多发性硬化风险基因座在感染后神经综合征中的影响。
Impact of multiple sclerosis risk loci in postinfectious neurological syndromes.
作者信息
Martinelli-Boneschi Filippo, Currò Riccardo, Santoro Silvia, Berzero Giulia, Sorosina Melissa, Ferrè Laura, Mascia Elisabetta, Peroni Silvia, Comi Giancarlo, Gugliemi Angelo, Vegezzi Elisa, Callegari Ilaria, Filippi Massimo, Cortese Andrea, Esposito Federica, Clarelli Ferdinando, Marchioni Enrico
机构信息
Dino Ferrari Centre, Neuroscience Section, Department of Pathophysiology and Transplantation (DEPT), University of Milan, Via Francesco Sforza 35, 20122 Milan, Italy; Neurology Unit and MS Centre, Foundation IRCCS Ca' Granda Ospedale Maggiore Policlinico, Via Francesco Sforza 35, 20122 Milan, Italy.
Department of Brain and Behavioral Sciences, University of Pavia, via Forlanini 6, 27100 Pavia, Italy; Fondazione Istituto Neurologico Nazionale IRCCS Mondino, via Mondino 2, 27100 Pavia, Italy.
出版信息
Mult Scler Relat Disord. 2020 Sep;44:102326. doi: 10.1016/j.msard.2020.102326. Epub 2020 Jun 24.
BACKGROUND
The genetic component of multiple sclerosis (MS) is now set to 200 autosomal common variants. However, it is unclear how genetic knowledge be clinically used in the differential diagnosis between MS and other inflammatory conditions like adult-onset postinfectious neurological syndromes (PINS). The aim of this study was to investigate whether PINS and MS have a shared genetic background using an updated polygenic risk scores.
METHODS
Eighty-eight PINS patients have been consecutively recruited between 1996 and 2016 at Mondino Foundation of Pavia, diagnosed according to clinical, MRI and CSF findings and followed-up for several years. Patients were typed using Illumina array, and genotypes imputed using the 1000 Genomes Project reference panel. A weighted genetic risk score (wGRS) has been calculated based on autosomal MS risk loci derived from large-scale studies, and an HLA genetic burden (HLAGB) was also calculated on loci associated to MS.
RESULTS
PINS occurred as an episode of myelitis in 44% of patients, encephalomyelitis in 44%, and encephalitis in remaining cases, with an involvement of peripheral nervous system in 41% of patients. Mean age of onset was 50.1 years, and female:male ratio was 1.4. Patients were followed-up for a mean of 7.2 years, and at last visit 55% had a low disability grade (mRS 0-1). Disease was monophasic in 67% of patients, relapsing in 18% and chronic-progressive in 15%. The wGRS of PINS cases was comparable to 370 healthy controls, while significantly lower compared to 907 bout-onset MS (BOMS) cases (wGRS= 20.9 vs 21.2; p<0.0001). The difference was even larger for PINS with peripheral nervous system involvement (wGRS=20.6) vs BOMS.
CONCLUSION
The distinction between MS and PINS is not easy to make in clinical practice. However, our study shows that the new set of MS risk alleles does not confer increased susceptibility to PINS. These data support the importance to discriminate these cases from MS with pathophysiological and therapeutic implications.
背景
多发性硬化症(MS)的遗传成分目前已确定为200个常染色体常见变异。然而,尚不清楚如何将遗传学知识临床应用于MS与其他炎症性疾病(如成人感染后神经综合征(PINS))的鉴别诊断。本研究的目的是使用更新的多基因风险评分来调查PINS和MS是否具有共同的遗传背景。
方法
1996年至2016年期间,在帕维亚的蒙迪诺基金会连续招募了88例PINS患者,根据临床、MRI和脑脊液检查结果进行诊断,并进行了数年随访。使用Illumina阵列对患者进行基因分型,并使用千人基因组计划参考面板推算基因型。基于大规模研究得出的常染色体MS风险位点计算加权遗传风险评分(wGRS),并计算与MS相关位点的HLA遗传负担(HLAGB)。
结果
44%的患者PINS表现为脊髓炎发作,44%为脑脊髓炎,其余为脑炎,41%的患者累及周围神经系统。平均发病年龄为50.1岁,女性与男性比例为1.4。患者平均随访7.2年,最后一次随访时55%的患者残疾程度较低(改良Rankin量表0-1级)。67%的患者疾病为单相性,18%为复发型,15%为慢性进展型。PINS病例的wGRS与370名健康对照相当,但与907例发作性MS(BOMS)病例相比显著更低(wGRS = 20.9对21.2;p<0.0001)。对于伴有周围神经系统受累的PINS(wGRS = 20.6)与BOMS相比,差异更大。
结论
在临床实践中,MS和PINS之间的区分并不容易。然而,我们的研究表明,新的MS风险等位基因集不会增加PINS的易感性。这些数据支持了从MS中鉴别这些病例的重要性,这具有病理生理学和治疗意义。
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