Subnormal visual acuity after compliant amblyopia therapy: residual/refractory amblyopia or co-existing pathology? - a retrospective analysis.

IF 0.8 Q4 OPHTHALMOLOGY Strabismus Pub Date : 2024-03-01 Epub Date: 2024-02-04 DOI:10.1080/09273972.2023.2294997
Virender Sachdeva, Bidisha Bhattacharya, Snehal Ganatra, Ramesh Kekunnaya
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Abstract

Purpose: To assess the prevalence of alternate etiology/co-existing pathology among patients with amblyopia, and to characterize factors contributing to over-diagnosis of amblyopia. Methods: We retrospectively reviewed records of children (from 1 January 2016 to 31 December 2019) who were initially diagnosed as "amblyopia" but later an alternate diagnosis for subnormal vision was established. Patients who had a best corrected visual acuity (BCVA) of ≤20/32 (0.2 logMAR) after compliant amblyopia therapy were divided into 2 groups: those with refractory amblyopia (BCVA improvement from baseline <1 logMAR line) and residual amblyopia (BCVA improvement from baseline >1 logMAR line). Data was collected for presence/absence of amblyogenic risk factors, history, ocular examination, and investigations leading to the final alternate diagnosis. We analyzed the factors that contributed to the initial over-diagnosis of amblyopia using the diagnostic error evaluation and research (DEER) taxonomy tool. Results: During the study period, 508 children with an initial diagnosis of amblyopia met the study criteria. Among these 508 children, 466 were diagnosed to have amblyopia alone, while 26 children (5.1%, median age: 7 years, 17 boys: 9 girls) were revised to have an alternate diagnosis/co-existing pathology. These 26 patients comprised of 2 groups: children referred to us as amblyopia but rediagnosed to have an alternate diagnosis; and a second subset, initially diagnosed by us to have amblyopia, but later found to have alternate diagnosis/co-existing pathology. Subclinical optic neuritis (50%, 13 children), and occult macular dystrophy (OMD) (38.4%, 10 children) were the most frequent alternative diagnoses. Children with ametropic amblyopia (8/26, 30.7%) were most frequently misdiagnosed. Risk factors that led to an initial diagnosis of amblyopia were: high refractive error and heterotropia in 7 patients each (26.9%), anisometropia in 12 (46.1%), and prior pediatric cataract surgery in 4(15.3%). No improvement in BCVA in 21/26 (80.7%) children led to suspicion of co-existing etiology. Other clues were optic disc pallor (11), subnormal color vision (7), history of parental consanguinity in 7, and preceding febrile illness/rhinitis in 1 child. The DEER taxonomy tool suggested that the most common reasons for diagnostic errors were over-emphasis on amblyopia. Conclusion: Our study suggests that 5% of children diagnosed with amblyopia might have co-existing/alternate etiology. Most common co-existing etiologies were subclinical optic neuropathy, and OMD. No improvement in BCVA, subtle history and examination findings prompted further workup. Not considering co-existing etiologies was the most common reason for an initial overdiagnosis of amblyopia.

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顺应性弱视治疗后视力异常:残留/难治性弱视还是并存病理?- 回顾性分析。
目的:评估替代病因/并存病理在弱视患者中的流行率,并确定导致弱视过度诊断的因素。研究方法我们回顾性地查看了最初被诊断为 "弱视",但后来被确定为视力不正常的替代诊断的儿童记录(2016 年 1 月 1 日至 2019 年 12 月 31 日)。将接受弱视治疗后最佳矫正视力(BCVA)≤20/32(0.2 logMAR)的患者分为两组:难治性弱视组(BCVA比基线提高1 logMAR线)。收集的数据包括是否存在致弱视风险因素、病史、眼部检查和导致最终替代诊断的检查。我们使用诊断错误评估与研究(DEER)分类工具分析了导致最初过度诊断弱视的因素。研究结果在研究期间,有 508 名初次诊断为弱视的儿童符合研究标准。在这508名儿童中,466名儿童被诊断为单纯性弱视,26名儿童(5.1%,年龄中位数:7岁,17名男孩:9名女孩)被修正为有其他诊断/并存病症。这26名患者包括两组:一组是被转诊为弱视,但重新诊断为其他诊断的儿童;另一组是最初被诊断为弱视,但后来发现有其他诊断/并存病理的儿童。亚临床视神经炎(50%,13名儿童)和隐性黄斑营养不良(OMD)(38.4%,10名儿童)是最常见的替代诊断。各向异性弱视儿童(8/26,30.7%)最常被误诊。导致最初诊断为弱视的风险因素有:高度屈光不正和异性斜视各占 7 例(26.9%),异性斜视占 12 例(46.1%),曾接受过小儿白内障手术占 4 例(15.3%)。21/26(80.7%)名患儿的视力均无改善,这让人怀疑是否存在并存病因。其他线索还包括视盘苍白(11 例)、色觉异常(7 例)、7 例父母有近亲结婚史、1 例患儿曾患发热性疾病/鼻炎。DEER分类工具表明,诊断错误最常见的原因是过度强调弱视。结论我们的研究表明,5%被诊断为弱视的儿童可能有并存/替代病因。最常见的并存病因是亚临床视神经病变和OMD。BCVA没有改善、病史和检查结果不明确,都需要进一步检查。未考虑并存病因是最初过度诊断弱视的最常见原因。
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来源期刊
Strabismus
Strabismus OPHTHALMOLOGY-
CiteScore
1.60
自引率
11.10%
发文量
30
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