A Randomized, Controlled, Partially Masked, Phase 3b Study to Assess the Injection Burden, Efficacy, Safety, and Long-Term Preservation of Visual Acuity of Surabgene Lomparvovec (ABBV-RGX-314) in a Real-World Context in Subjects With Neovascular Age-Related Macular Degeneration (nAMD)

Neovascular age-related macular degeneration (nAMD), also known as "wet" AMD, is the abnormal growth of new blood vessels in the light-sensitive tissue at the back of the eye called the retina. The purpose of this study is to assess how safe and effective Surabgene Lomparvovec is in treating participants with Neovascular age-related macular degeneration (nAMD).
Surabgene Lomparvovec (ABBV-RGX-314) is an investigational gene therapy being developed for the treatment of neovascular age-related macular degeneration (nAMD). Participants will be placed into 1 of 3 groups, called treatment arms. Each group receives different treatment. Adult participants aged 50 and older years with a diagnosis of previously treated nAMD will be enrolled. Around 561 participants will be enrolled in the study at approximately 150 sites worldwide.
Participants in groups 1 and 2 will receive a single subretinal dose of ABBV-RGX-314. Participants in group 3 will receive Ranibizumab as needed throughout the study. Ranibizumab will be given as an intravitreal injection (injection into the jelly-like tissue that fills the eyeball injection), and ABBV-RGX-314 will be given as a subretinal (between the retina and the back of the eye) injection. The Assessment Period begins after randomization (1:1:1) to one of the ABBV-RGX-314 treatment groups or control at Week -2 and lasts up to 5 years.
There may be higher treatment burden for participants in this trial compared to their standard of care. Participants will attend regular monthly visits during the study at a hospital or clinic. The effect of the treatment will be checked by medical assessments, blood tests, checking for side effects and completing questionnaires.

开始日期2025-11-05

申办/合作机构

AbbVie, Inc.

NCT06942520

/ Recruiting临床2期

A Randomized, Open Label, Controlled, Phase 2 Clinical Study to Evaluate the Efficacy and Safety of RGX-314 AAV Gene Therapy Administered Via Subretinal Delivery in Participants With Center Involved Diabetic Macular Edema

Phase 2 open label, randomized, active controlled, dose-ranging trial in adults with Center Involved - Diabetic Macular Edema (CI - DME)

开始日期2025-03-18

申办/合作机构

Sierra Eye Associates

[+1]

NCT05407636

/ Recruiting临床3期

A Randomized, Partially Masked, Controlled, Phase 3 Clinical Study to Evaluate the Efficacy and Safety of RGX-314 Gene Therapy in Participants With nAMD

ABBV-RGX-314 (also known as RGX-314) is being developed as a novel one-time gene therapy for the treatment of neovascular (wet) age-related macular degeneration (wet AMD). Wet AMD is characterized by loss of vision due to new, leaky blood vessel formation in the retina. Wet AMD is a significant cause of vision loss in the United States, Europe and Japan, with up to 2 million people living with wet AMD in these geographies alone. Current anti-vascular endothelial growth factor (VEGF) therapies have significantly changed the landscape for treatment of wet AMD, becoming the standard of care due to their ability to prevent progression of vision loss in the majority of patients. These therapies, however, require life-long intraocular injections, typically repeated every four to 12 weeks in frequency, to maintain efficacy. Due to the burden of treatment, patients often experience a decline in vision with reduced frequency of treatment over time. ABBV-RGX-314 is being developed as a potential one-time treatment for wet AMD.

开始日期2022-01-13

申办/合作机构

AbbVie, Inc.

[+1]

100 项与 Surabgene Lomparvovec 相关的临床结果

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100 项与 Surabgene Lomparvovec 相关的转化医学

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100 项与 Surabgene Lomparvovec 相关的专利（医药）

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项与 Surabgene Lomparvovec 相关的文献（医药）

2025-10-03·Translational Vision Science & Technology

Computational Fluid Dynamics Modeling of Intravitreal Ranibizumab Bolus Versus Subretinal ABBV-RGX-314 Transgene Product in Human Eyes

Article

作者: Kazemi, Mohammad ; Tamhane, Mitalee ; Shen, Jie ; Park, Jenny

Purpose:

ABBV-RGX-314 is being developed for neovascular age-related macular degeneration (nAMD). Computational fluid dynamics (CFDs) modeling in the eye enables simulation of drug distribution incorporating geometry and substructures of the eye across species. Given the similarity between ranibizumab and ABBV-RGX-314 transgene product (TP), ranibizumab intraocular pharmacokinetic (PK) data from literature were used to simulate intraocular drug distribution of ABBV-RGX-314 TP. This investigation aims to use CFD modeling to estimate retinal TP level based on aqueous humor (AH) TP level following subretinal (SR) injection of ABBV-RGX-314 in patients with nAMD.

Methods:

Ocular distribution of ranibizumab following a single intravitreal (IVT) injection was modeled in both monkey and human eyes independently. Following model validation, ABBV-RGX-314 TP distribution in human eyes was simulated following retinal transduction of ABBV-RGX-314.

Results:

Iterative simulations were performed to achieve similar AH ABBV-RGX-314 TP levels in patients with nAMD from phase I/IIa Study RGX-314-001. The CFD simulation estimated corresponding retinal TP concentrations of 1.86 to 5.50 µg/g at steady-state, which was assumed to be reached by 28 days and falls within the range of the estimated retinal ranibizumab trough retinal ranibizumab concentration (Ctrough; 0.718-5.37 µg/g) following monthly and every other month (EOM) dosing of 0.5 mg ranibizumab in patients with nAMD.

Conclusions:

The current study results predict that the 2 pivotal trial ABBV-RGX-314 doses (6.4E10 and 1.3E11 genome copies/eye) are expected to achieve and maintain sufficient retinal ABBV-RGX-314 TP levels for the treatment of nAMD.

Translational Relevance:

CFD modeling effectively bridges limited human ocular PK data with rich preclinical data, supporting model-informed drug development (MIDD) for clinical dose selection.

2025-05-24·EXPERT OPINION ON PHARMACOTHERAPY

Beyond the injection: delivery systems reshaping retinal disease management

Review

作者: Harris, Alon ; Ciulla, Thomas A. ; Akotoye, Christian ; Rowe, Lucas W.

INTRODUCTION:

Intravitreal injections remain the standard for treating common retinal diseases including age-related macular degeneration (AMD), diabetic macular edema (DME) and diabetic retinopathy. However, frequent administration creates significant treatment burden due to limited drug half-life and the chronic nature of these conditions.

AREAS COVERED:

This review summarizes emerging drug delivery techniques and therapies for retinal disease that have achieved FDA approval within the past five years or have advanced to Phase 3 development, including intravitreal sustained-release platforms and alternative delivery routes (suprachoroidal, subretinal, topical, and subcutaneous). Specific innovations discussed include the ranibizumab port delivery system, EYP-1901 (Duravyu, vorolanib implant), KSI-301 (tarcocimab tedromer), KSI-501, OTX-TKI (Axpaxli, axitinib implant), 4D-150, revakinagene taroretcel-lwey (Encelto, NT-501, encapsulated cell therapy), Xipere (triamcinolone acetonide injectable suspension), AU-011 (belzupacap sarotalocan targeted delivery), ABBV-RGX-314, elamipretide, and OCS-01 (high concentration dexamethasone).

EXPERT OPINION:

Promising innovations include sustained-release intravitreal implants, topical and subcutaneous delivery systems, and targeted methods like suprachoroidal and subretinal injections, each with unique advantages and limitations. Challenges include overcoming the blood-retinal barrier, surgical complications with implantable devices, and ensuring patient adherence. Advances in smart delivery systems, drug formulations, and predictive models, alongside interdisciplinary collaboration, will be crucial in achieving personalized, effective, and sustainable retinal therapies.

2025-01-01·EYE

Exploring new horizons in neovascular age-related macular degeneration: novel mechanisms of action and future therapeutic avenues

Review

作者: Shirian, Jonathan D ; Shirian, Jonathan D. ; Shukla, Priya ; Singh, Rishi P. ; Singh, Rishi P

Abstract:

Neovascular age-related macular degeneration (nAMD) can lead to significant vision impairment through the growth of abnormal neovascular membranes in the choroid. Despite advancements with current anti-vascular endothelial growth factor (VEGF) therapies, challenges such as frequent injections, inadequate response, and patient-related concerns persist. Emerging therapeutics aim to reduce vision-loss through a variety of mechanisms. Gene therapies, including RGX-314 and Ixo-vec, express an anti-VEGF protein, and 4D-150, expresses an anti-VEGF protein and a VEGF-C inhibitory miRNA. Anti-VEGF associated therapeutics include OPT-302, targeting VEGF-C and VEGF-D, BI 836880, which inhibits VEGF-A and Ang-2 activity, and Tarcocimab tedromer, inhibiting all VEGF-A isoforms. Agents with novel mechanisms of action include UBX1325, which inhibits an anti-apoptotic protein, Restoret (EYE103), a Wnt agonist, and the tyrosine kinase inhibitors, EYP-1901, OTX-TKI, CLS-AX, and KHK4951.

200

项与 Surabgene Lomparvovec 相关的新闻（医药）

2026-02-22

·瞳神书院Phoenix

年龄相关性黄斑变性：疾病机制、治疗突破与可及性挑战

引言年龄相关性黄斑变性是导致全球老年人中心视力丧失乃至失明的首要原因。尽管年龄标准化患病率有所下降，但绝对患病人数与疾病负担正因人口老龄化而急剧攀升，预计到2050年全球受影响人数将超过2100万，其中低收入与中等收入国家的负担尤为沉重。一：疾病概述与流行病学全景 1.1 年龄相关性黄斑变性（AMD）：定义、分型与临床进程年龄相关性黄斑变性是一种慢性、进行性的眼底疾病，主要累及视网膜中心区域的黄斑，该区域负责精细视觉和中心视力。其发病与年龄增长密切相关，在发展中国家的重要性也日益凸显。根据病理特征和临床表现，AMD主要分为两种类型：干性（非新生血管性）AMD ：这是最常见的类型，约占所有AMD病例的80%-90%。其特征是视网膜色素上皮细胞逐渐萎缩、功能丧失，并伴随玻璃膜疣的积累。干性AMD通常进展缓慢，早期可能无症状或仅有轻度视力模糊，但晚期可发展为地图状萎缩，导致中心视力出现不可逆的暗点。湿性（新生血管性）AMD ：虽然仅占病例的约10%-20%，但却是导致严重、快速视力丧失的主要原因。其病理基础是脉络膜新生血管异常生长并侵入视网膜下，这些血管脆弱易漏，引起出血、渗出和视网膜水肿，可在短时间内严重破坏黄斑结构与功能。值得注意的是，干性AMD有可能进展为湿性AMD，因此对干性AMD患者的定期监测至关重要。 1.2 全球疾病负担（GBD）深度解析：趋势、差异与核心驱动因素 GBD 2021全球合作团队的研究为我们提供了迄今为止最详尽、时空跨度最大的AMD全球负担评估（数据覆盖1990-2021年，并预测至2050年），其核心发现揭示了当前面临的严峻挑战与未来趋势。 1.2.1 绝对负担的急剧攀升与“成功中的挑战” 研究最引人瞩目的结论是：全球因AMD导致视力受损（中度至重度视力丧失及失明）的绝对人数在1990年至2021年间翻了一倍多，从364万激增至806万。同期，用于衡量疾病总负担的伤残调整生命年（DALYs）也从30万增加到58万，增幅达91%。这清晰地表明，AMD正在影响越来越多的人，并导致巨大的健康寿命损失。然而，另一个关键指标—— 年龄标准化患病率与DALY率 ——却在同期呈现下降趋势（患病率从每10万人99.50例降至94.00例；DALY率从8.38降至6.78）。这种“绝对数上升，率下降”的矛盾现象，深刻揭示了全球AMD负担动态的核心：人口增长与老龄化是驱动患者总数飙升的主导力量，而医疗水平的提高、风险因素的控制则在减缓年龄调整后的发病速率方面取得了部分成功。这是一个典型的“成功中的挑战”范例：医疗卫生进步取得了成效，但社会人口结构的变化带来了更大的绝对压力。 1.2.2 显著的社会经济与地域不平等 GBD研究按社会人口指数（SDI）进行的分层分析，凸显了疾病负担分布的不平等性。年龄标准化率的下降在高SDI地区最为持续和明显。这与健康可及性与质量指数与AMD负担呈负相关的发现一致，即医疗系统更发达、质量更高的地区，能够更有效地管理和减轻AMD带来的疾病负担。相反，中低SDI地区，尤其是低收入和中等收入国家，正面临着双重压力：一方面，这些地区人口老龄化速度可能更快；另一方面，其医疗体系在诊断、治疗和长期管理AMD方面的能力相对薄弱。研究特别指出，引入具有成本效益的治疗和诊断方法，同时在LMICs实施烟草管制，对于减轻全球AMD负担具有至关重要的意义。这直接呼应了关于LMICs中经济有效治疗方法的搜索发现，即抗VEGF疗法等高成本治疗手段在这些地区的可及性严重受限。 1.2.3 风险因素的量化：烟草的关键作用与可控性 GBD 2021研究的一个重要贡献是量化了可改变风险因素对AMD负担的影响。吸烟被明确确定为AMD的关键可改变风险因素。数据显示，全球范围内，烟草使用对AMD相关DALYs的贡献率从1990年的12.45%下降至2021年的9.96%（降幅20%）。这一下降很可能与同期全球许多地区推行的烟草控制政策有关。研究的预测模型进一步强化了这一观点：消除烟草使用，可以将2050年预计受AMD影响的男性人数从902万降至817万，女性人数从1232万降至1115万，总计减少约193万人。这一数据为公共卫生政策制定者提供了强有力的经济学和公共健康论据，表明针对性的烟草控制不仅是肺癌等疾病的预防策略，也是减少未来AMD致残负担、节约长期医疗与社会成本的高效干预手段。这与关于烟草控制政策的搜索结果高度吻合，即严格的烟草控制立法、征税和公众教育是降低吸烟率及相关疾病（包括AMD）负担的有效措施。 1.2.4 对未来（至2050年）的严峻预测基于当前趋势的预测显示，若不采取更有效的全球干预，到2050年，全球受AMD影响的总人数预计将达到惊人的2134万，其中男性约902万，女性约1232万。这一预测远超人口线性增长的速度，提示随着战后“婴儿潮”一代全面进入高龄，AMD的流行将进入一个前所未有的高峰期。这将对全球的眼科医疗服务体系、社会保障系统乃至经济生产力构成巨大挑战。 1.3 干性与湿性AMD的流行病学与临床负担差异尽管GBD 2021等宏观研究通常不区分干湿性AMD的报告数据，但临床和流行病学研究清楚地表明两者在负担构成上存在本质差异。患病率与发病率：干性AMD在病例数量上占据绝对主导。湿性AMD虽然病例数较少，但其发病率随年龄增长而急剧上升。视力损害贡献度：尽管干性AMD患者基数庞大，但湿性AMD是导致快速、严重中心视力丧失的元凶，承担了AMD所致大部分法定盲和重度视力损伤的归因风险。因此，在计算DALYs时，湿性AMD因其导致的残疾权重更高，对总负担的贡献比例远高于其患病人数比例。治疗反应与疾病管理：这是两者最根本的差异点。目前，针对湿性AMD已有明确有效的治疗方案——即抗血管内皮生长因子（抗VEGF）玻璃体内注射，它能有效抑制新生血管生长、减轻水肿，稳定甚至改善视力。然而，这种治疗需要频繁、长期的注射和监测，给患者和医疗系统带来沉重负担。对于干性AMD，尤其是其晚期形式地图状萎缩（GA），长期以来缺乏被证实能逆转或显著延缓视力丧失的疗法，管理主要侧重于补充抗氧化剂（如AREDS2配方）和定期监测。近年来，一些针对GA的补体抑制剂等新药已在美国等地获批，标志着干性AMD治疗领域的重大突破，但其长期效果、可及性和成本仍是待解难题。这种“有药可治但负担重”与“无药可治但患者多”的悖论，构成了AMD临床管理与公共卫生应对的复杂局面。二：临床诊疗现状、挑战与可及性困境 2.1 诊断技术与筛查策略早期诊断和分型对于AMD的管理至关重要。标准诊断流程依赖于全面的眼科检查，包括： 1) 视力检查：评估中心视力受损程度。 2) 眼底检查：使用检眼镜直接观察视网膜，可发现玻璃膜疣、色素改变、出血或渗出。 3) 光学相干断层扫描（OCT）：这是当前诊断和监测AMD，尤其是湿性AMD的金标准工具。它能非侵入性地提供视网膜横断面的高分辨率图像，精确显示视网膜各层厚度、积液、玻璃膜疣和新生血管膜的存在与变化。 4) 荧光素血管造影（FA）和吲哚菁绿血管造影（ICGA）：通过静脉注射造影剂，动态观察视网膜和脉络膜血管的循环情况，有助于明确湿性AMD中新生血管的类型、位置和活动性，尤其在OCT图像不典型时。在筛查层面，随着技术发展，人工智能（AI）辅助的眼底影像分析正在成为一个极具潜力的方向。这有望在基层医疗、社区筛查和资源有限地区，大幅提高筛查效率和覆盖范围，实现早发现、早转诊。 2.2 现有治疗范式及其局限性 2.2.1 干性AMD的治疗长期以来，干性AMD的治疗选择非常有限。年龄相关性眼病研究（AREDS和AREDS2）表明，特定配方的抗氧化剂和矿物质补充剂（含维生素C、E、锌、铜、叶黄素、玉米黄质）可以降低高风险人群进展为晚期AMD的风险约25% (Fleckenstein M, et al. JAMA. 2024)。然而，这仅是预防性措施，对于已形成的GA无效。近年来，针对补体通路过度激活的药物研发取得突破。例如，美国FDA已批准pegcetacoplan和avacincaptad pegol等补体C3或C5抑制剂用于治疗GA。这些药物通过玻璃体内注射，被证明可以减缓GA病灶的扩大速度。然而，它们尚不能恢复已丧失的视力，且同样面临长期注射、高成本和安全性监测的挑战。 2.2.2 湿性AMD的治疗：抗VEGF疗法的统治与困境自2000年代中期以来，抗VEGF疗法彻底改变了湿性AMD的治疗格局，使其从一种几乎注定致盲的疾病转变为一种多数情况下可控制的慢性病。目前主流的抗VEGF药物包括雷珠单抗、阿柏西普和贝伐珠单抗。疗效与标准方案：这些药物通过阻断VEGF来抑制新生血管和血管渗漏。标准的治疗方案初始阶段需要每月注射，之后根据“治疗并延长”或“按需治疗”方案进行调整，以维持视力稳定。临床试验和真实世界数据证实，规律治疗能显著改善或维持绝大多数患者的视力 (Fleckenstein M, et al. JAMA. 2024)。主要挑战： 1) 治疗负担：需要终身、频繁的玻璃体内注射和定期OCT复查，给患者带来极大的身体、心理和经济压力，也是导致治疗依从性下降和视力结果不佳的主要原因。 2) 经济成本：抗VEGF药物本身价格昂贵，加上注射操作和监测的费用，使得湿性AMD成为眼科领域医疗成本最高的疾病之一。在高收入国家，这已对医保基金构成压力；在LMICs，这直接导致了巨大的治疗可及性鸿沟。 3) 治疗反应不均一：部分患者对抗VEGF治疗反应不佳，视力仍持续下降。为了克服这些挑战，产业界正致力于开发长效抗VEGF疗法，旨在延长注射间隔。此外，基因疗法的终极目标是通过一次性治疗，让眼内细胞持续表达抗VEGF蛋白，从而可能实现“一劳永逸”或极大减少注射频率。 2.3 资源有限环境下的可及性危机与应对策略在低收入和中等收入国家（LMICs），AMD的诊断和治疗面临“缺乏数据、公众意识不足和医疗资源有限”的系统性挑战。抗VEGF疗法在高收入国家是可及的标准治疗，但在LMICs，其应用受限于高昂的药物成本、不完善的保险覆盖、专科医生和诊疗中心短缺，以及冷链物流等基础设施落后的问题。在此背景下，探索和推广具有成本效益的替代方案成为当务之急：药物替代：使用贝伐珠单抗作为雷珠单抗或阿柏西普的廉价替代品，是许多LMICs（如印度）普遍采用的策略。尽管需要谨慎处理分装带来的无菌和合规风险，但其成本可能仅为专利药物的百分之一，显著降低了治疗门槛。生物类似药：随着原研抗VEGF药物专利到期，其生物类似药的上市有望通过市场竞争进一步拉低价格，提高可及性。服务模式创新：任务转移与简化诊疗：培训中级眼科保健人员进行部分诊断甚至注射操作，可以缓解专科医生短缺的压力。远程医疗与AI筛查：利用智能手机眼底照相设备结合AI分析，或通过远程医疗平台将基层拍摄的图像传输给中心医院的专家进行诊断，可以扩大筛查和随访覆盖范围，尤其适用于偏远地区。尽管存在互联网接入和数字素养的障碍，但其潜力巨大。优化治疗流程：采用“治疗并延长”等个性化方案，在确保疗效的前提下尽可能减少就诊和注射次数，可以降低患者交通和时间成本，提高系统效率。这些策略的成功实施，离不开政府卫生部门、国际非政府组织、制药企业以及本地医疗机构的共同规划和投入。三：超越视力的多重影响：心理、社会与经济维度 AMD的影响远不止于视力图表上的数字下降。它是一种对患者整体健康、心理健康、社会功能和经济状况产生深远影响的全身性疾病。 3.1 精神心理健康：显著的抑郁风险大量研究证实，AMD患者罹患抑郁症的风险显著高于普通同龄人。韩国一项全国性队列研究（Hwang S, et al. Ophthalmology. 2023）更是量化了这一风险，指出AMD诊断会使抑郁症的风险增加15%。视力丧失导致阅读、驾驶、识别人脸、从事爱好等日常活动能力受限，极大地削弱了患者的独立性和生活质量，容易引发无助感、社会隔离和自尊心下降，这些都是抑郁症的重要诱因。鉴于这一高风险，将心理社会支持整合到AMD标准护理中至关重要。搜索结果显示，多种干预措施被证明有效：问题解决疗法（PST）：教导患者以结构化的方式应对因视力下降带来的具体日常问题，被多项研究证明能有效预防或减轻AMD患者的抑郁症状，尤其在短期内效果显著。认知行为疗法（CBT）原则与自我管理：帮助患者调整对视力损失的负面认知，学习使用残存视力的技巧，管理情绪。社会支持与团体干预：加入患者支持小组、接受定向行走训练、学习使用辅助器具，能有效减少孤独感，重建社会连接，是预防抑郁的关键。职业治疗：通过改善患者进行日常活动的能力，提升其功能独立性和自信心，从而缓解抑郁。眼科医生在接诊AMD患者时，应有意识地进行简单的抑郁筛查，并建立向心理健康专业人员转诊的通道。 3.2 全因死亡率与全身健康关联一项发表于《柳叶刀-全球健康》的系统综述与荟萃分析（Ehrlich JR, et al. 2021）证实，视力损伤与全因死亡率增加存在显著关联。这种关联的机制可能是多方面的：视力障碍增加跌倒、骨折和意外伤害的风险；影响患者管理其他慢性病的能力；限制身体活动，加剧社会孤立，进而对心血管和免疫系统产生负面影响。因此，有效管理AMD、维持最佳视觉功能，可能对延长患者的总体健康寿命具有积极意义。 3.3 沉重的社会经济负担 AMD造成的经济负担是直接医疗成本与间接生产力损失的总和。直接医疗成本：包括药物费用、注射操作费、诊断检查费、门诊费以及可能的住院和手术费用。在高收入国家，每位湿性AMD患者每年的治疗费用可达数万美元。全球每年的相关医疗成本估计高达数百亿美元。间接成本与社会成本：生产力损失：患者本人可能因视力下降而提前退休、减少工作时间或工作效率降低。此外，患者家属也可能需要投入大量时间提供照料，影响其自身的工作和收入。一项研究估计，全球因视力损伤和盲导致的经济生产力损失极其巨大 (Marques AP, et al. EClinicalMedicine. 2021)。社会支持系统支出：社会需要为视力残疾者提供康复服务、辅助设备、交通补贴和社会保障福利。无形负担：生活质量的下降、痛苦的增加等无法用金钱衡量的损失。对于中低收入国家而言，AMD的经济负担尤为沉重。由于缺乏有效的治疗可及性，患者可能更早、更彻底地丧失劳动能力和独立性，不仅个人和家庭陷入贫困，国家也损失了宝贵的劳动力资源。四：创新前沿：从基因治疗到数字健康的突破性进展 4.1 基因治疗：追求“一次性治愈”的梦想基因治疗旨在通过病毒载体将编码治疗性蛋白的基因直接递送到眼内细胞，使其能够长期、持续地表达目标蛋白，从而理论上实现单次或极少数治疗即可长期控制疾病。针对湿性AMD ：主要策略是让眼内细胞持续表达抗VEGF蛋白。 RGX-314 （RegenxBio公司）是该领域的领先候选产品之一。其II/III期临床试验正在评估其安全性和减少抗VEGF注射需求的疗效，目标是在2020年代后期支持其生物制剂许可申请（BLA）。早期数据显示其在减少注射次数方面有潜力，且安全性可接受。其他如 ABP 938 等产品也处于不同研发阶段。针对干性AMD（GA）：策略更多样，包括靶向补体系统或提供神经营养因子以保护视网膜细胞。挑战与展望：基因治疗面临长期安全性和有效性验证、免疫反应、载体递送效率、高昂的研发与生产成本等挑战。然而，其“一劳永逸”的潜力使其成为改变AMD治疗范式的最大希望之一。基因编辑技术未来甚至可能直接纠正致病基因变异，提供真正的治愈可能。 4.2 干细胞治疗：旨在修复与再生干细胞治疗侧重于替代AMD中受损或死亡的视网膜色素上皮细胞，甚至感光细胞，以期恢复视力功能。主要使用人多能干细胞（包括胚胎干细胞或诱导多能干细胞）分化成RPE细胞，然后移植到患者视网膜下。进展与试验：例如， OpRegen （由胚胎干细胞衍生的RPE细胞组成）的临床试验已显示出初步的安全性和一些结构改善的迹象。挑战：该领域面临细胞纯化、移植后存活与整合、免疫排斥、潜在致瘤风险以及手术复杂性等多重挑战。目前，干细胞治疗更可能首先应用于晚期地理状萎缩，作为“细胞贴片”来替代萎缩区域。 4.3 新型药物递送系统为了延长抗VEGF药物的作用时间，减少注射频率，除了开发新分子实体，还在积极研究新型递送技术：长效缓释植入物：将药物封装在生物可降解或非降解的微型植入物中，通过一次手术植入眼内，在数月甚至数年内缓慢释放药物。口服或局部给药：研发能够穿透血-眼屏障的口服小分子VEGF抑制剂或眼药水，是更具便利性的探索方向，但目前疗效尚未能媲美眼内注射。 4.4 数字健康与人工智能（AI）的深度融合数字技术正在重塑AMD的筛查、诊断、监测和管理全流程。 AI辅助诊断与分级：如前所述，AI算法分析眼底彩照或OCT图像，可达到甚至超过人类专家的准确度，实现大规模、低成本的自动化筛查和分级，尤其适用于基层和资源匮乏地区。远程监测与居家管理：家用OCT设备、智能手机适配的眼底镜头，允许患者在家中定期自查。图像通过安全平台上传，由AI初步分析或医生远程审阅，可以及时发现疾病复发或进展的迹象，实现更精准的“按需”复诊，减少不必要的奔波，优化医疗资源分配。预测模型：利用机器学习分析多模态数据，预测个体患者进展为晚期AMD的风险，实现真正的个性化预防和管理。这些技术的整合，有望构建一个更高效、更可及、更以患者为中心的AMD智慧医疗生态系统。五：多方协作与系统性解决方案：构建可持续的应对体系应对AMD这一复杂的全球性公共卫生挑战，任何单一主体都无法独力完成。需要制药公司、支付方（政府医保、商业保险）、政策制定者、医疗机构、患者组织以及科研机构形成合力，构建一个可持续的应对体系。 5.1 制药企业的角色与策略创新研发创新：持续投入研发更有效、更长效、更便利的新疗法（基因治疗、新型生物药、小分子药物），是企业的根本使命。定价与可及性策略：在追求投资回报的同时，需承担社会责任，制定差异化的全球定价策略。在高中收入国家，通过价值定价和风险共担协议来证明其产品的成本效益。在LMICs，则必须探索切实可行的价格削减、自愿许可（授权本地生产）、或与政府/国际组织建立公私合作伙伴关系（PPP）。支持真实世界研究与患者支持项目：资助或开展真实世界研究，积累药物在更广泛人群中长期使用的证据。设立患者援助项目，为经济困难的患者提供药物或费用支持。 5.2 支付方与政策制定者的核心作用卫生技术评估（HTA）与报销决策：医保部门应基于严格的卫生技术评估，科学、及时地将有价值的新疗法纳入报销目录。对于像基因治疗这样前期成本极高的“一次性”疗法，需要设计创新的支付模式，如分期付款、按疗效付费、长期年金支付等，以分摊财务风险。公共卫生政策制定： 1) 烟草控制：GBD研究提供了烟草导致AMD负担的量化证据。政府应坚定推行并加强全面的烟草控制措施，这将是预防AMD最具成本效益的公共卫生投资之一。 2) 筛查与早诊早治体系：在国家眼健康规划中，将老年人AMD筛查纳入考虑。利用AI和远程医疗技术，建立高效、低成本的筛查网络，促进早期转诊和治疗。 3) 医疗资源规划与培训：加强眼科服务体系建设，特别是在基层和农村地区。培训足够的眼科医生和中级眼保健人员，确保诊断和治疗能力。促进多方合作平台：政府或国际组织可以牵头建立“AMD治疗合作网络”，汇聚药企、医保、医院、学者，共同研究治疗规范、成本效益模型和数据共享，以优化整体医疗资源配置。 5.3 医疗机构与专业学会的责任规范诊疗与质量控制：制定并推广基于证据的临床诊疗指南，规范抗VEGF治疗的启动、调整和监测流程，确保治疗质量和患者视力获益最大化。多学科协作：在眼科诊所内或与社区医疗、精神心理科、康复科建立协作机制，为AMD患者提供“一站式”的综合管理，包括视力康复、心理评估与干预、社会服务转介等。拥抱技术创新：积极引入并合理应用AI诊断工具、远程医疗平台，提高诊疗效率，扩大服务覆盖面。 5.4 患者组织与社会力量倡导与发声：代表患者群体，向政府、药企和医保机构倡导更可及的药物、更合理的政策和更全面的支持服务。教育与支持：为患者和家属提供疾病知识教育、心理支持、经验分享平台，帮助他们更好地应对疾病，提高自我管理能力。参与研究：鼓励患者参与临床试验和真实世界研究，为医学进步贡献数据。结论与展望年龄相关性黄斑变性已然是一个不容忽视的全球健康危机。一方面，我们拥有比以往任何时候都更强大的科学武器：从能有效控制湿性AMD的抗VEGF疗法，到初见曙光的干性AMD新药；从可能改变治疗范式的基因与干细胞治疗，到能重塑诊疗流程的人工智能与数字健康技术。另一方面，将这些科学突破转化为全球患者，特别是LMICs患者可及、可负担的福祉，仍然横亘着成本、基础设施、人力资源和政策协调的巨大鸿沟。参考信息 Trends in the global disease burden of age-related macular degeneration from 1990 to 2021 Global, regional, and national burden of age-related macular degeneration, 1990–2019: an age-period-cohort analysis based on the Global Burden of Disease 2019 Study Global burden of low vision and blindness due to age-related macular degeneration from 1990 to 2021 and projections for 2050 Tackling an Age-Related Macular Degeneration in the Low and Middle Income Countries Eyes on the future: A clear outlook on Age-related Macular Degeneration An overview of multidisciplinary rehabilitation for age-related macular degeneration at the Henry Ford Center for Visual Rehabilitation and Research The Clinical Effectiveness and Cost-Effectiveness of Screening for Age-Related Macular Degeneration in Japan: A Markov Modeling Study Global burden of smoking-associated age-related macular degeneration: Spatiotemporal trends from 1990 to 2021 and projections to 2040 Protocol for a mixed-methods randomised controlled trial evaluating the psychosocial effects of an expressive arts-based intervention on adults with age-related macular degeneration Depression in patients with age-related macular degeneration and diabetic retinopathy can be reduced with self-care tools Psychologische Interventionen und Psychotherapie bei älteren Patienten mit Depression Decoding Age-Related Macular Degeneration: From Molecular Pathways to Cutting-edge Therapies Morphological and Functional Assessment of the Optic Nerve Head and Retinal Ganglion Cells in Dry vs Chronically Treated Wet Age-Related Macular Degeneration Economic burden of late-stage age-related macular degeneration in Bulgaria, Germany, and the US Recommendation of the Retina International age-related macular degeneration (AMD) Communications taskforce Efficacy and Safety of Ranibizumab Biosimilar QL1205 in Neovascular Age-Related Macular Degeneration: A Phase III Randomized Trial

2026-02-09

·雪球

$Regenxbio(RGNX)$REGENXBIO计划与FDA合作

$Regenxbio(RGNX)$REGENXBIO计划与FDA合作，寻找前进路径，目标是重新提交BLAROCKVILLE,Md.,Feb.9,2026/PRNewswire/--REGENXBIOInc.(Nasdaq:RGNX)todayannouncedthattheU.S.FoodandDrugAdministration(FDA)hasissuedaCompleteResponseLetter(CRL)regardingitsBiologicsLicenseApplication(BLA)forRGX-121(clemidsogenelanparvovec)forthetreatmentofMucopolysaccharidosisII(MPSII),anultra-rareneurodegenerativediseasealsoknownasHuntersyndrome.马里兰州罗克维尔，2026年2月9日/PRNewswire/--REGENXBIO公司（纳斯达克股票代码：RGNX）今日宣布，美国食品药品监督管理局（FDA）已就其用于治疗黏多糖贮积症II型（MPSII，也称为亨特综合征）的RGX-121（clemidsogenelanparvovec）生物制品许可申请（BLA）发布了一份完整回应函（CRL）。这是一种超罕见的神经退行性疾病。InMay2025,theFDAacceptedtheRGX-121BLAundertheacceleratedapprovalpathway.IntheFebruary7,2026CRL,theFDAstatedthatithadagreedtothestudyprotocolinprincipleandoutlinedseveralreasonsfornotapprovingthegenetherapy,includinguncertaintyregardingthestudyeligibilitycriteriatoadequatelydefineapopulationwithneuronopathicdisease(vs.attenuateddisease),thecomparabilityofthenaturalhistoryexternalcontroltothestudypopulation,andtheappropriatenessofCSFHSD2S6asasurrogateendpointreasonablylikelytopredictclinicalbenefit.TheCRLlistsseveralpotentialpathsforward,includinganewstudy,treatingadditionalpatientsandconductinglonger-termfollowup,andusinganuntreatedcontrolarm,allofwhichwouldbechallenginginanultra-rarediseasepopulation,likeMPSII.2025年5月，FDA接受了RGX-121BLA的加速审批通道。在2026年2月7日的完整回应函中，FDA表示原则上同意研究方案，并列出了不批准该基因疗法的几个原因，包括对如何充分定义患有神经病变疾病（而非轻型疾病）人群的研究资格标准存在不确定性、自然史外部对照与研究人群之间的可比性问题，以及脑脊液HSD2S6作为预测临床效益的可能性较大的替代终点是否合适的问题。CRL列出了一些潜在的后续路径，包括进行一项新的研究、治疗更多患者并进行长期随访、使用未治疗的对照组，所有这些在像MPSII这样的超罕见病人群中都是具有挑战性的。"Thisdecisionisdevastatingforthefamiliesofboyslivingwiththisprogressive,life-threateningdisease,"saidCurranSimpson,PresidentandCEOofREGENXBIO."WeareconcernedaboutFDA'sfeedbackregardingtheoveralldevelopmentpathandevaluationofthedatainthecontextoftheurgentneedforthisirreversibleultra-raredisease.Weremainconfidentinthequalityandvolumeofevidencedemonstratingthelong-termpotentialofRGX-121topositivelychangethetrajectoryofHuntersyndrome.Thisprogramhasbeenindevelopmentforover10years.Weareincrediblygratefultoallthepatients,theirfamilies,investigators,andsitestaffwhohavesupportedthisprogramandourcontinuedeffortstobringamuch-needednewtreatmentoptiontotheHuntersyndromecommunity.Wewillcontinuethoseefforts."“这一决定对那些患有这种渐进式的、危及生命的疾病的男孩家庭来说是一个毁灭性的打击。”REGENXBIO总裁兼首席执行官CurranSimpson表示，“我们对FDA关于整体开发路径和在评估数据背景下的反馈感到担忧，尤其是考虑到这一不可逆的超罕见疾病迫切的治疗需求。我们仍然对证明RGX-121长期潜力能够积极改变Hunter综合征进程的数量众多且高质量的证据充满信心。该项目已经开发了十多年。我们非常感谢所有支持该项目以及我们持续努力为Hunter综合征社区带来亟需的新治疗选择的患者、他们的家人、研究人员和现场工作人员。我们将继续努力。”ThroughoutactivediscussionsduringtheBLAprocess,REGENXBIObelievedithadaddressedthepointsraisedintheCRLthroughthesubmissionofadditionaldataandresponsestonumerousinformationrequests.Independent,leadingglobalMPSandbiomarkerexpertsconductedanalysesandreviewswiththeFDA,aswell.Ultimately,theFDAdidnotagreethedatasetprovidedsubstantialevidenceofeffectivenesstosupportapprovalofRGX-121forthetreatmentofMPSII.在BLA审查过程中积极讨论期间，REGENXBIO认为它通过提交额外数据和回复大量信息请求解决了CRL中提出的问题。独立的全球领先的MPS和生物标志物专家也与FDA一起进行了分析和审查。最终，FDA并不认为提供的数据集提供了支持批准RGX-121治疗MPSII的有效性的实质性证据。REGENXBIOplanstorequestaTypeAmeetingtodiscusstheCRL,aswellastheplannedBLAresubmissiontoprovideadditionalevidencefromglobalMPSIIexpertstofurtherclarifytheneuronopathicpatientpopulationandadditionallonger-termclinicaldatatosupportevidenceofeffectiveness.REGENXBIOintendstofindapathforwardasquicklyaspossiblewiththegoalofresubmittingtheBLA.REGENXBIO计划请求召开A类会议，讨论CRL以及计划中的BLA重新提交事宜，以提供来自全球MPSII专家的额外证据，进一步明确神经病变患者群体，并提供额外的长期临床数据来支持有效性证据。REGENXBIO希望尽快找到一条前进路径，目标是重新提交BLA。"MPSIIisaverycomplexdisease,butitsimpactiswellestablished,resultinginirreversiblebraindamageforthemajorityofpatients;withoutappropriatetreatmentsstoppingthisneurocognitivedecline,theneuronopathicMPSIIchildwilldieprematurely,usuallyintheirmid-teens,"saidJosephMuenzer,M.D.,Ph.D.,Director,MuenzerMPSResearchandTreatmentCenter,BrysonDistinguishedProfessorintheDivisionofGeneticsandMetabolism,DepartmentofPediatricsGenetics,UniversityofNorthCarolinaatChapelHill."IremainencouragedbytheclinicaldatabehindRGX-121.Newinnovationslikegenetherapycouldmakeasignificantimpactforthesepatients,andtimeispreciousforthesefamilies."“MPSII是一种非常复杂的疾病，但其影响已经被充分证实，大多数患者会出现不可逆的脑损伤；如果不采取适当的治疗阻止这种神经认知能力下降，患有神经病变的MPSII儿童通常会在十几岁时早逝。”JosephMuenzer博士说道，他是MuenzerMPS研究与治疗中心主任，Bry杰出教授，北卡罗来纳大学教堂山分校儿科遗传学系遗传学与代谢科成员。“我依然受到RGX-121背后的临床数据鼓舞。像基因疗法这样的创新可能对这些患者产生重大影响，而时间对这些家庭来说非常宝贵。”"I'veseenthesevereimpactofMPSIIonpatientsandtheirfamiliesfirsthandandamextremelydisheartenedbytoday'snews,"saidTerriKlein,PresidentandCEO,NationalMPSSociety."Familiesknowthedevastatingtrajectoryofthisdiseasealltoowellandhavewaited20yearsfornewtreatmentoptions.Theycannotwaitanylonger.Drugdevelopmentforultra-rarediseasemustbestreamlinedtoallownewmedicinestoreachpatients.WeurgetheFDAtofindaswiftpathforwardsothatboyslivingwithMPSIIandtheirfamilieshavethechanceforabetterlife."“我亲眼目睹了MPSII对患者及其家庭造成的严重影响，因此对今天的消息感到极度失望。”国家MPS协会主席兼首席执行官TerriKlein表示，“家属们深知这种疾病的毁灭性轨迹，并且已经等待了20年的新治疗选择。他们不能再等了。对于超罕见疾病的药物研发必须简化，以便让新药更快地到达患者手中。我们敦促FDA找到快速前进的方法，使那些患MPSII的男孩及其家庭有机会过上更好的生活。”AboutRGX-121(clemidsogenelanparvovec)RGX-121isapotentialone-timegenetherapyforthetreatmentofboyswithMPSII,designedtodelivertheiduronate-2-sulfatase(IDS)genetotheCNS.DeliveryoftheIDSgenewithincellsintheCNScouldprovideapermanentsourceofsecretediduronate-2-sulfatase(I2S)proteinbeyondtheblood-brainbarrier,allowingforlong-termcrosscorrectionofcellsthroughouttheCNS.RGX-121expressedproteinisstructurallyidenticaltonormalI2S.关于RGX-121（clemidsogenelanparvovec）RGX-121是一种潜在的一次性基因疗法，用于治疗患有MPSII的男孩，旨在将艾杜糖醛酸-2-硫酸酯酶（IDS）基因递送到中枢神经系统（CNS）。在CNS内的细胞中递送IDS基因可以提供一个永久性的分泌型艾杜糖醛酸-2-硫酸酯酶（I2S）蛋白来源，超越血脑屏障，从而实现整个CNS细胞的长期交叉校正。RGX-121表达的蛋白质在结构上与正常I2S完全相同。TheBLAforRGX-121forMPSIIwassupportedbypositivebiomarker,functionalandsafetydatafromtheCAMPSIITEI/II/IIItrial,includingoutto12months.RGX-121hasbeenwelltoleratedinallpatientsdosedacrossallphasesoftheCAMPSIITEtrial.CAMPSIITEI/II/III试验的积极生物标志物、功能和安全性数据（最长至12个月）支持了RGX-121治疗MPSII的BLA申请。在CAMPSIITE试验的所有阶段中，所有接受治疗的患者对RGX-121的耐受性良好。RGX-121hasreceivedOrphanDrugProduct,RarePediatricDisease,FastTrackandRegenerativeMedicineAdvancedTherapy(RMAT)designationsfromtheFDAandadvancedtherapymedicinalproducts(ATMP)classificationfromtheEuropeanMedicinesAgency.RGX-121已获得FDA授予的孤儿药产品、罕见儿科疾病、快速通道及再生医学高级治疗（RMAT）称号，并获得欧洲药品管理局的先进治疗药物产品（ATMP）分类。AboutMucopolysaccharidosisTypeII(MPSII)MPSII,orHunterSyndrome,isarare,X-linkedrecessivediseasecausedbyadeficiencyinthelysosomalenzymeI2Sleadingtoanaccumulationofglycosaminoglycans(GAGs),includingheparansulfate(HS)intissueswhichultimatelyresultsincell,tissue,andorgandysfunction,includinginthecentralnervoussystem(CNS).Insevereformsofthedisease,earlydevelopmentalmilestonesmaybemet,butdevelopmentaldelayisreadilyapparentby18to24months.SpecifictreatmenttoaddresstheneurologicalmanifestationsofMPSIIremainsasignificantunmetmedicalneed.KeybiomarkersofI2SenzymaticactivityinMPSIIpatientsincludeitssubstrateCSFHSD2S6,whichhasbeenshowntocorrelatewithneurocognitivemanifestationsofthedisorder.关于黏多糖贮积症II型（MPSII）MPSII（亨特综合症）是一种罕见的X连锁隐性疾病，由溶酶体酶I2S缺乏导致糖胺聚糖（GAGs）积累所致，其中包括组织中的硫酸肝素（HS），最终导致细胞、组织和器官功能障碍，包括中枢神经系统（CNS）。在疾病的严重形式下，早期发育里程碑可能得以达成，但在18至24个月时发育迟缓显而易见。针对MPSII神经学表现的具体治疗方法仍然是重要的未满足医疗需求。MPSII患者的I2S酶活性的关键生物标志物包括其底物CSFHSD2S6，已被证明与该疾病的神经认知表现相关。ABOUTREGENXBIOInc.REGENXBIOisabiotechnologycompanyonamissiontoimprovelivesthroughthecurativepotentialofgenetherapy.Sinceitsfoundingin2009,REGENXBIOhaspioneeredthefieldofAAVgenetherapy.REGENXBIOisadvancingalate-stagepipelineofone-timetreatmentsforrareandretinaldiseases,includingRGX-202forthetreatmentofDuchenne;clemidsogenelanparvovec(RGX-121)forthetreatmentofMPSIIandRGX-111forthetreatmentofMPSI,bothinpartnershipwithNipponShinyaku;andsurabgenelomparvovec(ABBV-RGX-314)forthetreatmentofwetAMDanddiabeticretinopathy,incollaborationwithAbbVie.ThousandsofpatientshavebeentreatedwithREGENXBIO'sAAVplatform,includingthosereceivingNovartis'ZOLGENSMA.REGENXBIO'sinvestigationalgenetherapieshavethepotentialtochangethewayhealthcareisdeliveredformillionsofpeople.Formoreinformation,pleasevisit.关于REGENXBIO公司REGENXBIO是一家生物技术公司，致力于通过基因疗法的治愈潜力改善生活。自2009年成立以来，REGENXBIO一直是AAV基因疗法领域的先驱。REGENXBIO正在推进一系列针对罕见病和视网膜疾病的晚期一次性治疗管线，包括用于治疗杜氏肌营养不良症的RGX-202；与日本新药株式会社合作开发的clemidsogenelanparvovec(RGX-121)用于治疗MPSII和RGX-111用于治疗MPSI；以及与艾伯维公司合作开发的surabgenelomparvovec(A

2026-02-09

·PRNewswire

REGENXBIO Announces Regulatory Update on RGX-121 BLA for MPS II

FDA issues Complete Response Letter for RGX-121 (clemidsogene lanparvovec) for treatment of Mucopolysaccharidosis II (MPS II) REGENXBIO plans to work with FDA on a path forward with the goal of resubmitting the BLA ROCKVILLE, Md., Feb. 9, 2026 /PRNewswire/ -- REGENXBIO Inc. (Nasdaq: RGNX) today announced that the U.S. Food and Drug Administration (FDA) has issued a Complete Response Letter (CRL) regarding its Biologics License Application (BLA) for RGX-121 (clemidsogene lanparvovec) for the treatment of Mucopolysaccharidosis II (MPS II), an ultra-rare neurodegenerative disease also known as Hunter syndrome. In May 2025, the FDA accepted the RGX-121 BLA under the accelerated approval pathway. In the February 7, 2026 CRL, the FDA stated that it had agreed to the study protocol in principle and outlined several reasons for not approving the gene therapy, including uncertainty regarding the study eligibility criteria to adequately define a population with neuronopathic disease (vs. attenuated disease), the comparability of the natural history external control to the study population, and the appropriateness of CSF HS D2S6 as a surrogate endpoint reasonably likely to predict clinical benefit. The CRL lists several potential paths forward, including a new study, treating additional patients and conducting longer-term follow up, and using an untreated control arm, all of which would be challenging in an ultra-rare disease population, like MPS II. "This decision is devastating for the families of boys living with this progressive, life-threatening disease," said Curran Simpson, President and CEO of REGENXBIO. "We are concerned about FDA's feedback regarding the overall development path and evaluation of the data in the context of the urgent need for this irreversible ultra-rare disease. We remain confident in the quality and volume of evidence demonstrating the long-term potential of RGX-121 to positively change the trajectory of Hunter syndrome. This program has been in development for over 10 years. We are incredibly grateful to all the patients, their families, investigators, and site staff who have supported this program and our continued efforts to bring a much-needed new treatment option to the Hunter syndrome community. We will continue those efforts." Throughout active discussions during the BLA process, REGENXBIO believed it had addressed the points raised in the CRL through the submission of additional data and responses to numerous information requests. Independent, leading global MPS and biomarker experts conducted analyses and reviews with the FDA, as well. Ultimately, the FDA did not agree the data set provided substantial evidence of effectiveness to support approval of RGX-121 for the treatment of MPS II. REGENXBIO plans to request a Type A meeting to discuss the CRL, as well as the planned BLA resubmission to provide additional evidence from global MPS II experts to further clarify the neuronopathic patient population and additional longer-term clinical data to support evidence of effectiveness. REGENXBIO intends to find a path forward as quickly as possible with the goal of resubmitting the BLA. "MPS II is a very complex disease, but its impact is well established, resulting in irreversible brain damage for the majority of patients; without appropriate treatments stopping this neurocognitive decline, the neuronopathic MPS II child will die prematurely, usually in their mid-teens," said Joseph Muenzer, M.D., Ph.D., Director, Muenzer MPS Research and Treatment Center, Bryson Distinguished Professor in the Division of Genetics and Metabolism, Department of Pediatrics Genetics, University of North Carolina at Chapel Hill. "I remain encouraged by the clinical data behind RGX-121. New innovations like gene therapy could make a significant impact for these patients, and time is precious for these families." "I've seen the severe impact of MPS II on patients and their families firsthand and am extremely disheartened by today's news," said Terri Klein, President and CEO, National MPS Society. "Families know the devastating trajectory of this disease all too well and have waited 20 years for new treatment options. They cannot wait any longer. Drug development for ultra-rare disease must be streamlined to allow new medicines to reach patients. We urge the FDA to find a swift path forward so that boys living with MPS II and their families have the chance for a better life." About RGX-121 (clemidsogene lanparvovec) RGX-121 is a potential one-time gene therapy for the treatment of boys with MPS II, designed to deliver the iduronate-2-sulfatase (IDS) gene to the CNS. Delivery of the IDS gene within cells in the CNS could provide a permanent source of secreted iduronate-2-sulfatase (I2S) protein beyond the blood-brain barrier, allowing for long-term cross correction of cells throughout the CNS. RGX-121 expressed protein is structurally identical to normal I2S. The BLA for RGX-121 for MPS II was supported by positive biomarker, functional and safety data from the CAMPSIITE I/II/III trial, including out to 12 months. RGX-121 has been well tolerated in all patients dosed across all phases of the CAMPSIITE trial. RGX-121 has received Orphan Drug Product, Rare Pediatric Disease, Fast Track and Regenerative Medicine Advanced Therapy (RMAT) designations from the FDA and advanced therapy medicinal products (ATMP) classification from the European Medicines Agency. About Mucopolysaccharidosis Type II (MPS II) MPS II, or Hunter Syndrome, is a rare, X-linked recessive disease caused by a deficiency in the lysosomal enzyme I2S leading to an accumulation of glycosaminoglycans (GAGs), including heparan sulfate (HS) in tissues which ultimately results in cell, tissue, and organ dysfunction, including in the central nervous system (CNS). In severe forms of the disease, early developmental milestones may be met, but developmental delay is readily apparent by 18 to 24 months. Specific treatment to address the neurological manifestations of MPS II remains a significant unmet medical need. Key biomarkers of I2S enzymatic activity in MPS II patients include its substrate CSF HS D2S6, which has been shown to correlate with neurocognitive manifestations of the disorder. ABOUT REGENXBIO Inc. REGENXBIO is a biotechnology company on a mission to improve lives through the curative potential of gene therapy. Since its founding in 2009, REGENXBIO has pioneered the field of AAV gene therapy. REGENXBIO is advancing a late-stage pipeline of one-time treatments for rare and retinal diseases, including RGX-202 for the treatment of Duchenne; clemidsogene lanparvovec (RGX-121) for the treatment of MPS II and RGX-111 for the treatment of MPS I, both in partnership with Nippon Shinyaku; and surabgene lomparvovec (ABBV-RGX-314) for the treatment of wet AMD and diabetic retinopathy, in collaboration with AbbVie. Thousands of patients have been treated with REGENXBIO's AAV platform, including those receiving Novartis' ZOLGENSMA®. REGENXBIO's investigational gene therapies have the potential to change the way healthcare is delivered for millions of people. For more information, please visit . FORWARD-LOOKING STATEMENTS This press release includes "forward-looking statements," within the meaning of Section 27A of the Securities Act of 1933, as amended, and Section 21E of the Securities Exchange Act of 1934, as amended. These statements express a belief, expectation or intention and are generally accompanied by words that convey projected future events or outcomes such as "believe," "may," "will," "estimate," "continue," "anticipate," "assume," "design," "intend," "expect," "could," "plan," "potential," "predict," "seek," "should," "would" or by variations of such words or by similar expressions. The forward-looking statements include statements relating to, among other things, REGENXBIO's future operations, clinical trials, costs and cash flow. REGENXBIO has based these forward-looking statements on its current expectations and assumptions and analyses made by REGENXBIO in light of its experience and its perception of historical trends, current conditions and expected future developments, as well as other factors REGENXBIO believes are appropriate under the circumstances. However, whether actual results and developments will conform with REGENXBIO's expectations and predictions is subject to a number of risks and uncertainties, including the timing of enrollment, commencement and completion and the success of clinical trials conducted by REGENXBIO, its licensees and its partners, the timing of commencement and completion and the success of preclinical studies conducted by REGENXBIO and its development partners, the timing or likelihood of payments from AbbVie or Nippon Shinyaku, the monetization of any priority review voucher, the timely development and launch of new products, the ability to obtain and maintain regulatory approval of product candidates, the ability to obtain and maintain intellectual property protection for product candidates and technology, trends and challenges in the business and markets in which REGENXBIO operates, the size and growth of potential markets for product candidates and the ability to serve those markets, the rate and degree of acceptance of product candidates, and other factors, many of which are beyond the control of REGENXBIO. Refer to the "Risk Factors" and "Management's Discussion and Analysis of Financial Condition and Results of Operations" sections of REGENXBIO's Annual Report on Form 10-K for the year ended December 31, 2024, and comparable "risk factors" sections of REGENXBIO's Quarterly Reports on Form 10-Q and other filings, which have been filed with the SEC and are available on the SEC's website at . All of the forward-looking statements made in this press release are expressly qualified by the cautionary statements contained or referred to herein. The actual results or developments anticipated may not be realized or, even if substantially realized, they may not have the expected consequences to or effects on REGENXBIO or its businesses or operations. Such statements are not guarantees of future performance and actual results or developments may differ materially from those projected in the forward-looking statements. Readers are cautioned not to rely too heavily on the forward-looking statements contained in this press release. These forward-looking statements speak only as of the date of this press release. Except as required by law, REGENXBIO does not undertake any obligation, and specifically declines any obligation, to update or revise any forward-looking statements, whether as a result of new information, future events or otherwise. Zolgensma® is a registered trademark of Novartis Gene Therapies. All other trademarks referenced herein are registered trademarks of REGENXBIO. CONTACTS: Dana Cormack Corporate Communications [email protected] George E. MacDougall Investor Relations [email protected] SOURCE REGENXBIO Inc. 21% more press release views with Request a Demo

基因疗法孤儿药快速通道临床申请临床研究

100 项与 Surabgene Lomparvovec 相关的药物交易

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适应症	最高研发状态	国家/地区	公司	日期
脉络膜新生血管	临床3期	美国	AbbVie, Inc.	2022-01-13
脉络膜新生血管	临床3期	日本	AbbVie, Inc.	2022-01-13
脉络膜新生血管	临床3期	加拿大	AbbVie, Inc.	2022-01-13
脉络膜新生血管	临床3期	法国	AbbVie, Inc.	2022-01-13
脉络膜新生血管	临床3期	德国	AbbVie, Inc.	2022-01-13
脉络膜新生血管	临床3期	匈牙利	AbbVie, Inc.	2022-01-13
脉络膜新生血管	临床3期	意大利	AbbVie, Inc.	2022-01-13
脉络膜新生血管	临床3期	西班牙	AbbVie, Inc.	2022-01-13
脉络膜新生血管	临床3期	英国	AbbVie, Inc.	2022-01-13
II型糖原贮积病	临床3期	美国	AbbVie, Inc.	2022-01-13

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研究	分期	人群特征	评价人数	分组	结果	评价	发布日期


EURETINA2025	临床1/2期	湿性年龄相关性黄斑变性	10	ABBV-RGX-314 (bilateral choroidal neovascularization secondary to age-related macular degeneration)	襯製衊糧蓋鑰憲鏇齋廠(夢壓淵鹽遞鹽鹹願築鹹) = 觸蓋窪觸鏇網獵蓋鏇願觸選艱網衊蓋廠鏇衊襯 (繭淵顧遞鏇壓壓顧鏇顧 ) 更多	积极	2025-09-04
NCT04514653 (AAVIATE, Corporate Publications) 人工标引	临床2期	湿性黄斑变性	106	ABBV-RGX-314	襯簾夢憲選蓋齋簾夢築(齋蓋夢繭獵壓醖獵積觸) = in the study eye were mild or moderate and included conjunctival hemorrhage, increased intraocular pressure, episcleritis, and conjunctival hyperemia. 襯艱夢夢觸鏇壓蓋範繭 (顧獵範憲齋獵餘餘遞遞 ) 更多	积极	2024-01-16
EURETINA2023	N/A	年龄相关性黄斑变性	-	RGX-314	餘膚簾鹹選鑰蓋醖膚餘(鹽淵顧糧繭壓觸繭顧選) = No new drug-related ocular adverse events (AEs) have been reported in Cohorts 1-4 憲獵夢積襯襯壓遞襯淵 (艱襯壓艱網選簾蓋遞顧 ) 更多	-	2023-10-05
EURETINA2023	N/A	糖尿病性黄斑水肿	-	RGX-314 at a dose level of 2.5 x E11 GC/eye	齋壓鑰製選製鏇衊築糧(齋廠網衊簾鹽艱襯範選) = three cases of mild intraocular inflammation through 6 months which resolved with topical corticosteroids 淵鹹憲積憲餘築顧觸簾 (鹹選壓鹽鬱淵艱製醖廠 ) 更多	-	2023-10-05
EURETINA2023	N/A	糖尿病性黄斑水肿	-	RGX-314 at an increased dose level of 5 x E11 GC/eye		-	2023-10-05
Phase I/IIa (ARVO2023)	临床1/2期	湿性年龄相关性黄斑变性	42	RGX-314	觸選鹹鹽艱鑰鹽觸廠壓(膚夢廠顧齋糧齋壓顧膚) = no new drug-related ocular adverse events reported in Cohorts 1-4 and one drug-related adverse event of significantly decreased BCVA in Cohort 5 積製築顧遞願壓窪衊艱 (醖夢願襯糧糧築繭窪艱 )	积极	2023-04-23
NCT04567550 (ALTITUDE, Corporate Publications) 人工标引	临床2期	糖尿病性视网膜病变	60	RGX-314	觸齋鹽蓋鏇獵簾壓襯顧(艱繭觸鏇選窪鹹艱醖齋) = 簾夢壓簾遞齋簾夢齋廠壓鹹繭窪鏇廠選窪餘鹹 (膚醖遞鑰觸鑰積襯窪顧 ) 更多	积极	2022-11-02
NCT04567550 (ALTITUDE, Corporate Publications) 人工标引	临床2期	糖尿病性视网膜病变	60	control	觸齋鹽蓋鏇獵簾壓襯顧(艱繭觸鏇選窪鹹艱醖齋) = 壓蓋鏇簾鑰蓋蓋觸網醖壓鹹繭窪鏇廠選窪餘鹹 (膚醖遞鑰觸鑰積襯窪顧 ) 更多	积极	2022-11-02
NCT04567550 (ALTITUDE, Corporate Publications) 人工标引	临床2期	糖尿病性视网膜病变	20	RGX-314	網淵齋獵鹹築廠夢膚憲(淵觸糧鬱簾獵網襯鹹選) = 獵鑰淵廠蓋觸鬱製觸遞鹹積壓願選製壓鑰醖網 (鹽蓋願襯鹹觸願壓築鹽 ) 更多	积极	2022-09-13
NCT04567550 (ALTITUDE, Corporate Publications) 人工标引	临床2期	糖尿病性视网膜病变	20	Observational	網淵齋獵鹹築廠夢膚憲(淵觸糧鬱簾獵網襯鹹選) = 鑰鑰廠醖齋鏇窪網淵簾鹹積壓願選製壓鑰醖網 (鹽蓋願襯鹹觸願壓築鹽 ) 更多	积极	2022-09-13
NCT04514653 (AAVIATE, PRNewswire) 人工标引	临床2期	湿性年龄相关性黄斑变性	19	RGX-314	鏇遞觸衊齋築鹽淵選繭(淵積壓蓋衊鑰觸獵構糧) = 糧築鬱鑰艱範壓遞壓簾選網鹹範廠簾選築顧繭 (鏇蓋製廠選顧鹽鑰選淵 ) 更多	积极	2021-10-01
NCT04514653 (AAVIATE, PRNewswire) 人工标引	临床2期	湿性年龄相关性黄斑变性	19	Ranibizumab	鏇遞觸衊齋築鹽淵選繭(淵積壓蓋衊鑰觸獵構糧) = 夢廠獵蓋艱製獵繭夢襯選網鹹範廠簾選築顧繭 (鏇蓋製廠選顧鹽鑰選淵 ) 更多	积极	2021-10-01
EURETINA2021	N/A	湿性年龄相关性黄斑变性	-	RGX-314	壓壓廠齋醖夢鑰選鹽憲(醖鹽構鹽蓋構糧製淵積) = 20 serious adverse events (SAEs) reported in 13 patients, including one possibly drug-related SAE of significant decrease in vision in Cohort 5 簾廠繭網積淵醖築鑰鏇 (鹹廠築積鏇網夢繭夢觸 ) 更多	-	2021-09-01
RGX-314 (ASGCT2020)	临床1/2期	湿性年龄相关性黄斑变性	42	RGX-314 gene therapy	膚製襯淵廠齋觸艱遞鏇(積築廠鏇憲鏇範壓憲鹽) = improved central retinal thickness (-83 µm) 憲窪願網鏇積築積願齋 (鹽顧獵艱憲齋窪壓廠鑰 ) 更多	积极	2020-04-28