Apogee Therapeutics Announces Results Up to 9 Months From Phase 1 Trial of APG777, Its Novel Half-Life Extended Anti-IL-13 Antibody for the Treatment for Atopic Dermatitis and Other Inflammatory Diseases
Apogee Therapeutics Announces Results Up to 9 Months From Phase 1 Trial of APG777, Its Novel Half-Life Extended Anti-IL-13 Antibody for the Treatment for Atopic Dermatitis and Other Inflammatory Diseases
Pharmacokinetic data up to 9 months continue to support potential best-in-class profile, including a half-life of approximately 75 days, approximately three to five times that of currently approved treatments for moderate-to-severe AD
药代动力学数据长达9个月,继续支持潜在的最佳类别特性,包括约75天的半衰期,大约是目前批准用于中重度阿尔茨海默病治疗的三到五倍
Key biomarker data from single doses of APG777 show near complete inhibition of pSTAT6 and sustained TARC inhibition up to 9 months
来自APG777单剂量的关键生物标志数据显示几乎完全抑制pSTAT6,并在长达9个月的时间内持续抑制TARC
Proof-of-concept data from the ongoing APG777 Phase 2 clinical trial in patients with moderate-to-severe atopic dermatitis are expected in 2H 2025
预计在2025年下半年,正在进行中的APG777第2期临床试验在中重度特应性皮炎患者中的概念验证数据将会出现
APG777 has the potential to demonstrate improved clinical responses from greater exposures in induction and maintenance dosing of every 3- or 6-months
APG777有可能通过每3到6个月的诱导和维持剂量提高暴露水平,展现出改善临床反应的潜力
SAN FRANCISCO and WALTHAM, Mass., Oct. 24, 2024 (GLOBE NEWSWIRE) -- Apogee Therapeutics, Inc., (Nasdaq: APGE), a clinical-stage biotechnology company advancing novel biologics with potential for differentiated efficacy and dosing in the largest inflammatory and immunology (I&I) markets, including for the treatment of atopic dermatitis (AD), asthma, chronic obstructive pulmonary disease (COPD) and other I&I indications, today announced updated positive results from its ongoing Phase 1 clinical trial of APG777, a novel half-life extended anti-IL-13 antibody for the treatment for atopic dermatitis and other inflammatory diseases, in healthy volunteers up to nine months. These data will be presented at the American College of Allergy, Asthma & Immunology's (ACAAI) 2024 Annual Scientific Meeting, held in Boston from October 24-28, 2024.
旧金山和马萨诸塞州沃尔瑟姆,2024年10月24日(环球新闻社)——生态疗法公司爱文思控股(Nasdaq:APGE)是一家临床阶段生物技术公司,在最大的炎症和免疫学(I&I)市场中推进具有差异化疗效和剂量的新型生物制品,包括用于特应性皮炎(AD)、哮喘、慢性阻塞性肺病(COPD)和其他I&I适应症的治疗。今天,该公司宣布了其正在进行的APG777新型半衰期延长抗IL-13抗体对特应性皮炎和其他炎症性疾病的临床一期试验的更新积极结果,该试验已经进行了长达九个月的健康志愿者。这些数据将在美国过敏、哮喘及免疫学学院(ACAAI)2024年度科学会议上展示,该会议于2024年10月24日至28日在波士顿举行。
Today's results build on the Phase 1 positive interim data announced in March 2024. This updated dataset includes findings from the 40 enrolled participants across three single-ascending dose (SAD) cohorts, now with nine months of follow-up, and two multiple-ascending dose (MAD) cohorts, now with six months of follow-up. Findings demonstrated that APG777, in single doses up to 1,200mg or multiple doses of 300mg, showed a well-tolerated safety profile. Pharmacokinetic (PK) data was consistent with what was previously reported, including a half-life of approximately 75 days, dose proportional increases in Cmax and AUC, and low variability. APG777's pharmacodynamic (PD) profile showed near complete inhibition of pSTAT6 and sustained TARC inhibition up to 9 months. These findings further support Apogee's ongoing Phase 2 clinical trial of APG777 in patients with moderate-to-severe AD, with the potential for improved clinical responses from greater exposures in induction and significantly less frequent dosing in maintenance at every three or six months compared to every two-to-four week dosing with currently approved biologic therapies. The company expects to report 16-week topline data from Part A of the trial in the second half of 2025.
今天的结果是在2024年3月宣布的第一阶段积极中间数据基础上发展而来的。这些更新的数据集包括来自40名已入组志愿者的三个单升剂量(SAD)队列的发现,现在随访长达九个月,并包括两个多升剂量(MAD)队列,现在随访长达六个月。研究结果显示,APG777在单次剂量高达1,200毫克或多次300毫克剂量下,表现出良好耐受的安全性特征。药代动力学(PK)数据与先前报告一致,包括约75天的半衰期、Cmax和AUC的剂量比例增加以及低变异性。APG777的药效动力学(PD)特征表明近乎完全抑制pSTAT6并使TARC抑制持续达到9个月。这些发现进一步支持爱文思控股正在进行的APG777在中重度AD患者中的二期临床试验,带来了诱导期更大曝光强度和维持期明显较少剂量频率(每三到六个月一次)的潜力,相较于目前已批准的生物制品治疗每两至四周一次的剂量。该公司预计将于2025年下半年报告该试验A部分的16周头顶数据。
"Results from our Phase 1 trial of APG777 continue to support a potential best-in-class PK and PD profile of APG777, in particular a near-complete inhibition of pSTAT6 and sustained TARC inhibition out to nine months following a single dose," said Carl Dambkowski, M.D., Chief Medical Officer of Apogee. "Furthermore, we are pleased to see that APG777 continues to be well tolerated, and with APG777's PK profile, we remain confident that we can achieve maintenance dosing of every 3- to 6- months in patients with moderate-to-severe AD. We are on track to report initial data from Part A of our Phase 2 clinical trial in patients with moderate to severe AD in the second half of next year. We look forward to sharing more on APG777 and providing an update on our progress across all programs as well as highlighting our combination strategy in further detail at our R&D Day on December 2nd."
Apogee公司首席医疗官卡尔·丹布科夫斯基博士表示:“我们第一阶段对APG777的试验结果持续支持APG777具有潜在的最优Pk和PD特征,特别是对pSTAT6的近乎完全抑制以及单剂量后持续抑制TARC达九个月的效果。”“此外,我们很高兴看到APG777仍然被患者良好耐受,考虑到APG777的Pk特征,我们有信心能够在中度至重度AD患者中实现每3到6个月的维持剂量给药。我们正计划在明年下半年对中度至重度AD患者的第二阶段临床试验A部分的初步数据进行报告。我们期待在12月2日举行的研发日活动上详细介绍APG777的更多信息,同时更新所有项目的进展,并详细阐述我们的组合策略。”
Key Findings from the Phase 1 APG777 Results Up to 9 Months:
第1阶段APG777的关键发现结果长达9个月:
- Dose proportional PK was observed, with a half-life of ~75 days, approximately three to five times that of currently approved treatments for moderate-to-severe AD consistent with previously reported interim results.
- APG777 demonstrated dose proportional increases in Cmax and AUC from 300mg up to 1,200mg across all SAD and MAD cohorts.
- Single and multiple doses of APG777 resulted in rapid and sustained effect on PD markers for up to nine months.
- Single doses of APG777 showed rapid, near-complete inhibition of pSTAT6, one of the first downstream markers of IL-13 pathway inhibition, up to nine months (limit of available follow up in SAD cohort);
- MAD cohorts showed similar inhibition of pSTAT6 through available follow-up. Single doses of APG777 suppressed TARC, an inflammatory mediator and the most strongly correlated biomarker to AD severity, with deep and sustained inhibition for up to nine months.
- APG777 was generally well-tolerated at doses up to 1,200 mg.
- Treatment-emergent adverse events were generally mild-to-moderate and unrelated to APG777.
- There were no serious adverse events or dose-dependent trends observed up to time of data cut.
- 观察到剂量与Pk成正比,半衰期约为75天,约为目前批准的中度至重度AD治疗方案的三到五倍,与先前报告的中期结果一致。
- APG777表现出Cmax和AUC呈剂量成比例增加,从300mg到1,200mg在所有SAD和MAD队列中均有体现。
- APG777的单一和多剂量导致对PD标志物的快速和持久影响长达九个月。
- 单剂量APG777显示出对pSTAT6的迅速、几乎完全的抑制作用,pSTAT6是IL-13通路抑制的首个下游标记物之一,持续时间长达九个月(SAD队列中可获得的随访数据的极限);
- MAD队列通过可获得的随访数据显示了对pSTAT6的类似抑制作用。单剂量APG777抑制了TARC,这是一种炎症介质,与AD严重程度最强相关的生物标志物,深度且持续地抑制长达九个月。
- APG777在最高达到1,200毫克的剂量下一般耐受良好。
- 治疗出现的不良事件通常为轻到中度,并与APG777无关。
- 在数据截止时未观察到严重不良事件或剂量相关趋势。
Apogee's poster presentation from ACAAI can be found on the Publications page of the company website.
Apogee在ACAAI的海报展示可在公司网站的出版页面找到。
About APG777
APG777 is a novel, subcutaneous extended half-life monoclonal antibody targeting IL-13 – a critical cytokine in inflammation and a primary driver of AD. In our head-to-head preclinical studies, APG777 demonstrated equivalent or better potency to lebrikizumab in the inhibition of IL-13 signaling. Based on its potentially best-in-class PK profile, APG777 has the potential for improved clinical responses from greater exposures of drug in induction and dosing as infrequently as once every three or six months. AD is a chronic inflammatory skin disorder which can lead to sleep disturbance, psychological distress, elevated infection risk and chronic pain, all of which significantly impact quality of life. Today's treatments are associated with many challenges, including frequent injection regimens that can lead to poor patient compliance. APG777 represents the first clinical-stage product candidate from the company's strategic collaboration with Paragon Therapeutics, Inc., an innovative discovery engine for biologics.
关于APG777
APG777是一种新型的皮下延长半衰期单克隆抗体,靶向IL-13——一种重要的炎症细胞因子,是AD的主要驱动因素。在我们进行的对比临床研究中,APG777在抑制IL-13信号方面表现出与lebrikizumab相当或更好的效力。基于其潜在的一流Pk特性,APG777有可能通过更高的药物暴露,使诱导和每三到六个月一次的服药得以改善临床反应。AD是一种慢性炎症性皮肤疾病,可能导致睡眠障碍、心理困扰、感染风险升高和慢性疼痛,所有这些都会严重影响生活质量。现今的治疗方案存在诸多挑战,包括频繁的注射方案可能导致患者依从性差。APG777代表了公司与Paragon Therapeutics, Inc.的战略合作中首个处于临床阶段的产品候选药物,后者是生物制品创新发现引擎。
About Apogee
Apogee Therapeutics is a clinical-stage biotechnology company advancing novel biologics with potential for differentiated efficacy and dosing in the largest I&I markets, including for the treatment of AD, asthma, COPD and other I&I indications. Apogee's antibody programs are designed to overcome limitations of existing therapies by targeting well-established mechanisms of action and incorporating advanced antibody engineering to optimize half-life and other properties. APG777, the company's most advanced program, is being initially developed for the treatment of AD, which is the largest and one of the least penetrated I&I markets. With four validated targets in its portfolio, Apogee is seeking to achieve best-in-class efficacy and dosing through monotherapies and combinations of its novel antibodies. Based on a broad pipeline and depth of expertise, the company believes it can deliver value and meaningful benefit to patients underserved by today's standard of care. For more information, please visit .
关于Apogee:Apogee Therapeutics是一家处于临床阶段的生物技术公司,正在推进在最大的炎症和免疫(I&I)市场中具有差异化疗效和给药潜力的新型生物制品,包括治疗特应性皮炎(AD)、哮喘、慢性阻塞性肺疾病(COPD)和其他I&I适应症。Apogee的抗体计划旨在通过针对确定的作用机制,并结合先进的抗体工程来优化半衰期和其他特性,克服现有疗法的局限性。该公司最先进的APG777计划最初用于治疗AD,这是最大和最未渗透的I&I市场之一。根据其广泛管道和专业知识的基础,该公司相信它能通过其新型抗体的单一疗法和联合疗法实现最佳疗效和剂量,并为今天的治疗标准无法满足的患者提供有意义的益处。欲了解更多信息,请访问www.apogeetherapeutics.com。
Apogee Therapeutics是一家临床阶段的生物技术公司,正在推进具有差异化疗效和剂量潜力的新型生物制品,包括用于治疗AD、哮喘、COPD和其他I&I适应症。 Apogee的抗体项目旨在通过瞄准成熟机制和采用先进的抗体工程来优化半衰期和其他属性,以克服现有疗法的局限性。该公司最先进的项目APG777最初被开发用于治疗AD,这是最大且渗透率最低的I&I市场之一。凭借其组合中的四个验证靶点,Apogee希望通过其新型抗体的单药疗法和组合实现最佳疗效和剂量。基于其广泛的产品管线和专业知识,该公司相信自己可以为今天标准治疗无法满足的患者提供价值和有意义的益处。欲了解更多信息,请访问。
Forward Looking Statements
Certain statements in this press release may constitute "forward-looking statements" within the meaning of the federal securities laws, including, but not limited to, statements regarding: Apogee's plans for its current and future product candidates and programs, particularly APG777; its plans for current and future clinical trials; expected timing for release of data from Apogee's Phase 2 clinical trial of APG777 in AD; the potential clinical benefit, dosing schedule and half-life of APG777; plans for Apogee's other product candidates, and any other potential programs, including combination therapies. Words such as "may," "might," "will," "objective," "intend," "should," "could," "can," "would," "expect," "believe," "design," "estimate," "predict," "potential," "develop," "plan" or the negative of these terms, and similar expressions, or statements regarding intent, belief, or current expectations, are forward-looking statements. While Apogee believes these forward-looking statements are reasonable, undue reliance should not be placed on any such forward-looking statements, which are based on information available to the company on the date of this release. These forward-looking statements are based upon current estimates and assumptions and are subject to various risks and uncertainties (including, without limitation, those set forth in Apogee's filings with the U.S. Securities and Exchange Commission (the SEC)), many of which are beyond the company's control and subject to change. Actual results could be materially different. Risks and uncertainties include: global macroeconomic conditions and related volatility, expectations regarding the initiation, progress, and expected results of Apogee's preclinical studies, clinical trials and research and development programs; expectations regarding the timing, completion and outcome of Apogee's clinical trials; the unpredictable relationship between preclinical study results and clinical study results; the timing or likelihood of regulatory filings and approvals; liquidity and capital resources; and other risks and uncertainties identified in Apogee's Annual Report on Form 10-K for the year ended December 31, 2023, filed with the SEC on March 5, 2024, Quarterly Report on 10-Q for the quarterly period ended June 30, 2024, filed with the SEC on August 12, 2024, and subsequent disclosure documents we may file with the SEC. Apogee claims the protection of the Safe Harbor contained in the Private Securities Litigation Reform Act of 1995 for forward-looking statements. Apogee expressly disclaims any obligation to update or alter any statements whether as a result of new information, future events or otherwise, except as required by law.
前瞻性声明
本新闻稿中的某些声明可能构成《联邦证券法》中所述的"前瞻性声明",包括但不限于有关Apogee当前和未来产品候选药物和项目(尤其是APG777)的计划;当前和未来临床试验的计划;预期发布APG777用于治疗AD的2期临床试验数据的时间;APG777的潜在临床益处、剂量方案和半衰期;Apogee其他产品候选药物的计划,以及任何其他潜在项目,包括联合疗法。诸如"可能"、"也许"、"将会"、"目标"、"打算"、"应该"、"能够"、"愿意"、"期望"、"相信"、"设计"、"估计"、"预测"、"潜力"、"发展"、"计划"或这些词语的否定形式,以及类似表达,或涉及意图、信念或目前期望的声明均属于前瞻性声明。尽管Apogee认为这些前瞻性声明是合理的,但不应过分依赖任何此类前瞻性声明,因为这些声明基于公司在本发布日期可获得的信息。这些前瞻性声明基于目前的估计和假设,并受各种风险和不确定性的影响(包括但不限于Apogee在美国证券交易委员会(SEC)提交的文件中所列的风险和不确定因素),其中许多超出公司的控制范围并可能发生变化。实际结果可能截然不同。风险和不确定因素包括:全球宏观经济状况及相关波动,对Apogee的临床前研究、临床试验和研发项目的启动、进展和预期结果的期望;对Apogee的临床试验的时间、完成和结果的期望;临床前研究结果与临床研究结果之间不可预测的关系;监管申报和批准的时间或可能性;流动性和资本资源;以及Apogee在2023年12月31日结束的年度10-k报告,于2024年3月5日向SEC提交,在2024年6月30日结束的季度10-Q报告,于2024年8月12日向SEC提交,以及我们可能向SEC提交的后续披露文件中确定的其他风险和不确定因素。Apogee声称依据1995年《私人证券诉讼改革法案》中包含的安全港对前瞻性声明享有保护。Apogee明确否认更新或更改任何声明的义务,除非法律要求。
Investor Contact:
Noel Kurdi
VP, Investor Relations
Apogee Therapeutics, Inc.
Noel.Kurdi@apogeetherapeutics.com
投资者联系人:
Noel Kurdi
VP, 投资者关系
Apogee Therapeutics公司
Noel.Kurdi@apogeetherapeutics.com
Media Contact:
Dan Budwick
1AB Media
dan@1abmedia.com
媒体联系人:
Dan Budwick
1Ab Media
dan@1abmedia.com
译文内容由第三方软件翻译。
