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2021-12-28

申办/合作机构

AbbVie, Inc.

[+1]

NCT05210803

/ Enrolling by invitationN/A

A Long-term Follow-Up Study to Evaluate the Safety and Efficacy of Suprachoroidal Administration of RGX-314 for Participants With Neovascular Age-Related Macular Degeneration

This is a prospective, observational study designed to evaluate the long-term safety and efficacy of RGX-314. Eligible participants are those who were previously enrolled in a clinical study of nAMD in which they received suprachoroidal space (SCS) administration of RGX-314. Enrollment of each participant in the current study should occur after the participant has completed either the end of study or early discontinuation visit in the previous (parent) clinical study. Participants will be followed for up to 5 years after RGX-314 administration (inclusive of the parent study). As such, the total study duration for each participant may vary depending on when they enroll in the current study following RGX-314 administration in the parent study.

开始日期2021-12-20

申办/合作机构

AbbVie, Inc.

NCT04832724

/ Completed临床2期

A Phase 2, Open-label Study to Explore the Pharmacodynamics of Two Doses in Two Formulations of RGX-314 Gene Therapy Administered Via Subretinal Delivery in Participants With Neovascular Age-related Macular Degeneration

RGX-314 is being developed as a novel one-time gene therapy for the treatment of neovascular (wet) age-related macular degeneration (nAMD) also referred to as Wet AMD. Wet AMD is characterized by loss of vision due to new, leaky blood vessel formation in the retina. The purpose of this phase 2, open label study is to evaluate whether different doses of RGX-314 from two different formulations (clinical versus eventual commercial formulation) perform the same in humans when delivered by subretinal administration

开始日期2021-02-22

申办/合作机构

AbbVie, Inc.

100 项与 RGX-314 相关的临床结果

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100 项与 RGX-314 相关的转化医学

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100 项与 RGX-314 相关的专利（医药）

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项与 RGX-314 相关的文献（医药）

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.

2024-12-01·AMERICAN JOURNAL OF OPHTHALMOLOGY

Subretinal Gene Therapy for Treatment of Retinal and Choroidal Vascular Diseases

作者: Gahn, Greggory M ; Khan, Hannah ; Aziz, Aamir A ; Khan, Huma ; Sulahria, Humza ; Mojumder, Ohidul ; Khanani, Ibrahim ; Khanani, Zoha A ; Khanani, Arshad M ; Mishra, Kapil

OBJECTIVE:

This review article discusses investigational subretinal gene therapies for retinal vascular diseases, including AVA-101, an adeno-associated viral (AAV) 2 vector expressing soluble vascular endothelial growth factor (VEGF) receptor 1, ABBV-RGX-314, an AAV8 vector expressing an anti-VEGF-A antibody fragment, and EXG102-031, an AAV8 vector expressing a recombinant protein that blocks VEGF family members and angiopoietin 2.

DESIGN:

Review article CONCLUSION: Subretinal injection is a commonly used delivery route for investigational gene therapy agents which is theorized to provide relative immune privilege, thereby reducing the risk of inflammation, while providing high transgene expression in photoreceptors and retinal pigment epithelium. Subretinal injection of AVA-101 demonstrated safety and tolerability in Phase I and IIa trials, but failed to maintain visual acuity and control exudation. In contrast, subretinal injection of some doses of ABBV-RGX-314 have shown evidence of controlling exudation and the maintaining vision, as well as safety and tolerability, leading to two ongoing pivotal trials comparing subretinal delivery of two different doses of ABBV-RGX-314 versus intravitreal injections of 0.5mg ranibizumab or 2mg aflibercept. These preliminary results are an encouraging and welcome development in the search for efficacious, long-duration treatments for retinal vascular diseases.

2024-06-28·POSTGRADUATE MEDICAL JOURNAL

Advancements in the treatment of age-related macular degeneration: a comprehensive review

Review

作者: Papaioannou, Christos

Abstract:

Age-related macular degeneration (AMD) stands as a leading cause of irreversible blindness, particularly affecting central vision and impeding daily tasks. This paper provides a thorough exploration of AMD, distinguishing between its two main subtypes—Wet and Dry AMD—while shedding light on the prevalence and risk factors, including age, genetics, and smoking.The focus shifts to the current and future treatment landscape, examining both Dry and Wet AMD. Regarding Dry AMD, interventions such as antioxidant supplementation and ongoing clinical trials offer hope. Notable among these is Pegcetacoplan which is the only Food and Drug Administration (FDA)-approved medication, displaying promising results in reducing geographic atrophy lesions.For Wet AMD, anti-Vascular Endothelial Growth Factor therapies like Ranibizumab (Lucentis®) have been instrumental, and newer drugs like Faricimab and OPT-302 show comparable efficacy with extended dosing intervals. Additionally, gene therapies such as RGX-314 present a potential paradigm shift, reducing or eliminating the need for frequent injections. Biosimilars offer cost-effective alternatives.The paper also delves into the integration of technology and artificial intelligence in AMD management, highlighting the role of smartphone apps for patient monitoring and artificial intelligence algorithms for diagnosis and surveillance. Furthermore, patient perspectives on artificial intelligence demonstrate a positive correlation between understanding and trust.The narrative concludes with a glimpse into ground-breaking technologies, including retinal implants and bionic chips, offering hope for vision restoration. Overall, this paper underscores the multifaceted approach in addressing AMD, combining traditional and innovative strategies, paving the way for a more promising future in AMD treatment.

136

项与 RGX-314 相关的新闻（医药）

2025-01-28

·ir.clearsidebio.com

Clearside Biomedical Announces Multiple Medical Meeting Presentations Focused on the Advantages of Suprachoroidal Delivery and Key Differentiators in its CLS-AX Clinical Program

- Upcoming Presentations at Angiogenesis and Macula Society Conferences to Feature CLS-AX Sub-Group Analyses from ODYSSEY Wet AMD Trial - - CLS-AX Targets Flexible Dosing of Biologics with Duration of Tyrosine Kinase Inhibitors - ALPHARETTA, Ga., Jan. 28, 2025 (GLOBE NEWSWIRE) -- Clearside Biomedical, Inc. (Nasdaq: CLSD), a biopharmaceutical company revolutionizing the delivery of therapies to the back of the eye through the suprachoroidal space (SCS®), announced today recent and upcoming presentations at ophthalmic medical meetings highlighting Clearside’s suprachoroidal delivery technology and promising pipeline, including its Phase 3 ready CLS-AX program for the treatment of neovascular age-related macular degeneration (wet AMD). “Our medical meetings this quarter continue to demonstrate the commercial, clinical and regulatory expertise that establishes Clearside as the leader in suprachoroidal delivery,” said Victor Chong, MD, MBA, Chief Medical Officer and EVP, Head of Research and Development. “We are excited about the potential of our CLS-AX program and look forward to presenting additional data from our Phase 2b ODYSSEY trial at upcoming meetings. We believe suprachoroidal CLS-AX has the potential to deliver comparable 6-month therapeutic effect in most wet AMD patients, similar to other intravitreal TKIs in development, while allowing physicians to have more individualized and flexible dosing options, instead of rescue, for patients who need more frequent therapy. We also believe suprachoroidal delivery enables the precise application of therapy to the retina, which may result in improved safety over other intravitreal treatment options.” Recent Sessions on Suprachoroidal Drug Delivery Utilizing Clearside’s SCS Microinjector®: Hawaiian Eye & Retina 2025 (January 18-24, 2025) Presentation: Where Are We with Suprachoroidal Delivery Presenter: Judy E. Kim, MD, University of Texas Southwestern Medical Center Presentation: Suprachoroidal Delivery of Investigational ABBV-RGX-314 for Diabetic Retinopathy: The Phase II ALTITUDE® Study Presenter: Margaret Chang, MD, MS, Retinal Consultants Medical Group Presentation: Tyrosine Kinases Inhibitors Presenter: Rishi P. Singh, MD, Cleveland Clinic Presentation: Suprachoroidal Delivery of Triamcinolone Injectable Suspension for Post-Operative Cystoid Macular Edema Presenter: Irena Tsui, MD, Doheny Eye Center UCLA 3rd Annual Ophthalmic Drug Delivery Summit (January 28-30, 2025) Presentation: Advancing Targeted, Compartmentalized, & Long-Acting Depot Delivery Suprachoroidal Delivery of Particulate Formulations Presenter: Viral Kansara, PhD, Vice President, Preclinical Development, Clearside Biomedical Upcoming Sessions on CLS-AX Wet AMD Program Angiogenesis, Exudation, and Degeneration 2025 (Virtual; February 8, 2025) Presentation: Phase 2b CLS-AX ODYSSEY Trial Results Presenter: Roger Goldberg, MD, MBA, Bay Area Retinal Associates Medical Group The Macula Society 48th Annual Meeting (February 12-15, 2025) Presentation: Top Line Results from ODYSSEY: A Phase 2b Study of Suprachoroidally Administered CLS-AX in Participants with Neovascular Age-related Macular Degeneration Presenter: Thomas A. Ciulla, MD, MBA, Chief Medical Advisor-Retina and Chair, Scientific Advisory Board, Clearside Biomedical 5th Annual Wet AMD & Diabetic Eye Disease Drug Summit (March 18-20, 2025) Presentation: Transforming wAMD Treatment: Long-Lasting, Flexible Dosing with Suprachoroidal TKI Delivery Presenter: Victor Chong, MD, MBA, Chief Medical Officer, Clearside Biomedical About Clearside’s Suprachoroidal Space (SCS®) Injection Platform and SCS Microinjector® Clearside’s patent protected, proprietary suprachoroidal space (SCS®) injection treatment approach offers unprecedented access to the back of the eye, where sight-threatening disease often occurs. The Company’s unique platform is inherently flexible and intended to work with established and new formulations of medications. Clearside’s patented SCS Microinjector® can deliver a wide variety of drug candidates into the suprachoroidal space, providing targeted delivery to potentially improve efficacy and compartmentalization of medication to reduce or eliminate toxic effects on non-diseased cells. The SCS Microinjector is comprised of a syringe with a custom-designed hub and two 30-gauge hollow microneedles of varying lengths, each approximately one millimeter, optimizing insertion and suprachoroidal administration of drugs. About ODYSSEY Phase 2b Clinical Trial ODYSSEY was a randomized, double-masked, parallel-group, active-controlled, multicenter, 36-week, Phase 2b clinical trial in participants with wet AMD previously treated with intravitreal anti-vascular endothelial growth factor (VEGF) standard of care therapy. A total of 60 participants were treated for 36 weeks and randomized to either CLS-AX (1 mg) or aflibercept (2 mg) with a 2:1 randomization schedule (40 participants in CLS-AX arm and 20 participants in aflibercept arm). CLS-AX was administered via suprachoroidal injection using Clearside’s SCS Microinjector, and aflibercept was administered via intravitreal injection. Participants in the trial were determined to have active disease with a median duration of wet AMD diagnosis of 9.9 months. The ODYSSEY trial achieved its objectives, including primary outcomes in mean change from baseline in best corrected visual acuity and safety and tolerability of CLS-AX, and secondary outcomes in visual function and ocular anatomy, the need for supplemental treatment, and treatment burden as measured by total injections over the trial duration. CLS-AX demonstrated compelling intervention-free rates with 100% of CLS-AX participants not requiring any additional treatment up to 3 months, 90% up to 4 months, 81% up to 5 months, and 67% up to 6 months after the initial CLS-AX dose. In the CLS-AX group, the injection frequency was reduced by approximately 84% compared to the average monthly injections in the 24 weeks prior to screening. About CLS-AX (axitinib injectable suspension) Clearside is developing CLS-AX as a longer-acting therapy for the treatment of retinal diseases. CLS-AX (axitinib injectable suspension) is a proprietary suspension of axitinib for suprachoroidal injection. Axitinib is a tyrosine kinase inhibitor (TKI), currently approved as an oral tablet formulation to treat advanced renal cell carcinoma, that achieves pan-VEGF blockade, directly inhibiting VEGF receptors-1, -2, and -3 with high potency and specificity. Clearside believes this broad VEGF blockade may have efficacy advantages over existing retinal therapies by acting at a different level of the angiogenesis cascade and may benefit patients who sub-optimally respond to current, more narrowly focused anti-VEGF therapies. Suprachoroidal injection of this proprietary suspension of axitinib has demonstrated meaningful potential in Phase 1/2a and Phase 2b wet AMD clinical trials in which CLS-AX was well tolerated and demonstrated a positive safety profile. With suprachoroidal administration of axitinib, there is the potential to achieve prolonged duration and targeted delivery to affected tissue layers by compartmentalizing axitinib behind the retina, thereby limiting drug exposure to the front of the eye. About Clearside Biomedical, Inc. Clearside Biomedical, Inc. is a biopharmaceutical company revolutionizing the delivery of therapies to the back of the eye through the suprachoroidal space (SCS®) to improve patient outcomes. Clearside’s SCS injection platform, utilizing the Company’s patented SCS Microinjector®, enables an in-office, repeatable, non-surgical procedure for the targeted and compartmentalized delivery of a wide variety of therapies to the macula, retina, or choroid to potentially preserve and improve vision in patients with sight-threatening eye diseases. Clearside is developing its own pipeline of small molecule product candidates for administration via its SCS Microinjector. The Company’s lead program, CLS-AX (axitinib injectable suspension), is in development for the treatment of neovascular age-related macular degeneration (wet AMD). Planning for a Phase 3 program is underway. In addition, Clearside is evaluating various small molecules for the potential long-acting treatment of geographic atrophy (GA). Clearside developed and gained approval for its first product, XIPERE® (triamcinolone acetonide injectable suspension) for suprachoroidal use, which is available in the U.S. through a commercial partner. Clearside also strategically partners its SCS injection platform with companies utilizing other ophthalmic therapeutic innovations. For more information, please visit clearsidebio.com or follow us on LinkedIn and X. Cautionary Note Regarding Forward-Looking Statements Any statements contained in this press release that do not describe historical facts may constitute forward-looking statements as that term is defined in the Private Securities Litigation Reform Act of 1995. These statements may be identified by words such as “believe”, “expect”, “may”, “plan”, “potential”, “will”, and similar expressions, and are based on Clearside’s current beliefs and expectations. These forward-looking statements include statements regarding the potential benefits of CLS-AX, Clearside’s suprachoroidal delivery technology and Clearside’s SCS Microinjector®. These statements involve risks and uncertainties that could cause actual results to differ materially from those reflected in such statements. Risks and uncertainties that may cause actual results to differ materially include uncertainties inherent in the conduct of clinical trials, Clearside’s reliance on third parties over which it may not always have full control and other risks and uncertainties that are described in Clearside’s Annual Report on Form 10-K for the year ended December 31, 2023, filed with the U.S. Securities and Exchange Commission (SEC) on March 12, 2024, Clearside’s Quarterly Report on Form 10-Q for the quarter ended September 30, 2024, filed with the SEC on November 12, 2024, and Clearside’s other periodic reports filed with the SEC. Any forward-looking statements speak only as of the date of this press release and are based on information available to Clearside as of the date of this release, and Clearside assumes no obligation to, and does not intend to, update any forward-looking statements, whether as a result of new information, future events or otherwise. Source: Clearside Biomedical, Inc. Investor and Media Contacts: Jenny Kobin Remy Bernarda ir@clearsidebio.com

临床结果临床2期临床3期上市批准

2025-01-15

·派真生物PackGene

行业资讯 | 8.1亿美元！两款AAV基因疗法对外授权合作达成

2025年1月14日，REGENXBIO公司与Nippon Shinyaku（日本新药株式会社）宣布了关于AAV基因治疗领域的一项独家合作计划，旨在开发和商业化用于治疗黏多糖贮积症II型（MPS II，又称亨特综合征）的基因疗法RGX-121以及用于治疗黏多糖贮积症I型（MPS I，又称赫勒综合征）的基因疗法RGX-111。根据合作协议，REGENXBIO将获得1.1亿美元的预付款，并有可能在达到特定里程碑时获得高达7亿美元的额外付款。此外，REGENXBIO还将从在美国和亚洲地区的净销售额中获得一定比例的专利使用费。 REGENXBIO将继续负责这两种AAV基因治疗药物的制造工作，并保留对RGX-121优先审查凭证的所有权利及由此产生的任何收益。Nippon Shinyaku则将负责在美国和亚洲地区该基因疗法的商业化工作。预计此次交易将在2025年第一季度末完成，但需满足常规条件并获得必要的监管批准。这次合作结合了双方各自专业业务上的优势，以期为患有MPS II和MPS I的患者提供潜在的变革性治疗方法。 REGENXBIO的总裁兼首席执行官Curran M. Simpson表示，这次与Nippon Shinyaku的合作令人兴奋，因为它充分利用了双方的优势。RGX-121有望成为首个获批用于MPS II（亨特综合征）的基因疗法，预计最早在2025年末获得FDA批准。RGX-111在I/II期研究中显示出非常有希望的结果。凭借Nippon Shinyaku在罕见病领域的专长和强大的商业化能力，双方期待共同努力将这两种有前景的候选药物推向市场，造福患者。 Nippon Shinyaku的总裁Toru Nakai也表达了对此次合作的信心，非常高兴能与REGENXBIO这样的基因治疗开发和制造企业合作。 REGENXBIO是一家临床阶段生物技术公司，自2009年成立以来，它一直致力于AAV基因疗法的开发。该公司正在推进一系列针对视网膜和罕见疾病的AAV基因疗法的研发，包括与AbbVie合作开发用于治疗湿性AMD和糖尿病视网膜病变的ABBV-RGX-314，以及用于治疗Duchenne肌营养不良症的RGX-202等。目前，成千上万的患者已经接受了基于REGENXBIO的AAV基因治疗技术平台开发的创新基因疗法的治疗，其中包括诺华公司的用于治疗脊髓性肌肉萎缩症的AAV基因药物ZOLGENSMA（该款药物使用了REGENXBIO公司NAV®基因输送技术平台开发的AAV9病毒载体）。关于派真生物

引进/卖出基因疗法优先审批

2025-01-15

·Pharmaceutical Technology

Regenxbio and Nippon Shinyaku forge $810m gene therapy deal

The partnership centres on two of Regenxbio’s gene therapies, RGX-121 and RGX-111. Credit: Jinda Noipho via Getty Images. Regenxbio has entered into a strategic collaboration worth $810m with Japan-based Nippon Shinyaku to advance gene therapies targeting the rare metabolic disorder mucopolysaccharidosis (MPS). Under the terms of the deal, which centres on two of Regenxbio’s assets – RGX-121 and RGX-111 – Regenxbio will receive $110m upfront and is eligible for up to $700m in development, regulatory, and sales milestones. Nippon Shinyaku gains rights to co-develop and commercialise the therapies in specified markets. MPS includes a group of rare, inherited metabolic disorders caused by the absence or malfunctioning of specific enzymes required to break down glycosaminoglycans (GAGs), complex sugar molecules. The accumulation of GAGs leads to progressive tissue and organ damage, developmental delays, and in severe cases, early mortality. The most advanced candidate in the partnership, RGX-121 (clemidsogene lanparvovec), targets Hunter syndrome, also known as MPS II, a condition caused by a mutation in the iduronate-2-sulfatase (IDS) gene. RGX-121 is designed to deliver a functional copy of the IDS gene, addressing the underlying cause of the disease. Symptoms of Hunter syndrome include cognitive impairment, skeletal abnormalities, and organ enlargement. In September 2024, Regenxbio reported positive results from the Phase II/III CAMPSIITE trial (NCT03566043) of RGX-121, showing an 85% median reduction of cerebrospinal fluid (CSF) levels of heparan sulphate (HS) D2S6, a key biomarker linked to disease activity. In June 2024, the company announced progress with the US Food and Drug Administration (FDA) to pursue an accelerated approval pathway, with a rolling biologics license application (BLA) submission underway. An accelerated approval decision is expected in 2025, and Regenxbio retains rights to a priority review voucher (PRV) for RGX-121. The second asset, RGX-111, is being developed for mucopolysaccharidosis type I (MPS I), caused by mutations in the α-l-iduronidase (IDUA) gene. The gene therapy aims to deliver a functional copy of the IDUA gene directly to the central nervous system (CNS), potentially slowing cognitive decline and other symptoms. Interim data from an ongoing Phase I/II trial (NCT03580083) has shown a favourable safety profile and promising biomarker data indicative of CNS activity. Regenxbio continues to advance its broader pipeline of gene therapies for rare diseases. The company’s wet age-related macular degeneration (wAMD) programme, ABBV-RGX-314, partnered with AbbVie, is being evaluated in two pivotal trials , ATMOSPHERE (NCT04704921) and ASCENT (NCT05407636). Plans are also underway for a Phase III study of the therapy in diabetic retinopathy. Additionally, the company is progressing RGX-202, a gene therapy for Duchenne muscular dystrophy. Following positive data from a Phase I/II trial, Regenxbio has aligned with the FDA on an accelerated approval pathway, with a BLA submission anticipated in 2026. Cell & Gene Therapy coverage on Pharmaceutical Technology is supported by Cytiva . Editorial content is independently produced and follows the highest standards of journalistic integrity. Topic sponsors are not involved in the creation of editorial content. Free Whitepaper Optimise your cell therapy process: a guide to cell thawing Typically carried out at the point of care, errors in cell therapy thawing could compromise treatment efficacy, leading to significant patient impact as well as high costs and a compromised reputation for the product’s developer. This guide addresses how cell thawing has historically developed into the new techniques used today, along with the physical and biological implications of key metrics and components such as warming rate and ice structure. Also included are reviews of key studies from scientific literature and a consideration of the interactions between cooling and warming rates, as applicable to cell and gene therapies. Thank you. You will receive an email shortly. Please check your inbox to download the Whitepaper. By Cytiva Thematic By downloading this Whitepaper, you acknowledge that GlobalData may share your information with Cytiva Thematic and that your personal data will be used as described in their Privacy Policy

基因疗法临床3期临床结果优先审批引进/卖出

100 项与 RGX-314 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.	2021-12-28
脉络膜新生血管	临床3期	日本	AbbVie, Inc.	2021-12-28
脉络膜新生血管	临床3期	加拿大	AbbVie, Inc.	2021-12-28
脉络膜新生血管	临床3期	法国	AbbVie, Inc.	2021-12-28
脉络膜新生血管	临床3期	德国	AbbVie, Inc.	2021-12-28
脉络膜新生血管	临床3期	匈牙利	AbbVie, Inc.	2021-12-28
脉络膜新生血管	临床3期	意大利	AbbVie, Inc.	2021-12-28
脉络膜新生血管	临床3期	波多黎各	AbbVie, Inc.	2021-12-28
脉络膜新生血管	临床3期	西班牙	AbbVie, Inc.	2021-12-28
脉络膜新生血管	临床3期	英国	AbbVie, Inc.	2021-12-28

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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


NCT04514653 (AAVIATE, Corporate Publications) 人工标引	临床2期	湿性黄斑变性	106	ABBV-RGX-314	觸餘選積艱壓齋構築夢(鑰鑰鬱範繭鹹憲鏇簾衊) = in the study eye were mild or moderate and included conjunctival hemorrhage, increased intraocular pressure, episcleritis, and conjunctival hyperemia. 蓋蓋壓鹹鹽觸廠鑰夢範 (衊遞鹽觸壓壓壓網鏇構 ) 更多	积极	2024-01-16
EURETINA2023	N/A	糖尿病性黄斑水肿	-	RGX-314 at a dose level of 2.5 x E11 GC/eye	壓顧鏇網夢顧觸觸膚齋(顧網選膚鬱蓋構糧獵遞) = three cases of mild intraocular inflammation through 6 months which resolved with topical corticosteroids 醖廠艱簾廠築網廠構獵 (鹹齋鏇鹹獵製選範鑰艱 ) 更多	-	2023-10-05
				RGX-314 at an increased dose level of 5 x E11 GC/eye
EURETINA2023	N/A	年龄相关性黄斑变性	-	RGX-314	網壓積餘鏇積蓋廠簾顧(製壓艱積範壓製鏇繭鹹) = No new drug-related ocular adverse events (AEs) have been reported in Cohorts 1-4 獵夢網築選蓋廠選淵淵 (醖蓋醖顧鹽簾憲窪願願 ) 更多	-	2023-10-05
NCT04567550 (ALTITUDE, Corporate Publications) 人工标引	临床2期	糖尿病性视网膜病变	60	RGX-314	鹹糧積鬱艱鬱夢鏇蓋餘(構構憲鏇鑰鏇積構窪鹹) = 壓襯繭鹽鹹壓醖製範鹽遞衊觸網網蓋膚廠醖糧 (鏇艱鏇範衊簾壓構築觸 ) 更多	积极	2022-11-02
				control	鹹糧積鬱艱鬱夢鏇蓋餘(構構憲鏇鑰鏇積構窪鹹) = 襯醖壓鑰顧積醖願衊憲遞衊觸網網蓋膚廠醖糧 (鏇艱鏇範衊簾壓構築觸 ) 更多
NCT04567550 (ALTITUDE, Corporate Publications) 人工标引	临床2期	糖尿病性视网膜病变	20	RGX-314	醖獵鹽選製繭顧襯夢壓(壓淵構壓鬱網夢簾衊齋) = 鬱鑰選遞築繭壓製醖壓築蓋窪願鹹構繭艱襯夢 (蓋網壓觸積衊獵鹹繭衊 ) 更多	积极	2022-09-13
				Observational	醖獵鹽選製繭顧襯夢壓(壓淵構壓鬱網夢簾衊齋) = 衊夢鏇衊窪窪醖膚遞鏇築蓋窪願鹹構繭艱襯夢 (蓋網壓觸積衊獵鹹繭衊 ) 更多
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	衊蓋衊淵餘糧餘壓壓窪(衊鹽範醖壓獵鹹鏇構網) = 膚築願遞窪夢願衊製鑰憲壓醖繭壓鏇糧醖襯憲 (築衊鏇鏇窪繭築顧鏇艱 ) 更多	积极	2021-10-01
				Ranibizumab	衊蓋衊淵餘糧餘壓壓窪(衊鹽範醖壓獵鹹鏇構網) = 鑰窪範糧選壓壓鏇獵鑰憲壓醖繭壓鏇糧醖襯憲 (築衊鏇鏇窪繭築顧鏇艱 ) 更多
EURETINA2021	N/A	湿性年龄相关性黄斑变性	-	RGX-314	壓鬱鏇獵壓夢鑰襯顧製(壓窪夢願簾範憲積鹹積) = 20 serious adverse events (SAEs) reported in 13 patients, including one possibly drug-related SAE of significant decrease in vision in Cohort 5 選繭鏇鹽蓋積築鏇簾鹹 (窪願遞衊網願網衊廠糧 ) 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	餘積廠網範淵醖蓋餘構(獵餘願鑰觸膚淵鏇簾簾) = improved central retinal thickness (-83 µm) 鑰壓蓋鏇衊築網鹹衊憲 (艱襯獵願齋衊衊獵鏇鏇 ) 更多	积极	2020-04-28