De Angelis Floriana, Cameron James R, Eshaghi Arman, Parker Richard, Connick Peter, Stutters Jonathan, Plantone Domenico, Doshi Anisha, John Nevin, Williams Thomas, Calvi Alberto, MacManus David, Barkhof Frederik, Chandran Siddharthan, Weir Christopher J, Toosy Ahmed, Chataway Jeremy
Queen Square Multiple Sclerosis Centre, Department of Neuroinflammation, UCL Queen Square Institute of Neurology, Faculty of Brain Sciences, University College London, London, UK
University College London Hospitals, Biomedical Research Centre, National Institute for Health and Care Research, London, UK.
J Neurol Neurosurg Psychiatry. 2025 Jun 12;96(7):647-654. doi: 10.1136/jnnp-2024-334801.
Optical coherence tomography (OCT) inner retinal metrics reflect neurodegeneration in multiple sclerosis (MS). We explored OCT measures as biomarkers of disease severity in secondary progressive MS (SPMS).
We investigated people with SPMS from the Multiple Sclerosis-Secondary Progressive Multi-Arm Randomisation Trial OCT substudy, analysing brain MRIs, clinical assessments and OCT at baseline and 96 weeks. We measured peripapillary retinal nerve fibre layer (pRNFL) and macular ganglion cell-inner plexiform layer (GCIPL) thicknesses. Statistical analysis included correlations, multivariable linear regressions and mixed-effects models.
Of the 212 participants recruited at baseline, 192 attended at 96 weeks follow-up. Baseline pRNFL and GCIPL thickness correlated with Symbol Digit Modalities Test (SDMT) (respectively, r=0.33 (95% CI 0.20 to 0.47); r=0.39 (0.26 to 0.51)) and deep grey matter volume (respectively, r=0.21 (0.07 to 0.35); r=0.28 (0.14 to 0.41)).pRNFL was associated with Expanded Disability Status Scale (EDSS) score change (normalised beta (B)=-0.12 (-0.23 to -0.01)). Baseline pRNFL and GCIPL were associated with Timed 25-Foot Walk change (T25FW) (respectively, B=-0.14 (-0.25 to -0.03); B=-0.20 (-0.31 to -0.10)) and 96-week percentage brain volume change (respectively, B=0.14 (0.03 to 0.25); B=0.23 (0.12 to 0.34)). There were significant annualised thinning rates: pRNFL (-0.83 µm/year) and GCIPL (-0.37 µm/year).
In our cohort of people with SPMS and long disease duration, OCT measures correlated with SDMT and deep grey matter volume at baseline; EDSS, T25FW and whole brain volume change at follow-up.
光学相干断层扫描(OCT)的视网膜内层指标可反映多发性硬化症(MS)中的神经退行性变。我们探讨了OCT测量作为继发进展型MS(SPMS)疾病严重程度生物标志物的作用。
我们对来自多发性硬化症继发进展型多臂随机试验OCT子研究的SPMS患者进行了调查,分析了基线期和96周时的脑部MRI、临床评估和OCT。我们测量了视乳头周围视网膜神经纤维层(pRNFL)和黄斑神经节细胞-内丛状层(GCIPL)的厚度。统计分析包括相关性分析、多变量线性回归和混合效应模型。
在基线期招募的212名参与者中,192人参加了96周的随访。基线期的pRNFL和GCIPL厚度与符号数字模式测验(SDMT)相关(分别为r = 0.33(95%CI 0.20至0.47);r = 0.39(0.26至0.51))以及深部灰质体积(分别为r = 0.21(0.07至0.35);r = 0.28(0.14至0.41))。pRNFL与扩展残疾状态量表(EDSS)评分变化相关(标准化β(B)=-0.12(-0.23至-0.01))。基线期的pRNFL和GCIPL与25英尺步行时间变化(T25FW)相关(分别为B = -0.14(-0.25至-0.03);B = -0.20(-0.31至-0.10))以及96周时脑体积变化百分比(分别为B = 0.14(0.03至0.25);B = 0.23(0.12至0.34))。存在显著的年化变薄率:pRNFL(-0.83 µm/年)和GCIPL(-0.37 µm/年)。
在我们这个病程较长的SPMS患者队列中,OCT测量在基线期与SDMT和深部灰质体积相关;在随访期与EDSS、T25FW和全脑体积变化相关。
