- Initiating Registrational Cohorts with Update on Path to Registration by Year-End 2024 -
- Virtual Investor Event Today at 8:00 a.m. ET -
WALTHAM, Mass., Sept. 03, 2024 (GLOBE NEWSWIRE) -- Dyne Therapeutics, Inc. (Nasdaq: DYN), a clinical-stage muscle disease company focused on advancing innovative life-transforming therapeutics for people living with genetically driven diseases, today announced new clinical data from its ongoing Phase 1/2 DELIVER trial of DYNE-251 in patients with Duchenne muscular dystrophy (DMD) who are amenable to exon 51 skipping demonstrating unprecedented dystrophin expression and functional improvement in multiple cohorts.
"We believe these data reinforce the opportunity to transform the treatment paradigm for individuals living with Duchenne. In DELIVER, DYNE-251 achieved the highest level of dystrophin expression reported for an exon 51 skipping therapy and improvement in multiple functional endpoints across multiple cohorts that continued with time on therapy," said Wildon Farwell, M.D., MPH, chief medical officer of Dyne. "Our goal has always been to drive dystrophin levels that lead to functional benefit for patients – these data suggest that the distribution across cardiac, diaphragm and other skeletal muscles observed preclinically with the FORCE platform is translating in the clinic. Importantly, treatment with DYNE-251 resulted in meaningful improvements in SV95C, a digital outcome measure approved as a primary endpoint for Duchenne clinical trials in Europe. With these exciting data, we are moving quickly to initiate registrational cohorts in DELIVER, and we continue to pursue expedited approval pathways and plan to provide an update on our path to registration by the end of this year."
This assessment of the DELIVER trial evaluating DYNE-251 includes 6-month biomarker and functional data from 8 male patients enrolled in the 20 mg/kg (approximate PMO dose) cohort who were randomized to receive DYNE-251 or placebo once every four weeks, and 12-month functional data from 6 participants in the 10 mg/kg cohort.1 DYNE-251 demonstrated dose dependent exon skipping and dystrophin expression and improvement in multiple functional endpoints in both cohorts. Key findings include:
Dystrophin expression: DYNE-251 demonstrated unprecedented dystrophin expression as measured by Western blot. Patients treated with 20 mg/kg of DYNE-251 Q4W had a mean absolute dystrophin expression of 3.71% of normal (unadjusted for muscle content), more than 10-fold higher than the 0.3% reported in a clinical trial of the weekly standard of care, eteplirsen.2 When adjusting for muscle content, the DYNE-251 treated group reached 8.72% mean absolute dystrophin, which is greater than levels reported by peptide conjugate PMOs in clinical development.3
Function: Meaningful improvements in multiple functional endpoints were observed in both the 20 mg/kg and 10 mg/kg DYNE-251 Q4W groups, including North Star Ambulatory Assessment (NSAA), Stride Velocity 95th Centile (SV95C), 10-Meter Walk/Run Time (10-MWR), Time to Rise from Floor. The 10 mg/kg cohort showed continued improvement in all reported measures from 6 months to 12 months.1
Safety and Tolerability: Safety and tolerability data are based on 54 participants enrolled in the DELIVER trial. DYNE-251 demonstrated a favorable safety profile and the majority of treatment emergent adverse events were mild or moderate.4 No related serious treatment emergent adverse events have been identified other than in two participants at the 40 mg/kg dose level with events potentially related to study drug and both participants have recovered. Approximately 675 doses have been administered to date in the DELIVER trial, representing over 50 patient-years of follow-up.
Key Milestones for DELIVER and ACHIEVE Trials
Based on these data and regulatory interactions, Dyne is initiating registrational cohorts in the DELIVER trial and plans to provide an update on the path to registration by the end of 2024.
Dyne is also executing its ongoing Phase 1/2 ACHIEVE clinical trial of DYNE-101 in myotonic dystrophy type 1. The safety profile of DYNE-101 continues to be favorable and includes safety data up to the 6.8 mg/kg Q8W cohort.5 The company continues to engage with global regulators, including the U.S. Food and Drug Administration, and plans to provide an update on the path to registration for DYNE-101, including additional clinical data, by the end of 2024.
Virtual Investor Event
Dyne will host a video webcast event to discuss these DELIVER data today, September 3, 2024, at 8:00 a.m. ET and a replay will be accessible for 90 days following the presentation. An accompanying slide presentation for the event and an updated corporate presentation will also be available. To access these presentations and register for the live webcast and replay, please visit the Investors & Media section of Dyne's website at and the live event may also be accessed here.
About the DELIVER Trial
DELIVER is a Phase 1/2 global clinical trial evaluating DYNE-251, consisting of a 24-week multiple ascending dose (MAD) randomized placebo-controlled period, a 24-week open-label extension and a 96-week long-term extension. The trial, which is designed to be registrational, is enrolling ambulant and non-ambulant males with Duchenne muscular dystrophy (DMD) who are ages 4 to 16 and have mutations amenable to exon 51 skipping. The primary endpoints are safety, tolerability and change from baseline in dystrophin levels as measured by Western blot. Secondary endpoints include measures of muscle function, exon skipping and pharmacokinetics. For more information on the DELIVER trial, visit (NCT05524883).
About DYNE-251
DYNE-251 is an investigational therapeutic being evaluated in the Phase 1/2 global DELIVER clinical trial for people living with DMD who are amenable to exon 51 skipping. DYNE-251 consists of a phosphorodiamidate morpholino oligomer (PMO) conjugated to a fragment antibody (Fab) that binds to the transferrin receptor 1 (TfR1) which is highly expressed on muscle. It is designed to enable targeted muscle tissue delivery and promote exon skipping in the nucleus, allowing muscle cells to create a truncated, functional dystrophin protein, with the goal of stopping or reversing disease progression. DYNE-251 has been granted fast track, orphan drug and rare pediatric disease designations by the U.S. Food and Drug Administration for the treatment of DMD mutations amenable to exon 51 skipping.
In addition to DYNE-251, Dyne is building a global DMD franchise and has preclinical programs targeting other exons, including 53, 45 and 44.
About Duchenne Muscular Dystrophy (DMD)
DMD is a rare disease caused by mutations in the gene that encodes for dystrophin, a protein critical for the normal function of muscle cells. These mutations, the majority of which are deletions, result in the lack of dystrophin protein and progressive loss of muscle function. DMD occurs primarily in males and affects an estimated 12,000 to 15,000 individuals in the U.S. and 25,000 in Europe. Loss of strength and function typically first appears in pre-school age boys and worsens as they age. As the disease progresses, the severity of damage to skeletal and cardiac muscle often results in patients experiencing total loss of ambulation by their early teenage years and includes worsening cardiac and respiratory symptoms and loss of upper body function by the later teens. There is no cure for DMD and currently approved therapies provide limited benefit.
About Dyne Therapeutics
Dyne Therapeutics is a clinical-stage muscle disease company focused on advancing innovative life-transforming therapeutics for people living with genetically driven diseases. With its proprietary FORCE platform, Dyne is developing modern oligonucleotide therapeutics that are designed to overcome limitations in delivery to muscle tissue. Dyne has a broad pipeline for serious muscle diseases, including clinical programs for myotonic dystrophy type 1 (DM1) and Duchenne muscular dystrophy (DMD) and a preclinical program for facioscapulohumeral muscular dystrophy (FSHD). For more information, please visit , and follow us on X, LinkedIn and Facebook.
1. | During the OLE period, all participants in 10 mg/kg cohort were dose escalated to 20 mg/kg Q4W regimen. |
2. | No head-to-head trials have been conducted comparing DYNE-251 to eteplirsen. Eteplirsen data may not be directly comparable due to differences in trial protocols, dosing regimens and patient populations. Accordingly, these cross-trial comparisons may not be reliable. Eteplirsen data from J Neuromuscul Dis. 2021; 8(6): 989–1001. |
3. | No head-to-head trials have been conducted comparing DYNE-251 to SRP-5051. SRP-5051 data may not be directly comparable due to differences in trial protocols, dosing regimens, methodologies for calculating muscle content adjusted dystrophin and patient populations. Accordingly, these cross-trial comparisons may not be reliable. SRP-5051 data from Clinical Update: MOMENTUM (Study SRP-5051-201, Part B) Jan. 29, 2024. |
4. | DYNE-251 safety data as of August 21, 2024. |
5. | DYNE-101 safety data as of August 20, 2024. |
- 开始注册阶段,并更新2024年年底注册进程 -
- 今天上午8:00举行虚拟投资者活动 -
戴纳基(Dyne Therapeutics)是一家总部位于马萨诸塞州沃尔瑟姆的医疗公司。戴纳基(Dyne Therapeutics)是一家纳斯达克(Nasdaq)上市的临床阶段的肌肉疾病公司,专注于推动创新的治疗方法,提高生活质量,并改善患有遗传性疾病的患者的情况。今天,戴纳基(Dyne Therapeutics)宣布从其正在进行的DYNE-251第1/2期DELIVER试验中发布了新的临床数据,该试验针对可选择进行外显子51跳跃的杜氏肌萎缩患者(DMD),显示出前所未有的肌酸蛋白表达和功能改善的结果。
"我们相信这些数据强化了改变患有杜欧肌病患者治疗范式的机会。在DELIVER中,DYNE-251实现了外显子51跳跃疗法报告的最高水平的肌营养蛋白表达,以及在多个队列中随着治疗时间的延长而改善的多个功能终点指标," 戴纳的首席医务长Wildon Farwell博士,MPH表示。"我们的目标一直是促进导致患者获益的肌营养蛋白水平 - 这些数据表明,在临床中观察到的使用FORCE平台之前在心脏、隔膜和其他骨骼肌肉上的分布正在得到转化。值得注意的是,使用DYNE-251治疗导致了SV95C的有意义改善,这是欧洲杜欧肌肉营养不良临床试验的主要终点的数字结果测量。凭借这些令人振奋的数据,我们正在迅速启动DELIVER中的注册阶段,并继续探索加快批准途径,并计划在年底前更新我们的注册进程"。
对评估DYNE-251的DELIVER试验进行的评估包括20mg/kg(约PMO剂量)队列中8名男性患者的6个月生物标志物和功能数据,他们随机接受DYNE-251或安慰剂,每四周一次,并10mg/kg队列中的6名参与者的12个月功能数据。DYNE-251展示了剂量依赖的外显子跳跃和肌营养蛋白表达,以及在两个队列中的多个功能终点的改善。主要发现包括:
DYNE-251在Western blot检测中表现出前所未有的肌营养蛋白表达。接受20 mg/kg DYNE-251 Q4W治疗的患者,绝对肌营养蛋白表达平均值为3.71%,超过了临床试验中每周标准照护eteplirsen报道的0.3%的10倍以上。在调整肌肉含量后,DYNE-251治疗组的绝对肌营养蛋白平均达到了8.72%,高于临床开发中的肽共轭PMOs报告的水平。
功能:20 mg/kg和10 mg/kg DYNE-251 Q4W组中观察到多个功能终点的有意义改善,包括North Star步行评估(NSAA),步态速度95百分位数(SV95C),10米步行/开多时间(10-MWR),从地板上起立时间。10 mg/kg队列在6个月至12个月间所有报道的指标持续改善。
安全性与耐受性:安全性和耐受性数据基于DELIVER试验中纳入的54位参与者。DYNE-251显示出良好的安全配置文件,大多数治疗相关不良事件为轻度或中度。除了40 mg/kg剂量水平的两位参与者可能与研究药物有关的事件,未发现其他相关严重治疗相关不良事件,两位参与者均已康复。到目前为止,在DELIVER试验中已经施用了大约675个剂量,代表了超过50位患者年的随访。
DELIVER和ACHIEVE试验的关键里程碑
根据这些数据和监管互动,戴纳基正在启动DELIVER试验的注册队列,并计划于2024年底前提供有关注册路径的更新。
戴纳基还在进行DYNE-101在肌无力性肌营养不良类型1的正在进行的第1/2期ACHIEVE临床试验。 DYNE-101的安全性数据仍然良好,包括Q8W剂量组的安全数据高达6.8毫克/千克。5公司将继续与全球监管机构,包括美国食品和药物管理局,保持接触,并计划于2024年底前提供关于DYNE-101的注册路径的更新,包括更多临床数据。
虚拟投资者活动
About Duchenne Muscular Dystrophy (DMD)
关于DELIVER试验
About Dyne Therapeutics
About DYNE-251
DYNE-251 is an investigational therapeutic being evaluated in the Phase 1/2 global DELIVER clinical trial for people living with DMD who are amenable to exon 51 skipping. DYNE-251 consists of a phosphorodiamidate morpholino oligomer (PMO) conjugated to a fragment antibody (Fab) that binds to the transferrin receptor 1 (TfR1) which is highly expressed on muscle. It is designed to enable targeted muscle tissue delivery and promote exon skipping in the nucleus, allowing muscle cells to create a truncated, functional dystrophin protein, with the goal of stopping or reversing disease progression. DYNE-251 has been granted fast track, orphan drug and rare pediatric disease designations by the U.S. Food and Drug Administration for the treatment of DMD mutations amenable to exon 51 skipping.
除了DYNE-251,戴纳基正在建立一个全球DMD特许经营权,并有针对其他外显子(包括53、45和44)的临床前项目。
关于杜兴肌营养不良(DMD)
DMD是一种由编码肌细胞正常功能所必需蛋白质——肌铺干而造成的罕见疾病的突变基因引起的。其中大多数突变是缺失突变,导致缺乏肌铺干蛋白质和肌肉功能渐失的进展。DMD主要发生在男性,并影响大约12,000至15,000名美国人和25,000名欧洲人。力量和功能的丧失通常首先出现在学龄前的男孩身上,并随着年龄的增长而恶化。随着疾病的进展,骨骼和心脏肌肉受损的严重程度通常导致患者在13岁左右完全丧失行走能力,并在后期青少年时期出现加重的心脏和呼吸症状以及失去上肢功能的状况。目前没有DMD的治愈方法,当前批准的治疗方法只能提供有限的益处。
关于戴纳基(Dyne Therapeutics)
1. | DYNE-101的安全数据截至2024年8月20日。 |
2. | Contacts: |
3. | Investors |
| areilly@dyne-tx.com |
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