100% of Patients Achieve Remission Within 30 Days in Cohort 1 of Bispecific Mipletamig Frontline AML Trial
100% of Patients Achieve Remission Within 30 Days in Cohort 1 of Bispecific Mipletamig Frontline AML Trial
Two of three patients achieved both complete remission and MRD-negative status
三名患者中有两名达成完全缓解和MRD阴性状态
High response rates observed in earlier studies continue in ongoing mipletamig trial
早期研究中观察到的高反应率在正在进行的mipletamig试验中持续存在
Cohort 2 enrollment commencing
第二队列入组即将开始
SEATTLE, WA / ACCESSWIRE / December 12, 2024 / Aptevo Therapeutics ("Aptevo") (Nasdaq:APVO), a clinical-stage biotechnology company focused on developing novel bispecific immune-oncology therapeutics based on its proprietary ADAPTIR and ADAPTIR-FLEX platform technologies, today announced 100% of patients achieved remission* within 30 days, in Cohort 1 of the RAINIER frontline acute myeloid leukemia (AML) Phase 1b trial, including two patients who experienced complete remission with minimal residual disease (MRD)-negative status (100% elimination of cancer cells). The results build on data from the prior trial, in which 100% of frontline patients also achieved remission. *(Remission = complete remission (CR) and, complete remission with blood markers that have not yet recovered (CRi).
西雅图,WA / ACCESSWIRE / 2024年12月12日 / Aptevo Therapeutics ("Aptevo") (纳斯达克:APVO),是一家专注于基于其专有的ADAPTIR和ADAPTIR-FLEX平台技术开发新型双特异性免疫肿瘤治疗的临床阶段生物技术公司,今天宣布在RAINIER前线急性髓细胞性白血病(AML)第10亿期试验的第一队列中,100%的患者在30天内达成缓解*,其中包括两名患者经历了完全缓解且最小残留疾病(MRD)-阴性状态(癌细胞完全消除)。这些结果建立在之前试验的数据上,其中100%的前线患者也达成了缓解。*(缓解 = 完全缓解(CR)和尚未恢复血液标志物的完全缓解(CRi)。
"We are very excited by these Cohort 1 results as they add to an already compelling story that highlights mipletamig's potential to elevate the frontline AML treatment paradigm. We now have a 100% rate of remission in Cohort 1 of RAINIER. We saw a 100% rate of remission in frontline patients treated with the combination in our completed dose expansion trial. Remarkably, 86% of patients across both trials went into remission within 30 days of receiving their first treatment," said Marvin White, President and CEO of Aptevo. "It's also important to note that mipletamig continues to demonstrate a favorable safety and tolerability profile, reinforcing its potential as a transformative addition to the standard of care combination. Cohort 2 enrollment is commencing, marking the next step in the study. We look forward to sharing new results as they become available."
“我们对这些第一队列的结果感到非常兴奋,因为它们增添了一个令人信服的故事,突显了mipletamig成为前线AML治疗范式的潜力。我们现在在RAINIER的第一队列中有100%的缓解率。在我们完成的剂量扩展试验中,接受组合治疗的前线患者的缓解率也是100%。令人瞩目的是,86%的患者在接受首次治疗后30天内达成缓解,”Aptevo的总裁兼首席执行官Marvin White说道。“同样重要的是,mipletamig继续展现出良好的安全性和耐受性特征,加强了其成为标准护理组合中变革性补充的潜力。第二队列的入组即将开始,标志着研究的下一步。我们期待分享新的结果,因为它们将逐步公布。”
Mipletamig, a CD3 x CD123 bispecific antibody, is being investigated as frontline therapy in combination with venetoclax and azacitidine, a current standard of care for AML. These latest results further reinforce mipletamig's potential as a transformative treatment, supported by impressive efficacy, safety, and tolerability data from two prior clinical trials involving 90 patients.
Mipletamig是一种CD3 x CD123双特异性抗体,正在作为前线治疗与venetoclax和azacitidine联合使用,这些是AML的当前标准护理。这些最新结果进一步强化了mipletamig作为变革性治疗的潜力,由来自两项涉及90名患者的先前临床试验的令人印象深刻的疗效、安全性和耐受性数据支持。
"Achieving remission in all three Cohort 1 patients is highly encouraging, particularly when viewed alongside prior trial results. Notably, two of these three patients achieved MRD-negative status, a critical outcome indicating that even the most sensitive diagnostic methods detect no remaining cancer cells. This result is strongly associated with longer-lasting remissions and improved survival rates," said Dirk Huebner, MD, Chief Medical Officer at Aptevo. "What makes these outcomes even more compelling is that one of the MRD-negative patients had a TP53 mutation, a subgroup known for its poor prognosis due to chemotherapy resistance, genetic instability, and overall treatment challenges. This growing body of data underscores mipletamig's potential to address some of the most difficult hurdles in AML treatment, delivering deep and durable responses for patients with the greatest need."
"在所有三位1组患者中实现缓解令人鼓舞,尤其是考虑到先前的试验结果。值得注意的是,这三名患者中有两名达到了MRD阴性状态,这一关键结果表明即使是最敏感的诊断方法也未检测到残留的癌细胞。这一结果与持久的缓解和提高的生存率密切相关," Aptevo的首席医疗官Dirk Huebner博士说。"这些结果更引人注目的是,其中一名MRD阴性患者有TP53突变,这是一个以化疗耐药、基因不稳定和整体治疗挑战而著称的亚组。这些不断增长的数据强调了mipletamig在解决AML治疗中的一些最困难障碍的潜力,为最需要的患者提供深层和持久的反应。"
About RAINIER
关于RAINIER
RAINIER, a frontline AML study, is a Phase 1b/2 dose optimization, multi-center, multi-cohort, open label study of up to 39 patients who are being treated across five dose levels ranging from 9 mcg - 140 mcg in combination with venetoclax and azacitidine (ven/aza). Subjects will be adults aged 18 or older, newly diagnosed with AML who are not eligible for intensive induction chemotherapy. Phase 1b consists of 28-day cycles of treatment in five sequential cohorts. Aptevo has partnered with Prometrika (), a premier contract research organization for the trial. RAINIER will be conducted in two parts. First, a Phase 1b dose optimization study in frontline AML patients followed by a Phase 2 study.
RAINIER是一项前线AML研究,是一项1b/2期剂量优化、多中心、多队列、开放标签的研究,最多包含39名患者,他们在与Venetoclax和Azacitidine(ven/aza)联合治疗的五个剂量水平中接受治疗,剂量范围为9微克-140微克。受试者将是年龄在18岁或以上的新诊断AML患者,且不符合严格诱导化疗的条件。第10亿期包含五个连续队列的28天治疗周期。Aptevo与Prometrika()合作,这是该试验的顶级合同研究组织。RAINIER将分为两部分进行。第一部分是针对前线AML患者的第10亿期剂量优化研究,随后是第2期研究。
About Mipletamig
关于Mipletamig
Aptevo's wholly owned lead proprietary drug candidate, mipletamig, targeting AML, MDS and other leukemias, is differentiated by design to redirect the immune system of the patient to destroy leukemic cells and leukemic stem cells expressing the target antigen CD123, which is a compelling target for AML due to its overexpression on leukemic stem cells and AML blasts. This antibody-like recombinant protein therapeutic is designed to engage both leukemic cells and T cells of the immune system and bring them closely together to trigger the destruction of leukemic cells. Mipletamig is purposefully designed to reduce the likelihood and severity of CRS by use of a unique CD3 derived from CRIS-7 vs. the CD3 used by other competitors. Mipletamig has received orphan drug designation ("orphan status") for AML according to the Orphan Drug Act. Mipletamig has been evaluated in 90 patients over two trials to date. RAINIER, Aptevo's Phase 1b/2 frontline AML program, was initiated in 3Q24.
Aptevo全资拥有的领先专有药物候选者mipletamig,针对AML、MDS及其他白血病,设计上旨在重新定向患者的免疫系统以破坏表达靶抗原CD123的白血病细胞和白血病干细胞,这是一个针对AML的引人注目的靶点,因为其在白血病干细胞和AML母细胞上过表达。这种类似抗体的重组蛋白治疗旨在使白血病细胞与免疫系统的T细胞紧密结合,以触发对白血病细胞的破坏。Mipletamig特意设计以降低CRS的可能性和严重性,通过使用与其他竞争者不同的CD3(来自CRIS-7的独特CD3)来实现。根据孤儿药法,Mipletamig已获得AML的孤儿药资格(“孤儿状态”)。迄今为止,Mipletamig在90名患者中进行了两项试验评估。RAINIER,Aptevo的1b/2期前线AML项目,计划于2024年第3季度启动。
About Aptevo Therapeutics
关于Aptevo Therapeutics
Aptevo Therapeutics Inc. (Nasdaq:APVO) is a clinical-stage biotechnology company focused on developing novel bispecific immunotherapies for the treatment of cancer. The company has two clinical candidates. Mipletamig is currently being evaluated in RAINIER, a Phase 1b/2 trial for the treatment of frontline acute myeloid leukemia in combination with standard of care venetoclax + azacitidine. Mipletamig has orphan status for AML according to the Orphan Drug Act. ALG.APV-527, a bispecific conditional 4-1BB agonist that is only active upon simultaneous binding to 4-1BB and 5T4, is being co-developed with Alligator Bioscience and is being evaluated in a Phase 1 clinical trial for the treatment of multiple solid tumor types likely to express 5T4. Aptevo has three pre-clinical candidates with different mechanisms of action designed to target a range of solid tumors. All pipeline candidates were created from two proprietary platforms, ADAPTIR and ADAPTIR-FLEX. The Aptevo mission is to improve treatment outcomes and transform the lives of cancer patients. For more information, please visit .
Aptevo Therapeutics Inc.(纳斯达克:APVO)是一家临床阶段的生物技术公司,专注于开发新型双特异性免疫疗法以治疗癌症。该公司有两个临床候选药物。Mipletamig目前正在RAINIER进行评估,这是一个针对前线急性髓系白血病的1b/2期试验,联合使用标准护理药物venetoclax + azacitidine。根据《孤儿药法》,Mipletamig获得了急性髓系白血病的孤儿药资格。ALG.APV-527是一种仅在同时与4-1Bb和5T4结合时才活跃的双特异性条件4-1Bb激动剂,正在与Alligator Bioscience共同开发,并正在1期临床试验中评估,用于治疗可能表达5T4的多种实体肿瘤。Aptevo拥有三个不同作用机制的临床前候选药物,旨在靶向多种实体肿瘤。所有管道候选药物均来自两个专有平台,ADAPTIR和ADAPTIR-FLEX。Aptevo的使命是改善治疗结果,改变癌症患者的生活。更多信息,请访问。
Safe Harbor Statement
安全港声明
This press release includes forward-looking statements within the meaning of the Private Securities Litigation Reform Act of 1995. All statements, other than statements of historical fact, including, without limitation, Aptevo's expectations about the activity, efficacy, safety, tolerability and durability of its therapeutic candidates and potential use of any such candidates, including in combination with other drugs, as therapeutics for treatment of disease, its expectations regarding the effectiveness of its ADAPTIR and ADAPTIR-FLEX platforms, statements related to the progress of Aptevo's clinical programs, including statements related to anticipated clinical and regulatory milestones, whether further study of mipletamig in a Phase 1b dose optimization trial focusing on multiple doses of mipletamig in combination with venetoclax + azacitidine on a targeted patient population will continue to show remissions, let alone at a rate of 100%, whether Aptevo's final remission data or trial results will vary from its earlier assessment, whether Aptevo's strategy will translate into an improved overall survival in AML, especially among patient subgroups with poor prognosis, whether further study of ALG.APV-527 across multiple tumor types will continue to show clinical benefit, the possibility and timing of future preliminary or interim data readouts for ALG.APV-527, statements related to the progress of and enthusiasm for Aptevo's clinical programs, statements related to Aptevo's ability to generate stockholder value, whether Aptevo will continue to have momentum in its business in the future, and any other statements containing the words "may," "continue to," "believes," "knows," "expects," "optimism," "potential," "designed," "promising," "plans," "will" and similar expressions are intended to identify forward-looking statements. These forward-looking statements are based on Aptevo's current intentions, beliefs, and expectations regarding future events. Aptevo cannot guarantee that any forward-looking statement will be accurate. Investors should realize that if underlying assumptions prove inaccurate or unknown risks or uncertainties materialize, actual results could differ materially from Aptevo's expectations. Investors are, therefore, cautioned not to place undue reliance on any forward-looking statement.
本新闻稿包含1995年《私人证券诉讼改革法》意义上的前瞻性声明。除了历史事实的陈述外,所有声明均包括但不限于Aptevo对其治疗候选药物的活性、疗效、安全性、耐受性和持久性的预期及其潜在用途(包括与其他药物联合使用作为疾病治疗的治疗选项),对其ADAPTIR和ADAPTIR-FLEX平台效力的预期,涉及Aptevo临床项目进展的声明,包括有关预期临床和监管里程碑的声明,mipletamig在10亿剂量优化试验中的进一步研究是否会继续显示缓解,何况以100%的比例,Aptevo的最终缓解数据或试验结果是否会与其早期评估有所不同,Aptevo的策略是否会转化为急性髓系白血病的整体生存改善,尤其是在预后不良的患者亚组中,ALG.APV-527在多种肿瘤类型中的进一步研究是否会继续显示临床获益,ALG.APV-527未来初步或中期数据结果的可能性和时间,涉及Aptevo临床项目进展及其热情的声明,涉及Aptevo创造股东价值能力的声明,Aptevo在未来是否会继续保持业务的动力,以及任何其他含有“可能”、“继续”、“相信”、“知道”、“期待”、“乐观”、“潜力”、“设计”、“有前途”、“计划”、“将会”等类似表述的声明,旨在识别前瞻性声明。这些前瞻性声明基于Aptevo对未来事件的当前意图、信念和预期。Aptevo不能保证任何前瞻性声明的准确性。投资者应意识到,如果基础假设被证明不准确或未知风险或不确定性出现,实际结果可能会与Aptevo的预期有实质性差异。因此,投资者被警告不要过分依赖任何前瞻性声明。
There are several important factors that could cause Aptevo's actual results to differ materially from those indicated by such forward-looking statements, including a deterioration in Aptevo's business or prospects; further assessment of preliminary or interim data or different results from later clinical trials; adverse events and unanticipated problems, adverse developments in clinical development, including unexpected safety issues observed during a clinical trial; and changes in regulatory, social, macroeconomic and political conditions. For instance, actual results may differ materially from those indicated by such forward-looking statements as a result of various important factors, including the uncertainties inherent in the results of preliminary or interim data and preclinical studies being predictive of the results of later-stage clinical trials, initiation, enrollment and maintenance of patients, and the completion of clinical trials, the availability and timing of data from ongoing clinical trials, the trial design includes combination therapies that may make it difficult to accurately ascertain the benefits of mipletamig, expectations for the timing and steps required in the regulatory review process, expectations for regulatory approvals, the impact of competitive products, our ability to enter into agreements with strategic partners or raise funds on acceptable terms or at all and other matters that could affect the availability or commercial potential of Aptevo's product candidates, business or economic disruptions due to catastrophes or other events, including natural disasters or public health crises such as the coronavirus (referred to as COVID-19), geopolitical risks, including the current war between Russia and Ukraine, war between Israel and Hamas, and macroeconomic conditions such as economic uncertainty, rising inflation and interest rates, continued market volatility and decreased consumer confidence. These risks are not exhaustive, Aptevo faces known and unknown risks. Additional risks and factors that may affect results are set forth in Aptevo's filings with the Securities and Exchange Commission, including its Annual Report on Form 10-K for the fiscal year ended December 31, 2023, and its subsequent reports on Form 10-Q and current reports on Form 8-K. The foregoing sets forth many, but not all, of the factors that could cause actual results to differ from Aptevo's expectations in any forward-looking statement. Any forward-looking statement speaks only as of the date of this press release, and, except as required by law, Aptevo does not assume any obligation to update any forward-looking statement to reflect new information, events, or circumstances.
有几个重要因素可能导致Aptevo的实际结果与这些前瞻性声明中所示的结果有重大差异,包括Aptevo的业务或前景恶化;对初步或中期数据的进一步评估或后续临床试验的不同结果;不良事件和意外问题,临床开发中出现的不利进展,包括在临床试验中观察到的意外安全性问题;以及监管、社会、宏观经济和政治条件的变化。例如,实际结果可能因各种重要因素而与这些前瞻性声明中所示的结果存在重大差异,包括初步或中期数据以及临床前研究结果的不确定性,能否预测后期临床试验的结果,患者的启动、招募和维持,临床试验的完成,来自正在进行的临床试验的数据的可用性和时机,试验设计包括的组合疗法可能使准确评估mipletamig的益处变得困难,监管审查过程中的预期时间和步骤,监管批准的预期,对竞争产品的影响,我们和战略伙伴达成协议的能力或以可接受的条款筹集资金的能力,以及可能影响Aptevo产品候选人的可用性或商业潜力的其他事项,因灾害或其他事件(包括自然灾害或公共卫生危机,如新冠病毒(称为COVID-19))而导致的业务或经济中断,地缘政治风险,包括俄罗斯与乌克兰之间当前的战争,以色列与哈马斯之间的战争,以及经济不确定性、日益上升的通货膨胀和利率、市场持续波动以及消费者信心下降等宏观经济条件。这些风险并不详尽,Aptevo面临已知和未知的风险。可能影响结果的其他风险和因素列在Aptevo提交给证券交易委员会的文件中,包括截至2023年12月31日财年的10-k表格年度报告及其后续10-Q表格和8-k表格的当前报告。上述内容列出了许多但不是所有可能导致实际结果与Aptevo在任何前瞻性声明中的期望不符的因素。任何前瞻性声明仅在本新闻稿发布之日有效,除法律要求外,Aptevo不承担更新任何前瞻性声明以反映新信息、事件或情况的义务。
CONTACT:
联系方式:
Miriam Weber Miller
Head, Investor Relations & Corporate Communications
Aptevo Therapeutics
Email: IR@apvo.com or Millerm@apvo.com
Phone: 206-859-6628
米里亚姆·韦伯·米勒
投资者关系及企业传播负责人
Aptevo Therapeutics
电子邮件:IR@apvo.com 或 Millerm@apvo.com
电话:206-859-6628
SOURCE: Aptevo Therapeutics
来源:Aptevo Therapeutics
译文内容由第三方软件翻译。
