ITeos Therapeutics Presents Interim A2A-005 Clinical Trial Data, Translational, and Preclinical Data From Inupadenant at ESMO Immuno-Oncology Congress
ITeos Therapeutics Presents Interim A2A-005 Clinical Trial Data, Translational, and Preclinical Data From Inupadenant at ESMO Immuno-Oncology Congress
- Inupadenant + carboplatin/pemetrexed in Phase 2 A2A-005 trial demonstrated a 63.9% overall response rate (ORR) and a median PFS of 7.7 months for all evaluable patients across the cohorts
- Recommended Phase 2 dose (RP2D) of inupadenant 80mg + carboplatin/pemetrexed demonstrated 73.3% ORR, with 64.6% of patients achieving landmark 6-month PFS
- Inupadenant + carboplatin/pemetrexed safety profile was manageable and tolerable, with no dose-dependent toxicity observed
- Inupadenant deprioritized to focus resources on other programs
- 在A2A-005 II期臨床試驗中,inupadenant與鉑金/pemetrexed聯合使用顯示出63.9%的總體反應率(ORR),並且在所有可評估患者中,平均無進展生存期(PFS)爲7.7個月
- inupadenant 80mg與鉑金/pemetrexed聯合使用的推薦II期劑量(RP2D)顯示出73.3%的ORR,其中64.6%的患者達到了標誌性6個月的PFS
- inupadenant與鉑金/pemetrexed的安全性可控且耐受性良好,沒有觀察到劑量依賴性毒性
- inupadenant被降級優先級,以集中資源於其他項目
WATERTOWN, Mass. and GOSSELIES, Belgium, Dec. 12, 2024 (GLOBE NEWSWIRE) -- iTeos Therapeutics, Inc. (Nasdaq: ITOS), a clinical-stage biopharmaceutical company pioneering the discovery and development of a new generation of immuno-oncology therapeutics for patients, today announced the presentation of clinical, translational, and preclinical data from its adenosine A2A receptor (A2AR) antagonist program, inupadenant, including interim data from the dose escalation portion of A2A-005, the Phase 2 trial assessing inupadenant and platinum-doublet chemotherapy in post-immunotherapy metastatic non-small cell lung cancer (NSCLC) patients, at the European Society for Medical Oncology Immuno-Oncology (ESMO IO) Congress 2024.
馬薩諸塞州沃特敦和比利時戈塞利耶,2024年12月12日(GLOBE NEWSWIRE)—— iTeos Therapeutics, Inc.(納斯達克代碼:ITOS),一家臨床階段的生物製藥公司,開創了針對患者的新一代免疫腫瘤治療藥物的發現和開發,今天宣佈了其腺苷A2A受體(A2AR)拮抗劑項目inupadenant的臨床、轉化和前臨床數據的展示,包括A2A-005 II期試驗中inupadenant與鉑金雙藥化療在接受免疫治療的轉移性非小細胞肺癌(NSCLC)患者中的劑量遞增部分的中期數據,在2024年歐洲醫學腫瘤學會免疫腫瘤學(ESMO IO)大會上進行了展示。
"We believe our presentations at ESMO IO on the adenosine pathway demonstrate the strong efforts our research and discovery team have put into understanding this immunosuppressive mechanism," said Michel Detheux, Ph.D., president and chief executive officer of iTeos. "While the initial signal for inupadenant's RP2D in the A2A-005 trial compared to chemotherapy alone is encouraging and supports its differentiated, insurmountable profile, we as well as our scientific and clinical advisory boards believe it does not meet sufficient level of clinical activity to warrant further investment. We remain committed to focusing our resources on developing differentiated, first- or best-in-class therapies and look forward to providing updates on our pipeline in 2025."
「我們相信我們在ESMO IO關於腺苷通路的報告展示了我們的研究和發現團隊在理解這種免疫抑制機制方面所做的努力,」iTeos的總裁兼首席執行官Michel Detheux博士表示。「雖然在A2A-005試驗中,與單獨化療相比,inupadenant的RP2D初始信號令人鼓舞,並支持其差異化的、不容忽視的特徵,但我們和我們的科學及臨床顧問委員會認爲,其臨床活動水平尚不足以進一步投資。我們仍然致力於集中資源開發差異化的第一類或最佳類療法,並期待在2025年提供我們研發管線的更新。」
Mini Oral Sessions
Title: Inupadenant Combined with Chemotherapy in Patients with Non-Squamous NSCLC Progressing On or After Immune Checkpoint Inhibitor Therapy: Results from Dose-Finding Part of the A2A-005 Trial
Summary: As of the October 29, 2024 data cutoff, the topline data from the dose escalation portion of A2A-005 presented at the ESMO IO Congress were based on 36 patients eligible for safety and efficacy evaluation. Patients received inupadenant at 40mg, 60mg, or 80mg twice daily (BID) in combination with carboplatin/pemetrexed. All patients had a minimum follow-up of 6 months. Patient baseline characteristics were balanced across arms, with a slight imbalance of more patients with brain metastases in the 40mg and 80mg cohorts and ECOG status 0 favoring the 80mg cohort.
迷你口腔會議
標題:在接受免疫檢查點抑制劑治療後惡化的非鱗狀非小細胞肺癌患者中使用Inupadenant聯合化療:A2A-005試驗的劑量發現部分結果
摘要:截至2024年10月29日的數據截止,A2A-005劑量遞增部分在ESMO IO大會上報告的頂線數據基於36名符合安全性和療效評估的患者。患者每天兩次(BID)接受40mg、60mg或80mg的Inupadenant與卡鉑/培美曲塞聯合治療。所有患者的最短隨訪時間爲6個月。患者的基線特徵在各組之間均衡,但在40mg和80mg組中腦轉移患者略多,且ECOG狀態0偏向80mg組。
- The primary endpoint of the safety of inupadenant in combination with carboplatin/pemetrexed was observed to be manageable and tolerable, with no dose dependent toxicities.
- The secondary endpoint of ORR was 63.9% across all patients (53.3% at 40mg, 66.7% at 60mg, and 73.3% at 80mg).
- The secondary endpoint of mPFS was 7.7 months across all patients (5.6 months at 40mg and 6.6 months at 60mg; mPFS remains unreached at 80mg).
- The exploratory biomarker of CXCL13, a B-cell chemokine and lymphoid structure marker associated with clinical activity, was observed to be restored by inupadenant after depletion by chemotherapy, with quicker restoration kinetics in patients with PFS greater than 6 months.
- As of the data cutoff, 8 patients remained on treatment (1 at 40mg, 1 at 60mg, and 6 at 80mg). The median follow-up was 9.7 months (10.6 months at 40mg, 13.1 months at 60mg, and 8.2 months at 80mg).
- Inupadenant與卡鉑/培美曲塞聯合治療的主要終點安全性被觀察到是可控和耐受的,未觀察到劑量依賴性毒性。
- 客觀緩解率(ORR)的次要終點在所有患者中爲63.9%(40mg爲53.3%,60mg爲66.7%,80mg爲73.3%)。
- 次要終點中的中位無進展生存期(mPFS)在所有患者中爲7.7個月(40mg爲5.6個月,60mg爲6.6個月;80mg的mPFS尚未達到)。
- CXCL13的探索性生物標誌物,這是一種與臨床活動相關的b細胞趨化因子和淋巴結構標記,在化療消耗後被inupadenant恢復,且在無進展生存期超過6個月的患者中恢復動力學更快。
- 截至數據截止時,8名患者仍在接受治療(1名在40mg,1名在60mg,6名在80mg)。中位隨訪爲9.7個月(40mg時爲10.6個月,60mg時爲13.1個月,80mg時爲8.2個月)。
| Response Measure | Inupadenant 40mg + carboplatin / pemetrexed BID | Inupadenant 60mg + carboplatin / pemetrexed BID | Inupadenant 80mg + carboplatin / pemetrexed BID | Overall | ||||
| (N=15) | (N=6) | (N=15) | (N=36) | |||||
| ORR, % | 53.3% | 66.7% | 73.3% | 63.9% | ||||
| n (95% CI) |
n=8 (26.6–78.7) |
n=6 (22.3–95.7) |
n=15 (44.9–92.2) |
n=36 (46.2–79.2) |
||||
| Complete response, n (%) | 0 | 0 | 2 (13.3%) | 2 (5.6%) | ||||
| Partial response, n (%) | 8 (53.3%) | 4 (66.7%) | 9 (60.0%) | 21 (58.3%) | ||||
| Stable disease, n (%) | 7 (46.7%) | 1 (16.7%) | 3 (20.0%) | 11 (30.6%) | ||||
| Progressive disease, n (%) | 0 | 0 | 1 (6.7%) | 1 (2.8%) | ||||
| Not evaluable/no assessment, n (%) | 0 | 1 (16.7%) | 0 | 1 (2.8%) | ||||
| mPFS, months | 5.6 | 6.6 | NC | 7.7 | ||||
| Event n (%) (95% CI) |
13 (86.7%) (4.1-8.3) |
5 (83.3%) (0.4-NC) |
6 (40.0%) (4.9-NC) |
24 (66.7%) (5.1-11.0) |
||||
| Landmark 6-Month PFS % |
46.7% (21.2-68.7) |
50.0% (11.1-80.4) |
64.6% (34.7-83.5) |
54.5% (36.8-69.1) |
||||
| 反應測量 | Inupadenant 40mg + 卡鉑 / 培美曲塞 BID | Inupadenant 60mg + 卡鉑 / 培美曲塞 BID | Inupadenant 80mg + 卡鉑 / 培美曲塞 BID | 總體 | ||||
| (N=15) | (N=6) | (N=15) | (N=36) | |||||
| ORR, % | 53.3% | 66.7% | 73.3% | 63.9% | ||||
| n (95% 置信區間) |
樣本量=8 (26.6–78.7) |
樣本量=6 (22.3–95.7) |
樣本量=15 (44.9–92.2) |
n=36 (46.2–79.2) |
||||
| 完全響應,n (%) | 0 | 0 | 2 (13.3%) | 2 (5.6%) | ||||
| 部分反應,n (%) | 8 (53.3%) | 4 (66.7%) | 9 (60.0%) | 21 (58.3%) | ||||
| 穩定病情,n (%) | 7 (46.7%) | 1 (16.7%) | 3 (20.0%) | 11 (30.6%) | ||||
| 進行性疾病,n (%) | 0 | 0 | 1 (6.7%) | 1 (2.8%) | ||||
| 不可評估/無評估,n (%) | 0 | 1 (16.7%) | 0 | 1 (2.8%) | ||||
| 無進展生存期,單位:月 | 5.6 | 6.6 | 北卡羅來納州 | 7.7 | ||||
| 事件 n (%) (95% 置信區間) |
13 (86.7%) (4.1-8.3) |
5 (83.3%) (0.4-NC) |
6 (40.0%) (4.9-NC) |
24 (66.7%) (5.1-11.0) |
||||
| 里程碑 6 個月 PFS % | 46.7% (21.2-68.7) |
50.0% (11.1-80.4) |
64.6% (34.7-83.5) |
54.5% (36.8-69.1) |
||||
CI, confidence interval; NC, not calculable
CI,置信區間;NC,不可計算
Title: The A2AR Antagonist Inupadenant Promotes Humoral Responses in Patients
Summary: Based on monotherapy clinical and translational data, inupadenant demonstrated modulation of humoral responses in patient blood and tumor tissue, supporting our previous finding that expression of antibody-secreting cells (ASCs) in tumor tissue is associated with non-progression in patient disease. Furthermore, CXCL13 expression, a protein involved in immune cell recruitment, activation, and adaptive immune response regulation, increased in patients treated with inupadenant and more rapidly and extensively in non-progressors compared to progressors. These findings confirm inupadenant plays a key role in B cell maturation restoration and may play a substantial role in delaying progression in end-stage patients.
標題:A2AR拮抗劑Inupadenant促進患者的體液免疫反應
摘要:根據單藥臨床和轉化數據,inupadenant顯示了對患者血液和腫瘤組織的體液反應的調節,支持我們之前的發現:腫瘤組織中抗體分泌細胞(ASCs)的表達與患者疾病的非進展相關。此外,CXCL13的表達,作爲參與免疫細胞招募、激活和適應性免疫反應調節的蛋白質,在接受inupadenant治療的患者中增加,並且在非進展患者中相較進展患者更快速和廣泛。這些發現確認inupadenant在B細胞成熟恢復中發揮關鍵作用,並可能在延緩末期患者疾病進展中發揮重要作用。
Poster Sessions
Title: The A2AR Antagonist Inupadenant Promotes Humoral Responses in Preclinical Models
Summary: In preclinical models, inupadenant counteracted the A2AR-mediated inhibition of B cell maturation into ASCs and immunoglobulin production in both in vitro and ex vivo systems by modulating B cells at the level of the germinal center (GC). These findings suggest that inupadenant restores or even enhances B cell maturation towards ASCs and GC reactions in both secondary lymphoid organs as well as the tumor in the presence of A2AR signaling. Furthermore, this process is essential for producing high-affinity antibodies and potentially for sustained anti-tumor immunity.
海報會議
標題:A2AR拮抗劑inupadenant在臨床前模型中促進體液反應
摘要:在臨床前模型中,inupadenant抵消了A2AR介導的B細胞向ASCs和免疫球蛋白生成成熟的抑制作用,在體外和體外實驗中通過調節B細胞在生髮中心(GC)水平的作用。這些發現表明,inupadenant恢復甚至增強了B細胞朝向ASCs和GC反應的成熟,無論是在二級淋巴器官還是在腫瘤中存在A2AR信號的情況下。此外,這個過程對於產生高親和力抗體和潛在的持續抗腫瘤免疫非常重要。
Title: A Novel Tumor Adenosine Signature to Guide Indication Selection for Adenosine Pathway inhibitor
Summary: Based on the spatial quantification of adenosine in human tumors, we developed the first adenosine gene signature, demonstrating its potential for indication selection. This new signature, derived from 249 differentially expressed genes (DEGs) associated with metabolism and immune activation, showed high predictive power across tumor types. Furthermore, the adenosine signature was higher in tumors compared to healthy tissue and exhibited variable expression and prognostic value across tumor subtypes. These findings suggest that the adenosine signature represents a powerful tool for prioritizing tumor types which may benefit most from adenosine-targeting therapies and for understanding the mechanisms of adenosine-mediated immunosuppression.
標題:一種新型腫瘤腺苷特徵指導腺苷通路抑制劑的適應症選擇
摘要:基於對人類腫瘤中腺苷的空間量化,我們開發了第一個腺苷基因特徵,展示了其在適應症選擇中的潛力。這種新特徵源於與代謝和免疫激活相關的249個差異表達基因(DEGs),在各種腫瘤類型中顯示出高預測能力。此外,腺苷特徵在腫瘤中比在健康組織中的水平更高,並且在不同的腫瘤亞型中表現出變量表達和預後價值。這些發現表明,腺苷特徵代表了一種強有力的工具,可以優先考慮可能最受益於腺苷靶向療法的腫瘤類型,並幫助理解腺苷介導的免疫抑制機制。
About iTeos Therapeutics, Inc.
iTeos Therapeutics is a clinical-stage biopharmaceutical company pioneering the discovery and development of a new generation of immuno-oncology therapeutics for patients. iTeos Therapeutics leverages its deep understanding of tumor immunology and immunosuppressive pathways to design novel product candidates with the potential to restore the immune response against cancer. The Company's innovative pipeline includes three clinical-stage programs targeting novel, validated immunosuppressive pathways designed with optimized pharmacologic properties for improved clinical outcomes, including the TIGIT/CD226 axis and the adenosine pathway. iTeos Therapeutics is headquartered in Watertown, MA with a research center in Gosselies, Belgium.
關於iTeos Therapeutics, Inc.
iTeos Therapeutics是一家臨床階段的生物製藥公司,致力於開發新一代免疫腫瘤治療藥物,爲患者提供創新選擇。iTeos Therapeutics憑藉對腫瘤免疫學和免疫抑制途徑的深入理解,設計出具有恢復對抗癌症免疫應答潛力的新型產品候選藥物。公司的創新管線包括三個臨床階段項目,針對新開發的、經過驗證的免疫抑制途徑,具有優化的藥理特性以改善臨床效果,包括TIGIT/CD226軸和腺苷途徑。iTeos Therapeutics總部位於馬薩諸塞州的沃特敦,並在比利時的戈塞利斯設有研究中心。
About Inupadenant (EOS-850)
Inupadenant is a next-generation small molecule antagonist targeting adenosine A2A receptor (A2AR), the primary receptor on immune cells whose activation by adenosine suppresses innate and adaptive immune cell responses leading to inhibition of antitumor responses. Optimized for potency, high selectivity of A2AR, and activity at high adenosine concentrations in solid tumors, inupadenant is uniquely designed with its insurmountable profile to inhibit the ATP-adenosine pathway and has the potential for enhanced antitumor activity as compared to other A2AR antagonists in clinical development. The therapeutic candidate is in Phase 2 development.
關於Inupadenant(柚子-850)
Inupadenant是一種新一代小分子拮抗劑,靶向腺苷A2A受體(A2AR),該受體是免疫細胞上的主要受體,腺苷激活它會抑制先天性和適應性免疫細胞的應答,從而抑制抗腫瘤應答。Inupadenant經過優化,具有強效、高選擇性A2AR特性,並在固體腫瘤中能夠在高濃度腺苷下發揮活性,獨特設計的不可逾越特性使其能夠抑制ATP-腺苷途徑,並有潛力相比於其他臨床開發中的A2AR拮抗劑增強抗腫瘤活性。該治療候選藥物目前處於第二階段開發中。
Internet Posting of Information
iTeos routinely posts information that may be important to investors in the 'Investors' section of its website at . The Company encourages investors and potential investors to consult our website regularly for important information about iTeos.
信息的互聯網發佈
iTeos定期在其網站的「投資者」部分發布對投資者可能很重要的信息。該公司鼓勵投資者和潛在投資者定期查看我們的網站,以獲取關於iTeos的重要信息。
Forward-Looking Statements
This press release contains forward-looking statements. Any statements that are not solely statements of historical fact are forward-looking statements. Words such as "believe," "anticipate," "plan," "expect," "will," "may," "intend," "prepare," "look," "potential," "possible" and similar expressions are intended to identify forward-looking statements. These forward-looking statements include statements relating to the potential benefits of inupadenant and the adenosine gene signature; and iTeos remaining committed to focusing its resources on developing differentiated, first- or best-in-class therapies.
前瞻性聲明
本新聞稿包含前瞻性聲明。任何不僅僅是歷史事實的聲明均爲前瞻性聲明。諸如「相信」、「預期」、「計劃」、「期待」、「將」、「可能」、「打算」、「準備」、「關注」、「潛在」、「可能」等類似表達旨在識別前瞻性聲明。這些前瞻性聲明包括與inupadenant和腺苷基因特徵的潛在益處以及iTeos致力於集中資源開發差異化的、首個或最佳療法的聲明。
These forward-looking statements involve risks and uncertainties, many of which are beyond iTeos' control. Actual results could materially differ from those stated or implied by these forward-looking statements as a result of such risks and uncertainties. Known risk factors include the following: success in preclinical testing and early clinical trials does not ensure that later clinical trials will be successful, and early results from a clinical trial do not necessarily predict final results; interim and early data may change as more patient data become available and are subject to audit and verification procedures; the data for our product candidates may not be sufficient for obtaining regulatory approval to move into later stage trials or to commercialize products; iTeos may not be able to execute on its business plans, including meeting its expected or planned regulatory milestones and timelines, research and clinical development plans, and bringing its product candidates to market, for various reasons, some of which may be outside of iTeos' control, including possible limitations of company financial and other resources, manufacturing limitations that may not be anticipated or resolved for in a timely manner, negative developments in the field of immuno-oncology, and regulatory, court or agency decisions such as decisions by the United States Patent and Trademark Office with respect to patents that cover our product candidates; and those risks identified under the heading "Risk Factors" in iTeos' Annual Report on Form 10-Q for the period ended September 30, 2024 filed with the Securities and Exchange Commission (SEC) as well as other SEC filings made by the Company which you are encouraged to review.
這些前瞻性聲明涉及風險和不確定性,許多風險和不確定性超出了iTeos的控制範圍。由於這些風險和不確定性,實際結果可能與這些前瞻性聲明中所述或暗示的結果有重大不同。已知的風險因素包括以下幾點:在臨床前測試和早期臨床試驗中取得成功並不確保後續臨床試驗會成功,早期臨床試驗的結果不一定能預測最終結果;隨着更多患者數據的可用,臨時和早期數據可能會發生變化,並受審核和驗證程序的影響;我們的產品候選者的數據可能不足以獲得監管批准,以進入後期試驗或商品化產品;出於多種原因,包括可能超出iTeos控制範圍的原因,iTeos可能無法執行其業務計劃,包括實現其預計或規劃的監管里程碑和時間表、研究和臨床開發計劃,並將其產品候選者投放市場,其中一些原因可能包括公司財務和其他資源的可能限制、可能無法及時預見或解決的製造業限制、免疫腫瘤領域的負面發展,以及監管、法院或機構的決策,例如美國專利商標局關於涵蓋我們產品候選者的專利的決策;以及在iTeos截至2024年9月30日的10-Q表格年報中「風險因素」章節下識別的風險以及公司向證券交易委員會(SEC)提交的其他SEC文件,鼓勵您查閱。
Any of the foregoing risks could materially and adversely affect iTeos' business, results of operations and the trading price of iTeos' common stock. We caution investors not to place undue reliance on the forward-looking statements contained in this press release. iTeos does not undertake any obligation to publicly update its forward-looking statements other than as required by law.
以上任何風險都可能對iTeos的業務、運營結果以及iTeos普通股的交易價格產生重大不利影響。我們提醒投資者不要過度依賴本新聞稿中包含的前瞻性聲明。iTeos沒有義務公開更新其前瞻性聲明,除非法律要求。
For further information, please contact:
如需更多信息,請聯繫:
Investor Contact:
Carl Mauch
iTeos Therapeutics, Inc.
carl.mauch@iteostherapeutics.com
投資者聯繫人:
卡爾·毛赫
iTeos Therapeutics, Inc.
carl.mauch@iteostherapeutics.com
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media@iteostherapeutics.com
媒體聯繫人:
media@iteostherapeutics.com