Objective response rate of 39% with manageable safety profile in patients with non-small cell lung cancer (NSCLC) harboring EGFR Exon 20 insertion mutations treated with zipalertinib who had progressed after prior amivantamab treatment
CAMBRIDGE, Mass., June 01, 2024 (GLOBE NEWSWIRE) -- Cullinan Therapeutics, Inc. (Nasdaq: CGEM), a biopharmaceutical company focused on developing modality-agnostic targeted therapies, today announced positive initial data in patients receiving zipalertinib after prior treatment with amivantamab enrolled in its pivotal Phase 2b REZILIENT1 clinical trial.
As of a January 12, 2024 data cut-off, 31 patients had been enrolled. Patients had received a median of three prior systemic anti-cancer regimens, including prior platinum-based chemotherapy, prior anti-PD1/L1 therapy, and prior epidermal growth factor receptor (EGFR) tyrosine kinase inhibitor (TKI) therapy.
At data cut-off, 18 patients were evaluable for response and showed similar anti-tumor activity compared with those post prior chemotherapy in the previously reported Phase 1/2a part of the study.
| Module C (post chemo
and Ami+/- other
exon20ins treatment)
(N=18) | Phase 1/2a results
(post chemo)1
(N=39) |
ORR (confirmed) | 39% | 41% |
DCR2 | 94% | 97% |
DOR (months) | NE | NE |
PFS (months) | NE | 12 |
NE: Not yet estimable
ORR: Objective response rate; DCR: Disease control rate; DOR: Duration of response; PFS: Progression-free survival
1 Piotrowska Z, et al. JCO 2023
2 DCR= (PR+SD) / response-evaluable patients
PR: Partial response; SD: Stable disease
Zipalertinib demonstrated a manageable safety profile, similar to what has been previously reported. There were no grade 4 or grade 5 treatment-related adverse events.
"In an evolving treatment landscape, this is the first ever clinical data to systematically characterize the potential of an irreversible and selective EGFR exon20 insertion mutation TKI such as zipalertinib in patients who were heavily pre-treated and had received amivantamab. Given the recent approval of amivantamab as a first line treatment in combination with chemotherapy, we are encouraged by the initial results of the Phase 2b portion of the REZILIENT1 clinical trial, which show that in a post-amivantamab setting, zipalertinib demonstrated promising efficacy, similar to that in patients who progressed after platinum-based chemotherapy alone, and had a manageable safety profile," said Jeffrey Jones, MD, MBA, Chief Medical Officer, Cullinan Therapeutics. "With a comprehensive development plan for zipalertinib, this data further strengthens our confidence in its potential to address a significant unmet need for patients with NSCLC harboring EGFR exon20 insertion mutations. We remain on track to complete enrollment in the pivotal Phase 1/2b REZILIENT1 trial by the end of this year."
Zipalertinib has a unique chemical structure that is distinct from other exon20 insertion directed agents, which makes it highly selective for mutant exon 20 versus wild-type EGFR. Cullinan entered into a partnership with Taiho in 2022, with an upfront cash payment of $275M and additional payments totaling $130M to be made for US regulatory approvals in 1L and 2L+ NSCLC. Cullinan also retains a 50/50 profit share in the U.S.
Cullinan and Taiho have a broad development program for zipalertinib through a suite of REZILIENT studies, including two ongoing pivotal studies in 1L and 2L+ exon20 insertion NSCLC as well as studies in other patient populations such as patients with active brain metastases and those with uncommon EGFR mutations. Both Module B2 (post chemo only) and Module C (post approved ex20ins treatments) of the pivotal REZILIENT1 trial remain on track to complete enrollment by end of 2024, consistent with prior projections.
Virtual and Live Investor Event
Cullinan Therapeutics will host an Investor Event on Saturday, June 1, 2024, at 6:30 PM Central Time, during which Dr. Jeff Jones, Chief Medical Officer at Cullinan Therapeutics, will present an overview of this zipalertinib data along with CLN-619 data shared at the 2024 American Society of Clinical Oncology Annual Meeting. Alexander Spira, MD, PhD, FACP, FASCO, Director, Virginia Cancer Specialists Research Institute and Director, NEXT Oncology Virginia, will share an overview of the current treatment landscape for EGFR-mutated NSCLC. Investors and analysts are invited to register to attend in person by emailing Chad Messer, VP Investor Relations (cmesser@cullinantx.com). A live webcast will be available via the events page of the Company's investor relations website at and a replay will be available shortly after the conclusion of the live event.
About Zipalertinib
Zipalertinib (CLN-081/TAS6417) is an orally available small molecule designed to target activating mutations in EGFR. The molecule was engineered to inhibit EGFR variants with exon 20 insertion mutations, while sparing wild-type EGFR. Zipalertinib is designed as a next generation, irreversible EGFR inhibitor for the treatment of a genetically defined subset of patients with non-small cell lung cancer. Zipalertinib has received Breakthrough Therapy Designation from the FDA.
Zipalertinib is being developed by Taiho Oncology, Inc., its parent company, Taiho Pharmaceutical Co., Ltd., and Cullinan Therapeutics, Inc. Cullinan Pearl Corp., which Taiho Pharmaceutical Co., Ltd., acquired from Cullinan Therapeutics, Inc. in 2022, previously licensed the rights to zipalertinib in Greater China to Zai Lab Limited in 2020.
使用齊帕替尼治療的非小細胞肺癌(NSCLC)患者的客觀緩解率爲39%,安全性可控,這些患者在接受齊帕替尼治療後出現進展的表皮生長因子外顯子20插入突變
馬薩諸塞州劍橋,2024年6月1日(GLOBE NEWSWIRE)——專注於開發與模式無關的靶向療法的生物製藥公司庫裏南療法公司(納斯達克股票代碼:CGEM)今天公佈了參與其關鍵的2b 期 REZILIENT1 臨床試驗後接受齊帕勒替尼治療的患者的積極初步數據。
截至2024年1月12日的數據截止日期,已有31名患者入組。患者接受的三種全身抗癌方案中位數,包括先前的鉑類化療、先前的抗PD1/L1治療和先前的表皮生長因子受體(EGFR)酪氨酸激酶抑制劑(TKI)治療。
在數據截止時,在先前報告的1/2a期研究中,有18名患者進行了反應評估,並表現出與之前化療後的患者相似的抗腫瘤活性。
| 模塊 C(化療後)
還有 Ami+/-其他
exon20ins 治療)
(N = 18) | 第 1/2a 階段的結果
(化療後)1
(N=39) |
ORR(已確認) | 39% | 41% |
DCR2 | 94% | 97% |
DOR(月) | 沒有 | 沒有 |
PFS(月) | 沒有 | 12 |
NE:尚不可估計
ORR:客觀緩解率;DCR:疾病控制率;DOR:反應持續時間;PFS:無進展存活率
1 Piotrowska Z 等人JCO 2023
2 DCR= (PR+SD) /反應可評估的患者
PR:部分反應;SD:穩定疾病
Zipalertinib顯示出可控的安全性,與先前報道的類似。沒有4級或5級治療相關的不良事件。
“在不斷變化的治療環境中,這是有史以來第一份系統地描述了諸如齊帕勒替尼等不可逆和選擇性表皮生長因子外顯子20插入突變TKI在經過大量預治療並接受過阿米萬坦單抗的患者中可能出現的臨床數據。鑑於阿米凡坦單抗最近獲准作爲與化療聯合使用的一線療法,REZILIENT1 臨床試驗2b期的初步結果令我們感到鼓舞,該結果表明,在阿米萬坦單抗之後的環境中,齊帕樂替尼表現出令人鼓舞的療效,與僅接受鉑類化療後進展的患者類似,安全性可控的患者。” 工商管理碩士傑弗裏·瓊斯說,庫裏南療法首席醫學官。“通過zipalertinib的全面開發計劃,這些數據進一步增強了我們的信心,使其有潛力解決帶有表皮生長因子外顯子20插入突變的非小細胞肺癌患者大量未得到滿足的需求。我們仍有望在今年年底之前完成關鍵的 1/2b 期 REZILIENT1 試驗的入組。”
Zipalertinib具有獨特的化學結構,與其他外顯子20插入定向藥物截然不同,這使得它對突變外顯子20與野生型表皮生長因子具有很高的選擇性。庫裏南於2022年與Taiho建立了合作伙伴關係,預付了2.75億美元的現金,並額外支付了總額爲1.3億美元的款項,以獲得美國監管機構的1L和2L+非小細胞肺癌的批准。庫裏南在美國還保留了50/50的利潤份額。
Cullinan和Taiho通過一系列REZILIENT研究,爲齊帕勒替尼制定了廣泛的開發計劃,包括兩項正在進行的針對1L和2L+外顯子20插入的關鍵研究,以及對其他患者群體的研究,例如活性腦轉移患者和表皮生長因子異常突變患者。與先前的預測一致,這項關鍵的 REZILIENT1 試驗的模塊 B2(僅限化療後)和模塊 C(批准後的 ex20ins 治療)均有望在 2024 年底前完成入組。
虛擬和現場投資者活動
Cullinan Therapeutics將於美國中部時間2024年6月1日星期六下午6點30分舉辦投資者活動,在此期間,庫裏南療法首席醫學官傑夫·瓊斯博士將概述齊帕勒替尼的這些數據以及在2024年美國臨床腫瘤學會年會上分享的 CLN-619 數據。Alexander Spira,醫學博士,FACP,FASCO,弗吉尼亞癌症專家研究所所長兼弗吉尼亞NEXT Oncology主任,將概述表皮生長因子突變的非小細胞肺癌的當前治療格局。邀請投資者和分析師通過發送電子郵件給投資者關係副總裁查德·梅塞爾(cmesser@cullinantx.com)註冊親自出席。將通過公司投資者關係網站的活動頁面進行網絡直播,直播活動結束後不久將提供重播。
關於齊帕勒替尼
齊帕勒替尼(CLN-081/TAS6417)是一種口服可口服的小分子,旨在靶向表皮生長因子的激活突變。該分子經過精心設計,可抑制具有20外顯子插入突變的表皮生長因子變體,同時避免野生型表皮生長因子。Zipalertinib被設計爲下一代不可逆的表皮生長因子抑制劑,用於治療基因定義的非小細胞肺癌患者。Zipalertinib已獲得美國食品藥品管理局的突破性療法稱號。
Zipalertinib由大和腫瘤株式會社及其母公司大豐製藥有限公司和庫裏南製藥有限公司開發,庫裏南珍珠公司是大豐製藥有限公司於2022年從庫裏南治療公司手中收購的,此前曾於2020年將齊帕勒替尼在大中華區的版權許可給了Zai Lab Limited。
