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与萎缩素反应介导蛋白5相关的视神经病变:临床特征、影像学线索及预后

Collapsin response mediator protein 5-associated optic neuropathy: clinical characteristics, radiologic clues, and outcomes.

作者信息

Yan Rong, Mao Yu, Zeng Huiyang, Liu Qian, Jiang Hanqiu, Peng Jingting, Yang Qingling, Cui Shilei, Liu Lei, Guo Yanjun, Wang Jiawei

机构信息

Department of Neurology, Beijing Tongren Hospital, Capital Medical University, Beijing, China.

Department of Ophthalmology, Beijing Tongren Hospital, Capital Medical University, Beijing, China.

出版信息

Front Neurol. 2023 Jun 28;14:1163615. doi: 10.3389/fneur.2023.1163615. eCollection 2023.

Abstract

OBJECTIVE

Collapsin response mediator protein 5-associated optic neuropathy (CRMP5-ON) is a rare entity of autoimmune optic neuropathy. This study aimed to review the neuro-ophthalmic findings and outcomes in a series of patients with CRMP5-ON to further characterize its clinical phenotype, radiologic clues, and outcomes.

METHODS

This was a retrospective case series and a single-center medical chart review of all patients with CRPM5-seropositive ON at the Department of Neurology, Beijing Tongren Hospital, from December 1, 2020, to March 31, 2023. The main outcome measures were neuro-ophthalmic manifestations, radiologic characteristics, and clinical outcomes of CRMP5-ON; coexisting neural autoantibody, paraneoplastic associations, and the impact of immunosuppressant therapy.

RESULTS

Five patients were identified. Four (80%) were female, and the average age at onset was 59.4 years (range 53-69 years), with an average follow-up of 15.3 months (range 1.4-28.7 months). The average best-corrected visual acuity (BCVA) at nadir was 20/120 (range 20/20 to count fingers). Seven of ten affected eyes (70%) showed diffuse defects of the central field. Painless bilateral involvement and optic disk edema occurred in 100% of patients, combined with vitritis, uveitis, or retinitis in four (80%). Four patients (80%) had MRI abnormalities along the optic nerve (one patient with optic nerve enhancement and three patients had optic nerve sheath enhancement or peribulbar fat enhancement). Three patients (60%) had optic neuropathy with other neurologic symptoms. Four patients (80%) had confirmed cancer (two were small-cell lung carcinoma, one was papillary thyroid carcinoma and another was thymoma and invasive pulmonary adenocarcinoma). All cancers were identified after the presentation of the optic neuropathy. The intervention included IVIG, IVMP, surgery and chemotherapy. The average BCVA at the last follow-up was 20/50 (range 20/20 to count fingers). Three patients had surgery during the initial hospitalization, and were stable during the follow-up. Among two patients who received IVMP, both had improvement after treatment, although one patient had worsening non-ocular neurologic symptoms during the steroid taper.

CONCLUSION

CRMP5-ON presented with optic disc edema, often bilateral involved and combined with vitreitis, retinitis, or uveitis. CRMP5-ON can present with MRI optic nerve or perineural optic nerve enhancement, especially in the optic nerve sheath. CRMP5-ON is closely related to paraneoplastic neurologic syndrome. Cancer screening and intervention are crucial to prognosis.

摘要

目的

collapsin反应介导蛋白5相关视神经病变(CRMP5-ON)是一种罕见的自身免疫性视神经病变。本研究旨在回顾一系列CRMP5-ON患者的神经眼科检查结果及预后情况,以进一步明确其临床表型、影像学线索及预后。

方法

这是一项回顾性病例系列研究,对2020年12月1日至2023年3月31日在北京同仁医院神经内科就诊的所有CRPM5血清学阳性的视神经病变患者进行单中心病历回顾。主要观察指标为CRMP5-ON的神经眼科表现、影像学特征及临床预后;并存的神经自身抗体、副肿瘤综合征关联以及免疫抑制治疗的影响。

结果

共纳入5例患者。4例(80%)为女性,发病平均年龄为59.4岁(范围53 - 69岁),平均随访15.3个月(范围1.4 - 28.7个月)。最低点时的平均最佳矫正视力(BCVA)为20/120(范围20/20至指数)。10只受累眼中有7只(70%)表现为中心视野弥漫性缺损。所有患者(100%)均有无痛性双侧受累及视盘水肿,4例(80%)合并玻璃体炎、葡萄膜炎或视网膜炎。4例患者(80%)的视神经MRI有异常(1例视神经强化,3例视神经鞘强化或球周脂肪强化)。3例患者(60%)的视神经病变伴有其他神经系统症状。4例患者(80%)确诊患有癌症(2例为小细胞肺癌,1例为甲状腺乳头状癌,另1例为胸腺瘤及浸润性肺腺癌)。所有癌症均在视神经病变出现后被发现。干预措施包括静脉注射免疫球蛋白(IVIG)、静脉注射甲泼尼龙(IVMP)、手术及化疗。末次随访时的平均BCVA为20/50(范围20/20至指数)。3例患者在初次住院期间接受了手术,随访期间病情稳定。在接受IVMP治疗的2例患者中,2例治疗后均有改善,尽管1例患者在激素减量过程中非眼部神经系统症状加重。

结论

CRMP5-ON表现为视盘水肿,常为双侧受累,并合并玻璃体炎、视网膜炎或葡萄膜炎。CRMP5-ON可出现MRI视神经或视神经周围强化,尤其是视神经鞘强化。CRMP5-ON与副肿瘤性神经综合征密切相关。癌症筛查及干预对预后至关重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/06bd/10337587/a8a7d7a27e37/fneur-14-1163615-g001.jpg

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