FDA Grants Orphan Drug Status to UniQure's AMT-191, Aiming to Treat Fabry Disease
FDA Grants Orphan Drug Status to UniQure's AMT-191, Aiming to Treat Fabry Disease
uniQure N.V. (NASDAQ:QURE), a leading gene therapy company advancing transformative therapies for patients with severe medical needs, today announced that the U.S. Food and Drug Administration (FDA) has granted Orphan Drug Designation to AMT-191, uniQure's investigational gene therapy for the treatment of Fabry disease, a rare, inherited genetic disease. In August 2024, uniQure announced the dosing of the first patient in its U.S., multi-center, open-label Phase I/IIa trial of AMT-191.
uniQure N.V.(納斯達克:QURE)是一家領先的基因治療公司,致力於爲嚴重醫療需求患者推進變革性療法。今天宣佈,美國食品藥品監督管理局(FDA)已授予AMt-191孤兒藥品認定,用於治療Fabry病,一種罕見的遺傳性疾病。2024年8月,uniQure宣佈在其美國多中心、開放標籤的AMt-191 Phase I/IIa試驗中對首位患者進行了劑量給藥。
"This important designation highlights the need for new gene therapies like AMT-191 for patients with Fabry disease with the potential of delivering meaningful benefit given the suboptimal effectiveness of current chronic treatments," stated Walid Abi-Saab, M.D., chief medical officer of uniQure. "This designation supports our Phase I/IIa clinical trial and we look forward to rapidly generating clinical proof-of-concept data and providing initial data in 2025."
「這一重要認定凸顯了像AMt-191這樣的新基因療法對Fabry病患者的需求,有可能提供有意義的益處,考慮到當前慢性治療效果不佳,」uniQure首席醫療官Walid Abi-Saab博士表示。 「這一認定支持我們的I/IIa臨床試驗,我們期待快速生成臨床概念證據,並在2025年提供初步數據。」
In patients with Fabry disease, a pathogenic variant in the galactosidase alpha (GLA) gene leads to α-galactosidase A (aGAL-A) enzyme deficiency, which in turn results in a progressive accumulation of lipids in multiple cell types, including kidney and heart cells, eventually resulting in a multi-system disorder. AMT-191 is a one-time intravenously administered investigational AAV5-based gene therapy that uses a proprietary, highly potent promoter to deliver a GLA transgene designed to target the liver to produce GLA protein.
在患有Fabry病的患者中,α半乳糖苷酶A(aGAL-A)基因中的致病變異導致α-半乳糖苷酶A(aGAL-A)酶缺乏,進而導致脂質在多種細胞類型中逐漸積累,包括腎臟和心臟細胞,最終導致多系統障礙。AMt-191是一種一次性靜脈給藥的基因治療,使用專有的高效啓動子傳遞GLA基因,旨在靶向肝臟產生GLA蛋白。
The Phase I/IIa clinical trial of AMT-191 will be conducted in the United States. The multicenter, open-label trial consists of two cohorts with up to six adult male patients each: a low-dose cohort of 6x1013 gc/kg and a high-dose cohort of 3x1014 gc/kg delivered through a one-time intravenous infusion. Patients will continue to receive their regular enzyme replacement therapy until the criteria for withdrawal is met and will be followed for a period of 24 months. The trial will explore the safety, tolerability, and early signs of efficacy by measuring the expression of lysosomal enzyme aGLA-A. Additional details are available on (NCT06270316).
AMt-191的I/IIa期臨床試驗將在美國進行。多中心、開放標籤試驗包括兩個隊列,每個隊列有最多六名成年男性患者:一個6x 1013gc/kg的低劑量隊列和一個3 x 1014gc/kg的高劑量隊列,通過一次靜脈輸注給藥。患者將繼續接受他們的常規酶替代治療,直到滿足撤出標準,並將在24個月的時間內進行跟蹤。試驗將通過測量溶酶體酶aGLA-A的表達來探索安全性、耐受性和早期療效跡象。更多細節可在(NCT06270316)上了解。
The FDA's Orphan Drug Designation provides a special status for investigational drugs being developed for rare diseases considered to affect only up to 200,000 people in the United States. Orphan drug status provides certain incentives, including tax credits, grants and waiver of certain administrative fees for clinical trials as well as seven years of market exclusivity in the United States following drug approval.
美國食品藥品監督管理局的孤兒藥物認定爲專門爲罕見疾病開發的研究性藥物提供特殊地位,這些疾病被認爲僅在美國影響不到20萬人。孤兒藥物地位提供特定激勵措施,包括稅收減免、撥款以及豁免特定臨床試驗的行政費用,以及在美國獲得藥物批准後七年的市場排他性。
譯文內容由第三人軟體翻譯。