Insights into the pathophysiology and response of persistent spinal pain syndrome type 2 to spinal cord stimulation: a human genome-wide association study

医学 病理生理学 脊髓刺激 刺激 全基因组关联研究 神经科学 脊髓 生物信息学 内科学 基因 病理 单核苷酸多态性 基因型 遗传学 生物
作者
Gustavo Fabregat,David L. Cedeño,José De Andrés,Anushik Harutyunyan,Vicente Monsalve-Dolz,Ana Mínguez-Martí,Natalia Escrivá-Matoses,Juan Marcos Asensio‐Samper,Thiago Carnaval,Jesús Villoria,Raquel Rodríguez‐López,Ricardo Vallejo
出处
期刊:Regional Anesthesia and Pain Medicine [BMJ]
卷期号:50 (10): 806-814 被引量:2
标识
DOI:10.1136/rapm-2024-105517
摘要

Background Spinal cord stimulation (SCS) provides pain relief for some patients with persistent spinal pain syndrome type 2 (PSPS 2), but the precise mechanisms of action and prognostic factors for a favorable pain response remain obscure. This in vivo human genome-wide association study provides some pathophysiological clues. Methods We performed a high-density oligonucleotide microarray analysis of serum obtained from both PSPS 2 cases and pain-free controls who had undergone lower back spinal surgery at the study site. Using multivariate discriminant analysis, we tried to identify different expressions between mRNA transcripts from PSPS 2 patients relative to controls, SCS responders to non-responders, or SCS responders to themselves before starting SCS. Gene ontology enrichment analysis was used to identify the biological processes that best discriminate between the groups of clinical interest. Results Thirty PSPS 2 patients, of whom 23 responded to SCS, were evaluated together with 15 pain-free controls. We identified 11 significantly downregulated genes in serum of PSPS 2 patients compared with pain-free controls and two significantly downregulated genes once the SCS response became apparent. All were suggestive of enhanced inflammation, tissue repair mechanisms and proliferative responses among the former. We could not identify any gene differentiating patients who responded to SCS from those who did not respond. Conclusions This study points out various biological processes that may underlie PSPS 2 pain and SCS therapeutic effects, including the modulation of neuroimmune response, inflammation and restorative processes.

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