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Edgewise Therapeutics Announces Positive Topline Results From the CANYON Phase 2 Trial of Sevasemten in Individuals With Becker Muscular Dystrophy (Becker)

Edgewise Therapeutics Announces Positive Topline Results From the CANYON Phase 2 Trial of Sevasemten in Individuals With Becker Muscular Dystrophy (Becker)

Edgewise Therapeutics宣佈在貝克肌營養不良症(Becker)患者中進行的CANYON第二階段試驗中獲得積極的初步結果。
Businesswire ·  12/16 19:00

– Trial met primary endpoint of reduction in circulating levels of creatine kinase (CK), a biomarker associated with skeletal muscle damage, in the largest Becker interventional trial to date –

— 在迄今爲止最大的貝克爾介入試驗中,該試驗達到了肌酸激酶(CK)(一種與骨骼肌損傷相關的生物標誌物)循環水平降低的主要終點 —

– On the key secondary endpoint, sevasemten-treated patients showed stabilization of North Star Ambulatory Assessment (NSAA) with a trend towards improvement at 12 months compared to placebo –

— 在關鍵的次要終點上,與安慰劑相比,接受sevasemten治療的患者表現出穩定的北極星門診評估(NSAA),在12個月時有改善的趨勢 —

– Sevasemten was well-tolerated and no new safety concerns were observed –

— Sevasemten 耐受性良好,未觀察到新的安全問題 —

– Edgewise leadership to discuss CANYON findings on Monday, December 16 at 8:30 a.m. Eastern Time at a virtual investor event –

— Edgewise領導層將於美國東部時間12月16日星期一上午 8:30 在一次虛擬投資者活動中討論CANYON的調查結果—

BOULDER, Colo.--(BUSINESS WIRE)--Edgewise Therapeutics, Inc., (Nasdaq: EWTX), a leading muscle disease biopharmaceutical company, today announced positive topline results from the Phase 2 CANYON trial of sevasemten in individuals with Becker muscular dystrophy. Sevasemten is an orally administered first-in-class fast skeletal myosin inhibitor designed to protect muscle against contraction-induced damage in muscular dystrophies. The trial met its primary endpoint of change from baseline in CK. CANYON is the largest interventional trial to date in Becker and the first to achieve its primary endpoint.

科羅拉多州博爾德--(美國商業資訊)--領先的肌肉疾病生物製藥公司Edgewise Therapeutics, Inc.(納斯達克股票代碼:EWTX)今天宣佈了針對貝克爾肌肉萎縮症患者的sevasemten的CANYON二期試驗的積極結果。Sevasemten是一種口服給藥的同類首創的快速骨骼肌球蛋白抑制劑,旨在保護肌肉免受肌肉萎縮引起的損傷。該試驗達到了Ck與基線相比變化的主要終點。CANYON是迄今爲止貝克爾最大的介入試驗,也是第一個實現其主要終點的試驗。

NSAA, the key secondary endpoint of function, showed a trend towards improvement over time in the sevasemten-treated group. Plasma fast skeletal muscle troponin I (TNNI2), a target-specific biomarker of fast skeletal muscle damage, showed a significant reduction, compared to placebo. Additional functional measures, including the 10-meter walk/run, 4-stair climb and 100-meter timed test, showed trends towards improvement compared to placebo. Notably, the treatment population had more advanced disease than placebo.

NSAA是功能的關鍵次要終點,在sevasemten治療組中,隨着時間的推移顯示出改善的趨勢。與安慰劑相比,血漿快速骨骼肌肌鈣蛋白I(TNNI2)是快速骨骼肌損傷的靶標特異性生物標誌物,顯示出顯著降低。與安慰劑相比,其他功能指標,包括10米步行/跑步、4層樓梯和100米計時測試,顯示出改善的趨勢。值得注意的是,治療人群的疾病比安慰劑更晚期。

Sevasemten was well-tolerated, and no new safety concerns were observed in either the adult or adolescent patient populations. Ninety-nine percent of eligible participants from CANYON and other sevasemten trials in Becker have enrolled in MESA, the ongoing open label extension trial.

Sevasemten的耐受性良好,在成人或青少年患者群體中均未觀察到新的安全問題。來自CANYON和貝克爾其他sevasemten試驗的合格參與者中有99%已報名參加MESA,這是一項正在進行的開放標籤延期試驗。

"Becker muscular dystrophy is a devastating neuromuscular disease characterized by rapid progression once functional decline begins. This landmark study presents compelling biomarker data and promising signals that suggest the potential for functional stabilization with administration of sevasemten," said Craig M. McDonald, M.D., Distinguished Professor and Chair at the UC Davis Health Department of Physical Medicine and Rehabilitation, and a Principal Investigator in CANYON and GRAND CANYON. "Becker has no approved therapies. I look forward to the results of the GRAND CANYON pivotal cohort with the hope of bringing the first treatment option to this patient population."

「貝克爾肌肉萎縮症是一種毀滅性的神經肌肉疾病,其特徵是一旦功能衰退開始就會迅速發展。這項具有里程碑意義的研究提供了令人信服的生物標誌物數據和有希望的信號,表明施用sevasemten有可能實現功能穩定。」 加州大學戴維斯分校物理醫學與康復系傑出教授兼主任、CANYON和GRAND CANYON首席研究員克雷格·麥克唐納博士說。「貝克爾沒有批准的療法。我期待着GRAND CANYON關鍵隊列的結果,希望爲這些患者群體帶來第一個治療選擇。」

"We are very encouraged by the CANYON results in Becker and the potential of this novel muscle-targeted therapeutic," said Joanne Donovan, Ph.D., M.D., Chief Medical Officer, Edgewise. "This confirmed our previous observations in the ARCH study of significant decreases in biomarkers of muscle damage and similarly we are seeing evidence of preservation of function in Becker patients."

Edgewise首席醫學官喬安妮·多諾萬博士說:「CANYON在Becker中的研究結果以及這種新型肌肉靶向療法的潛力令我們感到非常鼓舞。」「這證實了我們先前在ARCH研究中觀察到的肌肉損傷生物標誌物顯著減少的觀察,同樣,我們也看到了貝克爾患者功能保留的證據。」

The Company is on track to complete recruitment in the GRAND CANYON cohort by the first quarter of 2025. Based on these positive Phase 2 results, the Company plans to engage the U.S. Food and Drug Administration (FDA) and European Medicines Agency about marketing authorization filing strategies for sevasemten in Becker.

該公司有望在2025年第一季度之前完成大峽谷人才的招聘。基於這些積極的第二階段結果,該公司計劃與美國食品藥品監督管理局(FDA)和歐洲藥品管理局就sevasemten在貝克爾的上市許可申請策略進行接觸。

The Company intends to submit the complete results of the CANYON study for publication at a future medical congress.

該公司打算提交CANYON研究的完整結果,以便在未來的醫學大會上發表。

Overview of CANYON and Clinical Results

CANYON 和臨床結果概述

CANYON, the largest interventional Becker trial, is a Phase 2, double-blind, randomized, placebo-controlled study to investigate the effect of sevasemten on the safety, pharmacokinetics, biomarkers, and functional measures of participants (NCT05291091). The trial was not powered for the functional endpoints. Forty adults and 29 adolescents with Becker muscular dystrophy were enrolled. This study had a 4-week screening period, a 12-month treatment period, followed by a 4-week follow-up period. The adult participants were randomized to sevasemten or placebo in a 3:1 ratio. The adolescent participants were randomized in a 2:1 ratio to sevasemten or placebo and were assessed for safety and tolerability. The data analysis included the complete adult safety population of 40 individuals. There was a notable imbalance between adult participants in the sevasemten and placebo groups with the sevasemten group having more advanced disease at baseline based on all functional measures and MRI.

CANYON是最大的介入性貝克爾試驗,是一項2期、雙盲、隨機、安慰劑對照的研究,旨在研究sevasemten對參與者的安全性、藥代動力學、生物標誌物和功能測量(NCT05291091)的影響。該試用版不支持功能端點。招收了40名患有貝克爾肌肉萎縮症的成年人和29名青少年。該研究的篩查期爲4周,治療期爲12個月,隨後爲期4周的隨訪期。成年參與者以 3:1 的比例被隨機分配到sevasemten或安慰劑。青少年參與者與sevasemten或安慰劑的比例以 2:1 的比例隨機分配,並接受了安全性和耐受性評估。數據分析包括40人的完整成人安全人群。sevasemten和安慰劑組的成年參與者之間存在明顯的不平衡,根據所有功能測量和核磁共振成像,sevasemten組在基線時患有更晚期的疾病。

Primary Endpoint: The primary endpoint to assess the efficacy of sevasemten compared to placebo was change from baseline in CK over the treatment period for adults. The results demonstrated a significant change from baseline in CK in the sevasemten-treated group (difference vs. placebo, 28% average decrease over months 6 through 12; p=0.02).

主要終點:評估sevasemten與安慰劑相比療效的主要終點是成人治療期間Ck的基線變化。結果顯示,在sevasemten治療組中,Ck與基線相比有顯著變化(與安慰劑的差異,在第6至12個月中平均下降28%;p=0.02)。

Key Secondary Endpoint: The key secondary endpoint was the change from baseline in NSAA total score in adults at month 12. NSAA is a scale commonly used to rate motor function. The between-group difference was 1.1 points, favoring sevasemten; p=0.16 across all adult participants. NSAA remained stable over time in the sevasemten treatment group, similar to the observations in the ARCH study. Further, while the placebo group was small in number (n=12), NSAA declined similarly to that observed in previous natural history studies.1,2,3

關鍵次要終點:關鍵次要終點是第12個月成人NSAA總分與基線的變化。NSAA 是一種常用於評估運動功能的量表。組間差異爲1.1分,有利於sevasemten;所有成年參與者的p=0.16分。與ARCH研究中的觀察結果類似,NSAA在sevasemten治療組中長期保持穩定。此外,儘管安慰劑組的數量很少(n=12),但NSAA的下降幅度與先前自然歷史研究中觀察到的相似。1,2,3

Other Secondary Endpoints: Plasma TNNI2 decreased 77% from baseline in the sevasemten-treated group compared to placebo, averaged over months 6 through 12 in adults; p<0.001.

其他次要終點:與安慰劑相比,sevasemten治療組的血漿 TNNI2 比基線下降了77%,成人的血漿在6至12個月內平均下降了77%;p

The 10-meter walk/run, 4-stair climb and 100-meter timed test showed trends towards improvement, compared to placebo. The Company continues to evaluate additional secondary and exploratory endpoints.

與安慰劑相比,10米步行/跑步、4層樓梯和100米計時測試顯示出改善的趨勢。該公司繼續評估其他次要和探索性終點。

Safety and Tolerability: Sevasemten was well-tolerated, and no new safety concerns were identified.

安全性和耐受性:Sevasemten的耐受性良好,沒有發現新的安全問題。

CANYON Implications to GRAND CANYON: The functional observations from the CANYON study support that the GRAND CANYON pivotal cohort's primary endpoint is powered at >95% to demonstrate a statistically significant NSAA difference at 18 months.

峽谷對大峽谷的影響:峽谷研究的功能觀測結果支持,大峽谷關鍵隊列的主要終點位於大於 95%,顯示出18個月時NSAA存在統計學上的顯著差異。

MESA, open label extension trial in adults with Becker: The Company is advancing MESA, an open-label extension trial to assess the long-term effect of sevasemten in individuals with Becker. MESA provides continued access to sevasemten to participants who were previously enrolled in ARCH, or completed CANYON, GRAND CANYON, or DUNE. To date, 99% of eligible participants completing these trials have enrolled in MESA.

MESA,針對成年貝克爾患者的開放標籤延期試驗:該公司正在推進MESA,這是一項開放標籤延期試驗,旨在評估sevasemten對Becker患者的長期影響。MESA 向之前註冊過 ARCH 或已完成峽谷、大峽谷或 DUNE 的參與者提供繼續使用 sevasemten 的權限。迄今爲止,完成這些試驗的合格參與者中有99%已加入MESA。

GRAND CANYON, a global pivotal cohort in Becker: GRAND CANYON, an expansion of the CANYON placebo-controlled trial, is a multi-center, randomized, double-blind, placebo-controlled cohort to evaluate the safety and efficacy of sevasemten in adults with Becker. The primary endpoint of GRAND CANYON is change from baseline in NSAA at 18 months. In addition, other functional assessments, biomarkers of muscle damage, MRI, patient-reported outcomes and safety will be assessed. GRAND CANYON is an 18-month cohort anticipated to recruit approximately 120 individuals with Becker. Data from GRAND CANYON, if positive, could support a marketing application. To learn more, go to clinicaltrials.gov (NCT05291091).

GRAND CANYON是《貝克爾:大峽谷》中的全球關鍵隊列,是CANYON安慰劑對照試驗的擴展,是一個多中心、隨機、雙盲、安慰劑對照的隊列,旨在評估sevasemten對成年貝克爾患者的安全性和有效性。大峽谷的主要終點是與NSAA的基線相比在18個月時發生變化。此外,還將評估其他功能評估、肌肉損傷的生物標誌物、核磁共振成像、患者報告的結果和安全性。大峽谷是一個爲期 18 個月的隊伍,預計將招募大約 120 名貝克爾成員。來自大峽谷的數據如果爲正數,則可以支持營銷應用程序。要了解更多信息,請訪問 clinicaltrials.gov (NCT05291091)。

Sevasemten has achieved notable regulatory milestones by securing FDA Orphan Drug Designation for the treatment of Becker and Duchenne, Rare Pediatric Disease Designation (RPDD) for the treatment of Duchenne, and Fast Track designations for the treatment of Becker and Duchenne. Further, sevasemten secured the EMA Orphan Drug Designations for the treatment of Becker and Duchenne.

Sevasemten通過獲得用於治療貝克爾和杜興納的美國食品藥品管理局孤兒藥認證、用於治療杜興氏的罕見兒科疾病認證(RPDD)以及治療貝克爾和杜興納的快速通道認證,取得了顯著的監管里程碑。此外,sevasemten獲得了EMA孤兒藥認證,用於治療貝克爾和杜興內。

Upcoming CANYON Data Presentations:

即將發佈的 CANYON 數據演示:

Virtual Investor Event

虛擬投資者活動

Members of the Edgewise management team will hold a live webcast on Monday, December 16, at 8:30 a.m. ET to discuss the CANYON data, and will be joined by Dr. McDonald, who will share his perspective of sevasemten and Becker. An accompanying slide presentation will also be available. To register for the live webcast and replay, please visit the Edgewise events page.

Edgewise管理團隊的成員將在美國東部時間12月16日星期一上午8點30分進行網絡直播,討論CANYON的數據,麥克唐納博士將與會,他將分享他對sevasemten和Becker的看法。還將提供隨附的幻燈片演示。要註冊網絡直播和重播,請訪問 Edgewise 活動頁面。

Patient Community Webinar

患者社區網絡研討會

Members of Edgewise management will hold a community webinar on Wednesday, December 18, 2024, at 1 p.m. ET to discuss these data and the GRAND CANYON pivotal study. To register for the community webinar, please click here.

Edgewise管理層成員將在美國東部時間2024年12月18日星期三下午1點舉行社區網絡研討會,討論這些數據和大峽谷的關鍵研究。要註冊參加社區網絡研討會,請點擊此處。

About Becker Muscular Dystrophy

關於貝克爾肌肉萎縮症

Becker is a rare, genetic, life-shortening, debilitating and degenerative neuromuscular disorder. The disease predominantly affects males and imposes significant physical, emotional, financial, and social impacts on the individual and their caregivers. Individuals with Becker experience contraction-induced muscle damage, which is the primary driver of muscle loss and impaired motor function in muscular dystrophies. Functional decline can begin at any age, and once that muscle loss occurs, the decline in function is irreversible and continues throughout the individual's life. Some individuals living with Becker experience heart failure from cardiomyopathy, which may result in heart transplantation or early death. Currently, there is no cure for Becker; early and long-term multidisciplinary care is critical for optimized disease management. There is a great need for more Becker-specific scientific research, clinical programs, and treatment guidelines to improve management of this disease. To learn more about Becker, go to .

貝克爾是一種罕見的、遺傳性的、會縮短壽命的、使人衰弱和退化的神經肌肉疾病。該疾病主要影響男性,並對個人及其護理人員造成重大的身體、情感、財務和社會影響。Becker 患者會出現收縮引起的肌肉損傷,這是肌肉萎縮症中肌肉流失和運動功能受損的主要驅動因素。功能衰退可以從任何年齡開始,一旦發生肌肉流失,功能下降是不可逆轉的,並且會持續到個人的一生。一些患有貝克爾的人會因心肌病而出現心力衰竭,這可能導致心臟移植或過早死亡。目前,貝克爾無法治癒;早期和長期的多學科護理對於優化疾病管理至關重要。迫切需要更多針對貝克爾的科學研究、臨床項目和治療指南,以改善這種疾病的管理。要了解有關 Becker 的更多信息,請訪問。

About Sevasemten (EDG-5506) for Becker and Duchenne Muscular Dystrophies

關於治療貝克爾和杜興納肌肉萎縮症的 Sevasemten (EDG-5506)

Sevasemten is an orally administered first-in-class fast skeletal myosin inhibitor designed to protect muscle against contraction-induced muscle damage in muscular dystrophies including Becker and Duchenne. Sevasemten presents a novel mechanism of action designed to selectively limit the exaggerated muscle damage caused by the absence or loss of functional dystrophin. By minimizing the progressive muscle damage that leads to functional impairment, sevasemten has the potential to benefit a broad range of patients suffering from debilitating neuromuscular disorders. Its unique mechanism of action provides the potential to establish sevasemten as a foundational therapy in dystrophinopathies, either as a single agent therapy or in combination with available therapies and those in development.

Sevasemten是一種口服給藥的同類首創的快速骨骼肌球蛋白抑制劑,旨在保護肌肉免受包括貝克爾和杜興納在內的肌肉萎縮引起的肌肉損傷。Sevasemten提出了一種新的作用機制,旨在選擇性地限制因功能性肌萎縮素缺失或喪失而造成的過度肌肉損傷。通過最大限度地減少導致功能障礙的漸進性肌肉損傷,sevasemten有可能使許多患有虛弱性神經肌肉疾病的患者受益。其獨特的作用機制有可能將sevasemten確立爲肌萎縮症的基礎療法,既可以作爲單一藥物療法,也可以與現有療法和正在開發的療法聯合使用。

Sevasemten is being studied in the Phase 2 CANYON study with a pivotal cohort GRAND CANYON in adults and adolescents with Becker muscular dystrophy. Sevasemten is also being studied in the ongoing Phase 2 trials, LYNX and FOX, in children and adolescents with Duchenne muscular dystrophy.

CANYON的2期研究正在對Sevasemten進行研究,該研究針對患有貝克爾肌肉萎縮症的成人和青少年的關鍵隊列GRAND CANYON。正在進行的針對杜興氏肌肉萎縮症兒童和青少年的LYNX和FOX二期試驗也在研究Sevasemten。

For more information on Edgewise's clinical trials .

了解有關 Edgewise 臨床試驗的更多信息。

About Edgewise Therapeutics

關於 Edgewise 療法

Edgewise Therapeutics is a leading muscle disease biopharmaceutical company developing novel therapeutics for muscular dystrophies and serious cardiac conditions. The Company's deep expertise in muscle physiology is driving a new generation of novel therapeutics. Sevasemten is an orally administered first-in-class fast skeletal myosin inhibitor in late-stage clinical trials in Becker and Duchenne muscular dystrophies. EDG-7500 is a novel cardiac sarcomere modulator for the treatment of hypertrophic cardiomyopathy and other diseases of diastolic dysfunction, currently in Phase 2 clinical development. The entire team at Edgewise is dedicated to our mission: changing the lives of patients and families affected by serious muscle diseases. To learn more, go to:  or follow us on LinkedIn, X, Facebook and Instagram.

Edgewise Therapeutics是一家領先的肌肉疾病生物製藥公司,開發針對肌肉萎縮症和嚴重心臟病的新療法。該公司在肌肉生理學方面的深厚專業知識正在推動新一代新療法的發展。Sevasemten是貝克爾和杜興氏肌肉萎縮症的後期臨床試驗中口服給藥的同類首創快速骨骼肌球蛋白抑制劑。EDG-7500 是一種用於治療肥厚型心肌病和其他舒張功能障礙疾病的新型心臟肉瘤調節劑,目前處於二期臨床開發階段。Edgewise 的整個團隊都致力於我們的使命:改變受嚴重肌肉疾病影響的患者和家屬的生活。要了解更多信息,請訪問:或在領英、X、臉書和Instagram上關注我們。

References

參考文獻

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[2] van de Velde Nm 等人。使用定量肌肉磁共振成像和功能評估來識別貝克爾肌肉萎縮症的最佳生物標誌物的選擇方法。神經病學. 2021; 97 (5): e513-e522. doi: 10.1212/WNL.0000000000012233。

[3] De Wel B, et al. Lessons for future clinical trials in adults with Becker muscular dystrophy: disease progression detected by muscle magnetic resonance imaging, clinical and patient-reported outcome measures. Eur J Neurol. 2024:e16282. doi:10.1111/ene.16282. Online ahead of print.

[3] De Wel b 等人。Becker肌肉萎縮症成人未來臨床試驗的經驗教訓:通過肌肉磁共振成像、臨床和患者報告的結果衡量標準來檢測疾病進展。Eur J Neurol. 2024:e16282. doi: 10.1111/ene.16282。印刷前在線。

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