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首页> 外文期刊>British journal of ophthalmology >The relationship between HLA-DRB1 alleles and optic neuritis in Irish patients and the risk of developing multiple sclerosis.
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The relationship between HLA-DRB1 alleles and optic neuritis in Irish patients and the risk of developing multiple sclerosis.

机译:爱尔兰患者的HLA-DRB1等位基因与视神经炎与发生多发性硬化症的风险之间的关系。

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摘要

AIMS: To investigate the role of the major histocompatibility complex in Irish patients with optic neuritis (ON) and determine whether HLA-DRB1 genotypes are a risk factor for the development of multiple sclerosis (MS) in such patients. METHOD: All patients were Caucasian, had Irish ancestry and had MRI of brain and optic nerves within 2-3 weeks of presentation. Patients were referred to a neurologist if MRI findings were consistent with a diagnosis of MS. HLA-DRB1 allele and phenotype frequencies for 78 patients with a clinical diagnosis of acute ON were compared with those for 250 healthy bone marrow donors. RESULTS: An ON/MS positive patient was 3.4 times more likely than an ON/MS negative patient to be DRB1*15 positive. No difference in age profile was detected between ON/MS positive and ON/MS negative patients or between the ON male and female subgroups. No gender or HLA-DRB1 association was identified for ON/MS negative patients. Female gender was significantly increased among ON/MS positive patients with a p value of 0.0053. CONCLUSIONS: DRB1*15 is a significant predisposing factor for ON. This ON patient cohort has also provided an opportunity to evaluate the relationship of HLA genotype with the risk of MS development. The findings of this study indicate that Irish individuals presenting with ON and who are HLA DRB1*15 positive have a higher risk than HLA DRB1*15 negative patients of presenting with MRI findings indicative of MS. This study has also demonstrated that female gender is a risk factor for developing MS in the Irish population.
机译:目的:调查主要组织相容性复合体在爱尔兰视神经炎(ON)患者中的作用,并确定HLA-DRB1基因型是否是此类患者发展为多发性硬化症(MS)的危险因素。方法:所有患者均为白种人,有爱尔兰血统,并在出现后2-3周内接受了脑和视神经的MRI检查。如果MRI检查结果与MS诊断一致,则将患者转介给神经科医生。将临床诊断为急性ON的78例患者的HLA-DRB1等位基因和表型频率与250名健康骨髓供体的HLA-DRB1等位基因和表型频率进行了比较。结果:ON / MS阳性患者DRB1 * 15阳性的可能性是ON / MS阴性患者的3.4倍。在ON / MS阳性和ON / MS阴性患者之间或ON男性和女性亚组之间未检测到年龄特征差异。未发现ON / MS阴性患者的性别或HLA-DRB1关联。在ON / MS阳性患者中,女性性别显着增加,p值为0.0053。结论:DRB1 * 15是ON的重要诱因。该ON患者队列还提供了机会来评估HLA基因型与MS发展风险的关系。这项研究的结果表明,患有ON且HLA DRB1 * 15阳性的爱尔兰患者比HLA DRB1 * 15阴性的MRI表现为MS的患者风险更高。这项研究还表明,女性是爱尔兰人口患MS的危险因素。

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