort was divided into 702 controls and 107 cases (prevalence, 13%). MCs were more commonly present in the lower (149/251, 59.4%) than in the upper (102/251, 40.6%) endplates. L4–5 endplates were the most commonly affected levels (30.7%). Type 2 MCs were the most commonly observed pattern (n=206, 82%). The rs2228570 SNP of VDR (p=0.02) and rs17099008 SNP of MMP20 (p=0.03) were significantly associated with MCs. CONCLUSIONS: Genetic polymorphisms of SNPs of VDR and MMP20 were significantly associated with MCs. Understanding the etiopathogenetic mechanisms of MCs is important for planning preventive and therapeutic strategies.
