SELLAS Life Sciences Reports Promising Data From Phase 2 Trial of SLS009 in Relapsed/Refractory Acute Myeloid Leukemia
SELLAS Life Sciences Reports Promising Data From Phase 2 Trial of SLS009 in Relapsed/Refractory Acute Myeloid Leukemia
The overall response rate (ORR) is 56% to date in patients with acute myeloid leukemia with myelodysplasia-related changes.SELLAS reports median overall survival over 7.7 months and a 56% overall response rate for AML patients using SLS009.
SELLAS报告使用SLS009的急性髓性白血病(AML)患者中位整体生存期超过7.7个月,整体反应率为56%。
Quiver AI Summary
Quiver AI 概要
SELLAS Life Sciences Group, Inc. has released promising new data from its Phase 2 clinical trial of SLS009, a CDK9 inhibitor for patients with relapsed or refractory acute myeloid leukemia (r/r AML). In the 30 mg dosing cohort, the median overall survival (mOS) has now exceeded 7.7 months at the latest follow-up, significantly higher than the historical expected mOS of 2.5 months for this patient population. Additionally, the overall response rate (ORR) in two expansion cohorts of patients with acute myeloid leukemia with myelodysplasia-related changes is 56%, surpassing the pre-established target of 33%. The drug has been well-tolerated with no new safety issues reported, further supporting its potential as a vital new treatment option for patients with challenging AML nuances.
SELLAS生命科学集团公司发布了其SLS009的第二阶段临床试验的新数据,SLS009是一种针对复发或难治性急性髓性白血病(r/r AML)患者的CDK9抑制剂。在30毫克剂量组中,最新随访中位整体生存期(mOS)现已超过7.7个月,显著高于该患者人群历史预期的2.5个月的mOS。此外,在两组患有与骨髓增生异常相关变化的急性髓性白血病患者中的整体反应率(ORR)为56%,超出了预先设定的33%的目标。该药物耐受性良好,没有报告新的安全性问题,进一步支持其作为患者难治性AML新治疗选择的潜力。
Potential Positives
潜在的积极因素
- Median Overall Survival (mOS) exceeds 7.7 months in patients relapsed or refractory to venetoclax-based regimens, significantly higher than the expected 2.5 months.
- Overall Response Rate (ORR) of 56% achieved in patients with Acute Myeloid Leukemia with Myelodysplasia Related Changes (AML MRC), surpassing the pre-specified target of 33%.
- SLS009 demonstrated a favorable safety profile with no new safety signals observed to date.
- Rapid enrollment in the expansion cohorts indicates a high demand for new treatment options in the underserved patient population of r/r AML.
- 在对venetoclax基础方案复发或难治的患者中,中位整体生存期(mOS)超过7.7个月,显著高于预期的2.5个月。
- 在患有与骨髓增生异常相关变化的急性髓性白血病患者中,整体反应率(ORR)达到56%,超出了先前规定的33%的目标。
- SLS009表现出良好的安全性特征,目前没有观察到新的安全信号。
- 在扩展队列中的快速入组表明对急性髓性白血病(r/r AML)患者这一服务不足的人群的新治疗选择需求旺盛。
Potential Negatives
潜在负面因素
- Median Overall Survival (mOS) has not yet been reached, which may signal uncertainty about the drug's efficacy in longer-term outcomes.
- The clinical trial's open-label design may raise concerns regarding bias in reporting and measuring efficacy outcomes.
- Despite positive preliminary response rates, the overall number of evaluable patients is low, which might not provide a robust understanding of treatment efficacy across a broader patient population.
- 中位总生存期(mOS)尚未达到,这可能表明对药物在长期结果中的有效性存在不确定性。
- 临床试验的开放标签设计可能会引发有关报告和测量有效性结果的偏倚的担忧。
- 尽管初步响应率积极,但可评估患者的整体数量较少,这可能无法提供对更广泛患者群体治疗有效性的稳健理解。
FAQ
常见问题
What are the latest survival results for SLS009 in AML patients?
SLS009在急性髓细胞白血病(AML)患者中的最新生存结果是什么?
The median overall survival (mOS) has not yet been reached but exceeds 7.7 months in the 30 mg BIW cohort.
中位总生存期(mOS)尚未达到,但在30 mg双周剂量组中超过7.7个月。
What is the overall response rate in the expansion cohorts for AML?
在急性髓细胞白血病(AML)扩展队列中的总体响应率是多少?
The overall response rate (ORR) is 56% to date in patients with acute myeloid leukemia with myelodysplasia-related changes.
迄今为止,急性髓性白血病伴骨髓异常增生改变患者的整体反应率(ORR)为56%。
How does SLS009 compare to historical treatment outcomes?
SLS009与历史治疗结果相比如何?
The expected mOS for patients in this setting is typically around 2.5 months, highlighting SLS009's positive impact.
在这种情况下,预计患者的中位生存期(mOS)通常约为2.5个月,突显了SLS009的积极影响。
What safety profile has been observed with SLS009?
SLS009观察到了什么样的安全性特征?
SLS009 was well-tolerated with no new safety signals reported in the enrolled patients.
SLS009耐受性良好,在入组患者中没有报告新的安全信号。
Where can I find more information about the clinical trial?
我在哪里可以找到有关临床试验的更多信息?
More details on the study can be found at clinicaltrial.gov with identifier NCT04588922.
有关该研究的更多详细信息,请访问clinicaltrial.gov,标识符为NCT04588922。
Disclaimer: This is an AI-generated summary of a press release distributed by GlobeNewswire. The model used to summarize this release may make mistakes. See the full release here.
免责声明:这是由GlobeNewswire分发的新闻稿的人工智能生成摘要。用于总结这份稿件的模型可能会出错。请在这里查看完整发布。
$SLS Hedge Fund Activity
$SLS对冲基金活动
We have seen 19 institutional investors add shares of $SLS stock to their portfolio, and 13 decrease their positions in their most recent quarter.
我们看到19家机构投资者在最近一个季度增加了$SLS股票的持股,13家减少了持股。
Here are some of the largest recent moves:
以下是最近的一些重大变动:
- ANSON FUNDS MANAGEMENT LP added 793,835 shares (+inf%) to their portfolio in Q3 2024
- VANGUARD GROUP INC added 506,523 shares (+28.4%) to their portfolio in Q3 2024
- EQUITABLE HOLDINGS, INC. removed 197,940 shares (-94.3%) from their portfolio in Q3 2024
- MILLENNIUM MANAGEMENT LLC removed 104,113 shares (-69.2%) from their portfolio in Q3 2024
- GEODE CAPITAL MANAGEMENT, LLC added 88,183 shares (+17.1%) to their portfolio in Q3 2024
- XTX TOPCO LTD added 62,785 shares (+inf%) to their portfolio in Q3 2024
- RENAISSANCE TECHNOLOGIES LLC added 60,491 shares (+186.4%) to their portfolio in Q3 2024
- ANSON基金管理公司在2024年第三季度增加了793,835股(+inf%)到他们的投资组合
- 先锋集团在2024年第三季度增加了506,523股(+28.4%)到他们的投资组合
- 公平控股公司在2024年第三季度从他们的投资组合中移除了197,940股(-94.3%)
- 千禧管理公司在2024年第三季度从他们的投资组合中移除了104,113股(-69.2%)
- GEODE资本管理公司在2024年第三季度增加了88,183股(+17.1%)到他们的投资组合
- XTX TOPCO LTD在2024年第三季度向其投资组合添加了62,785股(+inf%)
- RENAISSANCE TECHNOLOGIES LLC在2024年第三季度向其投资组合添加了60,491股(+186.4%)
To track hedge funds' stock portfolios, check out Quiver Quantitative's institutional holdings dashboard.
要跟踪对冲基金的股票投资组合,请查看Quiver Quantitative的机构持有情况仪表。
Full Release
完整发布
- Median Overall Survival (mOS) Not Yet Reached, Now Exceeds 7.7. Months at Latest Follow-Up in the 30 mg BIW Cohort in Patients Relapsed or Refractory to Venetoclax-Based Regimens -
- 中位整体生存率(mOS)尚未达到,目前在30 mg BIW患者中,超出7.7个月,最新随访时数据为止,患者复发或对Venetoclax治疗耐药 -
- Overall Response Rate (ORR) of 56% Achieved to Date in Patient with Acute Myeloid Leukemia with Myelodysplasia Related Changes (AML MRC) Prospectively Enrolled in Two Expansion Cohorts; Exceeding Prespecified Target Response Rate of 33% -
- 至今在急性髓性白血病(AML MRC)患者中,整体响应率(ORR)达到56%,该患者由两组扩展研究前瞻性招募;超出预设的33%目标响应率 -
NEW YORK, Dec. 09, 2024 (GLOBE NEWSWIRE) -- SELLAS Life Sciences Group, Inc. (NASDAQ: SLS) ("SELLAS" or the "Company"), a late-stage clinical biopharmaceutical company focused on the development of novel therapies for a broad range of cancer indications, today announced additional data from the expansion cohorts in the Phase 2 trial of SLS009, a highly selective CDK9 inhibitor, in relapsed/refractory acute myeloid leukemia (r/r AML).
纽约,2024年12月09日(全球新闻社)-- SELLAS Life Sciences Group, Inc.(纳斯达克:SLS)("SELLAS"或"公司"),一家专注于开发针对广泛癌症指征的新型治疗方法的后期临床生物制药公司,今天宣布了SLS009在复发/耐药急性髓性白血病(r/r AML)II期试验扩展组的额外数据。
"We are highly encouraged by the emerging data, which continue to show the potential of SLS009 to transform outcomes of these heavily pretreated AML patients," said Angelos Stergiou, MD, ScD h.c., President and Chief Executive Officer of SELLAS. "In the Cohort 3, the optimal dosing regimen of 30 mg BIW, in patients relapsed or refractory to venetoclax-based regimens, the median overall survival has not been reached but exceeds 7.7 months at latest follow-up, marking a significant milestone for patients in this setting, where the expected mOS is historically around 2.5 months. In addition, we are seeing more than 50% ORR to date in our expansion cohorts in patients with AML-myelodysplasia-related changes (AML-MRC) with ASXL1 mutation and mutations and cytogenic changes other than ASXL1, similar to the previously reported ORR in Cohort 3. We set up an aggressive threshold of 33% response rate before the trial started, and to date we achieved 56% in 5/9 evaluable patients. The rapid enrollment in the expansion cohorts further highlight the critical need for new treatments for our target patient population. These results support the potential of SLS009 to become an important new therapeutic option for this underserved patient population."
"我们对新出现的数据感到非常鼓舞,这些数据继续显示SLS009有潜力改变这些重度预处理AML患者的结果,"SELLAS的董事总裁及首席执行官Angelos Stergiou博士说。"在第三组中,30 mg BIW的最佳给药方案在复发或对Venetoclax治疗耐药的患者中,中位整体生存率尚未达到,但在最新随访中超过7.7个月,这对于预计mOS历史数据约为2.5个月的患者来说是一个重要的里程碑。此外,我们在AML-骨髓发育异常相关变化(AML-MRC)患者中看到超过50%的ORR,这些患者有ASXL1突变和除ASXL1之外的其他突变和细胞遗传学变化,类似于之前报告的第三组ORR。在试验开始前,我们设定了33%的响应率的激进门槛,到目前为止,我们在9名可评估患者中达到了56%。扩展组的快速招募进一步强调了我们目标患者群体对新治疗方案的迫切需求。这些结果支持SLS009作为这一被忽视患者群体的重要新治疗选择的潜力。"
Key Highlights from the updated topline data:
更新的顶线数据关键亮点:
-
As of December 4, 2024, data cutoff, 14 patients were enrolled in Cohort 3 and 14 in Cohort 4 and 5, of which 9 were evaluable at the time of analysis.
-
At latest follow-up, the mOS has not been reached yet but has exceeded 7.7 months in Cohort 3. This is particularly significant as the expected mOS for patients in this setting is typically 2.5 months.
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In expansion cohorts 4 and 5, in patients with AML-myelodysplasia-related changes (AML-MRC) with ASXL1 mutation (cohort 4) and mutations and cytogenic changes other than ASXL1 (cohort 5) the ORR was 56% in 9 evaluable for efficacy patients.
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SLS009 was well-tolerated with no new safety signals observed to date as the regimen remains safe in additional patients enrolled to date.
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截至2024年12月4日数据截止时,3组有14名患者入组,4组和5组各有14名患者,其中9名在分析时可评估。
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在最新的随访中,mOS尚未达到,但在3组中已超过7.7个月。这一点尤其重要,因为在这种情况下患者的预期mOS通常为2.5个月。
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在扩展组4和5中,AML相关的骨髓增生异常变化(AML-MRC)患者中,具有ASXL1突变(4组)及除ASXL1以外的突变和细胞遗传学变化(5组)的患者有效率为56%,在9名可评估有效性的患者中。
-
SLS009的耐受性良好,迄今未观察到新的安全信号,因为该方案在迄今入组的其他患者中仍然安全。
The Phase 2 clinical trial of SLS009 is an open-label, single-arm, multi-center study designed to evaluate the safety, tolerability, and efficacy of SLS009 in combination with venetoclax and azacitidine at two dose levels, 45 and 60 mg. In the 60 mg dose cohort patients were randomized into either a 60 mg dose once per week or a 30 mg dose two times per week. The trial was expanded to include two additional cohorts, one with ASXL1 mutated AML patients and one with patients with myelodysplasia-related molecular abnormalities other than ASXL1. In addition to response and survival analyses, the study aims to identify biomarkers for the target patient population and enrichment for further trials. For more information on the study, visit clinicaltrial.gov identifier
NCT04588922
.
SLS009的2期临床试验是一项开放标签、单臂、多中心研究,旨在评估SLS009与venetoclax和azacitidine联合使用的安全性、耐受性和有效性,分为两个剂量水平,分别为45 mg和60 mg。在60 mg剂量组中,患者随机分为每周一次60 mg或每周两次30 mg。该试验扩展为包含两个额外组,一个为ASXL1突变的AML患者,另一个为具有除ASXL1以外骨髓增生相关分子异常的患者。除了反应和生存分析外,研究旨在识别目标患者群体的生物标志物,并为进一步试验提供富集。有关该研究的更多信息,请访问clinicaltrial.gov标识符
NCT04588922
.
About SELLAS Life Sciences Group, Inc.
关于Sellas Life Sciences集团公司。
SELLAS is a late-stage clinical biopharmaceutical company focused on the development of novel therapeutics for a broad range of cancer indications. SELLAS' lead product candidate, GPS, is licensed from Memorial Sloan Kettering Cancer Center and targets the WT1 protein, which is present in an array of tumor types. GPS has the potential as a monotherapy and combination with other therapies to address a broad spectrum of hematologic malignancies and solid tumor indications. The Company is also developing SLS009 (formerly GFH009) - potentially the first and best-in-class differentiated small molecule CDK9 inhibitor with reduced toxicity and increased potency compared to other CDK9 inhibitors. Data suggests that SLS009 demonstrated a high response rate in AML patients with unfavorable prognostic factors including ASXL1 mutation, commonly associated with poor prognosis in various myeloid diseases. For more information on SELLAS, please visit .
Sellas是一家处于晚期临床阶段的生物制药公司,专注于开发针对广泛癌症指征的新型治疗药物。Sellas的首个产品候选药物GPS,是从纪念斯隆凯特琳癌症中心授权的,针对WT1蛋白,WT1蛋白存在于多种肿瘤类型中。GPS有潜力作为单独疗法或与其他疗法结合,来应对广泛的血液恶性肿瘤和实体瘤指征。该公司还在开发SLS009(以前称为GFH009)——潜在的首个且最佳的差异化小分子CDK9抑制剂,其毒性降低,效力增强,相较于其他CDK9抑制剂。数据显示,SLS009在具有不良预后因素的AML患者中表现出高反应率,包括与多种骨髓疾病中不良预后常相关的ASXL1突变。有关Sellas的更多信息,请访问。
Forward-Looking Statements
前瞻性声明
This press release contains forward-looking statements. All statements other than statements of historical facts are "forward-looking statements," including those relating to future events. In some cases, forward-looking statements can be identified by terminology such as "plan," "expect," "anticipate," "may," "might," "will," "should," "project," "believe," "estimate," "predict," "potential," "intend," or "continue" and other words or terms of similar meaning. These statements include, without limitation, statements related to the GPS clinical development program, including the REGAL study and the timing of future milestones related thereto. These forward-looking statements are based on current plans, objectives, estimates, expectations, and intentions, and inherently involve significant risks and uncertainties. Actual results and the timing of events could differ materially from those anticipated in such forward-looking statements as a result of these risks and uncertainties, which include, without limitation, risks and uncertainties with oncology product development and clinical success thereof, the uncertainty of regulatory approval, and other risks and uncertainties affecting SELLAS and its development programs as set forth under the caption "Risk Factors" in SELLAS' Annual Report on Form 10-K filed on March 28, 2024 and in its other SEC filings. Other risks and uncertainties of which SELLAS is not currently aware may also affect SELLAS' forward-looking statements and may cause actual results and the timing of events to differ materially from those anticipated. The forward-looking statements herein are made only as of the date hereof. SELLAS undertakes no obligation to update or supplement any forward-looking statements to reflect actual results, new information, future events, changes in its expectations, or other circumstances that exist after the date as of which the forward-looking statements were made.
本新闻稿包含前瞻性声明。除历史事实外的所有陈述均为“前瞻性声明”,包括与未来事件相关的声明。在某些情况下,可以通过诸如“计划”、“期望”、“预期”、“可能”、“或许”、“将”、“应该”、“项目”、“相信”、“估计”、“预测”、“潜在”、“打算”或“继续”和其他类似意义的词汇来识别前瞻性声明。这些声明包括但不限于与GPS临床开发计划相关的声明,包括REGAL研究及其相关未来里程碑的时间安排。这些前瞻性声明基于当前的计划、目标、估计、期望和意图,固有地涉及重大风险和不确定性。由于这些风险和不确定性,实际结果和事件的时间可能与预期有显著差异,包括但不限于肿瘤产品开发及其临床成功的不确定性、监管批准的不确定性,以及影响Sellas及其开发计划的其他风险和不确定性,这些风险和不确定性在Sellas于2024年3月28日提交的10-k表格年报中的“风险因素”标题下列出。Sellas当前不知晓的其他风险和不确定性也可能影响Sellas的前瞻性声明,并可能导致实际结果和事件的时间与预期显著不同。本声明中的前瞻性声明仅在此日期之前进行,Sellas没有义务更新或补充任何前瞻性声明,以反映实际结果、新信息、未来事件、期望的变化或在前瞻性声明发布后的其他情况。
Investor Contact
Bruce Mackle
Managing Director
LifeSci Advisors, LLC
SELLAS@lifesciadvisors.com
投资者联系
布鲁斯·麦克尔
常务董事
生命科学顾问公司
SELLAS@lifesciadvisors.com
Media Contact
Michael Fitzhugh
LifeSci Communications
mfitzhugh@lifescicomms.com
媒体联系
迈克尔·菲茨休
通信-半导体
mfitzhugh@lifescicomms.com