An Operationally Seamless Phase 2b/3, Multicenter, Randomized, Masked, Sham-controlled Study to Evaluate the Efficacy and Safety of Surabgene Lomparvovec (Sura-vec) Delivered Via Suprachoroidal Space (SCS) Injection Targeting Subjects With Diabetic Retinopathy Without Center Involved-Diabetic Macular Edema (CI-DME) (NAAVIGATE)

Diabetic Retinopathy (DR) is a common eye condition caused by diabetes, where high blood sugar levels damage the blood vessels in the back part of the eye (called the retina). Over time, this damage can lead to vision problems and even blindness if not treated. This study will assess surabgene lomparvovec (sura-vec) as a potential one-time gene therapy administered in the suprachoroidal space (SCS) for the treatment of diabetic retinopathy (DR) and prevention of vision-threatening events (VTEs) in participants with non-proliferative DR (NPDR) without center-involved diabetic macular edema (CI-DME).
This study will consist of 3 portions: a Phase 2b portion, a Phase 3 portion, and a bilateral treatment portion. Approximately 576 adult participants will be enrolled in the study across multiple sites in the United States and Puerto Rico.
In the Phase 2b and Phase 3 portions, participants will be randomized to different groups to receive sura-vec and prophylactic steroids or sham and artificial tears in their study eye. If assigned to sham, participants will be given an opportunity to cross over and receive treatment with sura-vec. In the bilateral treatment portion, participants will be enrolled to receive sura-vec and prophylactic steroids in both eyes. In all 3 portions, follow-up in the study will continue through 5 years following administration of sura-vec in each eye.
There may be higher treatment burden for participants in this trial compared to their standard of care. Participants will attend regular visits during the study at a 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2026-05-20

申办/合作机构

AbbVie, Inc.

NCT07007065

/ Recruiting临床3期

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

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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）

2026-05-01·CURRENT OPINION IN OPHTHALMOLOGY

Emerging solutions for neovascular age-related macular degeneration

Review

作者: Wubben, Thomas J ; Franco, Jovany J

Purpose of review:

To summarize emerging therapeutic strategies for neovascular (wet) age-related macular degeneration (nAMD), with emphasis on recent translational and clinical developments.

Recent findings:

The nAMD treatment landscape is rapidly evolving. Gene therapies (e.g. ABBV-RGX-314, ADVM-022, and 4D-150) have demonstrated sustained intraocular anti-VEGF expression with reduced injection burden in phase 2 and 3 programs, validating the ‘biofactory’ concept. Tyrosine kinase inhibitors delivered via intravitreal or suprachoroidal implants (e.g. EYP-1901, OTX-TKI, and CLS-AX) show potential for twice-yearly or less frequent dosing. Moreover, emerging therapeutic approaches increasingly target non-VEGF pathogenic pathways, reflecting a shift toward mechanistically diverse vascular stabilization and neuroprotection strategies. These include multitargeted biologics that couple anti-angiogenic and anti-inflammatory effects (e.g. KSI-501, IBI-302, and AG-73305), as well as agents modulating FGF2 signaling, Wnt activation, complement regulation, and cellular metabolism.

Summary:

Therapeutic innovation in nAMD is transitioning from incremental refinements in intravitreal anti-VEGF delivery to strategies aimed at extending durability or targeting alternative contributory pathways. Long-term safety, efficacy, and durability will determine which of these candidates redefine standard care.

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.

2025-07-01·International ophthalmology clinics

Gene Therapy in Age-related Macular Degeneration

Review

作者: Zhou, Henry W ; Kim, Leo A

Recent advances in gene therapy and salient features of the current AMD therapeutic landscape have led to increased interest in applying gene therapy approaches to AMD. This review will discuss approaches to drug administration, viral and non-viral delivery vectors, and current trials in gene therapy for both wet and dry AMD. Drug administration routes include subretinal, intravitreal, and suprachoroidal approaches. Viral vectors include adenoviral, lentiviral, and adeno-associated viral (AAV) vectors. Non-viral vectors include lipid nanoparticle (LNP) and polymer-based vectors. Current trials in wet AMD include ADVM-022 and RGX-314. Current trials in dry AMD include GT-005 and JNJ-1887.

210

项与 Surabgene Lomparvovec 相关的新闻（医药）

2026-05-20

·PRNewswire

REGENXBIO Announces Positive Topline Results from Pivotal Phase III AFFINITY DUCHENNE® Study of RGX-202

Achieved primary endpoint with high statistical significance; 93% of patients achieved microdystrophin expression above 10% (pStatistically significant correlation between RGX-202 microdystrophin expression and functional improvement (NSAA n=9), supporting validity of surrogate endpoint Well-tolerated, differentiated safety profile Company preparing for potential accelerated approval in 2027 Webcast to be held at 8:00 a.m. ET today May 14, 2026 -- REGENXBIO Inc. (Nasdaq: RGNX) announced positive topline and interim functional data from the pivotal Phase III portion of the Phase I/II/III AFFINITY DUCHENNE® trial of RGX-202, a potential best-in-class gene therapy for Duchenne Muscular Dystrophy. The trial met its primary endpoint with high statistical significance (p<0.0001), with 93% of participants reaching at least 10% microdystrophin expression at Week 12 (n=30). Additionally, RGX-202 demonstrated statistically significant correlation between microdystrophin expression and interim functional improvement. "These topline results are exciting for the Duchenne community," said Pat Furlong, Founding President of Parent Project for Muscular Dystrophy. "For decades, our community has pushed for therapies that can change the trajectory of this disease, and today's news gives us renewed optimism. Our families cannot wait; regulatory flexibility for innovative medicines to treat rare disease remains an urgent priority. We applaud the dedication of the patients and families who participated in this research and look forward to continued progress toward delivering stronger futures for people with Duchenne." "Duchenne muscular dystrophy is a rare, progressive neuromuscular disease characterized by worsening muscle weakness and loss of function, and there continues to be a critical unmet need for therapies that can reliably alter the course of the disease", said AFFINITY DUCHENNE principal investigator Aravindhan Veerapandiyan, M.D., Arkansas Children's Hospital. "It's encouraging to see robust microdystrophin expression, correlation with functional outcomes, and a manageable safety profile. These data give us hope and reinforce the potential of RGX-202 to positively impact disease progression in individuals with Duchenne." "RGX-202 is the first gene therapy in development for Duchenne to demonstrate strong, statistically significant correlation between microdystrophin expression and functional improvement, a landmark distinction in the field," said Steve Pakola, M.D., Chief Medical Officer of REGENXBIO. "Today's topline results underscore how our novel construct and differentiated therapeutic approach support a favorable safety profile and potential clinical benefit, including in older patients where progressive decline is expected. These data support the potential of RGX-202 to become a best-in-class gene therapy for Duchenne patients." The pivotal portion of the Phase I/II/III AFFINITY DUCHENNE trial evaluated RGX-202 at 2x1014 GC/kg in 31 ambulatory boys aged 1 year of age and older. Key topline interim results include safety (n=31), biomarker (n=30), and functional data (n=9 aged >4 years, 12 months post-treatment).1 More than 20 additional participants have been enrolled in the confirmatory trial of RGX-202 (n=30), and the Company expects to have completed dosing in all 60 patients across the pivotal and confirmatory trials by mid-year. 93% of participants achieved >10% RGX-202 microdystrophin expression at Week 12 (pMicrodystrophin expression averaged 71.1% across all participants, and 41.6% in older boys, aged >8 years. Additionally, 80% of participants achieved >40% microdystrophin expression. RGX-202 was appropriately localized to the sarcolemma, demonstrating that the differentiated construct with the inclusion of the C-Terminal (CT) domain is appropriately targeting the muscle. Additionally, robust vector copies per nucleus and percent positive fibers observed support the potential for sustained microdystrophin expression. Duchenne is a severe, progressive, degenerative muscle disease, affecting 1 in 3,500 to 5,000 boys born each year worldwide. Duchenne is caused by mutations in the Duchenne gene which encodes for dystrophin, a protein involved in muscle cell structure and signaling pathways. Without dystrophin, muscles throughout the body degenerate and become weak, eventually leading to loss of movement and independence, required support for breathing, cardiomyopathy and premature death. 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. The content above comes from the network. if any infringement, please contact us to modify.

临床结果

2026-05-19

·劲帆生物前沿

REGENXBIO RGX-202 DMD AAV疗法III期数据亮眼，为罕见病患者迎来全新治疗转机

新闻资讯全球AAV基因治疗领军企业REGENXBIO于2026年5月14日连发两大重磅公告：旗下杜氏肌营养不良症（DMD）基因疗法RGX-202关键性Ⅲ期研究达主要终点，数据惊艳；同日发布2026年第一季度财报，管线全面推进，现金储备可支撑至2027年初。 RGX-202：DMD治疗里程碑，Ⅲ期数据全线告捷 RGX-202是REGENXBIO自主研发的潜在同类最优（Best-in-class）DMD AAV基因疗法，旨在通过靶向表达新型微肌营养不良蛋白，从根源上修复DMD致病基因缺陷。核心设计优势：唯一含C端结构域的微肌营养不良蛋白，更接近天然蛋白，可有效保护肌肉功能；创新载体设计、主动短期免疫抑制方案以及行业领先纯度（完整衣壳＞80%），安全性更优。试验设计：Ⅰ/Ⅱ/Ⅲ期AFFINITY DUCHENNE®试验，关键Ⅲ期入组31例、≥1岁可行走男性患儿，给药剂量2×1014GC/kg；主要终点为第12周微肌营养不良蛋白表达率。顶线关键数据（2026年4月16日数据截止）： 1.主要终点（n=30）：93%患者微肌营养不良蛋白表达＞10%，统计学意义高度显著（p＜0.0001）；全体平均表达率71.1%，＞8岁大龄患儿达41.6%；80%患者表达＞40%。 2.功能疗效（n=9，治疗1年）：第12周蛋白表达水平与12个月后运动功能改善（NSAA评分、起立/行走/攀爬计时测试）呈极强统计学相关性（r=0.94，p=0.0002），首次证实蛋白表达可直接转化为功能获益，疾病进展显著逆转。 3.安全性（n=31）：耐受性良好，仅2例严重不良事件（8岁亚急性心肌炎、10岁无症状肝损伤），均数周内缓解无后遗症；常见轻中度反应为呕吐、疲劳、恶心，无长期肝损伤信号。 4.监管进展：与FDA沟通顺利，同意以蛋白表达作为替代终点，支持2027年加速获批计划；确证试验已入组20+例，预计2026年中完成全部60例给药。图1 给药1年后，RGX-202治疗组受试者各项功能评估指标均优于外部对照组图2 RGX-202微肌营养不良蛋白表达水平与机体功能改善呈正相关肌肉营养不良症家长互助项目创始主席Pat Furlong表示：“这份顶线数据让整个DMD病患群体倍感振奋。数十年来，我们一直期盼能够改变疾病发展进程的治疗手段，如今这一消息再次带来希望。患病家庭早已迫切等待新药落地，为罕见病创新药物开通灵活审批通道依旧是当下紧要任务。我们由衷感谢所有参与本次研究的患者与家属，也期待研发进程持续推进，助力杜氏肌营养不良患者拥有更好的未来。” 阿肯色州儿童医院、AFFINITY DUCHENNE试验首席研究员Aravindhan Veerapandiyan, M.D.称：“DMD是一类罕见的进行性神经肌肉疾病，患者肌肉力量持续减弱、身体功能不断衰退，临床上依旧极度缺乏能够有效干预疾病进程的治疗方案。此次试验中观察到可观的microdystrophin表达水平，且其与功能改善存在明确关联，同时药物安全性整体可控。这些数据令人备受鼓舞，也进一步印证RGX-202具备改善杜氏肌营养不良患者疾病进展的潜力。” REGENXBIO首席医疗官Steve Pakola, M.D.表示：“RGX-202是首款在杜氏肌营养不良研发领域，证实microdystrophin表达与功能改善存在显著统计学关联的在研基因疗法，是行业内具有里程碑意义的突破。本次顶线结果证实，我们独创的载体结构与差异化治疗策略，让药物具备良好安全属性与可观临床获益，即便是身体机能持续衰退的大龄患者也能从中获益。现有数据充分证明，RGX-202有望成为治疗杜氏肌营养不良的同类最优基因疗法。” 视网膜管线 sura-vec（ABBV-RGX-314）稳步冲刺关键节点与艾伯维（AbbVie）合作的湿性AMD/糖尿病视网膜病变AAV基因疗法sura-vec进展顺利：湿性AMD（脉络膜下腔给药）：ATMOSPHERE®/ASCENT®关键试验2026年Q4公布顶线数据，2027年启动全球监管申报。糖尿病视网膜病变（脉络膜上腔给药）：Ⅱb/Ⅲ期NAAVIGATE研究美国中心已启动入组，预计2026年Q2完成首例给药，触发艾伯维1亿美元里程碑付款。湿性AMD（脉络膜上腔给药）：Ⅱ期AAVIATE®试验已完成入组。罕见病管线 RGX-121解除临床暂停，全球布局加速 RGX-121（亨特综合征/MPS Ⅱ）：FDA解除部分临床暂停，公司正积极沟通后续开发路径；同系列RGX-111（Hurler综合征/MPS Ⅰ）同步推进，与日本新药（Nippon Shinyaku）合作开发。作为AAV基因治疗领域的先行者，REGENXBIO凭借RGX-202的突破性数据，首次在DMD领域证实基因治疗可实现“蛋白表达→功能改善”的直接关联，为全球DMD患者带来治愈曙光。新闻来源： https://ir.regenxbio.com/news-releases/news-release-details/regenxbio-reports-first-quarter-2026-financial-results-and https://ir.regenxbio.com/news-releases/news-release-details/regenxbio-announces-positive-topline-results-pivotal-phase-iii END 劲帆医药自主研发的Bac/Sf9昆虫杆状病毒系统，拥有多项全球领先的专利技术，在AAV病毒及疫苗规模化生产中，实现提速、降本、增效，为合作伙伴管线商业化竞争赋能。劲帆医药劲帆医药与国内外众多家药企、科研单位、医疗院所建立合作关系，已提供优质、高效、前沿的工具病毒和技术支持服务20000+。关于劲帆医药劲帆生物医药科技（武汉）有限公司简称“劲帆医药”，创立于2022年，提供一站式病毒载体、蛋白和疫苗CRO/CDMO服务，拥有全球领先的规模化AAV制备专利技术平台及病毒载体/cGMP级蛋白/疫苗生产车间，致力于推进基因治疗药物、蛋白药物、治疗性疫苗更有效，更安全，更经济，更可及，赋能客户，造福患者。联系我们电话：17720522078 官网：www.genevoyager.com 邮箱：marketing@genevoyager.com 地址：中国武汉东湖高新区光谷七路128号微信：Genevoyager2022 扫码进入官网扫码联系客服 1. 全球首款！AAV基因治疗迈入代谢病领域，Fractyl糖尿病疗法获批临床 2. 拜耳庞贝病AAV基因疗法完成全球首例给药，有望摆脱长期用药依赖！ 3. 临床数据亮眼！Atsena双管线推进，眼科基因疗法迎来突破 4. 全球首个遗传性耳聋AAV基因疗法Otarmeni获批上市，一次注射重获自然听力

2026-05-18

·PRNewswire

REGENXBIO to Participate in Upcoming Investor Conferences

ROCKVILLE, Md., May 18, 2026 /PRNewswire/ -- REGENXBIO Inc. (Nasdaq: RGNX) today announced it will participate in the following investor conferences: 2026 RBC Capital Markets Global Healthcare Conference Fireside Chat: Wednesday, May 20 at 9:30am ET Location: New York, NY Stifel 2026 Virtual Ophthalmology Forum Fireside Chat: Tuesday, May 26 at 9:30am ET Location: Virtual Live webcasts of select events can be accessed in the Investors section of REGENXBIO's website at . Archived replays of the webcasts will be available for approximately 30 days following the events. 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 . Contacts: Dana Cormack Corporate Communications [email protected] Investors: George E. MacDougall Investor Relations [email protected] SOURCE REGENXBIO Inc. 21% more press release views with Request a Demo

基因疗法

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
糖尿病性黄斑水肿	临床3期	美国	AbbVie, Inc.	2026-05-20
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

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临床结果

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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)	壓觸構壓餘繭鬱願鏇襯(顧簾顧構艱選鬱蓋窪壓) = 廠壓齋繭觸糧衊觸衊簾築窪築網繭醖餘膚糧選 (鏇鑰積醖積願淵繭遞鏇 ) 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	鑰襯壓簾憲鬱衊鹽製繭(構網淵窪製壓構鬱餘遞) = in the study eye were mild or moderate and included conjunctival hemorrhage, increased intraocular pressure, episcleritis, and conjunctival hyperemia. 糧製築鹽壓壓鏇選遞鬱 (簾積淵餘糧壓糧鑰顧觸 ) 更多	积极	2024-01-16
EURETINA2023	N/A	年龄相关性黄斑变性	-	RGX-314	簾齋遞憲鑰鏇壓選糧獵(襯鹹壓憲鹽鹽夢積顧獵) = No new drug-related ocular adverse events (AEs) have been reported in Cohorts 1-4 艱壓鏇壓醖範製壓糧鹹 (膚廠窪襯糧製構製範顧 ) 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	顧醖構獵膚選遞製鹽廠(憲鹹願鬱鹹衊選衊艱膚) = three cases of mild intraocular inflammation through 6 months which resolved with topical corticosteroids 蓋網淵壓蓋築積夢選構 (鹽製繭遞鏇壓鹽糧淵鹽 ) 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	鏇齋鑰餘製簾獵襯膚窪(鑰襯衊選獵鑰繭繭壓壓) = 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 襯積醖範衊糧餘襯鬱鹹 (簾醖鏇淵糧積製遞膚願 )	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	觸蓋鑰網獵夢憲製鏇鑰(鹽鑰醖衊遞願憲觸糧衊) = 艱繭遞艱製繭襯築製膚壓窪鑰繭網構簾醖衊遞 (蓋遞壓艱範網願憲網範 ) 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	觸蓋鑰網獵夢憲製鏇鑰(鹽鑰醖衊遞願憲觸糧衊) = 範範淵顧膚餘遞鏇遞衊壓窪鑰繭網構簾醖衊遞 (蓋遞壓艱範網願憲網範 ) 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	鹽獵廠獵糧觸夢壓憲遞(廠醖鬱製構構顧襯簾齋) = 艱積醖蓋願獵壓網淵鏇蓋觸襯構願窪築衊積築 (願製鬱淵齋獵壓窪鬱構 ) 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	鹽獵廠獵糧觸夢壓憲遞(廠醖鬱製構構顧襯簾齋) = 衊獵鑰鑰顧顧齋簾顧獵蓋觸襯構願窪築衊積築 (願製鬱淵齋獵壓窪鬱構 ) 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	齋築餘蓋鏇鹽鑰襯窪窪(衊膚獵製醖餘齋製簾顧) = 選鹹選鹹選鑰艱齋壓蓋醖鏇蓋網鏇鑰鏇膚廠衊 (選鹹齋鹹餘夢繭鹽網積 ) 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	齋築餘蓋鏇鹽鑰襯窪窪(衊膚獵製醖餘齋製簾顧) = 獵築淵築築衊獵構醖夢醖鏇蓋網鏇鑰鏇膚廠衊 (選鹹齋鹹餘夢繭鹽網積 ) 更多	积极	2021-10-01
EURETINA2021	N/A	湿性年龄相关性黄斑变性	-	RGX-314	膚窪醖糧鹹遞鏇鹹簾蓋(齋顧蓋衊願窪憲觸範築) = 20 serious adverse events (SAEs) reported in 13 patients, including one possibly drug-related SAE of significant decrease in vision in Cohort 5 觸鹹艱鏇鑰餘願鹹襯襯 (顧構餘廠憲觸遞繭繭簾 ) 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	艱衊廠網蓋鹹顧繭繭範(遞簾鏇齋憲廠蓋獵顧築) = improved central retinal thickness (-83 µm) 鏇鹽觸夢範艱醖構夢願 (糧鹹鬱衊選築觸醖鬱壓 ) 更多	积极	2020-04-28