- Shatsky, Rebecca A;
- Trivedi, Meghna S;
- Yau, Christina;
- Nanda, Rita;
- Rugo, Hope S;
- Davidian, Marie;
- Tsiatis, Butch;
- Wallace, Anne M;
- Chien, A Jo;
- Stringer-Reasor, Erica;
- Boughey, Judy C;
- Omene, Coral;
- Rozenblit, Mariya;
- Kalinsky, Kevin;
- Elias, Anthony D;
- Vaklavas, Christos;
- Beckwith, Heather;
- Williams, Nicole;
- Arora, Mili;
- Nangia, Chaitali;
- Roussos Torres, Evanthia T;
- Thomas, Brittani;
- Albain, Kathy S;
- Clark, Amy S;
- Falkson, Carla;
- Hershman, Dawn L;
- Isaacs, Claudine;
- Thomas, Alexandra;
- Tseng, Jennifer;
- Sanford, Amy;
- Yeung, Kay;
- Boles, Sarah;
- Chen, Yunni Yi;
- Huppert, Laura;
- Jahan, Nusrat;
- Parker, Catherine;
- Giridhar, Karthik;
- Howard, Frederick M;
- Blackwood, M Michele;
- Sanft, Tara;
- Li, Wen;
- Onishi, Natsuko;
- Asare, Adam L;
- Beineke, Philip;
- Norwood, Peter;
- Brown-Swigart, Lamorna;
- Hirst, Gillian L;
- Matthews, Jeffrey B;
- Moore, Brian;
- Symmans, W Fraser;
- Price, Elissa;
- Heditsian, Diane;
- LeStage, Barbara;
- Perlmutter, Jane;
- Pohlmann, Paula;
- DeMichele, Angela;
- Yee, Douglas;
- van ’t Veer, Laura J;
- Hylton, Nola M;
- Esserman, Laura J
Sequential adaptive trial designs can help accomplish the goals of personalized medicine, optimizing outcomes and avoiding unnecessary toxicity. Here we describe the results of incorporating a promising antibody-drug conjugate, datopotamab-deruxtecan (Dato-DXd) in combination with programmed cell death-ligand 1 inhibitor, durvalumab, as the first sequence of therapy in the I-SPY2.2 phase 2 neoadjuvant sequential multiple assignment randomization trial for high-risk stage 2/3 breast cancer. The trial includes three blocks of treatment, with initial randomization to different experimental agent(s) (block A), followed by a taxane-based regimen tailored to tumor subtype (block B), followed by doxorubicin-cyclophosphamide (block C). Subtype-specific algorithms based on magnetic resonance imaging volume change and core biopsy guide treatment redirection after each block, including the option of early surgical resection in patients predicted to have a high likelihood of pathologic complete response, which is the primary endpoint assessed when resection occurs. There are two primary efficacy analyses: after block A and across all blocks for six prespecified HER2-negative subtypes (defined by hormone receptor status and/or response-predictive subtypes). In total, 106 patients were treated with Dato-DXd/durvalumab in block A. In the immune-positive subtype, Dato-DXd/durvalumab exceeded the prespecified threshold for success (graduated) after block A; and across all blocks, pathologic complete response rates were equivalent to the rate expected for the standard of care (79%), but 54% achieved that result after Dato-DXd/durvalumab alone (block A) and 92% without doxorubicin-cyclophosphamide (after blocks A + B). The treatment strategy across all blocks graduated in the hormone-negative/immune-negative subtype. No new toxicities were observed. Stomatitis was the most common side effect in block A. No patients receiving block A treatment alone had adrenal insufficiency. Dato-DXd/durvalumab is a promising therapy combination that can eliminate standard chemotherapy in many patients, particularly the immune-positive subtype.ClinicalTrials.gov registration: NCT01042379 .
