Geographic atrophy

地理萎缩
  • 文章类型: Journal Article
    地理萎缩(GA),年龄相关性黄斑变性(AMD)的萎缩性晚期,是发达国家视力丧失的主要原因之一。基于遗传,组织学和临床前研究,先天免疫系统在GA的发生和发展中的作用已得到充分证实。小胶质细胞,主要的常驻免疫细胞,被认为是先天免疫的关键参与者,也是AMD发展的贡献者。光学相干断层扫描(OCT)可以识别具有特定特征的小的高反射视网膜病灶(HRF),这些特征被称为激活的小胶质细胞聚集体,可能是局部神经视网膜炎症的体内成像特征。这项研究的目的是评估不同黄斑萎缩性表型患者眼中小HRF的存在和数量。双眼有GA的患者(双侧GA:B-GA组),一只眼睛的GA和另一只眼睛的黄斑新血管(MNV)的患者(单侧GA:U-GA组)和广泛的黄斑萎缩伴假性玻璃疣(EMAP)的患者,萎缩性AMD的一种罕见且激进的变种,进行了回顾性分析。HRF,定义为具有中等反射率(类似于神经纤维层)且没有阴影锥的小尺寸(≤30μm)的孤立点状元件,被手动识别和量化。HRF的量与最佳矫正视力(BCVA)相关,GA病变大小,在近红外反射率(NIR)下测量,和蓝色波长眼底自发荧光(FAF)图像,某些GA特征(多灶性与单灶性GA;存在与不存在中央凹保留)和中央视网膜厚度(CRT)。46例患者(B-GA组26例,研究了U-GA组16例,EMAP组4例)。与B-GA患者和U-GA患者相比,EMAP患者更年轻(63.5±6.8岁vs80.4±8.4岁B-GA,和vs83.3±6.1年U-GA;分别为p=0.0004和p=<0.0001)。平均BCVA,NIR和FAF图像的平均GA面积,中央凹保留和多焦点与单焦点GA分布以及平均CRT在各组之间没有显着差异。在所有组中,NIR与FAF相比,GA区域更宽,B-GA和U-GA组(B-GA为11.7±7.6mm2vs10.6±7.1mm2,p=0.0087;U-GA为7.8±9.2mm2vs7.7±9.4mm2,p=0.004)。与B-GA和EMAP相比,U-GA中的HRF数量显着增加(47.4±7.1vs31.6±7.3B-GA和28.0±4.9EMAP,两者的p<0.0001),而B-GA和EMAP之间的平均HRF数没有显着差异(p=0.1960)。HRF计数仅与CRT相关,B-GA为阳性,U-GA为阴性。小的HRF的增加,反映了视网膜小胶质细胞的激活,表征单侧GA的眼睛(和对侧眼的MNV),但不表征双侧GA或EMAP的眼睛。需要更好地研究激活的小胶质细胞在GA眼视网膜中的作用,主要考虑减少萎缩性黄斑改变的发展或进展的实际和新的治疗策略。
    Geographic atrophy (GA), the atrophic late stage of age-related macular degeneration (AMD), is one of the leading causes of vision loss in developed countries. Based on genetic, histological and preclinical studies, the role of the innate immune system in the development and progression of GA is well established. Microglia, the principal resident immune cells, are recognized as key players in innate immunity and contributors to AMD development. Optical coherence tomography (OCT) allows to identify small hyperreflective retinal foci (HRF) with specific features known as aggregates of activated microglial cells as possible in vivo imaging feature of local neuroretinal inflammation. The purpose of this study was to evaluate the presence and amount of small HRF in the eyes of patients with different macular atrophic phenotypes. Patients with GA in both eyes (bilateral GA: B-GA group), patients with GA in one eye and macular new vessels (MNV) in the fellow-eye (unilateral GA: U-GA group) and patients with extensive macular atrophy with pseudodrusen (EMAP), a rare and aggressive variant of atrophic AMD, were retrospectively analyzed. HRF, defined as isolated punctiform elements of small dimensions (≤30 μm) with intermediate reflectivity (similar to that of the nerve fiber layer) and without a shadow cone, were manually identified and quantified. The amount of HRF was correlated to best corrected visual acuity (BCVA), GA lesion size, measured both at near infrared reflectance (NIR), and blue wavelength fundus autofluorescence (FAF) images, to some GA features (multifocal versus unifocal GA; presence versus absence of foveal sparing) and to central retinal thickness (CRT). Forty-six patients (26 in the B-GA group, 16 in the U-GA group and 4 in the EMAP group) were studied. Patients with EMAP were younger compared to patients with B-GA and to patients with U-GA (63.5 ± 6.8 years vs 80.4 ± 8.4 years B-GA, and vs 83.3 ± 6.1 years U-GA; p = 0.0004 and p= <0.0001, respectively). Mean BCVA, mean GA area at NIR and at FAF images, foveal sparing and multifocal versus unifocal GA distribution and mean CRT were not significantly different among groups. GA area was wider on NIR versus FAF in all groups, significantly in B-GA and U-GA groups (11.7 ± 7.6 mm2 vs 10.6 ± 7.1 mm2, p = 0.0087 in B-GA; 7.8 ± 9.2 mm2 vs 7.7 ± 9.4 mm2, p = 0.004 in U-GA). The number of HRF was significantly higher in U-GA compared to B-GA and to EMAP (47.4 ± 7.1 vs 31.6 ± 7.3 B-GA and 28.0 ± 4.9 EMAP, p < 0.0001 for both), while mean HRF number did not significantly differ between B-GA and EMAP (p = 0.1960). HRF count correlated only to CRT, positively in B-GA and negatively in U-GA group. The increase of small HRF, which mirrors retinal microglial activation, characterizes eyes with unilateral GA (and MNV in the fellow eye) but not eyes with bilateral GA or EMAP. The role of activated microglia in the retina of GA eyes needs to be better investigated, mainly considering the actual and new therapeutic strategies with which to reduce either the development or progression of the atrophic macular changes.
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  • 文章类型: Journal Article
    随着前两种用于治疗继发于年龄相关性黄斑变性(AMD)的地理萎缩(GA)的物质的批准,在临床实践中需要对接受补体抑制剂治疗的患者进行标准化监测.光学相干断层扫描(OCT)提供了对视网膜色素上皮(RPE)和神经感觉层的高分辨率访问,例如椭球区(EZ),与常规眼底自发荧光(FAF)相比,这进一步增强了对GA疾病进展和治疗效果的了解。此外,基于人工智能的方法允许以客观和标准化的方式识别和量化OCT上的GA相关病理。这项研究的目的是在迄今为止最大的成功的3期补体抑制剂治疗临床试验数据中,与基于阅读中心的手动FAF测量相比,全面评估GA的自动OCT监测。RPE损失的自动OCT分析显示与常规FAF上的手动GA测量具有高度且一致的相关性。OCT上的EZ损失通常大于RPE损失的面积,支持EZ损失超过潜在的RPE损失作为GA进展的基本病理生理学的假设。自动OCT分析非常适合监测在临床实践和临床试验中治疗的GA患者的疾病进展。
    With the approval of the first two substances for the treatment of geographic atrophy (GA) secondary to age-related macular degeneration (AMD), a standardized monitoring of patients treated with complement inhibitors in clinical practice is needed. Optical coherence tomography (OCT) provides high-resolution access to the retinal pigment epithelium (RPE) and neurosensory layers, such as the ellipsoid zone (EZ), which further enhances the understanding of disease progression and therapeutic effects in GA compared to conventional fundus autofluorescence (FAF). In addition, artificial intelligence-based methodology allows the identification and quantification of GA-related pathology on OCT in an objective and standardized manner. The purpose of this study was to comprehensively evaluate automated OCT monitoring for GA compared to reading center-based manual FAF measurements in the largest successful phase 3 clinical trial data of complement inhibitor therapy to date. Automated OCT analysis of RPE loss showed a high and consistent correlation to manual GA measurements on conventional FAF. EZ loss on OCT was generally larger than areas of RPE loss, supporting the hypothesis that EZ loss exceeds underlying RPE loss as a fundamental pathophysiology in GA progression. Automated OCT analysis is well suited to monitor disease progression in GA patients treated in clinical practice and clinical trials.
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  • 文章类型: Editorial
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  • 文章类型: Journal Article
    背景:本研究的目的是比较使用眼底自发荧光(FAF)和光学相干断层扫描(OCT)注释的地理萎缩(GA)面积半自动测量与cRORA(完全视网膜色素上皮和外部视网膜萎缩)标准。
    方法:从24例干性年龄相关性黄斑变性(AMD)患者的36只眼获得的36对FAF和OCT扫描中,在单个时间点对FAF和OCT的GA结果进行半自动注释。GA地区,焦点,周边,循环性,最小和最大费雷特直径,比较FAF和OCT注释与中心的最小距离。
    结果:在OCT上测得的GA总面积为4.74±3.80mm2。相比之下,在FAF上测得的总GA为13.47±8.64mm2(p<0.0001),平均差为8.72±6.35mm2。多变量回归分析显示,OCT和FAF之间的面积差异与OCT测量的总基线病变周长和最大病变直径(调整后的r2:0.52;p<0.0001)和FAF测量的总基线病变面积(调整后的r2:0.83;p<0.0001)之间存在显著相关性。
    结论:我们报道,在FAF上测得的GA面积与在OCT上测得的GA面积显著不同。为了确定这些发现的临床相关性,需要进一步的研究。
    BACKGROUND: The purpose of this study was to compare geographic atrophy (GA) area semi-automatic measurement using fundus autofluorescence (FAF) versus optical coherence tomography (OCT) annotation with the cRORA (complete retinal pigment epithelium and outer retinal atrophy) criteria.
    METHODS: GA findings on FAF and OCT were semi-automatically annotated at a single time point in 36 pairs of FAF and OCT scans obtained from 36 eyes in 24 patients with dry age-related macular degeneration (AMD). The GA area, focality, perimeter, circularity, minimum and maximum Feret diameter, and minimum distance from the center were compared between FAF and OCT annotations.
    RESULTS: The total GA area measured on OCT was 4.74 ± 3.80 mm2. In contrast, the total GA measured on FAF was 13.47 ± 8.64 mm2 (p < 0.0001), with a mean difference of 8.72 ± 6.35 mm2. Multivariate regression analysis revealed a significant correlation between the difference in area between OCT and FAF and the total baseline lesion perimeter and maximal lesion diameter measured on OCT (adjusted r2: 0.52; p < 0.0001) and the total baseline lesion area measured on FAF (adjusted r2: 0.83; p < 0.0001).
    CONCLUSIONS: We report that the GA area measured on FAF differs significantly from the GA area measured on OCT. Further research is warranted in order to determine the clinical relevance of these findings.
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  • 文章类型: Journal Article
    地理萎缩(GA)影响患者和护理人员,然而,人们对他们各自的负担却知之甚少。MOSAIC研究旨在确定临床,情感,以及GA患者和护理人员的经济负担。
    共有来自美国(美国)的28名GA患者和17名护理人员,联合王国,和澳大利亚参加了个性化定性访谈,随后对美国102名患者和102名护理人员进行了横断面定量调查.对采访记录进行了分析,以开发概念模型,然后用于指导定量调查的设计。适当时在项目级别和分数级别描述数据(国家眼科研究所视觉功能问卷[NEIVFQ]-39和Zarit负担访谈[ZBI])。对于患者/护理人员二重样本,通过相关系数和散点图研究了NEIVFQ-39评分和ZBI评分之间的关联.
    GA对患者视力相关生活质量产生了重大影响,日常生活活动,和日常生活的工具性活动。患者和护理人员确定的观点和关键问题之间存在相当大的重叠。83%的护理人员报告说,由于患者活动受限,不得不开车送患者去预约。例如,41%的人报告说,他们成为照顾者后的就业状况发生了变化,其中50%的人由于照顾而无法工作。患者和护理人员的负担在NEIVFQ-39子量表与综合评分和ZBI评分之间具有-0.63至-0.21的相关性。
    这项研究证实了对GA患者和护理人员的支持不足。这两个群体都需要扩大金融渠道,社会,精神卫生资源。
    这个总结是关于什么的?有地理萎缩的人,也叫GA,会失去视力,很难开车,阅读,和识别面孔。这会使他们的生活质量恶化。通常,有GA的人需要有人照顾他们。MOSAIC研究是为了找出GA如何影响健康,幸福,以及GA患者及其护理人员的财务状况。结果如何?采访了美国的一百零二名GA和102名护理人员。GA患者的平均年龄为68岁,护理人员的平均年龄为46岁。调查结果表明,大多数患有GA的人并不是因为视力不好而开车,而是依靠他们的照顾者开车去看医生和其他地方。由于视力恶化,他们也在家里读书和做事。有GA的人和护理人员都说他们感到压力很大。他们俩都担心花钱在需要使与GA生活更轻松的事情上。他们还对自己的财务状况感到压力,因为他们无法工作。患有GA的人最担心失去独立性,而护理人员则最担心GA所爱的人的未来。这项研究表明,GA对人们的健康和生活质量有严重影响,同时对他们的照顾者也有重大影响。
    UNASSIGNED: Geographic atrophy (GA) impacts both patients and caregivers, yet little is understood about their respective burdens. The MOSAIC study aimed to identify the clinical, emotional, and financial burden among patients with GA and caregivers.
    UNASSIGNED: A total of 28 patients with GA and 17 caregivers from the United States (US), the United Kingdom, and Australia participated in individualized qualitative interviews followed by a cross-sectional quantitative survey of 102 patients and 102 caregivers in the US. Interview transcripts were analyzed to develop conceptual models, which were then used to guide the design of quantitative surveys. Data were described at the item level and score level when appropriate (National Eye Institute Visual Function Questionnaire [NEI VFQ]-39 and Zarit Burden Interview [ZBI]). For the patient/caregiver dyad sample, the association between the NEI VFQ-39 scores and ZBI score was explored through correlation coefficients and scatterplots.
    UNASSIGNED: GA had a substantial impact on patients\' vision-related quality of life, activities of daily living, and instrumental activities of daily living. There was considerable overlap between perspectives and key concerns identified by patients and caregivers. Eighty-three percent of caregivers reported having to drive patients to appointments due to limited patient mobility, for example, and 41% reported a change in their employment status after becoming a caregiver, with 50% of them unable to work due to caregiving. The burden of patients and caregivers had a correlation ranging from -0.63 to -0.21 between NEI VFQ-39 subscale and composite scores and ZBI score.
    UNASSIGNED: This study confirms the paucity of support for both patients with GA and caregivers. Both groups require expanded access to financial, social, and mental health resources.
    What is this summary about? People with geographic atrophy, also called GA, can lose their eyesight and have a hard time driving, reading, and recognizing faces. This can worsen their quality of life. Often, people with GA need someone to care for them. The MOSAIC study was done to find out how GA affects health, happiness, and finances of people with GA and their caregivers. What were the results? One hundred and two people with GA and 102 caregivers in the United States were interviewed. The average age of people with GA was 68 years and of caregivers was 46 years. The findings showed that most people with GA did not drive because of their poor eyesight and instead counted on their caregivers to drive them to doctor appointments and other places. They also had a reading and doing things around their home because of their worsened eyesight. Both people with GA and caregivers said they felt stressed. They both worried about spending money on things they need to make living with GA easier. They also felt stressed about their finances because they could not work as much. People with GA worried most about losing their independence and caregivers worried most about the future of their loved one with GA. What do the results mean? This study showed that GA has a serious effect on people’s health and quality of life while also having a major impact on their caregivers.
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  • 文章类型: Editorial
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  • 文章类型: Journal Article
    目的:比较某些退行性和黄斑遗传性视网膜疾病(IRD)的黄斑视网膜色素上皮(RPE)萎缩进展率。
    方法:系统评价和荟萃分析。
    方法:该协议已在PROSPERO数据库中注册。Medline,Embase,WebofScience,Cochrane中央控制试验登记册,和GoogleScholar在2023年9月15日之前搜索了报道患有地理萎缩(GA)的未治疗眼睛的RPE萎缩增长率的文章,Stargardt病(STGD1),最好的疾病,弹性假性黄瘤(PXE),中央乳晕脉络膜营养不良(CACD),或模式营养不良,以前或现在没有黄斑新生血管形成,最短随访时间为12个月。Meta分析确定每种疾病的平均RPE萎缩增长率,成像模式(眼底自发荧光[FAF],光学相干断层扫描[OCT],或彩色眼底照相[CFP])和公制(mm2/年或mm/年)。纽卡斯尔-渥太华量表和Cochrane偏差风险工具评估了偏差的风险,和漏斗图用于评估小型研究效果。
    结果:来自4354个出版物,85项纳入荟萃分析:69项关于GA的研究(7815只眼),STGD1上有15只(1367只眼睛),两个上都有一只。两项关于PXE的研究仅有资格进行审查。没有其他疾病的研究符合我们的资格标准。使用FAF的GA的总平均RPE萎缩增长率为1.65mm2/年(95%置信区间[CI],1.49-1.81)和0.35毫米/年(95%CI,0.28-0.41);使用OCT,它是1.46mm2/年(95%CI,1.28-1.64)和0.34mm/年(95%CI,0.28-0.40);CFP为1.76mm2/年(95%CI,1.56-1.97)和0.30mm/年(95%CI,0.28-0.31)。对于STGD1,使用FAF为1.0mm2/年(95%CI,0.77-1.23)和0.20mm/年(95%CI,0.17-0.23);在OCT上,为0.80mm2/年(95%CI,0.72-0.88)。没有关于STGD1的研究报告了其他成像方式或指标的增长率。GA的生长速率快于STGD1(p<0.05)。较大的基线萎缩面积通常与较快的生长速率相关。
    结论:GA的RPE萎缩生长速率比STGD1快,但研究和成像模式之间差异很大。其他黄斑IRD的信息有限,这表明需要进一步的研究。
    OBJECTIVE: To compare the macular retinal pigment epithelium (RPE) atrophy progression rate of selected degenerative and macular inherited retinal diseases (IRD).
    METHODS: Systematic review and meta-analysis.
    METHODS: The protocol was registered on the PROSPERO database. Medline, Embase, Web of Science, Cochrane Central Register of Controlled Trials, and Google Scholar were searched up to 15/Sep/2023 for articles reporting the RPE atrophy growth rate in treatment-naïve eyes with geographic atrophy (GA), Stargardt disease (STGD1), Best disease, pseudoxanthoma elasticum (PXE), central areolar choroidal dystrophy (CACD), or pattern dystrophies with no previous or current macular neovascularization and a minimum follow-up time of 12 months. Meta-analyses determined mean RPE atrophy growth rates per disease, imaging modality (fundus autofluorescence [FAF], optical coherence tomography [OCT], or color fundus photography [CFP]) and metric (mm2/year or mm/year). The Newcastle-Ottawa scale and the Cochrane Risk-of-Bias tool assessed the risk of bias, and funnel plots were used to evaluate small-study effects.
    RESULTS: From 4354 publications, 85 were included for meta-analysis: 69 studies (7815 eyes) on GA, 15 (1367 eyes) on STGD1, and one on both. Two studies on PXE were only eligible for review. No studies for other diseases met our eligibility criteria. The overall mean RPE atrophy growth rate for GA using FAF was 1.65 mm2/year (95% confidence interval [CI], 1.49-1.81) and 0.35 mm/year (95% CI, 0.28-0.41); using OCT, it was 1.46 mm2/year (95% CI, 1.28-1.64) and 0.34 mm/year (95% CI, 0.28-0.40); and on CFP it was 1.76 mm2/year (95% CI, 1.56-1.97) and 0.30 mm/year (95% CI, 0.28-0.31). For STGD1, using FAF it was 1.0 mm2/year (95% CI, 0.77-1.23) and 0.20 mm/year (95% CI, 0.17-0.23); on OCT, it was 0.80 mm2/year (95% CI, 0.72-0.88). No studies on STGD1 reported the growth rate with other imaging modalities or metrics. Growth rates in GA were faster than in STGD1 (p<0.05). A larger baseline area of atrophy was generally associated with faster growth rates.
    CONCLUSIONS: The RPE atrophy growth rate in GA is faster than in STGD1 but with great variation between studies and imaging modalities. Limited information was available for other macular IRD, suggesting further research is needed.
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  • 文章类型: Journal Article
    背景:晚期年龄相关性黄斑变性(AMD)是视力丧失的主要原因。因此,人们对可以预测或预防晚期AMD发病的前兆病变感兴趣.一个这样的病变是视网膜色素上皮(RPE)和布鲁赫膜(BM)的浅分离,用各种术语来描述,包括双层标志(DLS)。
    方法:在本文中,我们的目的是检查和澄清不同的术语,这些术语指的是RPE和BM的浅分离。我们还回顾了与DLS相关的结果的当前证据:首先,DLS是否可以预测渗出性新生血管性AMD;其次,DLS是否具有针对地理萎缩的潜在保护特性。
    结果:用于描述RPE和BM的浅分离的术语范围反映了DLS可以呈现不同的特征。虽然血管化DLS似乎可以防止萎缩,但可以进展为渗出,非血管化DLS与萎缩风险增加相关.光学相干断层扫描(OCT)血管造影(OCTA)是识别和区分各种形式的DLS的主要方法。如果OCTA不可用或实际上不可能,DLS的简化分类为厚或薄,使用OCT,使血管化的可能性接近。正在研究通过将深度学习算法应用于OCT扫描来自动化DLS检测。
    结论:术语DLS仍然适用于描述RPE和BM的浅分离。该特征的检测和分类提供关于进展为晚期AMD的风险的有价值的信息。然而,DLS的出现及其在预测AMD进展中的价值在不同患者之间可能存在差异.随着进一步的研究,可以确认个性化的风险,以告知适当的治疗。
    年龄相关性黄斑变性(AMD)是一种可能在老年人中发展的眼病,通常是60岁以上的人。在疾病早期,人们通常没有任何症状,但是随着疾病的发展,可能会出现视力丧失。AMD的高级形式被称为新生血管性AMD(也称为“湿性”AMD)和高级干性AMD(称为地理萎缩;GA)。重要的是在眼部扫描中识别特征和体征,以帮助预测AMD患者是否会发展为晚期疾病,因为这将帮助医生计划最合适的治疗方法。眼睛扫描上的一个这样的特征是双层符号(DLS)。在这篇文章中,我们总结了用于DLS的不同名称,并评估DLS是否会增加早期AMD患者发生湿性AMD或GA的可能性。我们得出的结论是,DLS看起来因人而异,这导致DLS被称为各种名称。患有早期AMD和含有DLS的血管的人可能更有可能发展为湿性AMD;而患有早期AMD和没有血管的DLS的人可能更有可能发展为GA。使用光学相干断层扫描血管造影成像对眼睛拍照是识别DLS和确认其是否包含血管的主要方法。
    BACKGROUND: Advanced age-related macular degeneration (AMD) is a major cause of vision loss. Therefore, there is interest in precursor lesions that may predict or prevent the onset of advanced AMD. One such lesion is a shallow separation of the retinal pigment epithelium (RPE) and Bruch\'s membrane (BM), which is described by various terms, including double-layer sign (DLS).
    METHODS: In this article, we aim to examine and clarify the different terms referring to shallow separation of the RPE and BM. We also review current evidence on the outcomes associated with DLS: firstly, whether DLS is predictive of exudative neovascular AMD; and secondly, whether DLS has potential protective properties against geographic atrophy.
    RESULTS: The range of terms used to describe a shallow separation of the RPE and BM reflects that DLS can present with different characteristics. While vascularised DLS appears to protect against atrophy but can progress to exudation, non-vascularised DLS is associated with an increased risk of atrophy. Optical coherence tomography (OCT) angiography (OCTA) is the principal method for identifying and differentiating various forms of DLS. If OCTA is unavailable or not practically possible, simplified classification of DLS as thick or thin, using OCT, enables the likelihood of vascularisation to be approximated. Research is ongoing to automate DLS detection by applying deep-learning algorithms to OCT scans.
    CONCLUSIONS: The term DLS remains applicable for describing shallow separation of the RPE and BM. Detection and classification of this feature provides valuable information regarding the risk of progression to advanced AMD. However, the appearance of DLS and its value in predicting AMD progression can vary between patients. With further research, individualised risks can be confirmed to inform appropriate treatment.
    Age-related macular degeneration (AMD) is an eye disease that may develop in older people, usually those aged over 60 years. Early in the disease, people often do not show any symptoms, but as the disease progresses, vision loss may occur. The advanced forms of AMD are called neovascular AMD (also called “wet” AMD) and advanced dry AMD (called geographic atrophy; GA). It is important to identify features and signs on eye scans that can help to predict if someone with AMD will develop an advanced form of the disease because this will help doctors plan the most appropriate treatment. One such feature on eye scans is the double-layer sign (DLS). In this article, we summarise the different names used for DLS, and assess if having a DLS increases the likelihood of someone with early AMD developing wet AMD or GA. We conclude that how DLS looks varies between people, which leads to DLS being called by various names. Someone with early AMD and a DLS containing blood vessels may be more likely to develop wet AMD; whereas someone with early AMD and a DLS without blood vessels may be more likely to develop GA. Taking photos of the eye using optical coherence tomography angiography imaging is the main method of identifying DLS and confirming whether it contains blood vessels.
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  • 文章类型: Journal Article
    背景:年龄相关性黄斑变性(AMD)是视力丧失的主要原因。光生物调节(PBM)提供了一个有争议的方法来管理干性AMD,旨在通过线粒体活性调节停止或逆转进展。然而,PBM作为治疗干性AMD的潜在方法的有效性和临床意义仍存在争议.
    方法:我们系统地搜索了PubMed,Embase,和Cochrane数据库的随机对照试验(RCTs),比较了PBM和假手术在干性AMD患者中的应用。我们进行了试验序贯分析(TSA)和最小临床重要差异(MCID)计算,以使用具有95%置信区间(CI)的随机效应模型评估统计学和临床意义。
    结果:我们纳入了三个RCT,包括247只眼。汇总分析显示,与假对照相比,PBM显着改善了BCVA(MD1.76字母;95%CI:0.04至3.48)和玻璃疣体积(MD-0.12mmpa;95%CI:-0.22至-0.02)。然而,TSA表明,目前的样本量不足以得出可靠的结论.在GA面积中没有观察到显著差异。MCID分析表明,统计学上的显着结果并未转化为临床上的显着益处。在质量评估中,所有研究均被认为存在高偏倚风险.
    结论:本荟萃分析指出了目前关于PBM治疗干性AMD的证据基础的局限性,围绕小样本量的问题。统计学上显著的改善不能转化为临床益处。该研究强调需要更大的随机对照试验来验证PBM对干性AMD的治疗潜力。
    BACKGROUND: Age-related macular degeneration (AMD) is a leading cause of vision loss. Photobiomodulation (PBM) offers a controversial approach for managing dry AMD, aiming to halt or reverse progression through mitochondrial activity modulation. However, the efficacy and clinical relevance of PBM as a potential approach for managing dry AMD remain debated.
    METHODS: We systematically searched PubMed, Embase, and Cochrane databases for randomized controlled trials (RCTs) comparing PBM versus a sham in patients with dry AMD. We performed trial sequential analysis (TSA) and minimal clinically important difference (MCID) calculations to assess statistical and clinical significance applying a random-effects model with 95% confidence intervals (CI).
    RESULTS: We included three RCTs comprising 247 eyes. The pooled analysis showed that PBM significant improved BCVA (MD 1.76 letters; 95% CI: 0.04 to 3.48) and drusen volume (MD -0.12 mm³; 95% CI: -0.22 to -0.02) as compared with a sham control. However, the TSA indicated that the current sample sizes were insufficient for reliable conclusions. No significant differences were observed in GA area. The MCID analysis suggested that the statistically significant results did not translate into clinically significant benefits. In the quality assessment, all studies were deemed to have a high risk of bias.
    CONCLUSIONS: This meta-analysis points limitations in the current evidence base for PBM in dry AMD treatment, with issues around small sample sizes. Statistically significant improvements do not translate into clinical benefits. The research underscores need for larger RCTs to validate PBM\'s therapeutic potential for dry AMD.
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  • 文章类型: Journal Article
    关键信息:已知:地理萎缩可能与MNV或其他血管改变有关。在没有新生血管形成的情况下,GA中也可能存在视网膜内液体。新功能:增益是一种新颖的临床实体,其特征是GA和视网膜内新生血管网络。增益可以是渗出性或非渗出性的。
    KEY MESSAGES     : WHAT IS KNOWN : Geographic atrophy could be associated with MNV or other vascular alterations. Intraretinal fluid could be present in GA also without neovascularization. WHAT IS NEW : GAIN is a novel clinical entity characterized by GA and an intraretinal neovascular network. GAIN could be exudative or non-exudative.
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