BriaCell Presents Clinical Efficacy Data at ASCO 2024
BriaCell Presents Clinical Efficacy Data at ASCO 2024
"Our ASCO presentations highlight how Bria-IMT's activities – through diverse mechanisms including adaptive and innate responses - synergize with multiple mechanisms of action of checkpoint inhibitors," stated Dr. Williams, BriaCell's President and CEO. "We believe Bria-IMT has the potential to become a breakthrough novel treatment option for patients in advanced metastatic breast cancer."- BriaCell doubles Progression-Free-Survival (PFS) and Clinical Benefit Rate vs historical results in the literature
- Bria-IMT PFS compares favorably to PFS of most recent treatment in 48% of Antibody-Drug Conjugate (ADC) resistant patients
- Therapy well-tolerated with no Bria-IMT related discontinuations
- Clinical data highlight significant potential of Bria-IMT in advanced metastatic breast cancer
- Superiority of selected Phase 3 regimen and formulation confirmed
- Oral presentation by Mayo Clinic Professor and Principal Investigator, Saranya Chumsri, MD, on Monday June 3; 11:30 AM-1:00 PM CDT
- BriaCell将Progression-Free-Survival(PFS)和临床受益率与文献中的历史结果相比翻倍。Bria-IMT PFS与48%的抗体药物联合物(ADC)耐药患者中最近治疗的PFS相比有利。
- 该疗法耐受良好,无Bria-IMT相关的停止治疗情况。
- 临床数据突显Bria-IMT在晚期转移性乳腺癌中的重要潜力。
- 选择的第3期方案和配方的卓越性得到确认。
- 梅奥诊所教授和主要研究员Saranya Chumsri,MD于6月3日星期一上午11:30至下午1:00在口头汇报中分享。
- PHILADELPHIA和温哥华,2024年6月3日(全球新闻)- BriaCell Therapeutics Corp。(Nasdaq:BCTX,BCTXW)(TSX:BCT)(“BriaCell”或“公司”),一家临床阶段的生物技术公司,开发新型免疫疗法改变癌症治疗,宣布对其正在进行的随机第2阶段研究评估先导临床候选药Bria-IMT在晚期转移性乳腺癌患者中的阳性临床功效数据进行更新。两个海报展示、一个摘要和一个口头展示(由梅奥诊所肿瘤学教授和主要研究员Saranya Chumsri,MD主持)将在2024年美国临床肿瘤学会年会上展示。该会议于2024年6月3日(星期五)在芝加哥McCormick Place举行。
PHILADELPHIA and VANCOUVER, British Columbia, June 03, 2024 (GLOBE NEWSWIRE) -- BriaCell Therapeutics Corp. (Nasdaq: BCTX, BCTXW) (TSX: BCT) ("BriaCell" or the "Company"), a clinical-stage biotechnology company that develops novel immunotherapies to transform cancer care, announces positive clinical efficacy data updates of its ongoing randomized Phase 2 study evaluating lead clinical candidate Bria-IMT in patients with advanced metastatic breast cancer. Two poster sessions, one abstract, and one oral presentation session (by Principal Investigator and Professor of Oncology, Mayo Clinic, Saranya Chumsri, MD), will be presented at the 2024 American Society of Clinical Oncology (ASCO) Annual Meeting taking place today June 3, 2024 at McCormick Place, Chicago, IL.
“我们对这些经过重度治疗的患者的临床效果和安全数据都非常满意。由于这组患者治疗选择有限,而大多数治疗方法都伴随着严重的毒性反应,医生和患者经常选择拒绝进一步的无效和有毒药物而选择姑息治疗,"梅奥诊所肿瘤学教授和主要研究员Saranya Chumsri,MD说。"抗体药物联合物(ADC)和免疫检查点抑制剂(CPIs)已成为最新的治疗这些患者的方法。然而,大量晚期患者无法产生反应,所有患者最终都会产生耐药性,因此需要一种安全而有效的治疗。BriaCell的新型免疫疗法为这些患者提供了一种耐受性良好的治疗选择,超越现有批准的药物。"
"We are very impressed with both clinical efficacy and safety data in these heavily pretreated patients. Given the limited effective treatment options in this group of patients, and the fact that most treatments are associated with significant toxicities, physicians and patients often opt to decline further ineffective and toxic drugs in lieu of palliative care," Saranya Chumsri, MD, Principal Investigator and Professor of Oncology, Mayo Clinic. "Antibody-drug conjugates (ADCs) and immune checkpoint Inhibitors (CPIs) have emerged as the latest therapies to treat these patients. However, a large percentage of late-stage patients do not respond, and all patients inevitably develop resistance to them, making a safe and effective treatment an urgent medical need. BriaCell's novel immunotherapy offers a well-tolerated treatment option for these patients beyond the currently approved drugs."
“虽然免疫疗法已经成为多种癌症类型的有效治疗选择,但在乳腺癌中的应用相当有限。发掘新的策略,以增强各亚型乳腺癌对免疫疗法的响应能力,可以作为一种治疗机会。通过其独特的作用机制,Bria-IMT方案可选择性地激活适应性抗癌CD4+和CD8+ T细胞以及先天免疫反应(树突状和NK细胞),以激活患者的免疫系统而不产生严重的副作用,"迈阿密大学米勒医学院乳腺病组的临床研究负责人、Sylvester Comprehensive Cancer Center癌症康复计划的联合主任和Bria-IMT第2期研究的主要临床调查员Carmen Calfa,M.D.说。
"While immunotherapy has emerged as an active treatment option for multiple cancer types, its use in breast cancer is rather restricted to a minority of patients. Discovering new strategies, in order to enhance the responsiveness of various subtypes of breast cancer to immunotherapy, presents as a therapeutic opportunity. Through its unique mechanism of action, Bria-IMT regimen selectively activates adaptive cancer-fighting CD4+ and CD8+ T cells and innate responses (dendritic and NK cells) to activate patients' immune systems without producing serious side effects," stated Carmen Calfa, M.D., Clinical Research Lead for the breast site disease group at the University of Miami Miller School of Medicine, Co-Director of the Cancer Survivorship Program at Sylvester Comprehensive Cancer Center, and Principal Clinical Investigator of the Phase 2 Bria-IMT study.
"我们的ASCO讲演重点介绍了Bria-IMT通过多种机制,包括适应性和先天免疫反应,与多种检查点抑制剂的多种作用机制相互协同的活动,"BriaCell总裁兼首席执行官Williams博士说。"我们认为,Bria-IMT有可能成为晚期转移性乳腺癌患者的突破性新治疗选择。"
"Our ASCO presentations highlight how Bria-IMT's activities – through diverse mechanisms including adaptive and innate responses - synergize with multiple mechanisms of action of checkpoint inhibitors," stated Dr. Williams, BriaCell's President and CEO. "We believe Bria-IMT has the potential to become a breakthrough novel treatment option for patients in advanced metastatic breast cancer."
演示的详细信息总结如下。
The details of the presentations are summarized below.
口头汇报摘要
Oral Presentation Summary
出版物的摘要编号:1022
Abstract Number for Publication: 1022
Title: Outcomes of advanced/metastatic breast cancer (aMBC) treated with Bria-IMT, an allogeneic whole cell immunotherapy.
Session Type and Title: Rapid Oral Abstract – Breast Cancer—Metastatic
Session Date and Time: 6/3/2024; 11:30 AM-1:00 PM CDT
标题:aMBC 患者采用全病理细胞免疫治疗 Bria-IMT 的疗效
会话类型和标题:自适应口头摘要-乳腺癌-转移
会议日期和时间:2024年6月3日下午11:30至下午1:00 CDT
该展示详细介绍了BriaCell正在进行的使用免疫检查点抑制剂(retifanlimab)的随机第2阶段研究评估Bria-IMT的结果。随机化的目的是比较第一轮疗法早期或在第二轮疗法后期后给予CPI对患者是否有任何优势。还评估了两种不同的Bria-IMT配方;一种用干扰素γ处理,一种未经处理。进入研究的患者都经过了重度治疗,并在下表中列出了多个先前的治疗方案。
This presentation details the results of BriaCell's randomized Phase 2 study of Bria-IMT in combination with retifanlimab, an immune checkpoint inhibitor (CPI). The goal of randomization was to compare whether administration of the CPI early, in the first cycle of therapy, or later, late in the second cycle of therapy, offered any advantage. Two different formulations of Bria-IMT were also evaluated; one treated with interferon gamma and one untreated.
表1.Bria-IMT 第2期研究中的先前治疗方案
The patients entering the study were very heavily pretreated and had failed multiple prior therapies as shown in the Table 1 below.
进入研究的患者经过大量治疗,且以前存在多种治疗失败的情况,详见表1。
|
Table 1. Prior Therapies in the Bria-IMT Phase 2 Study | |
| Previous Therapies | Number of Patients (%) |
| Antibody-Drug Conjugates (ADC) | 23 (44%) |
| Immune Checkpoint Inhibitor (CPI) | 11 (20%) |
| Cyclin-Dependent Kinase (CDK) 4/6 Inhibitors | 34 (63%) |
| 表1. Bria-IMT第2阶段研究中的先前治疗 | |
| 以往疗法 | 患者数量(%) |
| 抗体药物结合物(ADC) | 23(44%) |
| 免疫检查点抑制剂(CPI) | 11(20%) |
| 周期蛋白依赖性激酶(CDK)4/6抑制剂 | 34(63%) |
A total of 54 patients were included in the Phase 1/2 study. Nearly half of these had been treated previously with an antibody drug conjugate and had progressed in their disease following this treatment. Another 20% had failed a prior immune checkpoint inhibitor. Nearly 2/3 of the patients had failed therapy with a CDK 4/6 inhibitor. On average they had failed six prior therapy attempts.
共有54名患者参加了第1/2阶段的研究,其中近一半的患者之前接受过抗体-药物结合物治疗,并在此次治疗后疾病进展。还有20%的患者未能成功进行先前的免疫检查点抑制剂治疗,将近2/3的患者治疗CDK 4/6抑制剂时疗效不佳,平均而言,他们之前进行了6次治疗尝试。在第2阶段研究中,32名患者中,有16名早期用CPI治疗,另外16名晚期用CPI治疗,在这两组间,进展无病生存期(PFS)无统计学差异。但是,CPI早期组略优的表现使其被选为第3阶段的治疗方案,整个第1/2阶段经验中,54名患者未与干扰素γ孵育的制剂表现出统计学显著的PFS改善,因此该制剂被选为第3阶段的治疗方案。具体数据见图1。
In the Phase 2 portion of the study, there were 32 patients with 16 treated with CPI early and 16 treated with CPI late. There was no statistically significant difference in progression-free survival (PFS) two groups. However, a slight advantage in the CPI early group has led this to be the selected regimen for the Phase 3 study. In the entire Phase 1/2 experience, with 54 patients, the formulation not incubated with interferon gamma showed a statistically significant improvement in PFS. Therefore, this formulation was selected for the Phase 3 study. The data are shown in Figure 1.
在第2阶段研究中,32例患者中的16例早期接受了CPI治疗,另16例晚期接受同类治疗。这两组之间没有统计学显著差异,但由于CPI早期组有轻微优势,使其成为第3阶段研究的所选疗法。在整个第1/2阶段的经验中,共54例患者,未与干扰素γ孵育的制剂显示出统计学显著的PFS改善,因此该制剂被选为第3阶段研究的治疗方案。具体数据见图1。
Figure 1. Effect of treatment sequence and formulation on PFS
图1。不同治疗顺序和配方对PFS的影响
Clinical benefit was seen in 55% of evaluable patients across all subtypes of breast cancer as shown in Figure 2 below.
在所有乳腺癌亚型中评估患者中,有55%的患者获得了临床上的益处,具体见图2。
Figure 2: Objective Response Rate (ORR) and Clinical Benefit Rate (CBR) in the Bria-IMT Phase 1/2 Study
图2:Bria-IMT 1/2期研究中的客观缓解率(ORR)和临床益处率(CBR)
The progression free survival rate and the clinical benefit rate as well as the objective response rate were markedly higher than those of similar patients treated with the treatment of their physician's choice in other studies. Notably, "Treatment of Physician's Choice" (TPC) will be the comparator in the Phase 3 study of Bria-IMT. This is noted in Table 2 below.
进展无病生存率、临床受益率和客观缓解率均显著高于其他治疗方案的同类患者。值得注意的是,医师选择的治疗方案(TPC)将成为Bria-IMT第3阶段研究的比较组,详见表2。
| Table 2. Comparative PFS, ORR and CBR in Similar Patients | ||||
| Study |
Prior Lines of Therapy (median, range) |
PFS (months) |
ORR (%) |
CBR (%) |
| BriaCell's Phase 2 study patients who received pivotal Phase 3 study formulation | 6 (2-13) | 3.9 | 9.5* | 55* |
| BriaCell's ADC Resistant Phase 2 patients who received pivotal Phase 3 study formulation | 6 (3-13) | 4.1 | 12** | 53** |
| Bardia, A. et. al. 1 | 4 (2-14) | 1.7 | 4 | 8 |
| Tripathy D. et. al. 2 | ≥4 in 91% | 1.9 | 3 | 10 |
| O'Shaughnessy J. et. al. non-TNBC 3 | 5 (2-14) | 2.3 | 4 | 7 |
| O'Shaughnessy J. et. al. TNBC 3 | 4 (2-10) | 1.6 | 5 | 10 |
| 表2. 同类患者的PFS,ORR和CBR比较 | ||||
| 学习 | 之前的店铺 疗法 (中位数,区间) |
PFS (月份) |
ORR (%) |
CBR (%) |
| BriaCell阶段2研究接受关键阶段3研究制剂的患者 | 6(2-13) | 3.9 | 9.5* | 55* |
| BriaCell的ADC耐药阶段2研究接受关键阶段3研究制剂的患者 | 6(3-13) | 4.1 | 12** | 53** |
| Bardia,A. et. al.1 | 4(2-14) | 1.7 | 4 | 8 |
| Tripathy D. et. al. 2 | ≥4占91% | 1.9 | 3 | 10 |
| O’ Shaughnessy J.等人的非TNBC3 | 5(2-14) | 2.3 | 4 | 7 |
| O’ Shaughnessy J.等人的TNBC3 | 4(2-10) | 1.6 | 5 | 10 |
*Data is for evaluable patients, n=42 with 12 not evaluable.
** Data is for evaluable patients, n = 17 with 6 not evaluable.
References: Data is shown for the intent to treat population for the control group treated with treatment of physician's choice, which is the comparator in the BriaCell Phase 3 study
1. Bardia A, et al. J Clin Oncol. 2024 May 20;42(15):1738-1744.
2. Tripathy D, et al. JAMA Oncol. 2022 Nov 1;8(11):1700-1701. jamaoncol.2022.4346. PMID: 36136348. This paper describes patients with brain metastases.
3. O'Shaughnessy J, et al. Breast Cancer Res Treat. 2022 Sep;195(2):127-139.
*数据适用于可评估的患者,n=42人,其中12人不可评估。
**数据适用于可评估的患者,n=17人,其中6人不可评估。
参考资料:数据适用于意向治疗人群,对照组受到医生选择的治疗,这是BriaCell第3期研究中的比较组
1. Bardia A等人。J Clin Oncol.2024年5月20日; 42(15): 1738-1744。
2. Tripathy D等人。JAMA Oncol.2022年11月1日; 8(11): 1700-1701. jamaoncol.2022.4346。PMID: 36136348。本文描述了具有脑转移的患者。
3. O’Shaughnessy J等人。Breast Cancer Res Treat.2022年9月; 195(2): 127-139。
For additional detailed information of the clinical data on the oral presentation, please visit BriaCell Doubles Progression-Free-Survival (PFS) and Reports Clinical Benefit Data at ASCO 2024.
如需有关口头报告的临床数据的详细信息,请访问BriaCell在ASCO 2024年实现双倍无进展生存并报告临床获益数据的网站。
Poster Presentation Summary
海报展示总结
The first poster described BriaCell's ongoing pivotal Phase 3 registrational study in advanced metastatic breast cancer. BriaCell is excited to collaborate on this important program with authors and BriaCell medical advisory board members Sara A. Hurvitz, MD, Professor of Medicine, Fred Hutchinson Cancer Center, Adam M. Brufsky, MD, PhD, Professor of Medicine, University of Pittsburgh School of Medicine, and Massimo Cristofanilli, MD, Professor of Medicine, Weill Cornell Medical College, Cornell University. The second poster described clinical data of Bria-IMT in metastatic breast cancer patients who failed antibody drug conjugates (ADCs) and is spearheaded by Chaitali Nangia, MD, Partner, Hoag Medical Group, and Carmen Calfa, MD, Professor of Medicine, University of Miami.
Abstract Number for Publication: TPS1137
Title: Study of the Bria-IMT regimen and CPI vs physicians' choice in advanced metastatic breast cancer (BRIA-ABC).
Based on Phase 2 clinical data showing numerous survival and clinical benefit outcomes in advanced breast cancer patients treated with the Bria-IMT regimen, the pivotal Phase 3 study has been designed as a multicenter randomized, open label comparison of the Bria-IMT regimen plus CPI in one arm versus Treatment of Physicians' Choice (TPC) in metastatic breast cancer patients with no approved alternative therapies available. Patients' eligibility includes treatment with 2 or more prior regimens. There will be another arm of the Bria-IMT regimen alone (monotherapy). For additional information on the pivotal Phase 3 study, please visit ClinicalTrials.gov as NCT06072612.
第一张海报介绍了BriaCell进行的先进转移性乳腺癌的关键性第3期注册研究。 BriaCell很高兴与作者和BriaCell医学顾问委员会成员Sara A. Hurvitz博士,医学教授,弗雷德·哈钦森癌症研究中心,Adam M. Brufsky博士,医学博士,匹兹堡大学医学院教授,以及Massimo Cristofanilli博士,医学教授,威尔康奈尔医学院,康奈尔大学合作进行这个重要项目。第二张海报描述了接替抗体药物复合物(ADC)治疗失败的转移性乳腺癌患者中Bria-IMT的临床数据,并由Chaitali Nangia博士领导,首席合伙人,Hoag医疗组,和Carmen Calfa博士,医学教授,迈阿密大学。
TPS1137的摘要号码
标题:BRIA-ABC中比较了Bria-IMT方案和CPI与医生选择治疗在先进的转移性乳腺癌治疗的研究。
基于Bria-IMT方案在治疗先进乳腺癌患者中显示出多种生存和临床获益结果的2期临床数据,关键性第3期研究已设计为多中心随机、开放标签比较Bria-IMT方案和与无可用替代治疗的转移性乳腺癌患者的医生选择治疗(TPC)。患者的资格包括治疗2种或更多种前期方案。还将有一个单独的Bria-IMT方案治疗组(单药治疗组)。有关关键性第3期研究的更多信息,请访问ClinicalTrials.gov作为NCT06072612。
Abstract Number for Publication: 1087
Title: SV-BR-1-GM after progression on ADC in patients with metastatic breast cancer.
1087的摘要号码
标题:在可移植性乳腺癌患者中,ADC进展后的SV-BR-1-GM。
Remarkable progression-free survival and clinical benefit of Bria-IMT in ADC resistant advanced metastatic breast cancer
Bria-IMT在对抗ADC耐药的晚期转移性乳腺癌中表现出卓越的无进展生存期和临床益处。
Phase 2 clinical data of the Bria-IMT regimen in 23 advanced metastatic breast cancer patients who failed multiple prior treatments including ADCs and CPIs (median of 6 prior treatments) are presented.
在23位ADC耐药的晚期转移性乳腺癌患者中,Bria-IMT方案的2期临床数据显示这些患者经历了多种先前的治疗方法,包括抗体药物联合化疗和细胞免疫治疗(CPI),及中位数达到6次。
Clinical efficacy
临床疗效
- In evaluable patients, the ORR was 12% and CBR was 53% which is remarkable versus similar data suggesting clinical benefit.
- Median PFS of 4.1 months with the Phase 3 formulation was ~twice that seen of patients in similar studies - 1.71 and 2.23 months - who received TPC. The PFS results suggest superior clinical efficacy given the larger number of prior treatments (median of 6) in Bria-IMT patients vs those of the other studies (median of 4).
- Subset specific clinical benefits: Study data to date suggests clinical benefit for multiple breast cancer subtypes including HR+/HER2- (the most common breast cancer subtype, testing positive for estrogen and/or progesterone receptors and negative for human epidermal growth factor receptor 2 or HER2) with a CBR following treatment, of 63% (5 of 8 patients); HER2+ subtype (a positive test for HER2) with a 100% CBR (2 of 2 patients) and HR-/HER2 low subtype (a negative test for estrogen and/or progesterone receptor and a negative test for HER2) showing a CBR of 66% (2 of 3 patients). See Table 3.
- 在可评估的患者中,ORR为12%,CBR为53%,这些数据相当显著,表明其在获得临床益处方面的疗效。
- 在3期制剂中,中位PFS为4.1个月,是类似研究中患者(中位数为1.7个月和2.2个月,他们接受了TPC)的2倍,这一PFS结果表明,Bria-IMT患者前期治疗次数较多(中位数为6),因此在临床疗效方面表现出了优势。1和其他研究中患者(中位数为4)相比。3亚组特定的临床益处:研究数据表明,针对多种乳腺癌亚型,包括HR+/HER2- (最常见的乳腺癌亚型,测试为雌激素和/或黄体酮受体阳性,且人类表皮生长因子受体2或HER2阴性) 的治疗后CBR可达到63%(8名患者中的5名);HER2+亚型(HER2阳性)的CBR可达100%(2名患者);HR-/HER2低亚型(雌激素和/或黄体酮受体阴性,HER2阴性)的治疗CBR为66%(3名患者中的2名)。详见表3。
- 亚集具体的临床效益:截止目前的研究数据显示出多个乳腺癌亚型中的临床效益,其中HR+/HER2-(最常见的乳腺癌亚型,其试验呈阳性,表明对雌激素和/或黄体酮受体呈阳性,而人表皮生长因子受体2或HER2检验呈阴性)在治疗后表现出63%(8名患者中5名)CBR;HER2+亚型(HER2阳性检测)在治疗后表现出100%的临床益处(2名患者中的2名);HR-/HER2偏低亚型(雌激素和/或黄酮激素受体阴性检测和HER2阴性检测)在治疗后显示出66%的临床益处(3名患者中2名)。详见表3。
| Table 3: Treatment Efficacy by Metastatic Breast Cancer Subtype in ADC-resistant patients | ||||
| Histology | All Patients (N) | Evaluable (N) Patients | Best ORR | Best CBR |
| All ADC Resistant | 23 | 17 | 12% (2 / 17) | 53% (9 / 17) |
| ER/PR + / HER2 low or - | 8 | 8 | 13% (1 / 8) | 63% (5 / 8) |
| HER2+ | 3 | 2 | 50% (1 / 2) | 100% (2 / 2) |
| TNBC | 12 | 7 | 0 | 29% (2 / 7) |
| 表3:针对ADC耐药性乳腺癌亚型的治疗效果 | ||||
| 组织 | 所有患者(N) | 可评估患者(N) | 最佳ORR | 最佳CBR |
| 所有ADC耐药患者 | 23 | 17 | 12%(17人中的2人) | 53%(17人中的9人) |
| ER/PR + / HER2低或-型 | 8 | 8 | 13%(8人中的1人) | 63%(8人中的5人) |
| HER2阳性 | 3 | 2 | 50%(1 / 2) | 100%(2 / 2) |
| TNBC | 12 | 7 | 0 | 29%(2 / 7) |
- Bria-IMT showed potential survival advantage over penultimate treatment in 48% of patients, likely by reversing immune exhaustion in patients irrespective of specific prior ADC.
- Bria-IMT显示,在48%的患者中显示出比次级处理潜在的生存优势,可能通过逆转患者的免疫耗竭来实现,而不考虑特定的前期ADC。
Safety profile
安全防护措施
Absence of both interstitial lung disease (ILD), a common serious adverse event with ADCs, and Bria-IMT-related treatment discontinuations underscore Bria-IMT's excellent tolerability and favorable safety profile.
Bria-IMT与ADCs的常见严重不良事件之一的间质性肺疾病(ILD)和治疗中止相关的缺失强调了Bria-IMT的良好耐受性和优良的安全性资料。
In summary, the data to date shows that Bria-IMT offers extended progression-free survival and clinical benefit in heavily pre-treated, ADC resistant breast cancer patients versus those in other similar studies. BriaCell is closely monitoring ADC resistant patients in its ongoing pivotal Phase 3 study of Bria-IMT and CPI in advanced metastatic breast cancer.
总之,迄今的数据显示,Bria-IMT相对于其他类似研究中的患者,可为经过大量预处理、ADC耐药的乳腺癌患者提供延长的无进展生存期和临床益处。BriaCell正在密切监测ADC耐药患者,在其进行的Bria-IMT和CPI在爱文思控股的晚期转移性乳腺癌中的关键第3期研究中。
Title: Differential efficacy of SV-BR-1-GM in inducing intracranial metastasis regression.
标题:SV-BR-1-GM在诱导颅内转移消退中的差异疗效。
Superior clinical benefit of Bria-IMT regimen - alone or combined with an immune check point inhibitor (CPI) in advanced breast cancer patients with CNS metastatic disease
Bria-IMT方案具有优异的临床益处-独立或者联合免疫检查点抑制剂(CPI)在患有中枢神经系统转移疾病的晚期乳腺癌患者中使用。
Central nervous system (CNS) metastases, including brain metastases and other intracranial metastases, is a dire clinical situation with very poor survival. Very few therapies have shown any effect on CNS or intracranial metastases in breast cancer and it is a serious unmet medical need.
包括脑转移和其他颅内转移瘤的中枢神经系统(CNS)转移瘤是一种严重的临床情况,患者生存率非常低。极少有疗法对乳腺癌CNS或颅内转移瘤有任何影响,这是一个严重的未满足的医学需求。
Clinical efficacy:
临床疗效:
- 83% (5/6) intracranial objective response rate (iORR) was reported in evaluable patients with central nervous system (CNS) metastases treated with the Bria-IMT regimen, either alone or in combination with an immune checkpoint inhibitor (i.e. PD-1 inhibitor pembrolizumab or retifanlimab). These patients failed multiple prior treatments including 2 antibody-drug conjugates in one case. This is illustrated in Figure 3.
- 使用Bria-IMT方案单独或与免疫检查点抑制剂(例如PD-1抑制剂pembrolizumab或retifanlimab)联合治疗有中枢神经系统(CNS)转移瘤的可评估患者报告了83%(5/6)的颅内客观缩小率(iORR),这些患者在多种前期治疗失败后,包括在一种情况下使用了2种抗体药物结合物。这在图3中有所说明。
Figure 3. Intracranial Tumor Responses in Patients with Intracranial Metastases Treated with Bria-IMT
图3.使用Bria-IMT治疗颅内转移瘤的颅内肿瘤反应
- Tumor reductions (≥30% reduction in the sum of diameters) were observed in heavily pretreated patients highlighting potential clinical benefit of Bria-IMT in managing CNS metastases
- This is a pre-planned subgroup analysis in the pivotal Phase 3 study of Bria-IMT providing another opportunity for approval
- 观察到重度预处理患者的肿瘤缩小(直径和的≥30%减小),强调了Bria-IMT在治疗CNS转移瘤中的潜在临床益处
- 这是Bria-IMT关键第3期研究中预先计划的亚组分析,为获得另一次批准提供了机会
Safety profile:
安全资料:
No treatment related discontinuation was reported.
未指出任何与治疗相关的中止。
In summary, Bria-IMT's tumor reductions observed in patients with intracranial disease underlines its potential clinical effectiveness in managing CNS metastatic disease in advanced breast cancer. BriaCell will continue to monitor the data in this subgroup of patients in its ongoing pivotal Phase 3 study in advanced metastatic breast cancer. Treatment of patients with CNS metastatic disease represents a potential additional indication for market approval of Bria-IMT.
总之,Bria-IMT在患有颅内疾病的患者中观察到的肿瘤缩小,突显了其在治疗晚期乳腺癌中CNS转移疾病方面的潜在临床有效性。BriaCell将继续监测其在关键第3期研究中患有CNS转移疾病的患者的数据。治疗患有CNS转移疾病的患者也是Bria-IMT获得市场批准的潜在额外适应症。
Copies of the poster presentations and abstracts are posted on
海报和摘要的副本已张贴在
References
参考文献
- Bardia A, et al. Final Results From the Randomized Phase III ASCENT Clinical Trial in Metastatic Triple-Negative Breast Cancer and Association of Outcomes by Human Epidermal Growth Factor Receptor 2 and Trophoblast Cell Surface Antigen 2 Expression. J Clin Oncol. 2024 May 20;42(15):1738-1744. doi: 10.1200/JCO.23.01409. Epub 2024 Feb 29. PMID: 38422473.
- Tripathy D, et al. Treatment with etirinotecan pegol for patients with metastatic breast cancer and brain metastases: final results from the Phase 3 ATTAIN randomized clinical trial. JAMA Oncol. 2022;8(7):1047-1052. doi:10.1001/jamaoncol.2022.0514.
- O'Shaughnessy J et al. Analysis of patients without and with an initial triple-negative breast cancer diagnosis in the Phase 3 randomized ASCENT study of sacituzumab govitecan in metastatic triple-negative breast cancer. Breast Cancer Res Treat. 2022 Sep;195(2):127-139. doi: 10.1007/s10549-022-06602-7. Epub 2022 May 11. PMID: 35545724; PMCID: PMC9374646.
- Bardia A等人。Ⅲ期ASCENT临床试验转移性三阴性乳腺癌的最终结果及与人类表皮生长因子受体2和滋养层细胞表面抗原2表达情况的相关性。J Clin Oncol。2024年5月20日;42(15):1738-1744。doi:10.1200/JCO.23.01409。Epub 2024年2月29日。PMID:38422473。
- Tripathy D等人。用于转移性乳腺癌和脑转移患者的依替腺苷酸聚乙二醇处理的最终结果:来自ATTAIN随机临床试验的第3阶段。JAMA Oncol。2022年;8(7):1047-1052。doi:10.1001/jamaoncol.2022.0514。
- O'Shaughnessy J等人。在Ⅲ期ASCENT研究中,分析没有和有最初三阴性乳腺癌诊断的患者,在转移性三阴性乳腺癌中应用sacituzumab govitecan的有效性和安全性。Breast Cancer Res Treat。2022年9月; 195(2):127-139。doi:10.1007/s10549-022-06602-7。Epub 2022年5月11日。PMID:35545724;PMCID:PMC9374646。
About BriaCell Therapeutics Corp.
关于BriaCell Therapeutics Corp。
BriaCell is a clinical-stage biotechnology company that develops novel immunotherapies to transform cancer care. More information is available at
BriaCell是一家临床阶段的生物技术公司,开发新型免疫疗法来改变癌症治疗。更多信息可在
Safe Harbor
免责声明
This press release contains "forward-looking statements" that are subject to substantial risks and uncertainties. All statements, other than statements of historical fact, contained in this press release are forward-looking statements. Forward-looking statements contained in this press release may be identified by the use of words such as "anticipate," "believe," "contemplate," "could," "estimate," "expect," "intend," "seek," "may," "might," "plan," "potential," "predict," "project," "target," "aim," "should," "will," "would," or the negative of these words or other similar expressions, although not all forward-looking statements contain these words. Forward-looking statements, including those about the presentation at the 2024 ASCO of two poster sessions, one abstract, and the delivery of an oral presentation by Dr. Saranya Chumsri, and the contents of all such materials and presentations; BriaCell's novel immunotherapy offering a well-tolerated treatment option for patients beyond the currently approved drugs; Bria-IMT having the potential to become a breakthrough novel treatment option for patients in advanced metastatic breast cancer; "Treatment of Physician's Choice" (TPC) being the comparator in the Phase 3 study of Bria-IMT; monotherapy becoming another arm of the Bria-IMT regimen; the potential clinical benefit of Bria-IMT in managing CNS metastases disease in advanced breast cancer; BriaCell continuing to monitor the data in the intracranial disease subgroup of patients in its ongoing pivotal Phase 3 study in advanced metastatic breast cancer; and the treatment of patients with CNS metastatic disease representing a potential additional indication for market approval of Bria-IMT, are based on BriaCell's current expectations and are subject to inherent uncertainties, risks, and assumptions that are difficult to predict. Further, certain forward-looking statements are based on assumptions as to future events that may not prove to be accurate. These and other risks and uncertainties are described more fully under the heading "Risks and Uncertainties" in the Company's most recent Management's Discussion and Analysis, under the heading "Risk Factors" in the Company's most recent Annual Information Form, and under "Risks and Uncertainties" in the Company's other filings with the Canadian securities regulatory authorities and the U.S. Securities and Exchange Commission, all of which are available under the Company's profiles on SEDAR+ at and on EDGAR at www.sec.gov. Forward-looking statements contained in this announcement are made as of this date, and BriaCell Therapeutics Corp. undertakes no duty to update such information except as required under applicable law.
本新闻稿包含“前瞻性声明”,受到重大风险和不确定性的影响。除了历史事实陈述外,本新闻稿中包含的所有其他陈述均属于前瞻性声明。前瞻性声明包括在本新闻稿中,如关于2024年ASCO会议上两个海报和一个口头陈述的演示,以及Saranya Chumsri博士的演示内容; BriaCell的新型免疫疗法为超出目前批准药物的患者提供了一个耐受性良好的治疗选择; Bria-IMT有可能成为晚期转移性乳腺癌患者的突破性新型治疗选择; “医生的选择治疗”(TPC)是Bria-IMT的第三期研究中的对照组; 单药治疗成为Bria-IMT方案的另一个治疗方案; Bria-IMT在治疗晚期乳腺癌中管理中枢神经系统转移疾病的潜在临床益处; BriaCell将继续监测进行中的面向晚期转移性乳腺癌的关键第三期研究中的颅内疾病亚组数据; 用于治疗中枢神经系统转移性疾病的患者的治疗代表Bria-IMT的潜在附加适应症,并且是市场批准的另一个适应症,都基于BriaCell目前的预期并且存在困难预测的固有不确定性和风险和假设。此外,某些前瞻性声明基于未来事件的假设,这些假设可能证明不准确。更进一步的风险和不确定性的描述,请参阅公司最新的管理层讨论与分析报告中的“风险和不确定性”一章,最新的年度信息表中的“风险因素”一章,以及公司在加拿大证券监管机构和美国证券交易委员会上的其他申报文书中的“风险和不确定性”。所有这些申报文书都可以在公司的SEDAR个人配置文件和EDGAR个人配置文件下找到 和 www.sec.gov中。本公告中包含的前瞻性声明均截至本日,并且BriaCell Therapeutics Corp.除适用法律规定外,无需更新此类信息。
Neither the Toronto Stock Exchange nor its Regulation Services Provider (as that term is defined in the policies of the Toronto Stock Exchange) accepts responsibility for the adequacy or accuracy of this release.
多伦多证券交易所及其监管服务提供商(根据多伦多证券交易所政策中此项术语的定义)不对本公告的充足性或准确性承担任何责任。
Contact Information
联系信息
Company Contact:
William V. Williams, MD
President & CEO
1-888-485-6340
info@briacell.com
公司联系人:
William V. Williams,MD
总裁兼首席执行官
1-888-485-6340
info@briacell.com
Media Relations:
Jules Abraham
CORE IR
julesa@coreir.com
媒体关系:
Jules Abraham
CORE IR
julesa@coreir.com
Investor Relations Contact:
CORE IR
investors@briacell.com
投资者关系联系人:
CORE IR
investors@briacell.com
Photos accompanying this announcement are available at
附带的照片可在以下网址获取
