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...
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宣佈在美國放射腫瘤學會第66屆年會上發佈了關於評估在患有固體腦轉移瘤或腦腦膜轉移瘤並攜帶PI0.3萬途徑突變的患者中同時接受帕硫治和放射治療的有前景Ⅰ期數據。
Treatment with 45mg paxalisib and radiotherapy demonstrated 67% partial response (PR)
使用45毫克帕硫治和放射治療展示了67%的部分緩解(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
至少超過三分之二的患者在最大耐受劑量(MTD)下實現顱內反應,這與僅接受全腦放療的歷史反應率相比較有利。
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 /路透社/ -- 納斯達克上市公司Kazia Therapeutics Limited(股票代碼:KZIA),一家專注於腫瘤治療藥物研發的公司,宣佈了一項第Ⅰ期研究(NCT04192981)評估同時接受帕硫治和放射治療(RT)用於治療患有固體腦轉移瘤(BM)或腦腦膜轉移瘤(LM)並攜帶PI0.3萬途徑突變的患者的數據在美國放射腫瘤學會第66屆年會(ASTRO 2024)上發佈,該年會於2024年9月29日至10月2日在華盛頓特區舉行。
"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."
「這項第1期研究觀察到的令人鼓舞的反應率表明,在患有PI0.3萬途徑突變的患者中,正在進行的研究中,通過同時給予帕硫治的腦內非抗性PI0.3萬抑制劑與放射治療相結合似乎是一種可行的治療方法,」 Kazia Therapeutics首席執行官約翰·弗倫德萬博士說。 「本研究還將展示來自這項研究的循環腫瘤DNA(ctDNA)等額外數據,並正在討論有關評估此獨特組合療法用於患有PI0.3萬突變腦轉移瘤患者的潛在關鍵性登記研究的討論,該研究將於2024年的某次科學大會上發佈。」
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 |
Presenter: |
Brandon S. Imber, M.D., M.A., Memorial Sloan Kettering Cancer Center |
Abstract |
1094 |
Scientific Session Title: |
CNS 4: Brain Mets and LMD |
Session Date/Time: |
October 1, 5:15-6:15 PM ET |
演講詳情: |
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標題: |
固體腫瘤腦轉移(BM)或寄生轉移(LM)患者同時接受Paxalisib和放療的多中心I期研究,這些患者攜帶PI0.3萬信號通路突變 |
報告人: |
Brandon S. Imber博士,紀念斯隆凱特琳癌症中心 |
摘要 |
1094 |
科學研討會標題: |
CNS 4:大腦轉移和腦膜瘤 |
會議日期/時間: |
愛文思控股於美國東部時間10月1日下午5:15-6:15 |
Summary Results from Part II of Phase 1 Study
第1期研究第II部分的摘要結果
- 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.
- 在具有PI0.3萬通路突變的晚期實體腫瘤大腦轉移患者中,帕克沙利帕與腦放療的同時每天最大劑量45毫克一般耐受良好;
- 該研究中報道的最常見不良事件是噁心、嘔吐和高血糖;
- 在放射腫瘤學中建立了分子選擇的、合理的組合研究的概念驗證,以評估安全性和最終療效;
- 45mg帕克沙利帕聯合放療治療表現出67%的部分緩解率; and
- 過半數MTD患者獲得了顱內反應,與單獨WBRt的歷史反應率相比具有優勢。
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.
第1期研究(n=17可評估對象)是一項兩部分的、由研究者發起的試驗,旨在評估paxalisib與放射治療聯合治療PI0.3萬通路突變固實瘤腦轉移患者的用藥。研究的第一部分確定了paxalisib與放射治療的MTD,同時展示了9名可評估患者中所有9名患者都表現出臨床活性的有希望跡象。第二部分是一個後續擴展隊列,進一步評估MTD(每日45mg)與放射治療聯合治療在多達12名額外患者中的安全性和有效性。
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.
每年大約有20萬名癌症患者在美國患上腦轉移。放療是腦轉移的主要治療手段,一般包括立體定向放射外科(SRS)或全腦放射治療(WBRT)或二者的某種組合。接受WBRt治療的患者的療效因腫瘤類型、顱內轉移的數量和體積而異,但有幾項最近的出版物引用總體反應率爲20-45%。腦轉移發病率的增加和現有治療的低反應率凸顯了對新治療選擇的需求。
About Kazia Therapeutics Limited
關於Kazia Therapeutics Limited
Kazia Therapeutics Limited (NASDAQ: KZIA) is an oncology-focused drug development company, based in Sydney, Australia.
Kazia Therapeutics Limited(NASDAQ:KZIA)是一家專注於腫瘤學藥物開發的公司,總部位於澳大利亞悉尼。
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.
我們的主要項目是paxalisib,這是一種能夠穿透血腦屏障的PI0.3萬/Akt/mTOR通路抑制劑,目前正在研發用於治療多種形式的腦癌。該藥物於2016年末從Genentech獲得授權,目前或曾經在該疾病中進行過十項臨床試驗。在2021年,一項完成的腦膠質母細胞瘤II期研究報告了早期的臨床活性信號,而GBm AGILE中關鍵研究、腦膠質母細胞瘤的一個關鍵研究已經完成,預計將在2024年的重大醫學會議上公佈paxalisib的研究數據。涉及paxalisib的其他臨床試驗仍在進行中,包括腦轉移瘤、瀰漫性中線膠質瘤和原發性中樞神經系統淋巴瘤,其中幾項試驗已經報告了令人鼓舞的中期數據。
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於2018年2月獲得FDA對於膠質母細胞瘤的孤兒藥物認定,並於2020年8月獲得FDA對於膠質母細胞瘤的快速通道認定。Paxalisib還於2023年7月獲得FDA對於攜帶PI0.3萬通路突變的固體腫瘤腦轉移的快速通道認定,該認定與放射療法聯合應用。此外,Paxalisib於2020年8月獲得FDA對於瀰漫性髓橋膠質瘤的罕見兒科疾病認定和孤兒藥物認定,以及於2022年6月和2022年7月獲得FDA對於非典型畸胎/橫紋肌瘤的罕見兒科疾病認定和孤兒藥物認定。
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 therapeutics也正在研發EVT801,這是一種VEGFR3的小分子抑制劑,該藥物於2021年4月從Evotec SE授權獲得。臨床前數據顯示,EVT801對多種腫瘤類型有效,並顯示出與免疫腫瘤學藥物的協同作用證據。一期研究已經完成,並於2024年9月在第15屆卵巢癌研討會上發佈了初步數據。欲了解更多信息,請訪問 或關注我們在X上的賬號@KaziaTx。
Forward-Looking Statements
前瞻性聲明
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.
此公告可能包含前瞻性聲明,可以通過使用諸如「可能」,「將會」,「估計」,「未來」,「前進」,「預期」或其他類似詞語來識別。任何描述kazia未來計劃,戰略,意圖,期望,目標,目標或前景的聲明,以及其他非歷史事實的陳述,也屬於前瞻性聲明,包括但不限於有關:與Kazia的臨床和臨床前試驗相關的結果和數據的時間安排,Kazia在其項目方面的戰略和計劃,包括paxalisib和EVT801,paxalisib作爲一種檢驗性PI3K/mTOR抑制劑的潛在益處,任何與監管機構提交申請或與監管機構討論的時間安排,以及paxalisib的潛在市場機會。此類聲明基於Kazia目前對未來事件和影響其業務的未來趨勢的期望和預測,並受到某些風險和不確定性的影響,這可能導致實際結果與前瞻性聲明中預期的結果有重大不同,包括與臨床和臨床前試驗以及產品開發相關的風險和不確定性,相關的監管批准,全球經濟狀況的影響等風險和不確定性。這些以及其他風險和不確定性在Kazia的年度報告中更詳細描述,已向美國證券交易委員會提交了20-F表格,以及向美國證券交易委員會提交的後續文件中。Kazia不承諾公開更新任何前瞻性聲明,除非根據適用法律要求。您不應該過度依賴這些前瞻性聲明,這些聲明僅適用於此公告的日期。
This announcement was authorized for release by Dr John Friend, CEO.
此公告經CEO約翰·弗蘭德博士授權發佈。
SOURCE Kazia Therapeutics Limited
來源:kazia therapeutics limited