BeyondSpring Presents Efficacy/Safety Results From a Phase 2 Study of Pembrolizumab Plus Plinabulin/Docetaxel in Metastatic NSCLC After Progressing on First-Line Immune Checkpoint Inhibitors at ESMO Congress 2024
BeyondSpring Presents Efficacy/Safety Results From a Phase 2 Study of Pembrolizumab Plus Plinabulin/Docetaxel in Metastatic NSCLC After Progressing on First-Line Immune Checkpoint Inhibitors at ESMO Congress 2024
At the database lock on 29 April 2024, 29 patients were enrolled and 19 were evaluable for stage 1 data analysis. All patients experienced disease progression after initial clinical benefit with ICI. Of the 19 evaluable patients (median age at 66.4 years; ranged 50-76 years), 68.4% were male and 31.6% were female; 57.9% were current or former smokers. Histology included 57.9% patients with non-squamous cell carcinoma and 42.1% with squamous cell carcinoma. The median follow-up was 8.67 months. Below is an efficacy summary table.- Median PFS at 8.63 months and Disease Control Rate of 89.5% in Previously Treated NSCLC Patients after Progression on PD-1/L1 Monotherapy or in Combination with Platinum Doublet Chemotherapy
- 先前接受過PD-1/L1單藥治療或與鉑雙聯化療的NSCLC患者,中位無進展生存期爲8.63個月,疾病控制率達89.5%。
Florham Park, N.J., September 16, 2024 – BeyondSpring Inc. (NASDAQ: BYSI) ("BeyondSpring" or the "Company"), a clinical-stage global biopharmaceutical company developing innovative cancer therapies, today presented interim phase 2 data on the 303 Study, a study in 2L/3L non-small cell lung cancer (NSCLC) after disease progression on 1L PD-1/L1 inhibitors with and without chemotherapy, with financial support from Merck & Co., Inc's (NYSE: MRK, known as MSD outside of the United States and Canada) Investigator Studies Program and provision of study drug, at the European Society for Medical Oncology (ESMO) Congress 2024, on September 14, 2024 in Barcelona, Spain.
2024年9月16日,新澤西州弗洛姆帕克-萬春醫藥公司(納斯達克股票代碼:BYSI)("萬春醫藥"或"公司"),一家臨床階段的全球生物製藥公司,正在開發創新的癌症療法,今天在西班牙巴塞羅那舉辦的2024年歐洲醫學腫瘤學會(ESMO)大會上,就303研究的中期2期數據進行了展示,該研究針對在一線PD-1/L1抑制劑治療出現疾病進展後的2線/3線非小細胞肺癌(NSCLC),研究同時考察了化療的情況,並得到了默沙東(紐約證交所股票代碼:MRk,在美國和加拿大以外地區稱爲MSD)的投資者研究計劃的財務支持和研究藥物的提供。
Docetaxel remains the standard of care for patients with 2L/3L NSCLC without targetable alterations who progress on 1L immune checkpoint inhibitors (ICI) with and without standard chemotherapy, with an overall response rate (ORR) of 12.8% and median PFS (mPFS) of 3.7 months in TROPION Lung-01 phase 3 studies. In metastatic NSCLC resistant to previous PD-1/L1 therapy1, PD-L1 and CTLA-4 inhibition alone or in combination with hypofractionated radiotherapy produced limited clinical benefits with ~11.5% ORR.
對於那些在1L免疫檢查點抑制劑聯合或不聯合標準化療後沒有可靶點改變的2L/3L NSCLC患者,多西他賽仍然是標準治療,並伴有12.8%的總體反應率(ORR)和3.7個月的中位無進展生存期(mPFS),這一結果來自TROPION Lung-01 3期研究。對於以前對PD-1/L1療法耐藥的轉移性非小細胞肺癌,僅PD-L1和CTLA-4抑制劑單獨使用或與低分段放療聯合使用對臨床效果的改善有限,ORR爲約11.5%。
This investigator-initiated, single-arm, open-label, phase 2 study (KeyPelms-004 or 303 Study) evaluates the efficacy and safety of a triple combination regimen of pembrolizumab plus plinabulin/docetaxel (NCT05599789). The study intends to enroll a total of 47 patients and is ongoing at Peking Union Medical College Hospital, Beijing, China with the principal investigator Dr. Mengzhao Wang, Chief of the Department of Respiratory and Critical Care Medicine. Here, we report on a planned formal interim analysis of 19 patients.
此研究是一項由研究者發起的、單臂的、開放標籤的2期研究(KeyPelms-004或303研究),旨在評估帕博利珠單抗聯合普拉奈布林/多西他賽的治療方案的療效和安全性(NCT05599789)。該研究計劃納入總共47名患者,並在中國北京的北京協和醫學院附屬醫院進行,由主要研究員王孟照醫生領導(呼吸與危重症醫學科主任)。在此,我們報告了19名患者的計劃中期分析結果。
At the database lock on 29 April 2024, 29 patients were enrolled and 19 were evaluable for stage 1 data analysis. All patients experienced disease progression after initial clinical benefit with ICI. Of the 19 evaluable patients (median age at 66.4 years; ranged 50-76 years), 68.4% were male and 31.6% were female; 57.9% were current or former smokers. Histology included 57.9% patients with non-squamous cell carcinoma and 42.1% with squamous cell carcinoma. The median follow-up was 8.67 months. Below is an efficacy summary table.
截至2024年4月29日的數據庫鎖定時,共有29名患者入組,19名患者可用於第一階段數據分析。所有患者在抗腫瘤藥初始治療後均經歷了疾病進展。在19名可用於分析的患者中(中位年齡66.4歲;範圍:50-76歲),68.4%爲男性,31.6%爲女性;57.9%是吸菸者或曾經吸菸者。組織學包括57.9%的非鱗狀細胞癌患者和42.1%的鱗狀細胞癌患者。中位隨訪時間爲8.67個月。以下是療效總結表。
| Primary Endpoint | Plinabulin + Pembrolizumab + Docetaxel (n=19) |
| Confirmed ORR (RECIST 1.1) | 21.1% |
| Secondary Endpoints | |
| Median PFS (RECIST 1.1) |
8.63 M (6 M PFS rate: 67.1%; 12 M PFS rate: 49.2%) |
| Median OS (Overall Survival) |
Not reached |
| Median DoR (Duration of Response) |
11.40 M |
|
Disease Control Rate (PR + SD > 4 months) |
89.5% |
| 一級終點 | Plinabulin + Pembrolizumab + Docetaxel (n=19) |
| 經核實的總體有效率 (RECISt 1.1) | 21.1% |
| 二級終點 | |
| 中位無進展生存期 (RECISt 1.1) | 8.63百萬 (600百萬 無進展生存率: 67.1%; 1200百萬 無進展生存率: 49.2%) |
| 中位OS (總體生存期) |
未達到 |
| 中位持續時間 (回應持續時間) |
11.40 M |
| 疾病控制率 (PR + SD > 4個月) |
89.5% |
- The combination was well tolerated. 6% of patients experienced grade 3 or higher treatment-related adverse effects. There were no treatment-related deaths.
- 該組合療法耐受良好。6%的患者經歷了3級或更高級別與治療相關的不良反應。沒有與治療相關的死亡。
"Plinabulin is a potent inducer of dendritic cell or DC maturation that leads to T cell activation. DC is the most potent antigen presenting cell (APC). This unique mechanism of action reinforces anti-tumor immune response with the potential to overcome acquired ICI resistance, which may derive from APC pathway mutation or T cell exhaustion. Compared to historical controls of 3-4 months of median PFS2, this study's early efficacy data doubled median PFS to 8.6 months, with an impressive disease control rate of almost 90%, which is encouraging and clinically meaningful for this severe unmet need," said Dr. Mengzhao Wang, principal investigator at Peking Union Medical College Hospital.
「Plinabulin是一種能夠有效誘導樹突狀細胞(DC)成熟並激活T細胞的藥物。DC是最強效的抗原呈遞細胞(APC)。這一獨特的作用機制強化了抗腫瘤免疫反應的能力,有潛力克服由APC通路突變或T細胞功能耗竭引起的繼發性免疫治療耐藥性。與歷史對照組3-4個月中位PFS2相比,該研究的早期療效數據將中位PFS延長爲8.6個月,疾病控制率幾乎達到90%,對於這一嚴重未滿足需求的治療手段來說,這是令人鼓舞且具有臨床意義的。」 北京協和醫學院醫院的主要研究員王夢照博士表示。
ESMO Congress 2024 (1330P): Phase 2 Study of Pembrolizumab plus Plinabulin and Docetaxel for Patients (pts) with Metastatic NSCLC after Failure on First-line Immune Checkpoint Inhibitor Alone or Combination Therapy: Initial Efficacy and Safety Results on Immune Re-sensitization
ESMO 2024年會(1330P):Pembrolizumab與Plinabulin和Docetaxel聯合治療轉移性非小細胞肺癌患者的II期研究,治療失效於一線免疫檢查點抑制劑單獨或聯合療法的初步療效和安全性結果:免疫復敏的初步療效和安全性結果。
- Presenter: Yan Xu, Peking Union Medical College Hospital, Beijing, China
- Poster Session: NSCLC, metastatic
- 主持人:Yan Xu,北京協和醫學院附屬醫院,中國
- 海報會議:轉移性非小細胞肺癌
References:
參考文獻:
- Schoenfeld et al. 2022, Lancet Oncology 23:279-291
- TROPION Lung-01:
- Schoenfeld等人,2022年,全球性醫學期刊《腫瘤學報》,23:279-291
- TROPION Lung-01:
About Plinabulin
關於Plinabulin
Plinabulin is a novel first-in-class dendritic cell maturation therapeutic with durable anti-cancer benefit observed across multiple clinical studies. As a reversible binder at a distinct tubulin pocket, plinabulin does not change tubulin dynamics or antagonize tubulin stabilizing agents, such as docetaxel, which contributes to its differentiated activity and tolerability compared to other tubulin binders. In addition, plinabulin significantly reduces chemotherapy induced neutropenia and could thereby increase docetaxel tolerability. Over 700 patients have been treated with plinabulin with good tolerability.
Plinabulin是一種新型的樹突狀細胞成熟治療藥物,經過多個臨床研究觀察到具有持久的抗癌益處。作爲在特定微管口袋可逆地結合的藥物,plinabulin不會改變微管動力學,也不會對微管穩定劑如紫杉醇等產生拮抗作用,這與其他微管結合劑相比,有不同的活性和耐受性。此外,plinabulin顯著減少化療誘導的中性粒細胞減少症,從而可能增加紫杉醇的耐受性。已有700多名患者接受了plinabulin治療,具有良好的耐受性。
About KeyPelms-004 or 303 Study
關於KeyPelms-004或303研究
303 Study is an open-label, single-arm Phase 2 Study of Plinabulin plus docetaxel and pembrolizumab for previously treated patients with metastatic NSCLC and progressive disease after anti-PD-(L)1 inhibitor alone or in combination with platinum-doublet chemotherapy. This study evaluates the efficacy and safety of this triple combination and is being conducted at Peking Union Medical College Hospital, Beijing, China. The regimen includes Pembrolizumab 200 mg IV every 3 weeks (Q3W) on Day 1, Docetaxel 75 mg/m2 IV Q3W on Day 1 and Plinabulin 30mg/m2 IV Q3W on Day 1 in a 21-day cycle. The primary endpoint is investigator-based ORR (RECIST 1.1). The secondary endpoints include PFS, OS, DoR, and safety. The study intends to enroll 47 patients with a formal interim analysis of 19 patients enrolled. The study is funded by Merck's Investigator Studies Program with provision of study drug and financial support.
303研究是一項開放標籤、單臂Ⅱ期研究,研究對象是曾接受過抗PD-(L)1單藥或聯合鉑雙t化療治療後,出現轉移性非小細胞肺癌並出現疾病進展的患者。這個研究評估了plinabulin聯合紫杉醇和帕博利珠單抗的三聯療法的療效和安全性,研究地點在中國北京的北京協和醫學院附屬醫院。方案包括帕博利珠單抗每3周200毫克靜脈注射(Q3W)第1天,紫杉醇每2平方米靜脈注射75毫克(Q3W)第1天,plinabulin每2平方米靜脈注射30毫克(Q3W)第1天,21天爲一個療程。主要終點是基於研究者評估的總體有效率(RECISt 1.1)。次要終點包括無進展生存期(PFS)、總生存期(OS)、反應持續時間(DoR)和安全性。該研究擬招募47名患者,並在招募19名患者後進行正式中期分析。這項研究由默沙東的研究員研究項目資助,提供研究藥物和財務支持。
About BeyondSpring
關於萬春醫藥
BeyondSpring is a global clinical-stage biopharmaceutical company developing innovative therapies to improve clinical outcomes for patients with high unmet medical needs. The Company is advancing its first-in-class lead asset, Plinabulin, a potent inducer of dendritic cell maturation, in late-stage clinical development as a direct anti-cancer agent in NSCLC and a variety of cancer indications. BeyondSpring's pipeline also includes three preclinical immuno-oncology assets. Additionally, BeyondSpring is an equity owner of SEED Therapeutics, Inc which is a pioneer in Target Protein Degradation technology and its application in innovative drug development. Learn more by visiting .
萬春醫藥是一家全球臨床階段的生物製藥公司,致力於開發創新療法,改善對臨床需求高但尚未滿足的患者的臨床結果。該公司正在推進其首個一類新藥鉑林,作爲一種直接的抗癌劑,在非小細胞肺癌和多種癌症適應症中作爲強效的樹突狀細胞成熟誘導劑的後期臨床開發。萬春醫藥的創新藥物管線還包括三個臨床前的免疫腫瘤學資產。此外,萬春醫藥是SEED Therapeutics, Inc 的股權擁有者, SEED Therapeutics是目標蛋白降解技術和其在創新藥物開發中的應用方面的先驅者。了解更多信息,請訪問。
Investor Contact:
投資者聯繫人:
IR@beyondspringpharma.com
IR@beyondspringpharma.com
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媒體聯繫人:
PR@beyondspringpharma.com
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譯文內容由第三人軟體翻譯。
