Predictors of 24-month onset of macular fibrosis in type 3 macular neovascularisation.

IF 3.7 2区 医学 Q1 OPHTHALMOLOGY British Journal of Ophthalmology Pub Date : 2024-08-22 DOI:10.1136/bjo-2023-324713
Paolo Forte, Vincenzo Fontana, Julia Muzio, Luca Di Cello, Paolo Corazza, Raffaella Rosa, Donatella Musetti, Aldo Vagge, Carlo Enrico Traverso, Massimo Nicolò
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Abstract

Aims: To explore prognostic multimarker models for progression to macular fibrosis (MF) over 24 months specific to type 3 macular neovascularisation (T3 MNV).

Methods: This retrospective, exploratory, single-centre, cohort study comprised 65 eyes of 43 Caucasian patients with treatment naive T3 MNV, all with a 24-month follow-up post anti-VEGF therapy using a strict pro-re-nata (PRN) regimen. Data on demographic features, clinical findings, frequency of intravitreal treatments and optical coherence tomography biomarkers were collected at baseline and after 12 and 24 months of follow-up. Logistic regression models (LRM) and receiver-operating curve (C-index) analyses were performed to evaluate the prognostic ability of the studied biomarkers in discriminating between MF affected and unaffected patients.

Results: At final follow-up, MF was present in 46.2% of eyes. Subretinal hyper-reflective material (SHRM) and subretinal pigment epithelium multilaminar hyper-reflectivity (multilaminae) emerged as significant predictors for MF, with adjusted odds ratios (OR) of 18.0 (95% CL 13.4 to 24.1) and 11.8 (95% CL 8.66 to 16.0), respectively. Additionally, the presence of multifocal lesions (OR 0.04, 95% CL 0.01 to 0.30) appeared to decrease the likelihood of MF. C-indexes for the selected LRMs ranged between 0.92 and 0.88, indicating a comparably high discriminant ability. Despite consistent treatment schedules between the two groups (MF: median intravitreal treatment (IVT) number=10.5, IQR=7; non-MF: median IVT=10, IQR=6), a decline in best-corrected visual acuity was noted in the group with MF onset over the 24-month follow-up (-13.0 ETDRS letters; 95% CL -22.1 to -3.9; p=0.006).

Conclusion: Our study identifies SHRM and multilaminae as relevant predictors of 24-month onset of MF in patients with T3 MNV. These findings enrich our understanding of the development of MF in T3 MNV and can guide improved risk prognostication. Future research should consider larger samples and prospective designs to validate these predictors.

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3 型黄斑新生血管在 24 个月后出现黄斑纤维化的预测因素。
目的:探讨3型黄斑新生血管(T3 MNV)在24个月内发展为黄斑纤维化(MF)的预后多标志物模型:这项回顾性、探索性、单中心队列研究包括43名白种人T3型黄斑新生血管患者的65只眼睛,这些患者均在接受抗血管内皮生长因子治疗后24个月内采用严格的PRN治疗方案。在基线以及随访 12 个月和 24 个月后,收集了有关人口统计学特征、临床表现、玻璃体内治疗频率和光学相干断层扫描生物标志物的数据。通过逻辑回归模型(LRM)和受体运行曲线(C-index)分析,评估所研究的生物标志物在区分MF患者和未受影响患者方面的预后能力:在最终随访中,46.2%的眼球存在MF。视网膜下高反射物质(SHRM)和视网膜下色素上皮多层高反射(multilaminae)是MF的重要预测指标,调整后的几率比(OR)分别为18.0(95% CL 13.4-24.1)和11.8(95% CL 8.66-16.0)。此外,存在多灶性病变(OR 0.04,95% CL 0.01 至 0.30)似乎会降低 MF 的可能性。所选 LRM 的 C 指数介于 0.92 和 0.88 之间,表明具有相当高的判别能力。尽管两组患者的治疗方案一致(MF:玻璃体内治疗(IVT)中位数=10.5,IQR=7;非MF:IVT中位数=10,IQR=6),但在24个月的随访中,发现MF发病组的最佳矫正视力有所下降(-13.0 ETDRS字母;95% CL -22.1至-3.9;P=0.006):我们的研究发现,SHRM和多层膜是T3 MNV患者24个月后发生MF的相关预测因素。这些发现丰富了我们对 T3 MNV 中 MF 发展的认识,并可指导改善风险预后。未来的研究应考虑采用更大的样本和前瞻性设计来验证这些预测因子。
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来源期刊
CiteScore
10.30
自引率
2.40%
发文量
213
审稿时长
3-6 weeks
期刊介绍: The British Journal of Ophthalmology (BJO) is an international peer-reviewed journal for ophthalmologists and visual science specialists. BJO publishes clinical investigations, clinical observations, and clinically relevant laboratory investigations related to ophthalmology. It also provides major reviews and also publishes manuscripts covering regional issues in a global context.
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