Rapport Therapeutics Announces New Phase 1 Data, Further Supporting RAP-219's Transformative Potential for CNS Disorders
Rapport Therapeutics Announces New Phase 1 Data, Further Supporting RAP-219's Transformative Potential for CNS Disorders
In the PET trial, RAP-219 achieved and exceeded target receptor occupancy, increasing support for the dosing regimen utilized in the ongoing Phase 2a trial in focal epilepsy; restricted neuroanatomical expression of TARP8 was confirmed
在PEt试验中,RAP-219达到了并超过了目标受体占有率,提高了对正在进行的2a期局灶性癫痫试验中使用的剂量方案的支持;确认了TARP8的限制性神经解剖表达。
In the MAD-2 trial, RAP-219 was observed to be generally well tolerated with faster titration and higher exposures than in the initial MAD trial
在MAD-2试验中,观察到RAP-219通常耐受良好,且比初始MAD试验具有更快的剂量递增和更高的暴露量。
Data underscore the potential broad therapeutic index of RAP-219 and dosing flexibility
数据强调了RAP-219潜在的广泛治疗指数和灵活的剂量方案。
Ongoing Phase 2a trial of RAP-219 in focal epilepsy is on track and topline data is expected in mid-2025
正在进行的RAP-219在局灶性癫痫的2a期试验进展顺利,预计将在2025年中期提供顶线数据。
BOSTON and SAN DIEGO, Jan. 09, 2025 (GLOBE NEWSWIRE) -- Rapport Therapeutics, Inc. (Nasdaq: RAPP), a clinical-stage biotechnology company dedicated to the discovery and development of small molecule precision medicines for patients suffering from central nervous system (CNS) disorders, today announced results from its positron emission tomography (PET) trial and second multiple ascending dose (MAD-2) trial for RAP-219. Data from the trials demonstrated that RAP-219 achieved target receptor occupancy (RO) associated with maximal efficacy in prior preclinical models within five days of dosing while maintaining a differentiated tolerability profile.
波士顿和圣地亚哥,2025年1月9日(环球新闻)——Rapport Therapeutics, Inc.(纳斯达克:RAPP),一家致力于为患有中枢神经系统(CNS)疾病的患者发现和开发小分子精准医疗的临床阶段生物技术公司,今天公布了其正电子发射断层扫描(PET)试验和第二个多次递增剂量(MAD-2)试验的结果。试验数据表明,RAP-219在给药五天内达到了与最大疗效相关的目标受体占有率(RO),同时保持了差异化的耐受性轮廓。
"These Phase 1 results reinforce our belief in RAP-219's distinct profile and potential to deliver transformative outcomes for patients," said Steve Paul, M.D., Rapport cofounder and chair of the board of directors. "The data demonstrate that neuroanatomical specificity can be achieved through RAP-219's selective targeting of a receptor-associated protein, and RAP-219 was able to quickly achieve target engagement and therapeutic exposures in the brain while maintaining a generally favorable tolerability profile. Additionally, the data provide further support for the dosing regimen selected for our ongoing Phase 2a trial in focal epilepsy."
"这些一期试验结果巩固了我们对RAP-219独特特征及其为患者带来变革性结果潜力的信心,"Rapport的联合创始人和董事会主席Steve Paul万.D.表示。"数据表明,通过RAP-219选择性靶向与受体相关的蛋白,可以实现神经解剖的特异性,并且RAP-219能够迅速在大脑中实现目标参与和治疗暴露,同时保持普遍良好的耐受性。此外,数据进一步支持我们为正在进行的2a期焦点癫痫试验选择的给药方案。"
A total of four Phase 1 trials have been conducted to date, with 100 healthy volunteers exposed to RAP-219. In these trials, RAP-219 was generally well tolerated in multiple repeat-dose studies with up to 28 days of dosing, with no serious adverse events (SAEs), no treatment emergent adverse events (TEAEs) greater than Grade 2, and no clinically relevant laboratory or electrocardiogram (ECG) abnormalities. Three treatment discontinuations occurred (3%) that were attributed to TEAEs. The trials also showed that favorable tolerability was achieved with various dosing and titration regimens. Rapport believes the pharmacokinetic (PK) and tolerability outcomes from these clinical trials provide compelling translational evidence of selectively targeting TARP8 associated AMPA receptors to significantly enhance the therapeutic index of AMPA receptor modulation.
迄今为止总共进行了四个一期试验,100名健康志愿者接触了RAP-219。在这些试验中,RAP-219在多次重复给药的研究中普遍耐受良好,最长可达28天,未出现严重不良事件(SAE),也没有出现超过2级的治疗引起的不良事件(TEAE),并且没有临床相关的实验室或心电图(ECG)异常。发生了三例(3%)因TEAE而中止治疗。试验还表明,通过各种给药和 titration 方案实现了良好的耐受性。Rapport认为,这些临床试验的药代动力学(PK)和耐受性结果提供了有力的转化证据,表明选择性靶向与 TARP8 相关的 AMPA 受体可以显著增强 AMPA 受体调节的治疗指数。
"Due to the non-specific nature of currently available and other investigational treatments, many patients continue to endure significant side effects, which limit therapeutic efficacy and diminish their quality of life," said Abe Ceesay, chief executive officer of Rapport. "RAP-219 was designed to overcome such limitations, and we believe these compelling new data support our approach as we advance our Phase 2a trial in focal epilepsy, with topline results expected in mid-2025."
“由于目前可用的非特定性质的其他研究治疗,许多患者继续经历显著的副作用,这限制了治疗效果并降低了他们的生活质量,”Rapport的首席执行官Abe Ceesay说。“RAP-219的设计旨在克服这些局限性,我们相信这些引人注目的新数据支持我们的做法,我们将在癫痫局灶性2a期试验中推进,顶线结果预计在2025年中期公布。”
Also announced today, Bradley Galer, M.D., has stepped down as chief medical officer of Rapport. A search for his successor is underway, and the Company is confident that the transition will not disrupt progress across its clinical programs. Dr. Galer will be assisting the transition, and the Company is grateful for his support and contributions to Rapport over the past two years.
今天还宣布,Bradley Galer万.D.已辞去Rapport的首席医疗官职务。正在寻找他的继任者,公司相信这一过渡不会影响其临床项目的进展。Galer博士将协助这次过渡,公司对他在过去两年对Rapport的支持和贡献表示感激。
Results from the recent PET and MAD-2 trials are below, based on preliminary analysis of the data. Clinical conduct of the PET and MAD-2 trials is complete, and the clinical study reports for both are in progress.
基于数据的初步分析,最近的PEt和MAD-2试验结果如下。PEt和MAD-2试验的临床实施已经完成,两个试验的临床研究报告正在进行中。
The PET trial (RAP-219-103) was an open label trial in healthy volunteers designed to confirm neuroanatomical expression of TARP8 and establish the relationship between PK and brain target RO with RAP-219. The trial included three cohorts: Cohort 1 was given the same dosing regimen currently being used in the Phase 2a trial in focal epilepsy (0.75 mg daily for 5 days, followed by 1.25 mg daily for 9 days), and lower doses were used in the other two cohorts to better characterize the plasma concentration versus RO relationship. Cohort 2 was given 0.25 mg daily for 14 days and Cohort 3 was given 0.25 mg daily for 7 days, followed by 0.5 mg daily for 7 days.
PEt试验(RAP-219-103)是一个开放标签试验,在健康志愿者中进行,旨在确认TARP8的神经解剖表达,并建立Pk与大脑靶标RO与RAP-219的关系。试验包括三个组别:第一组使用的剂量方案与正在进行的癫痫局灶性2a期试验中使用的相同(每天0.75毫克,为期5天,然后每天1.25毫克为期9天),其他两个组别使用较低剂量以更好地表征血浆浓度与RO的关系。第二组每天0.25毫克,持续14天;第三组每天0.25毫克,持续7天,然后每天0.5毫克,持续7天。
PET trial results are summarized below:
PEt试验结果总结如下:
- The PET data demonstrated that Cohort 1 (the dosing regimen utilized in the ongoing Phase 2a trial in focal epilepsy) exceeded the target RO range associated with maximal efficacy in prior preclinical models (50%-70%) within five days of dosing, while maintaining a differentiated tolerability profile generally consistent with prior Phase 1 trial findings.
- The trial confirmed that the expression of TARP8-containing AMPA receptors is enriched in the hippocampus and cerebral cortex and is minimal in the cerebellum and brain stem.
- Collectively, data from the PET and MAD-2 trials demonstrated that plasma concentrations and associated target RO could be achieved within 5 days.
- PEt数据显示,1组(在进行中的2a期局部癫痫试验中使用的给药方案)在给药五天内超过了与之前的前临床模型相关的最大疗效目标RO区间(50%-70%),同时保持了一种与之前的1期试验结果普遍一致的差异化耐受性特征。
- 试验确认含有TARP8的AMPA受体在海马体和大脑皮层中的表达丰富,而在小脑和脑干中则很少。
- 总的来说,PEt和MAD-2试验的数据表明,在5天内可实现血浆浓度及相关的目标RO。
The MAD-2 (RAP-219-104) trial was a double-blind, placebo-controlled trial in healthy volunteers and was the second MAD trial of RAP-219. The trial was designed to further evaluate safety and tolerability with continued dose escalation, as well as to shorten time to reach predicted therapeutic levels of RAP-219. The trial included three cohorts: Cohort 1 (0.75 mg for 3 days, 1.25 mg for 3 days, 1.75 mg for 2 days), Cohort 2 (0.75 mg for 2 days, 1.25 mg for 2 days, 1.75 mg for 4 days), and Cohort 3 (0.5 mg for 2 days, 1 mg for 2 days, 1.75 mg for 24 days).
MAD-2(RAP-219-104)试验是一项针对健康志愿者的双盲、安慰剂对照试验,是RAP-219的第二次MAD试验。该试验旨在进一步评估安全性和耐受性,并持续进行剂量递增,缩短达到预测的RAP-219治疗水平所需的时间。该试验包括三个组:1组(3天0.75 mg,3天1.25 mg,2天1.75 mg),2组(2天0.75 mg,2天1.25 mg,4天1.75 mg),3组(2天0.5 mg,2天1 mg,24天1.75 mg)。
MAD-2 trial results are summarized below:
MAD-2试验结果总结如下:
- RAP-219 was generally well tolerated. All TEAEs were Grade 1 or 2 and generally consistent with tolerability observed in prior Phase 1 trials.
- Unlike with many anti-seizure medications, no sedation or motoric impairments were observed with RAP-219, consistent with target biology and preclinical observations.
- Target exposures and RO were achieved within 5 days of dosing across various dosing regimens.
- RAP-219通常耐受良好。所有不良事件均为1级或2级,且与之前的1期试验中观察到的耐受性一致。
- 与许多抗惊厥药物不同,RAP-219未观察到镇静或运动功能障碍,这与靶向生物学和临床前观察结果一致。
- 在各种给药方案中,靶定暴露和RO在给药后的5天内达成。
A Phase 2a proof-of-concept trial is currently underway to evaluate RAP-219 in patients with refractory focal epilepsy, with topline results expected in mid-2025.
目前正在进行一项2a期概念验证试验,以评估RAP-219在难治性局灶性癫痫患者中的疗效,预计在2025年中期公布主要结果。
About RAP-219
RAP-219 is a clinical-stage AMPA receptor negative allosteric modulator designed to achieve neuroanatomical specificity through its selective targeting of AMPA-associated protein, TARP8. AMPA receptors are present throughout the brain, including in the cerebellum and brain stem, where their non-selective targeting has resulted in poor tolerability. In contrast, TARP8 expression is enriched in the hippocampus and cerebral cortex and is minimal in the cerebellum and brain stem. RAP-219 is designed to be highly potent and selective for TARP8. It has been observed to have a long half-life (8–14 days) and minimal drug-drug interactions, making it potentially well-suited for polypharmacy. With this profile, RAP-219 has the potential to provide improved activity, tolerability, and a higher therapeutic index, potentially providing more patients with sustained therapeutic benefits without intolerable side effects, as compared to traditional neuroscience medications. As AMPA receptors play critical roles in numerous neurological disorders, selective targeting of TARP8 may provide a pipeline-in-a-product opportunity. The Company is currently pursuing RAP-219 as a potentially differentiated treatment for patients with focal epilepsy, diabetic peripheral neuropathic pain, and bipolar mania.
关于RAP-219
RAP-219是一种临床阶段的AMPA受体负向别构调节剂,旨在通过选择性靶向与AMPA相关的蛋白TARP8实现神经解剖特异性。AMPA受体遍布整个大脑,包括小脑和脑干,其非选择性靶向导致了耐受性差。相比之下,TARP8在海马体和大脑皮层的表达丰富,而在小脑和脑干中表达很少。RAP-219被设计为对TARP8具有高度的效力和选择性。研究表明,其半衰期较长(8-14天)且药物间相互作用最小,使其可能非常适合多药联用。凭借这一特征,RAP-219有潜力提供改善的活性、耐受性和更高的治疗指数,可能为更多患者提供持续的治疗效果,而不会出现不可耐受的副作用,相较传统神经科学药物而言。由于AMPA受体在众多神经系统疾病中起着关键作用,选择性靶向TARP8可能提供一个产品中的管道机会。公司目前正在推进RAP-219,作为可能的差异化治疗方案,用于治疗局灶性癫痫、糖尿病周围神经病痛和双相躁狂。
About Rapport Therapeutics
Rapport Therapeutics is a clinical-stage biotechnology company dedicated to discovering and developing small molecule precision medicines for patients suffering from central nervous system (CNS) disorders. The Company's founders have made pioneering discoveries related to the function of receptor associated proteins (RAPs) in the brain. Their findings form the basis of Rapport's RAP technology platform, which enables a differentiated approach to generate precision small molecule product candidates with the potential to overcome many limitations of conventional neurology drug discovery. Rapport's precision neuroscience pipeline includes the Company's lead clinical program, RAP-219, designed to achieve neuroanatomical specificity through its selective targeting of a RAP expressed in only discrete regions of the brain. The Company is currently advancing RAP-219 in clinical trials in focal epilepsy, diabetic peripheral neuropathic pain, and bipolar mania. Additional preclinical and late-stage discovery stage programs are also underway, targeting CNS disorders including chronic pain and hearing disorders.
关于Rapport Therapeutics
Rapport Therapeutics是一家临床阶段的生物技术公司,专注于发现和开发用于治疗中枢神经系统(CNS)疾病的精密小分子药物。公司的创始人对大脑中受体相关蛋白(RAPs)的功能进行了开创性的发现。他们的研究成果构成了Rapport的RAP技术平台的基础,该平台使其能够采用差异化的方法生成精准的小分子产品候选,以克服传统神经学药物发现的许多局限。Rapport的精准神经科学管道包括公司的首个临床项目RAP-219,旨在通过选择性靶向仅在大脑特定区域表达的RAP,实现神经解剖特异性。公司目前正在临床试验中推进RAP-219,针对局灶性癫痫、糖尿病周围神经病痛和双相躁狂。此外,还在进行其他前临床和晚期发现阶段的项目,目标针对包括慢性疼痛和听力障碍在内的CNS疾病。
Forward-Looking Statements
This press release contains "forward-looking statements" within the meaning of Section 27A of the Securities Act of 1933 and Section 21E of the Securities Exchange Act of 1934, each as amended. The words "anticipate," "believe," "continue," "could," "estimate," "expect," "intend," "may," "plan," "potential," "predict," "project," "should," "target," "would" and similar expressions are intended to identify forward-looking statements, although not all forward-looking statements contain these identifying words. These forward-looking statements include, but are not limited to, express or implied statements regarding: the broad therapeutic index of RAP-219 and its ability to deliver transformative outcomes for patients; the clinical development of RAP-219 for the treatment of drug-resistant focal epilepsy, peripheral neuropathic pain and bipolar acute mania, including expected dosing flexibility; the expected timing of the results from ongoing clinical trials; the activity and tolerability of RAP-219, including its neuroanatomical specificity; and Rapport's RAP technology platform.
前瞻性声明
本新闻稿包含在1933年证券法第27A条和1934年证券交易法第21E条的意义下的“前瞻性声明”,两者均经过修订。 "预计"、"相信"、"继续"、"可能"、"估计"、"期望"、"打算"、"可以"、"计划"、"潜在"、"预测"、"项目"、"应该"、"目标"、"会"以及类似的表达旨在识别前瞻性声明,尽管并非所有前瞻性声明都包含这些识别词。这些前瞻性声明包括但不限于:关于RAP-219广泛的治疗指数及其为患者带来变革性结果的能力;RAP-219用于治疗药物抵抗性局灶性癫痫、周围神经痛和双相急性狂躁的临床开发,包括预期的剂量灵活性;来自正在进行的临床试验的结果的预期时间;RAP-219的活性和耐受性,包括其神经解剖特异性;以及Rapport的RAP技术平台。
Forward looking statements are based on management's current expectations and are subject to risks and uncertainties that could negatively affect Rapport's business, operating results, financial condition, and stock value. Factors that could cause actual results to differ materially from those currently anticipated include: risks relating to the company's research and development activities, including that interim, topline and preliminary data from our clinical trials that we announce or publish from time to time are subject to audit and verification procedures that could result in material changes in the final data; Rapport's ability to execute on its strategy including obtaining the requisite regulatory approvals on the expected timeline, if at all; uncertainties relating to preclinical and clinical development activities; the company's dependence on third parties to conduct clinical trials, manufacture its product candidates and develop and commercialize its product candidates, if approved; Rapport's ability to attract, integrate and retain key personnel; risks related to the company's financial condition and need for substantial additional funds in order to complete development activities and commercialize a product candidate, if approved; risks related to regulatory developments and approval processes of the U.S. Food and Drug Administration and comparable foreign regulatory authorities; risks related to establishing and maintaining Rapport's intellectual property protections; and risks related to the competitive landscape for Rapport's product candidates; as well as other risks described in "Risk Factors," in the company's Registration Statement on Form S-1, and most recent Quarterly Report on Form 10-Q, as well as discussions of potential risks, uncertainties, and other important factors in Rapport's subsequent filings with the Securities and Exchange Commission. Rapport expressly disclaims any obligation or undertaking to release publicly any updates or revisions to any forward-looking statements contained herein to reflect any change in its expectations or any changes in events, conditions or circumstances on which any such statement is based, except as required by law, and claims the protection of the safe harbor for forward-looking statements contained in the Private Securities Litigation Reform Act of 1995.
前瞻性声明基于管理层当前的预期,并受到可能对Rapport的业务、运营结果、财务状况和股票价值产生负面影响的风险和不确定性的影响。可能导致实际结果与目前预期大相径庭的因素包括:与公司研究和开发活动相关的风险,包括我们不时宣布或发布的临床试验的中期、顶线和初步数据受到审计和验证程序的影响,这可能导致最终数据的重大变化;Rapport实施其策略的能力,包括在预期时间内获得必要的监管批准,如果能获得的话;与临床前和临床开发活动相关的不确定性;公司对第三方进行临床试验、制造其产品候选药物以及开发和商业化其产品候选药物(如果获得批准)的依赖;Rapport吸引、整合和留住关键人员的能力;与公司财务状况以及需要大量额外资金以完成开发活动和商业化产品候选药物(如果获得批准)相关的风险;与美国食品和药物管理局及可比的外国监管机构的监管发展和批准过程相关的风险;与建立和维护Rapport的知识产权保护相关的风险;以及与Rapport产品候选药物的竞争环境相关的风险;以及在公司的S-1登记声明中的“风险因素”以及最近的10-Q季度报告中描述的其他风险,以及Rapport后续向证券交易委员会提交的文件中讨论的潜在风险、不确定性和其他重要因素。Rapport明确声明不承担任何义务或承诺公开发布任何前瞻性声明的更新或修订,以反映其预期的任何变化或任何此类声明所基于的事件、条件或情况的变化,法律要求的除外,并主张享有1995年私人证券诉讼改革法案中所包含的前瞻性声明的安全港保护。
CONTACT: Contact
Julie DiCarlo
Head of Communications & IR
Rapport Therapeutics
jdicarlo@rapportrx.com
联系方式:联系
朱莉·迪卡尔洛
传播与投资关系负责人
拉波特治疗技术
jdicarlo@rapportrx.com
