评估退行性颈脊髓病的遗传和非遗传风险因素。
Evaluation of Genetic and Nongenetic Risk Factors for Degenerative Cervical Myelopathy.
机构信息
Department of Orthopaedic Surgery.
Department of Genetics, Washington University School of Medicine, St. Louis, MO.
出版信息
Spine (Phila Pa 1976). 2023 Aug 15;48(16):1117-1126. doi: 10.1097/BRS.0000000000004735. Epub 2023 May 30.
STUDY DESIGN
Cohort study.
OBJECTIVE
We aimed to evaluate the associations of genetic and nongenetic factors with degenerative cervical myelopathy (DCM).
SUMMARY OF BACKGROUND DATA
There is mounting evidence for an inherited predisposition for DCM, but uncertainty remains regarding specific genetic markers involved. Similarly, nongenetic factors are thought to play a role.
MATERIALS AND METHODS
Using diagnosis codes from hospital records linked to the UK Biobank cohort, patients with cervical spondylosis were identified followed by the identification of a subset with DCM. Nongenetic variables evaluated included age, sex, race, Townsend deprivation index, body mass index, occupational demands, osteoporosis, and smoking. Genome-wide association analyses were conducted using logistic regression adjusted for age, sex, population principal components, and follow-up.
RESULTS
A total of 851 DCM cases out of 2787 cervical spondylosis patients were identified. Several nongenetic factors were independently associated with DCM including age [odds ratio (OR)=1.11, 95% CI=1.01-1.21, P =0.024], male sex (OR=1.63, 95% CI=1.37-1.93, P <0.001), and relative socioeconomic deprivation (OR=1.03, 95% CI=1.00-1.06, P =0.030). Asian race was associated with lower DCM risk (OR=0.44, 95% CI=0.22-0.85, P =0.014). We did not identify genome-wide significant (≤5×10 -8 ) single-nucleotide polymorphisms (SNPs) associated with DCM. The strongest genome-wide signals were at SNP rs67256809 in the intergenic region of the genes LINC02582 and FBXO15 on chromosome 18 ( P =1.12×10 -7 ) and rs577081672 in the GTPBP1 gene on chromosome 22 ( P =2.9×10 -7 ). No SNPs reported in prior DCM studies were significant after adjusting for replication attempts.
CONCLUSIONS
Increasing age, male sex, and relative socioeconomic deprivation were identified as independent risk factors for DCM, whereas Asian race was inversely associated. SNPs of potential interest were identified in GTPBP1 and an intergenic region on chromosome 18, but these associations did not reach genome-wide significance. Identification of genetic and nongenetic DCM susceptibility markers may guide understanding of DCM disease processes, inform risk, guide prevention and potentially inform surgical outcomes.
LEVEL OF EVIDENCE
Prognostic level III.
研究设计
队列研究。
目的
评估遗传和非遗传因素与退行性颈椎脊髓病(DCM)的关联。
背景资料概要
越来越多的证据表明 DCM 存在遗传易感性,但仍存在不确定的特定遗传标记。同样,非遗传因素也被认为发挥了作用。
材料和方法
使用来自与英国生物库队列相关联的医院记录中的诊断代码,确定患有颈椎病的患者,然后确定患有 DCM 的亚组患者。评估的非遗传变量包括年龄、性别、种族、汤森贫困指数、体重指数、职业需求、骨质疏松症和吸烟。使用逻辑回归分析进行全基因组关联分析,该分析针对年龄、性别、人群主成分和随访进行了调整。
结果
在 2787 例颈椎病患者中,共发现 851 例 DCM 病例。几个非遗传因素与 DCM 独立相关,包括年龄[比值比(OR)=1.11,95%置信区间(CI)=1.01-1.21,P=0.024]、男性(OR=1.63,95%CI=1.37-1.93,P<0.001)和相对社会经济贫困(OR=1.03,95%CI=1.00-1.06,P=0.030)。亚洲种族与较低的 DCM 风险相关(OR=0.44,95%CI=0.22-0.85,P=0.014)。我们没有发现与 DCM 相关的全基因组显著(≤5×10 -8 )单核苷酸多态性(SNP)。全基因组最强信号位于 18 号染色体上 LINC02582 和 FBXO15 基因间区的 SNP rs67256809(P=1.12×10 -7 )和 22 号染色体上 GTPBP1 基因的 SNP rs577081672(P=2.9×10 -7 )。在调整了复制尝试后,先前 DCM 研究中报告的没有 SNP 具有统计学意义。
结论
年龄增长、男性和相对社会经济贫困被确定为 DCM 的独立危险因素,而亚洲种族则呈负相关。在 GTPBP1 基因和 18 号染色体上的基因间区发现了有潜在意义的 SNP,但这些关联未达到全基因组显著水平。确定 DCM 易感性的遗传和非遗传标记可能有助于了解 DCM 疾病过程、指导风险、指导预防,并可能指导手术结果。
证据水平
预后 III 级。
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