PO.CTP01.03 · 进行中的临床试验

AACR Adaptive Biomarker-Driven Organ Preservation Trial in GE Adenocarcinomas (AACR-ADOPT-GEA)

海报缩略图:AACR Adaptive Biomarker-Driven Organ Preservation Trial in GE Adenocarcinomas (AACR-ADOPT-GEA)
编号 CT223 展板 18 时间 4/21 09:00–12:00 区域 Section 51 主讲 Ronan McLaughlin, MS
分会场 Phase II and Phase III Clinical Trials in Progress
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作者与单位

Elena Elimova1, Jaffer Ajani2, Samuel J. Klempner3, Kurt Schalper4, Zev Wainberg5, Yuan Ying2, Jan D. Baranski6, Scott Boerner4, Sienna M. Durbin7, Denise Gallagher6, Huh Won Jae4, Ronan A. McLaughlin1, Matthew R. Strickland3, Eric H. Rubin6, Lillian L. Siu1, Timothy A. Yap2, Patricia LoRusso4

1UHN Princess Margaret Cancer Centre, Toronto, ON, Canada,2University of Texas MD Anderson Cancer Center, Heuston, TX,3Massachusetts General Hospital, Boston, MA,4Yale School of Medicine, New Haven, CT,5University of California, Los Angeles, CA,6American Association for Cancer Research, Philadelphia, PA,7Massachusetts General Brigham Cancer Institute, Boston, MA

摘要 Abstract

Background: Localized gastroesophageal adenocarcinomas (GEA) are molecularly heterogeneous and often exhibit limited sensitivity to current systemic therapies. The 5-year survival rate with standard perioperative chemotherapy is ~40%, and only ~15% of patients achieve a pathologic complete response (pCR). AACR-ADOPT-GEA was designed to overcome these barriers and assess, for the first time in GEA, if organ preservation is achievable by delivering biomarker-matched targeted therapies to patients. Notably, several targetable biomarkers - HER2, MSI, EBV, and CLDN18.2 - have demonstrated therapeutic relevance in metastatic GEA. In AACR-ADOPT-GEA, we hypothesize that in biomarker-selected cohorts, addition of a targeted agent for treatment of locally advanced GEA can increase pCR rates and enable 5-year organ preservation in approximately 20% of patients. Methods: AACR-ADOPT-GEA (NCT07290985) is a prospective, multi-center, two-stage adaptive platform trial. Eligible participants include patients diagnosed with resectable (stage II or higher [≥T2 N0-3 M0 or T0-4a N1-3 M0] as per NCCN guidelines) adenocarcinoma of the stomach, esophagus, or gastroesophageal junction, have an ECOG performance score of 0-1, adequate organ function, to be a candidate for curative surgery, and test positive for one of the targetable tumor biomarkers. Participants may receive one cycle of FLOT/mFOLFOX during the screening period. Following screening and biomarker confirmation, participants will be enrolled into a corresponding sub-study and treated with a biomarker-specific targeted agent in addition to mFOLFOX plus an immune checkpoint inhibitor (ICI) for 4 months. Pre-operative treatment will be followed by surgery and an 8-month post-operative treatment consisting of the targeted agent and an ICI. This two-stage study is designed to assess pCR rates for each targeted regimen with an initial cohort of up to 24 patients in Stage I. An interim analysis will be conducted after enrollment of 12 evaluable patients in each sub-study to drop futile regimens. Those regimens achieving a pCR rate ≥25% (6 out of 24 patients) will graduate and proceed to Stage II where a machine learning predictive model, utilizing clinical data, tumor biology, and serial ctDNA dynamics will be developed to establish a signature predictive of pCR. In stage II, 97 patients will be enrolled to achieve 80% power to test the area under the ROC curve of 0.80 against 0.65 to predict pCR at a two-sided significance level of 0.05. During this stage, patients with a complete clinical/radiological response and predicted pCR after 4 months of treatment may omit surgery and continue on 8 months of maintenance therapy with protocol-specified surveillance. Those with residual disease will undergo surgical resection followed by postoperative therapy. Importantly, access to pre- and post-treatment tissue samples in Stage II will enable multiomic analyses for response/resistance biomarkers to catalyze future work in this area.
利益披露 Disclosure
E. Elimova, BMS ), Other, Consulting. Zymeworks ), Other, Consulting. Adaptimuune Consulting. Astellas Other, Consulting. Beigene Other, Consulting. Viracta Tx Other, Consulting. Novartis Other, Consulting. Jazz ), Other, Consulting Steering committee. Natera Other, Consulting. Abbvie Other, Consulting. Daiichi-Sankyo Other, Consulting. Roche Consulting. Amgen ), Other, Consulting. Astra Zeneca ), Other, Consulting Steering Committee. Bold therapeutics ). Arcus Biosciences ). Merck Other, Family memeber. J. Ajani, Jazz Pharmaceuticals, Zymeworks, and BeOne Medicines Other, Consultant. S. J. Klempner, Merck Other, consulting. Astellas Other, Consulting. Daiichi-Sankyo Other, Consulting. Natera Other, Consulting. Novartis Other, Consulting. AstraZeneca Other, Consulting. Mersana Other, consulting. Beigene Other, Consulting. Gilead Other, Consulting. Elevation Oncology Other, Consulting. EsoBiotec Other, Consulting. Eisai Other, Consulting. Boehringer-Ingelheim Other, Consulting. I-Mab Other, Consulting. Signet Therapeutics Other, Consulting. Torrey Coast Foundation, the Degregorio Foundation, the Gastric Cancer Foundation, Debbie’s Dream Foundation, NIH/NCI, StandUp2Cancer, AACR. ). K. Schalper, None. Z. Wainberg, Alligator, Amgen, Arcus, AstraZeneca, Bayer, Bristol Myers Squibb, Ipsen, Janssen, Lilly, Merck, Merck KGaA, Novartis, and Pfizer Other, Consultant or advisor. Merck, Novartis, and Plexxikon ). Amgen, Lilly, and Merck Travel. Y. Ying, AbbVie, Affinixttx, Aktis Oncology, Amgen, Astellas, Avance, BioNTech, Blueprint, BrainChildBio, Bristol Myers Squibb, Cassava Sciences, Century Therapeutics, Cogent,CoRegen, GT Medical, Kyowa Kirin Other, Dr. Yuan served as a statistical consultant to these companies. J. D. Baranski, None.. S. Boerner, None.. S. M. Durbin, None.. D. Gallagher, None.. H. Won Jae, None.. R. A. McLaughlin, None. M. R. Strickland, Astellas Pharma Other, Honoraria. Bristol Myers Squibb, Sedgwick Claims Management, Astellas Pharma, Bayer, encapsulate Other, Consulting or Advisory Role. UpToDate Other, Patents, Royalties, Other Intellectual Property: UpToDate Editor & Author. E. H. Rubin, Modex, PAQ, Eikon, Nurix, TCG Soleil, Generate, and Mestag. Other, Consultant (independent contractor) for these companies. L. L. Siu, Merck, Pfizer, AstraZeneca, Roche, GSK, Bayer, Voronoi, Arvinas, Marengo, Daiichi Sankyo, Amgen, LTZ Therapeutics, Tubulis, Incyte, EMD Serono, Accent Other, Consultant/Advisory role (self):. Merck, Novartis, Bristol-Myers Squibb, Pfizer, Boerhinger-Ingelheim, GSK, Roche/Genentech, AstraZeneca, Bayer, Abbvie, Amgen, EMD Serono, Daiichi Sankyo, Gilead, Marengo, Incyte ). Treadwell Therapeutics Other, Leadership role (spouse). T. A. Yap, Several Other, Dr. Yap reports other support from University of Texas MD Anderson Cancer Center; as Vice President, Head Clinical Development in the Therapeutics Discovery Division, which has a commercial interest in DNA damage response (DDR) and other inhibitors(IACS30380/ ART0380 was licensed to Artios), grants and personal fees from Acrivon, grants and personal fees from Artios, grants and personal fee. P. LoRusso, 1. AbbVie: Advisory Board Member (2018-2019) 2. Roche-Genentech: imCORE Alliance (2016-2019) 3. Takeda: Advisory Board (2017-2020; 2023-2024) 4. SOTIO: Consultant (2018-2019); IDMC (2023) 5. Agenus: Other, Advisory boards for these companies.

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