Kazia Therapeutics Announces Presentation of Promising Phase I Data Evaluating Concurrent Paxalisib and Radiation Therapy in Patients With Solid Tumor Brain Metastases or Leptomeningeal Metastases Harboring PI3K Pathway Mutations at the American...
Kazia Therapeutics Announces Presentation of Promising Phase I Data Evaluating Concurrent Paxalisib and Radiation Therapy in Patients With Solid Tumor Brain Metastases or Leptomeningeal Metastases Harboring PI3K Pathway Mutations at the American...
"The encouraging response rates observed from this Phase 1 study suggests that the concurrent administration of the investigational brain penetrant PI3K inhibitor, paxalisib, in combination radiation therapy appears to be a viable treatment approach for addressing the tumor radioresistance in patients harboring PI3K pathway mutations," said Kazia Therapeutics Announces Presentation of Promising Phase I Data Evaluating Concurrent Paxalisib and Radiation Therapy in Patients With Solid Tumor Brain Metastases or Leptomeningeal Metastases Harboring PI3K Pathway Mutations at the American Society for Radiation Oncology 66th Annual Meeting
Kazia Therapeutics宣布在美国放射肿瘤学会第66届年会上公布有前景的I期数据,评估实体瘤脑转移或带有PI0.3万路径突变的轻脑膜转移患者同时进行Paxalisib和放射治疗
Treatment with 45mg paxalisib and radiotherapy demonstrated 67% partial response (PR)
45mg paxalisib 和放射疗法的治疗显示出 67% 的部分反应 (PR)
Over two-thirds of the patients at maximum tolerated dose (MTD) achieved intracranial response which compares favorably to historical response rates for whole brain radiation therapy alone
超过三分之二的患者在最大耐受剂量(MTD)下实现了颅内反应,这与仅使用全脑放射治疗的历史反应率相比是有利的
SYDNEY, Oct. 2, 2024 /PRNewswire/ -- Kazia Therapeutics Limited (NASDAQ: KZIA), an oncology-focused drug development company, announced the presentation of data from a Phase I study (NCT04192981) evaluating concurrent paxalisib and radiation therapy (RT) in patients for the treatment of solid tumor brain metastases (BM) or leptomeningeal metastases (LM) harboring PI3K pathway mutations at the American Society for Radiation Oncology 66th Annual Meeting (ASTRO 2024), which is taking place from September 29 - October 2, 2024, in Washington, D.C.
悉尼,2024年10月2日 /PRNewswire/ — 专注于肿瘤学的药物开发公司Kazia Therapeutics Limited(纳斯达克股票代码:KZIA)宣布公布了一项I期研究(NCT04192981)的数据,该研究评估了患者同时进行paxalisib和放射治疗(RT)以治疗实体瘤脑转移(BM)或轻脑膜转移瘤(LM)含有 PI0.3万 mukanyan 途径的患者在美国放射肿瘤学会第 66 届年会(ASTRO 2024)上,该年会将于 2024 年 9 月 29 日至 10 月 2 日在华盛顿特区举行
"The encouraging response rates observed from this Phase 1 study suggests that the concurrent administration of the investigational brain penetrant PI3K inhibitor, paxalisib, in combination radiation therapy appears to be a viable treatment approach for addressing the tumor radioresistance in patients harboring PI3K pathway mutations," said John Friend, M.D., Chief Executive Officer of Kazia Therapeutics. "Additional data, including circulating tumor DNA (ctDNA) from this study will be presented at an upcoming 2024 scientific congress and discussions for a potential pivotal registration study to evaluate this unique combination therapy for patients with PI3K mutant brain metastases are ongoing."
Kazia Therapeutics首席执行官John Friendwand.D.表示:“从这项1期研究中观察到的令人鼓舞的反应率表明,在联合放射治疗中同时使用正在研究的脑穿透剂PI0.3万抑制剂paxalisib似乎是解决携带PI0.3万路径突变的患者肿瘤放射耐药的可行治疗方法。”“包括这项研究的循环肿瘤DNA(ctDNA)在内的其他数据将在即将举行的2024年科学大会上公布,有关一项潜在的关键注册研究的讨论正在进行中,该研究旨在评估这种针对PI0.3万突变脑转移患者的独特联合疗法。”
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Presentation details: |
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Title: |
Multi-Center Phase I Study of Concurrent Paxalisib and Radiation Therapy in Patients with Solid Tumor Brain Metastases (BM) or Leptomeningeal Metastases (LM) Harboring PI3K Pathway Mutations |
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Presenter: |
Brandon S. Imber, M.D., M.A., Memorial Sloan Kettering Cancer Center |
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Abstract |
1094 |
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Scientific Session Title: |
CNS 4: Brain Mets and LMD |
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Session Date/Time: |
October 1, 5:15-6:15 PM ET |
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演示详情: |
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标题: |
对带有PI0.3万通路突变的实体瘤脑转移(BM)或轻脑膜转移(LM)患者同时进行Paxalisib和放射治疗的多中心I期研究 |
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演示者: |
Brandon S. Imbervan.D.Van.A.,纪念斯隆·凯特琳癌症中心 |
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摘要 |
1094 |
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科学会议标题: |
CNS 4:Brain Mets 和 LMD |
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会话日期/时间: |
美国东部时间 10 月 1 日下午 5:15-6:15 |
Summary Results from Part II of Phase 1 Study
第一阶段研究第二部分的结果摘要
- Concurrent daily administration of paxalisib with brain radiotherapy was generally well-tolerated at a maximum dose of 45 mg per day in advanced solid tumor patients with brain metastases and PI3K pathway mutations;
- The most commonly reported adverse events in the study were nausea, vomiting and hyperglycemia;
- Established proof-of-principle for molecularly-selected, rational combination studies in radiation oncology to assess safety and ultimately efficacy;
- Treatment with 45mg paxalisib and radiotherapy demonstrated a 67% PR; and
- Over two-thirds of the patients at MTD achieved intracranial response which compares favorably to historical response rates for WBRT alone.
- 对于患有脑转移和PI0.30万路径突变的晚期实体瘤患者,每日同时给予paxalisib与脑放疗的耐受性通常良好,最大剂量为45 mg;
- 该研究中最常报告的不良事件是恶心、呕吐和高血糖;
- 为放射肿瘤学中分子选择的合理组合研究建立了原理验证,以评估安全性和最终疗效;
- 使用45mg paxalisib和放射疗法进行治疗的PR为67%;以及
- 超过三分之二的MTD患者实现了颅内反应,这与仅使用wbRT的历史缓解率相比是有利的。
The Phase 1 study (n=17 evaluable) was a two-part, investigator-initiated trial evaluating the use of paxalisib with radiation therapy for the treatment of patients with PI3K pathway mutation brain metastases from solid tumors. Part I of the study established the MTD of paxalisib in combination with radiation therapy, while also demonstrating promising signs of clinical activity in all nine evaluable patients. Part II was a follow-on expansion cohort to further evaluate safety and efficacy of the MTD (45mg daily) combined with radiation therapy in up to 12 additional patients.
1期研究(n=17可评估)是一项由研究人员发起的由两部分组成的试验,评估了将paxalisib与放射治疗一起用于治疗实体瘤PI0.30万路径突变脑转移患者。该研究的第一部分确定了paxalisib与放射治疗联合使用的MTD,同时还显示出所有九名可评估患者的临床活性迹象。第二部分是一个后续扩展队列,旨在进一步评估MTD(每天45mg)联合放射治疗对多达12名患者的安全性和有效性。
Approximately 200,000 cancer patients develop brain metastases in the United States each year. Radiotherapy is the mainstay of treatment for brain metastases, and generally consists of either stereotactic radiosurgery (SRS) or whole brain radiotherapy (WBRT) or some combination thereof. The efficacy in patients who receive WBRT differs according to the type of tumor and the number and volume of brain metastases, but several recent publications cite overall response rates of 20-45%. The increasing incidence of brain metastasis and the low response rates to existing treatments underscores the need for new treatment options.
在美国,每年约有20万名癌症患者出现脑转移。放射治疗是脑转移治疗的主要手段,通常包括立体定向放射外科(SRS)或全脑放射治疗(WBRT)或两者的某种组合。接受wBRT的患者的疗效因肿瘤类型以及脑转移的数量和体积而异,但最近的几份出版物指出,总体缓解率为20-45%。脑转移发生率的增加和对现有治疗的低反应率凸显了对新治疗选择的需求。
About Kazia Therapeutics Limited
关于卡齐亚治疗有限公司
Kazia Therapeutics Limited (NASDAQ: KZIA) is an oncology-focused drug development company, based in Sydney, Australia.
Kazia Therapeutics Limited(纳斯达克股票代码:KZIA)是一家专注于肿瘤学的药物开发公司,总部位于澳大利亚悉尼。
Our lead program is paxalisib, an investigational brain-penetrant inhibitor of the PI3K / Akt / mTOR pathway, which is being developed to treat multiple forms of brain cancer. Licensed from Genentech in late 2016, paxalisib is or has been the subject of ten clinical trials in this disease. A completed Phase 2 study in glioblastoma reported early signals of clinical activity in 2021, and a pivotal study in glioblastoma, GBM AGILE, has been completed with presentation of paxalisib arm data expected later in 2024 at a major medical conference. Other clinical trials involving paxalisib are ongoing in brain metastases, diffuse midline gliomas, and primary CNS lymphoma, with several of these trials having reported encouraging interim data.
我们的主要项目是paxalisib,这是一种正在研究的PI0.3万/ Akt/mTOR途径的脑穿透抑制剂,该通路正在开发用于治疗多种形式的脑癌。paxalisib于2016年底获得基因泰克的许可,目前或曾经是该疾病的十项临床试验的主题。一项已完成的胶质母细胞瘤2期研究报告了2021年临床活动的早期信号,胶质母细胞瘤的关键研究gbM AGILE已经完成,预计将在2024年晚些时候在一次大型医学会议上公布paxalisib组的数据。其他涉及paxalisib的临床试验正在进行中,涉及脑转移、弥漫性中线神经胶质瘤和原发性中枢神经系统淋巴瘤,其中一些试验报告了令人鼓舞的中期数据。
Paxalisib was granted Orphan Drug Designation for glioblastoma by the FDA in February 2018, and Fast Track Designation (FTD) for glioblastoma by the FDA in August 2020. Paxalisib was also granted FTD in July 2023 for the treatment of solid tumour brain metastases harboring PI3K pathway mutations in combination with radiation therapy. In addition, paxalisib was granted Rare Pediatric Disease Designation and Orphan Drug Designation by the FDA for diffuse intrinsic pontine glioma in August 2020, and for atypical teratoid / rhabdoid tumours in June 2022 and July 2022, respectively.
Paxalisib于2018年2月被美国食品药品管理局授予胶质母细胞瘤孤儿药称号,并于2020年8月被美国食品药品管理局授予胶质母细胞瘤快速通道认证(FTD)。Paxalisib还于2023年7月获得FTD许可,用于与放射疗法联合治疗携带PI0.3万通路突变的实体瘤脑转移。此外,paxalisib于2020年8月被美国食品药品管理局授予弥漫性内在脑桥神经胶质瘤的罕见儿科疾病认定和孤儿药认定,并分别于2022年6月和2022年7月授予非典型畸胎类/横纹样肿瘤的孤儿药称号。
Kazia is also developing EVT801, a small-molecule inhibitor of VEGFR3, which was licensed from Evotec SE in April 2021. Preclinical data has shown EVT801 to be active against a broad range of tumour types and has provided evidence of synergy with immuno-oncology agents. A Phase I study has been completed and preliminary data was presented at 15th Biennial Ovarian Cancer Research Symposium in September 2024. For more information, please visit or follow us on X @KaziaTx.
Kazia 还在开发 VEGFR3 的小分子抑制剂 EVT801,它于 2021 年 4 月获得了 Evotec SE 的许可。临床前数据表明,EVT801 对多种肿瘤类型具有活性,并提供了与免疫肿瘤学药物协同作用的证据。I期研究已经完成,初步数据已在2024年9月的第15届双年度卵巢癌研究研讨会上公布。欲了解更多信息,请访问或关注我们 X @KaziaTx。
Forward-Looking Statements
前瞻性陈述
This announcement may contain forward-looking statements, which can generally be identified as such by the use of words such as "may," "will," "estimate," "future," "forward," "anticipate," or other similar words. Any statement describing Kazia's future plans, strategies, intentions, expectations, objectives, goals or prospects, and other statements that are not historical facts, are also forward-looking statements, including, but not limited to, statements regarding: the timing for results and data related to Kazia's clinical and preclinical trials, Kazia's strategy and plans with respect to its programs, including paxalisib and EVT801, the potential benefits of paxalisib as an investigational PI3K/mTOR inhibitor, timing for any regulatory submissions or discussions with regulatory agencies, and the potential market opportunity for paxalisib. Such statements are based on Kazia's current expectations and projections about future events and future trends affecting its business and are subject to certain risks and uncertainties that could cause actual results to differ materially from those anticipated in the forward-looking statements, including risks and uncertainties: associated with clinical and preclinical trials and product development, related to regulatory approvals, and related to the impact of global economic conditions. These and other risks and uncertainties are described more fully in Kazia's Annual Report, filed on form 20-F with the SEC, and in subsequent filings with the United States Securities and Exchange Commission. Kazia undertakes no obligation to publicly update any forward-looking statement, whether as a result of new information, future events, or otherwise, except as required under applicable law. You should not place undue reliance on these forward-looking statements, which apply only as of the date of this announcement.
本公告可能包含前瞻性陈述,这些陈述通常可以通过使用 “可能”、“将”、“估计”、“未来”、“向前”、“预期” 或其他类似词语来识别。任何描述Kazia未来计划、战略、意图、预期、目标、目标或前景的陈述,以及其他非历史事实的陈述,也是前瞻性陈述,包括但不限于以下方面的陈述:与Kazia临床和临床前试验相关的结果和数据的时机、Kazia与其项目(包括paxalisib和 EVT801)相关的战略和计划、paxalisib作为研究PiNational的潜在益处 3K/mTOR 抑制剂,任何监管机构提交或讨论的时机监管机构,以及paxalisib的潜在市场机会。此类陈述基于Kazia当前对影响其业务的未来事件和未来趋势的预期和预测,并存在某些风险和不确定性,这些风险和不确定性可能导致实际结果与前瞻性陈述中的预期存在重大差异,包括风险和不确定性:与临床和临床前试验及产品开发有关,与监管批准有关以及与全球经济状况的影响有关。Kazia以20-F表格向美国证券交易委员会提交的年度报告以及随后向美国证券交易委员会提交的文件中对这些风险和不确定性进行了更全面的描述。除非适用法律要求,否则Kazia没有义务公开更新任何前瞻性陈述,无论是由于新信息、未来事件还是其他原因。您不应过分依赖这些前瞻性陈述,这些陈述仅在本公告发布之日适用。
This announcement was authorized for release by Dr John Friend, CEO.
该公告由首席执行官约翰·弗里德博士授权发布。
SOURCE Kazia Therapeutics Limited
来源 Kazia Therapeutics 有限公司
