XBiotech Results From Randomized Double-Blinded Phase 1/2 Study Suggest Potential Breakthrough Treatment for Advanced Pancreatic Cancer
XBiotech Results From Randomized Double-Blinded Phase 1/2 Study Suggest Potential Breakthrough Treatment for Advanced Pancreatic Cancer
Overall Survival (OS) defined as from time of randomization to death. Natrunix + ON+5FU+LV (n=3) vs Placebo + ON+5FU+LV arms (n=32) were analyzed in a Kaplan-Meier Survival plot using a product limit comparison method. Borderline statistically significance of p = 0.096, given the small sample size for survival analysis, suggests prolonged survival for subjects receiving Natrunix.
总体存活率(OS)定义为从随机分组到死亡。使用产品极限比较方法在卡普兰-迈尔生存图中分析了Natrunix + ON+5FU+LV(n=3)与安慰剂 + ON+5FU+LV 双臂(n=32)的对比。鉴于存活分析的样本量很小,p = 0.096的临界统计学意义表明接受Natrunix治疗的受试者的存活时间延长。
Findings Show Trends for Reduced Toxicities and Better Outcomes for Subjects Receiving ONIVYDE/5-FU Combination and Targeted anti-IL-1alpha Therapy
研究结果显示,接受ONIVYDE/5-FU组合和靶向抗IL-1α疗法的受试者有降低毒性和改善疗效的趋势
AUSTIN, Texas, June 18, 2024 (GLOBE NEWSWIRE) -- XBiotech (NASDAQ: XBIT) announced today data from its Phase 1/Phase 2 randomized, double-blind, placebo-controlled multi-center study for advanced pancreatic cancer. Known as 1-BETTER, the study examined Natrunix (anti-interleukin-1alpha) antibody in combination with an established chemotherapy regimen (ONIVYDE (ON) + 5-Fluorouracil (5FU) + Leucovorin (LV), a regimen that is already widely used for treating pancreatic cancer but is associated with difficult toxicities and less then ideal survival outcomes. Natrunix was being evaluated as an anti-cancer agent for use in cytotoxic chemotherapy combinations where the Company believes it might potentially also improve tolerability of the chemotherapy.
得克萨斯州奥斯汀,2024年6月18日(GLOBE NEWSWIRE)——xBIOTECH(纳斯达克股票代码:XBIT)今天公布了其针对晚期胰腺癌的1/2期随机、双盲、安慰剂对照的多中心研究的数据。这项名为1-BETTER的研究考察了Natrunix(抗白介素-1α)抗体与既定的化疗方案(ONIVYDE(ON)+ 5-氟尿嘧啶(5FU)+ Leucovorin(LV)的联合疗法,该方案已被广泛用于治疗胰腺癌,但毒性很大,存活结果不太理想。Natrunix被评估为一种用于细胞毒性化疗组合的抗癌药物,该公司认为它还可能提高化疗的耐受性。
The Phase 1 portion was a dose escalation study in metastatic pancreatic cancer patients to determine if dose limiting toxicities (DLTs) occurred in combination with the ON+5FU+LV regimen in second- or third-line setting. DLTs were not expected with Natrunix and none were seen. The Natrunix dose in the Phase 2 portion was thus the highest dose used in the Phase 1 portion.
第一阶段是针对转移性胰腺癌患者的剂量递增研究,旨在确定在二线或三线环境中与ON+5FU+LV方案联合使用时是否出现剂量限制毒性(DLT)。预计 Natrunix 不会有 DLT,也没有看到任何东西。因此,第二阶段部分的Natrunix剂量是第一阶段使用的最高剂量。
Sixty-five subjects were randomized into the Phase 2 study on a 1:1 basis to receive either Natrunix+ ON+5FU+LV (Arm1) or Placebo +ON+5FU+LV (Arm2). There were 33 subjects enrolled into Arm1 and 32 into Arm2. The Phase 2 treatment period was 24-weeks with subjects receiving therapy once every other week for a total of 12 cycles.
65名受试者以 1:1 的比例随机进入第二阶段研究,接受Natrunix+ ON+5FU+LV(Arm1)或安慰剂+ON+5FU+LV(Arm2)治疗。有33名受试者加入了Arm1,32名受试者加入了Arm2。第二阶段治疗期为24周,受试者每隔一周接受一次治疗,共12个周期。
Subjects included in the study had confirmed metastatic, unresectable, or recurrent pancreatic adenocarcinoma of exocrine pancreas and were required to have had disease progression after one prior gemcitabine-based therapy or one FOLFIRINOX and gemcitabine containing therapy. All patients were required to have at least one measurable lesion according to Response Evaluation Criteria in Solid Tumor (RECIST v1.1).
该研究中包括的受试者已证实胰腺外分泌转移性、不可切除的或复发的胰腺腺癌,并且必须在先前接受过一次基于吉西他滨的治疗或一次含有FOLFIRINOX和吉西他滨的治疗后出现疾病进展。根据实体瘤反应评估标准(RECIST v1.1),所有患者都必须有至少一个可测量的病变。
The primary endpoint for the Phase 2 study was to assess the safety and tolerability of Natrunix when used with the ON+5FU+LV combination. Overall, there were fewer adverse events (AEs) of any kind during the 24-week treatment period for the Natrunix arm compared to placebo (297 vs 336), with markedly fewer events in specific categories of adverse events during that time. There was a 28% reduction in the number of subjects experiencing significant adverse events (SAEs) in the Natrunix arm (9 out of 33) versus placebo (12 out of 32) that occurred during the 24-week treatment period. Subjects receiving the Natrunix ON+5FU+LV regimen also had about a 33% reduction in hospitalization (80 days versus 120 days) during the 24-week treatment period compared to subjects receiving placebo + ON+5FU+LV combination.
2期研究的主要终点是评估Natrunix与ON+5FU+LV组合使用时的安全性和耐受性。总体而言,与安慰剂相比,在24周的治疗期内,Natrunix组的任何种类的不良事件(AE)都较少(297对比336),在此期间,特定类别的不良事件明显减少。与在24周治疗期内发生的安慰剂(32人中有12人)相比,Natrunix组出现重大不良事件(SAE)的受试者(33人中有9人)减少了28%。与接受安慰剂+ ON+5FU+LV联合治疗的受试者相比,在24周的治疗期内,接受Natrunix ON+5FU+LV方案的受试者的住院时间也减少了约33%(80天对比120天)。
Subjects receiving the Natrunix combination also reported a 22% reduction in fatigue (28 vs 36), 32% improved appetite (19 vs 28) and 41% reduction in pain (17 vs 29) as of the last day of the 24-week treatment period compared to subjects receiving the placebo ON+5FU+LV combination.
接受Natrunix组合的受试者还报告说,与接受安慰剂ON+5FU+LV组合的受试者相比,截至24周治疗期的最后一天,疲劳减轻了22%(28对36),食欲改善了32%(19对28),疼痛减轻了41%(17对29)。
Severe diarrhea that can be life -threatening is a significant complication for the ON+5FU+LV regimen. There was a two-fold reduction (9% versus 19%) in the incidence of severe diarrhea during the 24-week treatment regimen for patients receiving the Natrunix + ON+5FU+LV combination compared to placebo + ON+5FU+LV.
可能危及生命的严重腹泻是ON+5FU+LV方案的重大并发症。与安慰剂+ ON+5FU+LV相比,在为期24周的治疗方案中,接受Natrunix + ON+5FU+LV组合的患者的严重腹泻发病率降低了两倍(9%对19%)。
Overall Survival (OS), one of the secondary endpoints for the Phase 2 study, was conventionally defined in as time from randomization to death. The sample size for the study included intent-to-treat analysis of 33 subjects randomized into the Natrunix + ON+5FU+LV arm versus 32 subjects in Placebo + ON+5FU+LV arm. A Kaplan-Meier Survival Curve using a product limit comparison method was performed. This data highlights the observation that no subjects in the placebo ON+5FU+LV group (n=32) survived for longer than 330 days, whereas 8 subjects in the Natrunix ON+5FU+LV arm (n=33) were still alive as of day 330. Considering the small sample size, the borderline statistically significant p-value of p = 0.096 suggests prolonged survival for subjects receiving the Natrunix regimen.
总体存活率(OS)是2期研究的次要终点之一,传统上定义为从随机分组到死亡的时间。该研究的样本量包括对33名随机进入Natrunix + ON+5FU+LV组的受试者的治疗意向分析,而安慰剂+ ON+5FU+LV组的32名受试者的治疗意向分析。使用产品极限比较方法绘制了卡普兰-迈尔生存曲线。这些数据突显了这样的观察,即安慰剂ON+5FU+LV组(n=32)中没有受试者的存活时间超过330天,而截至第330天,Natrunix ON+5FU+LV组(n=33)中有8名受试者还活着。考虑到样本量小,具有统计学意义的临界值 p = 0.096 表明接受 Natrunix 方案的受试者的存活时间延长。
The lead investigator for the study, David J. Park, MD Medical Oncologist, Medical Director for the providence St. Jude Crosson Institute, Fullerton, CA stated "Treatment of advanced pancreatic cancer in the second and third line settings presents significant challenges in terms of toxicity as well as efficacy. To observe these trends for reduced toxicity and potential survival benefit is remarkable, particularly given the limited sample size. The potential interaction between reduced toxicity, more time on treatment and improvement in survival makes intuitive sense for clinicians who treat these patients. These findings are extremely important."
该研究的首席研究员、加利福尼亚州富乐顿普罗维登斯圣裘德·克罗森研究所医学主任肿瘤内科医生大卫·帕克表示:“在二线和三线环境中治疗晚期胰腺癌在毒性和疗效方面都存在重大挑战。观察这些毒性降低和潜在生存益处的趋势是显著的,尤其是在样本量有限的情况下。对于治疗这些患者的临床医生来说,减少毒性、延长治疗时间和提高存活率之间的潜在相互作用在直观上是合理的。这些发现非常重要。”
While there was a relatively small number of pancreatic cancer patients enrolled in the Phase 2 portion of the study, in the Company's opinion, the findings show better outcomes for the Natrunix + ON+5FU+LV group as compared to the control arm. The Company believes that the reduced number of serious and adverse events, the significant reduction in hospitalization, and improved OS during the respective time periods described above for each of these metrics suggest that Natrunix could represent a breakthrough advance for the treatment of pancreatic cancer.
该公司认为,尽管参与该研究第二阶段的胰腺癌患者人数相对较少,但研究结果表明,与对照组相比,Natrunix + ON+5FU+LV组的预后更好。该公司认为,在上述每项指标的相应时间段内,严重和不良事件数量的减少、住院人数的显著减少以及操作系统的改善,表明Natrunix可能代表胰腺癌治疗的突破性进展。
About XBiotech
XBiotech is pioneering the discovery and development of targeted antibodies based on its True Human technology. The company's mission is to rethink the way antibody medicines are discovered and commercialized by advancing its robust pipeline of truly natural human antibodies for treating serious diseases such as inflammatory conditions like rheumatology, infectious disease, cardiovascular disease and cancer. XBiotech has several candidate products including Natrunix. Cloned from individual donors who possess natural immunity against certain targeted diseases, XBiotech's pipeline of True Human antibodies are intended to deliver unmatched safety and efficacy. Located just minutes from downtown Austin, the XBiotech campus headquarters includes GMP manufacturing facilities, research and testing laboratories, infectious disease research facilities, and quality control and clinical operations. For more information, visit www.xbiotech.com.
关于 xBiotech
xBiotech在基于其真人技术的基础上率先发现和开发靶向抗体。该公司的使命是通过推进其强大的真正天然的人体抗体产品线,重新思考抗体药物的发现和商业化的方式,这些抗体药物用于治疗风湿病、传染病、心血管疾病和癌症等炎症性疾病。xBiotech有几种候选产品,包括Natrunix。xBiotech的True Human抗体产品线从对某些靶向疾病具有自然免疫力的个人捐赠者中克隆而来,旨在提供无与伦比的安全性和有效性。xBiotech园区总部距奥斯汀市中心仅数分钟路程,包括GMP制造设施、研究和测试实验室、传染病研究设施以及质量控制和临床运营。欲了解更多信息,请访问 www.xbiotech.com。
Cautionary Note on Forward-Looking Statements and Study Results
This press release contains forward-looking statements, including declarations regarding management's beliefs and expectations that involve substantial risks and uncertainties. Forward-looking statements are subject to inherent risks and uncertainties in predicting future results and conditions that could cause the actual results to differ materially from those projected in these forward-looking statements. These risks and uncertainties are subject to the disclosures set forth in the "Risk Factors" section of certain of our SEC filings. Any forward-looking statements that we make in this press release speak only as of the date of this press release. We assume no obligation to update our forward-looking statements whether as a result of new information, future events or otherwise, after the date of this press release. The Company makes no representations regarding OS or any other metric beyond the time periods specifically discussed herein. There can be no assurance that any study results discussed in this press release will be replicated in future studies or that Natrunix will be approved by the Food and Drug Administration or any other regulator.
关于前瞻性陈述和研究结果的警示说明
本新闻稿包含前瞻性陈述,包括有关管理层信念和期望的声明,这些声明涉及重大风险和不确定性。前瞻性陈述在预测未来业绩和条件时存在固有的风险和不确定性,这些风险和不确定性可能导致实际结果与这些前瞻性陈述中的预测存在重大差异。这些风险和不确定性受我们在美国证券交易委员会某些文件的 “风险因素” 部分中披露的约束。我们在本新闻稿中所作的任何前瞻性陈述仅代表截至本新闻稿发布之日。在本新闻稿发布之日之后,无论是由于新信息、未来事件还是其他原因,我们都没有义务更新我们的前瞻性陈述。除了本文特别讨论的时间段外,公司对操作系统或任何其他指标不作任何陈述。无法保证本新闻稿中讨论的任何研究结果将在未来的研究中复制,也无法保证Natrunix将获得美国食品药品监督管理局或任何其他监管机构的批准。
Contact
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Wenyi Wei
wwei@xbiotech.com
Tel. 737-207-4600
魏文义
wwei@xbiotech.com
电话:737-207-4600
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