Your search keyword '"Asare, Smita"' showing total 134 results

1. Neoadjuvant Trebananib plus Paclitaxel-based Chemotherapy for Stage II/III Breast Cancer in the Adaptively Randomized I-SPY2 Trial-Efficacy and Biomarker Discovery.

Author

Albain, Kathy, Yau, Christina, Petricoin, Emanuel, Wolf, Denise, Lang, Julie, Chien, A, Haddad, Tufia, Forero-Torres, Andres, Wallace, Anne, Kaplan, Henry, Pusztai, Lajos, Euhus, David, Nanda, Rita, Elias, Anthony, Clark, Amy, Godellas, Constantine, Boughey, Judy, Isaacs, Claudine, Tripathy, Debu, Lu, Janice, Yung, Rachel, Gallagher, Rosa, Wulfkuhle, Julia, Brown-Swigart, Lamorna, Krings, Gregor, Chen, Yunn, Potter, David, Stringer-Reasor, Erica, Blair, Sarah, Asare, Smita, Wilson, Amy, Hirst, Gillian, Singhrao, Ruby, Buxton, Meredith, Clennell, Julia, Sanil, Ashish, Berry, Scott, Asare, Adam, Matthews, Jeffrey, DeMichele, Angela, Hylton, Nola, Melisko, Michelle, Perlmutter, Jane, Rugo, Hope, Symmans, W, Vant Veer, Laura, Yee, Douglas, Berry, Donald, and Esserman, Laura

Subjects

Female, Humans, Antineoplastic Combined Chemotherapy Protocols, Bayes Theorem, Breast Neoplasms, Neoadjuvant Therapy, Paclitaxel, Receptor, ErbB-2, Receptor, TIE-2, Recombinant Fusion Proteins, Trastuzumab

Abstract

PURPOSE: The neutralizing peptibody trebananib prevents angiopoietin-1 and angiopoietin-2 from binding with Tie2 receptors, inhibiting angiogenesis and proliferation. Trebananib was combined with paclitaxel±trastuzumab in the I-SPY2 breast cancer trial. PATIENTS AND METHODS: I-SPY2, a phase II neoadjuvant trial, adaptively randomizes patients with high-risk, early-stage breast cancer to one of several experimental therapies or control based on receptor subtypes as defined by hormone receptor (HR) and HER2 status and MammaPrint risk (MP1, MP2). The primary endpoint is pathologic complete response (pCR). A therapy graduates if/when it achieves 85% Bayesian probability of success in a phase III trial within a given subtype. Patients received weekly paclitaxel (plus trastuzumab if HER2-positive) without (control) or with weekly intravenous trebananib, followed by doxorubicin/cyclophosphamide and surgery. Pathway-specific biomarkers were assessed for response prediction. RESULTS: There were 134 participants randomized to trebananib and 133 to control. Although trebananib did not graduate in any signature [phase III probabilities: Hazard ratio (HR)-negative (78%), HR-negative/HER2-positive (74%), HR-negative/HER2-negative (77%), and MP2 (79%)], it demonstrated high probability of superior pCR rates over control (92%-99%) among these subtypes. Trebananib improved 3-year event-free survival (HR 0.67), with no significant increase in adverse events. Activation levels of the Tie2 receptor and downstream signaling partners predicted trebananib response in HER2-positive disease; high expression of a CD8 T-cell gene signature predicted response in HR-negative/HER2-negative disease. CONCLUSIONS: The angiopoietin (Ang)/Tie2 axis inhibitor trebananib combined with standard neoadjuvant therapy increased estimated pCR rates across HR-negative and MP2 subtypes, with probabilities of superiority >90%. Further study of Ang/Tie2 receptor axis inhibitors in validated, biomarker-predicted sensitive subtypes is warranted.

Published

2024

2. Protein signaling and drug target activation signatures to guide therapy prioritization: Therapeutic resistance and sensitivity in the I-SPY 2 Trial

Author

Gallagher, Rosa I, Wulfkuhle, Julia, Wolf, Denise M, Brown-Swigart, Lamorna, Yau, Christina, O’Grady, Nicholas, Basu, Amrita, Lu, Ruixiao, Campbell, Michael J, Magbanua, Mark J, Coppé, Jean-Philippe, Investigators, I-SPY 2, Asare, Smita M, Sit, Laura, Matthews, Jeffrey B, Perlmutter, Jane, Hylton, Nola, Liu, Minetta C, Symmans, W Fraser, Rugo, Hope S, Isaacs, Claudine, DeMichele, Angela M, Yee, Douglas, Pohlmann, Paula R, Hirst, Gillian L, Esserman, Laura J, van ‘t Veer, Laura J, and Petricoin, Emanuel F

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Women's Health, Precision Medicine, Breast Cancer, Genetics, Clinical Research, Cancer, 4.1 Discovery and preclinical testing of markers and technologies, Detection, screening and diagnosis, 5.1 Pharmaceuticals, Development of treatments and therapeutic interventions, Good Health and Well Being, Humans, Drug Resistance, Neoplasm, Neoadjuvant Therapy, Triple Negative Breast Neoplasms, Biomarkers, Gene Expression Profiling, I-SPY 2 Investigators, LCM, RPPA, biomarker, breast cancer, clinical trial, drug target, neoadjuvant, phosphoprotein, protein, resistance, Biomedical and clinical sciences

Abstract

Molecular subtyping of breast cancer is based mostly on HR/HER2 and gene expression-based immune, DNA repair deficiency, and luminal signatures. We extend this description via functional protein pathway activation mapping using pre-treatment, quantitative expression data from 139 proteins/phosphoproteins from 736 patients across 8 treatment arms of the I-SPY 2 Trial (ClinicalTrials.gov: NCT01042379). We identify predictive fit-for-purpose, mechanism-of-action-based signatures and individual predictive protein biomarker candidates by evaluating associations with pathologic complete response. Elevated levels of cyclin D1, estrogen receptor alpha, and androgen receptor S650 associate with non-response and are biomarkers for global resistance. We uncover protein/phosphoprotein-based signatures that can be utilized both for molecularly rationalized therapeutic selection and for response prediction. We introduce a dichotomous HER2 activation response predictive signature for stratifying triple-negative breast cancer patients to either HER2 or immune checkpoint therapy response as a model for how protein activation signatures provide a different lens to view the molecular landscape of breast cancer and synergize with transcriptomic-defined signatures.

Published

2023

3. Clinical significance and biology of circulating tumor DNA in high-risk early-stage HER2-negative breast cancer receiving neoadjuvant chemotherapy

Author

Magbanua, Mark Jesus M, Brown Swigart, Lamorna, Ahmed, Ziad, Sayaman, Rosalyn W, Renner, Derrick, Kalashnikova, Ekaterina, Hirst, Gillian L, Yau, Christina, Wolf, Denise M, Li, Wen, Delson, Amy L, Asare, Smita, Liu, Minetta C, Albain, Kathy, Chien, A Jo, Forero-Torres, Andres, Isaacs, Claudine, Nanda, Rita, Tripathy, Debu, Rodriguez, Angel, Sethi, Himanshu, Aleshin, Alexey, Rabinowitz, Matthew, Perlmutter, Jane, Symmans, W Fraser, Yee, Douglas, Hylton, Nola M, Esserman, Laura J, DeMichele, Angela M, Rugo, Hope S, and van 't Veer, Laura J

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Clinical Trials and Supportive Activities, Human Genome, Cancer, Genetics, Clinical Research, Cancer Genomics, Breast Cancer, Women's Health, Good Health and Well Being, Humans, Female, Breast Neoplasms, Triple Negative Breast Neoplasms, Circulating Tumor DNA, Neoadjuvant Therapy, Clinical Relevance, Antineoplastic Combined Chemotherapy Protocols, Biology, Receptor, ErbB-2, Receptor, erbB-2, circulating tumor DNA, gene expression, neoadjuvant chemotherapy, pathologic complete response, receptor subtype, residual cancer burden, Neurosciences, Oncology & Carcinogenesis, Biochemistry and cell biology, Oncology and carcinogenesis

Abstract

Circulating tumor DNA (ctDNA) analysis may improve early-stage breast cancer treatment via non-invasive tumor burden assessment. To investigate subtype-specific differences in the clinical significance and biology of ctDNA shedding, we perform serial personalized ctDNA analysis in hormone receptor (HR)-positive/HER2-negative breast cancer and triple-negative breast cancer (TNBC) patients receiving neoadjuvant chemotherapy (NAC) in the I-SPY2 trial. ctDNA positivity rates before, during, and after NAC are higher in TNBC than in HR-positive/HER2-negative breast cancer patients. Early clearance of ctDNA 3 weeks after treatment initiation predicts a favorable response to NAC in TNBC only. Whereas ctDNA positivity associates with reduced distant recurrence-free survival in both subtypes. Conversely, ctDNA negativity after NAC correlates with improved outcomes, even in patients with extensive residual cancer. Pretreatment tumor mRNA profiling reveals associations between ctDNA shedding and cell cycle and immune-associated signaling. On the basis of these findings, the I-SPY2 trial will prospectively test ctDNA for utility in redirecting therapy to improve response and prognosis.

Published

2023

4. Safety and efficacy of HSP90 inhibitor ganetespib for neoadjuvant treatment of stage II/III breast cancer.

Author

Lang, Julie E, Forero-Torres, Andres, Yee, Douglas, Yau, Christina, Wolf, Denise, Park, John, Parker, Barbara A, Chien, A Jo, Wallace, Anne M, Murthy, Rashmi, Albain, Kathy S, Ellis, Erin D, Beckwith, Heather, Haley, Barbara B, Elias, Anthony D, Boughey, Judy C, Yung, Rachel L, Isaacs, Claudine, Clark, Amy S, Han, Hyo S, Nanda, Rita, Khan, Qamar J, Edmiston, Kristen K, Stringer-Reasor, Erica, Price, Elissa, Joe, Bonnie, Liu, Minetta C, Brown-Swigart, Lamorna, Petricoin, Emanuel F, Wulfkuhle, Julia D, Buxton, Meredith, Clennell, Julia L, Sanil, Ashish, Berry, Scott, Asare, Smita M, Wilson, Amy, Hirst, Gillian L, Singhrao, Ruby, Asare, Adam L, Matthews, Jeffrey B, Melisko, Michelle, Perlmutter, Jane, Rugo, Hope S, Symmans, W Fraser, van 't Veer, Laura J, Hylton, Nola M, DeMichele, Angela M, Berry, Donald A, and Esserman, Laura J

Subjects

Clinical Research, Clinical Trials and Supportive Activities, Prevention, Breast Cancer, Cancer, 6.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions

Abstract

HSP90 inhibitors destabilize oncoproteins associated with cell cycle, angiogenesis, RAS-MAPK activity, histone modification, kinases and growth factors. We evaluated the HSP90-inhibitor ganetespib in combination with standard chemotherapy in patients with high-risk early-stage breast cancer. I-SPY2 is a multicenter, phase II adaptively randomized neoadjuvant (NAC) clinical trial enrolling patients with stage II-III breast cancer with tumors 2.5 cm or larger on the basis of hormone receptors (HR), HER2 and Mammaprint status. Multiple novel investigational agents plus standard chemotherapy are evaluated in parallel for the primary endpoint of pathologic complete response (pCR). Patients with HER2-negative breast cancer were eligible for randomization to ganetespib from October 2014 to October 2015. Of 233 women included in the final analysis, 140 were randomized to the standard NAC control; 93 were randomized to receive 150 mg/m2 ganetespib every 3 weeks with weekly paclitaxel over 12 weeks, followed by AC. Arms were balanced for hormone receptor status (51-52% HR-positive). Ganetespib did not graduate in any of the biomarker signatures studied before reaching maximum enrollment. Final estimated pCR rates were 26% vs. 18% HER2-negative, 38% vs. 22% HR-negative/HER2-negative, and 15% vs. 14% HR-positive/HER2-negative for ganetespib vs control, respectively. The predicted probability of success in phase 3 testing was 47% HER2-negative, 72% HR-negative/HER2-negative, and 19% HR-positive/HER2-negative. Ganetespib added to standard therapy is unlikely to yield substantially higher pCR rates in HER2-negative breast cancer compared to standard NAC, and neither HSP90 pathway nor replicative stress expression markers predicted response. HSP90 inhibitors remain of limited clinical interest in breast cancer, potentially in other clinical settings such as HER2-positive disease or in combination with anti-PD1 neoadjuvant chemotherapy in triple negative breast cancer.Trial registration: www.clinicaltrials.gov/ct2/show/NCT01042379.

Published

2022

5. Redefining breast cancer subtypes to guide treatment prioritization and maximize response: Predictive biomarkers across 10 cancer therapies

Author

Wolf, Denise M, Yau, Christina, Wulfkuhle, Julia, Brown-Swigart, Lamorna, Gallagher, Rosa I, Lee, Pei Rong Evelyn, Zhu, Zelos, Magbanua, Mark J, Sayaman, Rosalyn, O’Grady, Nicholas, Basu, Amrita, Delson, Amy, Coppé, Jean Philippe, Lu, Ruixiao, Braun, Jerome, Investigators, I-SPY2, Asare, Smita M, Sit, Laura, Matthews, Jeffrey B, Perlmutter, Jane, Hylton, Nola, Liu, Minetta C, Pohlmann, Paula, Symmans, W Fraser, Rugo, Hope S, Isaacs, Claudine, DeMichele, Angela M, Yee, Douglas, Berry, Donald A, Pusztai, Lajos, Petricoin, Emanuel F, Hirst, Gillian L, Esserman, Laura J, and van 't Veer, Laura J

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Cancer, Precision Medicine, Women's Health, Breast Cancer, Genetics, Clinical Research, Good Health and Well Being, Antineoplastic Combined Chemotherapy Protocols, Biomarkers, Tumor, Breast Neoplasms, Female, Humans, Neoadjuvant Therapy, Receptor, ErbB-2, Receptors, Estrogen, Receptors, Progesterone, I-SPY2 Investigators, Receptor, erbB-2, DNA repair, Immune, Luminal, breast cancer, clinical trial, immunotherapy, multiple arms, platinum, response prediction, subtyping, Neurosciences, Oncology & Carcinogenesis, Biochemistry and cell biology, Oncology and carcinogenesis

Abstract

Using pre-treatment gene expression, protein/phosphoprotein, and clinical data from the I-SPY2 neoadjuvant platform trial (NCT01042379), we create alternative breast cancer subtypes incorporating tumor biology beyond clinical hormone receptor (HR) and human epidermal growth factor receptor-2 (HER2) status to better predict drug responses. We assess the predictive performance of mechanism-of-action biomarkers from ∼990 patients treated with 10 regimens targeting diverse biology. We explore >11 subtyping schemas and identify treatment-subtype pairs maximizing the pathologic complete response (pCR) rate over the population. The best performing schemas incorporate Immune, DNA repair, and HER2/Luminal phenotypes. Subsequent treatment allocation increases the overall pCR rate to 63% from 51% using HR/HER2-based treatment selection. pCR gains from reclassification and improved patient selection are highest in HR+ subsets (>15%). As new treatments are introduced, the subtyping schema determines the minimum response needed to show efficacy. This data platform provides an unprecedented resource and supports the usage of response-based subtypes to guide future treatment prioritization.

Published

2022

6. Neoadjuvant T-DM1/pertuzumab and paclitaxel/trastuzumab/pertuzumab for HER2+ breast cancer in the adaptively randomized I-SPY2 trial.

Author

Clark, Amy S, Yau, Christina, Wolf, Denise M, Petricoin, Emanuel F, van 't Veer, Laura J, Yee, Douglas, Moulder, Stacy L, Wallace, Anne M, Chien, A Jo, Isaacs, Claudine, Boughey, Judy C, Albain, Kathy S, Kemmer, Kathleen, Haley, Barbara B, Han, Hyo S, Forero-Torres, Andres, Elias, Anthony, Lang, Julie E, Ellis, Erin D, Yung, Rachel, Tripathy, Debu, Nanda, Rita, Wulfkuhle, Julia D, Brown-Swigart, Lamorna, Gallagher, Rosa I, Helsten, Teresa, Roesch, Erin, Ewing, Cheryl A, Alvarado, Michael, Crane, Erin P, Buxton, Meredith, Clennell, Julia L, Paoloni, Melissa, Asare, Smita M, Wilson, Amy, Hirst, Gillian L, Singhrao, Ruby, Steeg, Katherine, Asare, Adam, Matthews, Jeffrey B, Berry, Scott, Sanil, Ashish, Melisko, Michelle, Perlmutter, Jane, Rugo, Hope S, Schwab, Richard B, Symmans, W Fraser, Hylton, Nola M, Berry, Donald A, Esserman, Laura J, and DeMichele, Angela M

Subjects

Humans, Breast Neoplasms, Paclitaxel, Maytansine, Receptor, erbB-2, Neoadjuvant Therapy, Adult, Aged, Middle Aged, Antibodies, Monoclonal, Humanized, Biomarkers, Tumor, Trastuzumab, Ado-Trastuzumab Emtansine, Receptor, ErbB-2, Clinical Trials and Supportive Activities, Clinical Research, Breast Cancer, Cancer, Evaluation of treatments and therapeutic interventions, 6.1 Pharmaceuticals

Abstract

HER2-targeted therapy dramatically improves outcomes in early breast cancer. Here we report the results of two HER2-targeted combinations in the neoadjuvant I-SPY2 phase 2 adaptive platform trial for early breast cancer at high risk of recurrence: ado-trastuzumab emtansine plus pertuzumab (T-DM1/P) and paclitaxel, trastuzumab and pertuzumab (THP). Eligible women have >2.5 cm clinical stage II/III HER2+ breast cancer, adaptively randomized to T-DM1/P, THP, or a common control arm of paclitaxel/trastuzumab (TH), followed by doxorubicin/cyclophosphamide, then surgery. Both T-DM1/P and THP arms 'graduate' in all subtypes: predicted pCR rates are 63%, 72% and 33% for T-DM1/P (n = 52), THP (n = 45) and TH (n = 31) respectively. Toxicity burden is similar between arms. Degree of HER2 pathway signaling and phosphorylation in pretreatment biopsy specimens are associated with response to both T-DM1/P and THP and can further identify highly responsive HER2+ tumors to HER2-directed therapy. This may help identify patients who can safely de-escalate cytotoxic chemotherapy without compromising excellent outcome.

Published

2021

7. Ganitumab and metformin plus standard neoadjuvant therapy in stage 2/3 breast cancer.

Author

Yee, Douglas, Isaacs, Claudine, Wolf, Denise M, Yau, Christina, Haluska, Paul, Giridhar, Karthik V, Forero-Torres, Andres, Jo Chien, A, Wallace, Anne M, Pusztai, Lajos, Albain, Kathy S, Ellis, Erin D, Beckwith, Heather, Haley, Barbara B, Elias, Anthony D, Boughey, Judy C, Kemmer, Kathleen, Yung, Rachel L, Pohlmann, Paula R, Tripathy, Debu, Clark, Amy S, Han, Hyo S, Nanda, Rita, Khan, Qamar J, Edmiston, Kristen K, Petricoin, Emanuel F, Stringer-Reasor, Erica, Falkson, Carla I, Majure, Melanie, Mukhtar, Rita A, Helsten, Teresa L, Moulder, Stacy L, Robinson, Patricia A, Wulfkuhle, Julia D, Brown-Swigart, Lamorna, Buxton, Meredith, Clennell, Julia L, Paoloni, Melissa, Sanil, Ashish, Berry, Scott, Asare, Smita M, Wilson, Amy, Hirst, Gillian L, Singhrao, Ruby, Asare, Adam L, Matthews, Jeffrey B, Hylton, Nola M, DeMichele, Angela, Melisko, Michelle, Perlmutter, Jane, Rugo, Hope S, Fraser Symmans, W, Van't Veer, Laura J, Berry, Donald A, and Esserman, Laura J

Subjects

Diabetes, Cancer, Breast Cancer, 6.1 Pharmaceuticals

Abstract

I-SPY2 is an adaptively randomized phase 2 clinical trial evaluating novel agents in combination with standard-of-care paclitaxel followed by doxorubicin and cyclophosphamide in the neoadjuvant treatment of breast cancer. Ganitumab is a monoclonal antibody designed to bind and inhibit function of the type I insulin-like growth factor receptor (IGF-1R). Ganitumab was tested in combination with metformin and paclitaxel (PGM) followed by AC compared to standard-of-care alone. While pathologic complete response (pCR) rates were numerically higher in the PGM treatment arm for hormone receptor-negative, HER2-negative breast cancer (32% versus 21%), this small increase did not meet I-SPY's prespecified threshold for graduation. PGM was associated with increased hyperglycemia and elevated hemoglobin A1c (HbA1c), despite the use of metformin in combination with ganitumab. We evaluated several putative predictive biomarkers of ganitumab response (e.g., IGF-1 ligand score, IGF-1R signature, IGFBP5 expression, baseline HbA1c). None were specific predictors of response to PGM, although several signatures were associated with pCR in both arms. Any further development of anti-IGF-1R therapy will require better control of anti-IGF-1R drug-induced hyperglycemia and the development of more predictive biomarkers.

Published

2021

8. Durvalumab with olaparib and paclitaxel for high-risk HER2-negative stage II/III breast cancer: Results from the adaptively randomized I-SPY2 trial.

Author

Pusztai, Lajos, Yau, Christina, Han, Hyo, Du, Lili, Wallace, Anne, String-Reasor, Erica, Boughey, Judy, Chien, A, Elias, Anthony, Beckwith, Heather, Nanda, Rita, Albain, Kathy, Clark, Amy, Kemmer, Kathleen, Kalinsky, Kevin, Isaacs, Claudine, Thomas, Alexandra, Helsten, Theresa, Forero-Torres, Andres, Liu, Minetta, Brown-Swigart, Lamorna, Petricoin, Emmanuel, Wulfkuhle, Julia, Asare, Smita, Wilson, Amy, Singhrao, Ruby, Sit, Laura, Berry, Scott, Sanil, Ashish, Asare, Adam, Matthews, Jeffrey, Perlmutter, Jane, Melisko, Michelle, Rugo, Hope, Schwab, Richard, Symmans, W, Yee, Doug, Vant Veer, Laura, DeMichele, Angela, Berry, Donald, Esserman, Laura, Hylton, Nola, Wolf, Denise, Shatsky, Rebecca, and Hirst, Gillian

Subjects

DNA repair inhibitor, breast cancer, clinical trial, immunotherapy, Adult, Aged, Aged, 80 and over, Antibodies, Monoclonal, Antineoplastic Combined Chemotherapy Protocols, Breast Neoplasms, Female, Follow-Up Studies, Humans, Middle Aged, Neoadjuvant Therapy, Paclitaxel, Phthalazines, Piperazines, Prognosis, Receptor, ErbB-2, Survival Rate, Young Adult

Abstract

The combination of PD-L1 inhibitor durvalumab and PARP inhibitor olaparib added to standard paclitaxel neoadjuvant chemotherapy (durvalumab/olaparib/paclitaxel [DOP]) was investigated in the phase II I-SPY2 trial of stage II/III HER2-negative breast cancer. Seventy-three participants were randomized to DOP and 299 to standard of care (paclitaxel) control. DOP increased pathologic complete response (pCR) rates in all HER2-negative (20%-37%), hormone receptor (HR)-positive/HER2-negative (14%-28%), and triple-negative breast cancer (TNBC) (27%-47%). In HR-positive/HER2-negative cancers, MammaPrint ultra-high (MP2) cases benefited selectively from DOP (pCR 64% versus 22%), no benefit was seen in MP1 cancers (pCR 9% versus 10%). Overall, 12.3% of patients in the DOP arm experienced immune-related grade 3 adverse events versus 1.3% in control. Gene expression signatures associated with immune response were positively associated with pCR in both arms, while a mast cell signature was associated with non-pCR. DOP has superior efficacy over standard neoadjuvant chemotherapy in HER2-negative breast cancer, particularly in a highly sensitive subset of high-risk HR-positive/HER2-negative patients.

Published

2021

9. PRoBE the cloud toolkit: finding the best biomarkers of drug response within a breast cancer clinical trial.

Author

O'Grady, Nicholas, Gibbs, David L, Abdilleh, Kawther, Asare, Adam, Asare, Smita, Venters, Sara, Brown-Swigart, Lamorna, Hirst, Gillian L, Wolf, Denise, Yau, Christina, van 't Veer, Laura J, Esserman, Laura, and Basu, Amrita

Subjects

I-SPY 2, breast cancer, clinical trials, cloud, data analysis, Networking and Information Technology R&D (NITRD), Genetics, Human Genome, Bioengineering, Cancer, Patient Safety

Abstract

ObjectivesIn this paper, we discuss leveraging cloud-based platforms to collect, visualize, analyze, and share data in the context of a clinical trial. Our cloud-based infrastructure, Patient Repository of Biomolecular Entities (PRoBE), has given us the opportunity for uniform data structure, more efficient analysis of valuable data, and increased collaboration between researchers.Materials and methodsWe utilize a multi-cloud platform to manage and analyze data generated from the clinical Investigation of Serial Studies to Predict Your Therapeutic Response with Imaging And moLecular Analysis 2 (I-SPY 2 TRIAL). A collaboration with the Institute for Systems Biology Cancer Gateway in the Cloud has additionally given us access to public genomic databases. Applications to I-SPY 2 data have been built using R Shiny, while leveraging Google's BigQuery tables and SQL commands for data mining.ResultsWe highlight the implementation of PRoBE in several unique case studies including prediction of biomarkers associated with clinical response, access to the Pan-Cancer Atlas, and integrating pathology images within the cloud. Our data integration pipelines, documentation, and all codebase will be placed in a Github repository.Discussion and conclusionWe are hoping to develop risk stratification diagnostics by integrating additional molecular, magnetic resonance imaging, and pathology markers into PRoBE to better predict drug response. A robust cloud infrastructure and tool set can help integrate these large datasets to make valuable predictions of response to multiple agents. For that reason, we are continuously improving PRoBE to advance the way data is stored, accessed, and analyzed in the I-SPY 2 clinical trial.

Published

2021

10. MK-2206 and Standard Neoadjuvant Chemotherapy Improves Response in Patients With Human Epidermal Growth Factor Receptor 2-Positive and/or Hormone Receptor-Negative Breast Cancers in the I-SPY 2 Trial.

Author

Chien, A Jo, Tripathy, Debasish, Albain, Kathy S, Symmans, W Fraser, Rugo, Hope S, Melisko, Michelle E, Wallace, Anne M, Schwab, Richard, Helsten, Teresa, Forero-Torres, Andres, Stringer-Reasor, Erica, Ellis, Erin D, Kaplan, Henry G, Nanda, Rita, Jaskowiak, Nora, Murthy, Rashmi, Godellas, Constantine, Boughey, Judy C, Elias, Anthony D, Haley, Barbara B, Kemmer, Kathleen, Isaacs, Claudine, Clark, Amy S, Lang, Julie E, Lu, Janice, Korde, Larissa, Edmiston, Kirsten K, Northfelt, Donald W, Viscusi, Rebecca K, Yee, Douglas, Perlmutter, Jane, Hylton, Nola M, Van't Veer, Laura J, DeMichele, Angela, Wilson, Amy, Peterson, Garry, Buxton, Meredith B, Paoloni, Melissa, Clennell, Julia, Berry, Scott, Matthews, Jeffrey B, Steeg, Katherine, Singhrao, Ruby, Hirst, Gillian L, Sanil, Ashish, Yau, Christina, Asare, Smita M, Berry, Donald A, and Esserman, Laura J

Subjects

Clinical Research, Clinical Trials and Supportive Activities, Cancer, Prevention, Breast Cancer, 6.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions, Adult, Aged, Antineoplastic Combined Chemotherapy Protocols, Breast Neoplasms, Doxorubicin, Female, Heterocyclic Compounds, 3-Ring, Humans, Middle Aged, Neoadjuvant Therapy, Paclitaxel, Protein Kinase Inhibitors, Proto-Oncogene Proteins c-akt, Receptor, ErbB-2, Receptors, Steroid, Trastuzumab, I-SPY 2 Consortium, Receptor, erbB-2, Clinical Sciences, Oncology and Carcinogenesis, Oncology & Carcinogenesis

Abstract

PurposeThe phosphatidylinositol 3-kinase/Akt/mammalian target of rapamycin is a key pathway of survival and therapeutic resistance in breast cancer. We evaluated the pan-Akt inhibitor MK-2206 in combination with standard therapy in patients with high-risk early-stage breast cancer.Patients and methodsI-SPY 2 is a multicenter, phase II, open-label, adaptively randomized neoadjuvant platform trial that screens experimental therapies and efficiently identifies potential predictive biomarker signatures. Patients are categorized by human epidermal growth factor receptor 2 (HER2), hormone receptor (HR), and MammaPrint statuses in a 2 × 2 × 2 layout. Patients within each of these 8 biomarker subtypes are adaptively randomly assigned to one of several experimental therapies, including MK-2206, or control. Therapies are evaluated for 10 biomarker signatures, each of which is a combination of these subtypes. The primary end point is pathologic complete response (pCR). A therapy graduates with one or more of these signatures if and when it has an 85% Bayesian predictive probability of success in a hypothetical phase III trial, adjusting for biomarker covariates. Patients in the current report received standard taxane- and anthracycline-based neoadjuvant therapy without (control) or with oral MK-2206 135 mg/week.ResultsMK-2206 graduated with 94 patients and 57 concurrently randomly assigned controls in 3 graduation signatures: HR-negative/HER2-positive, HR-negative, and HER2-positive. Respective Bayesian mean covariate-adjusted pCR rates and percentage probability that MK-2206 is superior to control were 0.48:0.29 (97%), 0.62:0.36 (99%), and 0.46:0.26 (94%). In exploratory analyses, MK-2206 evinced a numerical improvement in event-free survival in its graduating signatures. The most significant grade 3-4 toxicity was rash (14% maculopapular, 8.6% acneiform).ConclusionThe Akt inhibitor MK-2206 combined with standard neoadjuvant therapy resulted in higher estimated pCR rates in HR-negative and HER2-positive breast cancer. Although MK-2206 is not being further developed at this time, this class of agents remains of clinical interest.

Published

2020

11. Mechanism of action biomarkers predicting response to AKT inhibition in the I-SPY 2 breast cancer trial.

Author

Wolf, Denise M, Yau, Christina, Wulfkuhle, Julia, Brown-Swigart, Lamorna, Gallagher, Rosa I, Magbanua, Mark Jesus M, O'Grady, Nick, Hirst, Gillian, I-SPY 2 TRIAL Investigators, Asare, Smita, Tripathy, Debu, Berry, Don, Esserman, Laura, Chien, A Jo, Petricoin, Emanuel F, and van 't Veer, Laura

Subjects

I-SPY 2 TRIAL Investigators, Breast cancer, Predictive markers, Breast Cancer, Cancer, Genetics, Detection, screening and diagnosis, 4.2 Evaluation of markers and technologies

Abstract

The AKT inhibitor MK2206 (M) was evaluated in I-SPY 2 and graduated in the HER2+, HR-, and HR- HER2+ signatures. We hypothesized that AKT signaling axis proteins/genes may specifically predict response to M and tested 26 phospho-proteins and 10 genes involved in AKT-mTOR-HER signaling; in addition, we tested 9 genes from a previous study in the metastatic setting. One hundred and fifty patients had gene expression data from pretreatment biopsies available for analysis (M: 94, control: 56) and 138 had protein data (M: 87, control: 51). Logistic modeling was used to assess biomarker performance in pre-specified analysis. In general, phospho-protein biomarkers of activity in the AKT-mTOR-HER pathway appeared more predictive of response to M than gene expression or total protein biomarkers in the same pathway; however, the nature of the predictive biomarkers differed in the HER2+ and TN groups. In the HER2+ subset, patients achieving a pCR in M had higher levels of multiple AKT kinase substrate phospho-proteins (e.g., pmTOR, pTSC2). In contrast, in the TN subset responding patients had lower levels of AKT pathway phospho-proteins, such as pAKT, pmTOR, and pTSC2. Pathway mutations did not appear to account for these associations. Additional exploratory whole-transcriptome analysis revealed immune signaling as strongly associated with response to M in the HER2+ subset. While our sample size is small, these results suggest that the measurement of particular AKT kinase substrate phospho-proteins could be predictive of MK2206 efficacy in both HER2+ and TN tumors and that immune signaling may play a role in response in HER2+ patients.

Published

2020

12. Erratum: Author Correction: Surgical Standards for Management of the Axilla in Breast Cancer Clinical Trials with Pathological Complete Response Endpoint.

Author

Boughey, Judy C, Alvarado, Michael D, Lancaster, Rachael B, Symmans, W Fraser, Mukhtar, Rita, Wong, Jasmine M, Ewing, Cheryl A, Potter, David A, Tuttle, Todd M, Hieken, Tina J, Carter, Jodi M, Jakub, James W, Kaplan, Henry G, Buchanan, Claire L, Jaskowiak, Nora T, Sattar, Husain A, Mueller, Jeffrey, Nanda, Rita, Isaacs, Claudine J, Pohlmann, Paula R, Lynce, Filipa, Tousimis, Eleni A, Zeck, Jay C, Lee, M Catherine, Lang, Julie E, Mhawech-Fauceglia, Paulette, Rao, Roshni, Taback, Bret, Goodellas, Constantine, Chen, Margaret, Kalinsky, Kevin M, Hibshoosh, Hanina, Killelea, Brigid, Sanft, Tara, Hirst, Gillian L, Asare, Smita, Matthews, Jeffrey B, Perlmutter, Jane, Esserman, Laura J, and I-SPY2 Investigators

Subjects

I-SPY2 Investigators

Abstract

[This corrects the article DOI: 10.1038/s41523-018-0074-6.].

Published

2019

13. Residual cancer burden after neoadjuvant chemotherapy and long-term survival outcomes in breast cancer: a multicentre pooled analysis of 5161 patients

Author

Adamson, Kathi, Albain, Kathy S., Asare, Adam L., Asare, Smita M., Balassanian, Ron, Beckwith, Heather, Berry, Scott M., Berry, Donald A., Boughey, Judy C., Buxton, Meredith B., Chen, Yunn-Yi, Chen, Beiyun, Chien, A. Jo, Chui, Stephen Y., Clark, Amy S., Clennell, Julia L., Datnow, Brian, DeMichele, Angela M., Duan, Xiuzhen, Edmiston, Kirsten K., Elias, Anthony D., Ellis, Erin D., Esserman, Laura L., Euhus, David M., Fadare, Oluwole, Fan, Fang, Feldman, Michael D, Forero-Torres, Andres, Haley, Barbara B., Han, Hyo S., Harada, Shuko, Haugen, Patricia, Helsten, Teresa, Hirst, Gillian L., Hylton, Nola M., Isaacs, Claudine, Kemmer, Kathleen, Khan, Qamar J., Khazai, Laila, Klein, Molly E., Krings, Gregor, Lang, Julie E., LeBeau, Lauren G., Leyland-Jones, Brian, Liu, Minetta C., Lo, Shelly, Lu, Janice, Magliocco, Anthony, Matthews, Jeffrey B., Melisko, Michelle E., Mhawech-Fauceglia, Paulette, Moulder, Stacy L., Murthy, Rashmi K., Nanda, Rita, Northfelt, Donald W., Ocal, Idris T., Olopade, Olufunmilayo, Pambuccian, Stefan, Paoloni, Melissa, Park, John W., Parker, Barbara A., Perlmutter, Jane, Peterson, Garry, Pusztai, Lajos, Rendi, Mara, Rugo, Hope S., Sahoo, Sunati, Sams, Sharon, Sanil, Ashish, Sattar, Husain, Schwab, Richard B., Singhrao, Ruby, Steeg, Katherine, Stringer-Reasor, Erica, Symmans, W. Fraser, Tawfik, Ossama, Tripathy, Debasish, Troxell, Megan L., van't Veer, Laura J., Venters, Sara J., Vinh, Tuyethoa, Viscusi, Rebecca K., Wallace, Anne M., Wei, Shi, Wilson, Amy, Yau, Christina, Yee, Douglas, Zeck, Jay C., Osdoit, Marie, van der Noordaa, Marieke, Shad, Sonal, Wei, Jane, de Croze, Diane, Hamy, Anne-Sophie, Laé, Marick, Reyal, Fabien, Sonke, Gabe S, Steenbruggen, Tessa G, van Seijen, Maartje, Wesseling, Jelle, Martín, Miguel, del Monte-Millán, Maria, López-Tarruella, Sara, Boughey, Judy C, Goetz, Matthew P, Hoskin, Tanya, Gould, Rebekah, Valero, Vicente, Edge, Stephen B, Abraham, Jean E, Bartlett, John M S, Caldas, Carlos, Dunn, Janet, Earl, Helena, Hayward, Larry, Hiller, Louise, Provenzano, Elena, Sammut, Stephen-John, Thomas, Jeremy S, Cameron, David, Graham, Ashley, Hall, Peter, Mackintosh, Lorna, Godwin, Andrew K, Schwensen, Kelsey, Sharma, Priyanka, DeMichele, Angela M, Cole, Kimberly, Kim, Mi-Ok, van 't Veer, Laura J, Esserman, Laura J, and Symmans, W Fraser

Published

2022

14. Surgical Standards for Management of the Axilla in Breast Cancer Clinical Trials with Pathological Complete Response Endpoint.

Author

Boughey, Judy C, Alvarado, Michael D, Lancaster, Rachael B, Fraser Symmans, W, Mukhtar, Rita, Wong, Jasmine M, Ewing, Cheryl A, Potter, David A, Tuttle, Todd M, Hieken, Tina J, Carter, Jodi M, Jakub, James W, Kaplan, Henry G, Buchanan, Claire L, Jaskowiak, Nora T, Sattar, Husain A, Mueller, Jeffrey, Nanda, Rita, Isaacs, Claudine J, Pohlmann, Paula R, Lynce, Filipa, Tousimis, Eleni A, Zeck, Jay C, Lee, M Catherine, Lang, Julie E, Mhawech-Fauceglia, Paulette, Rao, Roshni, Taback, Bret, Chen, Margaret, Kalinsky, Kevin M, Hibshoosh, Hanina, Killelea, Brigid, Sanft, Tara, Hirst, Gillian L, Asare, Smita, Matthews, Jeffrey B, Perlmutter, Jane, Esserman, Laura J, and and I-SPY 2 Investigators

Subjects

and I-SPY 2 Investigators, Clinical Trials and Supportive Activities, Clinical Research, Patient Safety, Cancer

Abstract

Advances in the surgical management of the axilla in patients treated with neoadjuvant chemotherapy, especially those with node positive disease at diagnosis, have led to changes in practice and more judicious use of axillary lymph node dissection that may minimize morbidity from surgery. However, there is still significant confusion about how to optimally manage the axilla, resulting in variation among practices. From the viewpoint of drug development, assessment of response to neoadjuvant chemotherapy remains paramount and appropriate assessment of residual disease-the primary endpoint of many drug therapy trials in the neoadjuvant setting-is critical. Therefore decreasing the variability, especially in a multicenter clinical trial setting, and establishing a minimum standard to ensure consistency in clinical trial data, without mandating axillary lymph node dissection, for all patients is necessary. The key elements which include proper staging and identification of nodal involvement at diagnosis, and appropriately targeted management of the axilla at the time of surgical resection are presented. The following protocols have been adopted as standard procedure by the I-SPY2 trial for management of axilla in patients with node positive disease, and present a framework for prospective clinical trials and practice.

Published

2018

15. Supplementary Table S3 from Neoadjuvant Trebananib plus Paclitaxel-based Chemotherapy for Stage II/III Breast Cancer in the Adaptively Randomized I-SPY2 Trial—Efficacy and Biomarker Discovery

Author

Albain, Kathy S., primary, Yau, Christina, primary, Petricoin, Emanuel F., primary, Wolf, Denise M., primary, Lang, Julie E., primary, Chien, A. Jo, primary, Haddad, Tufia, primary, Forero-Torres, Andres, primary, Wallace, Anne M., primary, Kaplan, Henry, primary, Pusztai, Lajos, primary, Euhus, David, primary, Nanda, Rita, primary, Elias, Anthony D., primary, Clark, Amy S., primary, Godellas, Constantine, primary, Boughey, Judy C., primary, Isaacs, Claudine, primary, Tripathy, Debu, primary, Lu, Janice, primary, Yung, Rachel L., primary, Gallagher, Rosa I., primary, Wulfkuhle, Julia D., primary, Brown-Swigart, Lamorna, primary, Krings, Gregor, primary, Chen, Yunn Yi, primary, Potter, David A., primary, Stringer-Reasor, Erica, primary, Blair, Sarah, primary, Asare, Smita M., primary, Wilson, Amy, primary, Hirst, Gillian L., primary, Singhrao, Ruby, primary, Buxton, Meredith, primary, Clennell, Julia L., primary, Sanil, Ashish, primary, Berry, Scott, primary, Asare, Adam L., primary, Matthews, Jeffrey B., primary, DeMichele, Angela M., primary, Hylton, Nola M., primary, Melisko, Michelle, primary, Perlmutter, Jane, primary, Rugo, Hope S., primary, Symmans, W. Fraser, primary, van't Veer, Laura J., primary, Yee, Douglas, primary, Berry, Donald A., primary, and Esserman, Laura J., primary

Published

2024

16. Data from Neoadjuvant Trebananib plus Paclitaxel-based Chemotherapy for Stage II/III Breast Cancer in the Adaptively Randomized I-SPY2 Trial—Efficacy and Biomarker Discovery

Author

Albain, Kathy S., primary, Yau, Christina, primary, Petricoin, Emanuel F., primary, Wolf, Denise M., primary, Lang, Julie E., primary, Chien, A. Jo, primary, Haddad, Tufia, primary, Forero-Torres, Andres, primary, Wallace, Anne M., primary, Kaplan, Henry, primary, Pusztai, Lajos, primary, Euhus, David, primary, Nanda, Rita, primary, Elias, Anthony D., primary, Clark, Amy S., primary, Godellas, Constantine, primary, Boughey, Judy C., primary, Isaacs, Claudine, primary, Tripathy, Debu, primary, Lu, Janice, primary, Yung, Rachel L., primary, Gallagher, Rosa I., primary, Wulfkuhle, Julia D., primary, Brown-Swigart, Lamorna, primary, Krings, Gregor, primary, Chen, Yunn Yi, primary, Potter, David A., primary, Stringer-Reasor, Erica, primary, Blair, Sarah, primary, Asare, Smita M., primary, Wilson, Amy, primary, Hirst, Gillian L., primary, Singhrao, Ruby, primary, Buxton, Meredith, primary, Clennell, Julia L., primary, Sanil, Ashish, primary, Berry, Scott, primary, Asare, Adam L., primary, Matthews, Jeffrey B., primary, DeMichele, Angela M., primary, Hylton, Nola M., primary, Melisko, Michelle, primary, Perlmutter, Jane, primary, Rugo, Hope S., primary, Symmans, W. Fraser, primary, van't Veer, Laura J., primary, Yee, Douglas, primary, Berry, Donald A., primary, and Esserman, Laura J., primary

Published

2024

17. Supplementary Figure S1 from Neoadjuvant Trebananib plus Paclitaxel-based Chemotherapy for Stage II/III Breast Cancer in the Adaptively Randomized I-SPY2 Trial—Efficacy and Biomarker Discovery

Author

Albain, Kathy S., primary, Yau, Christina, primary, Petricoin, Emanuel F., primary, Wolf, Denise M., primary, Lang, Julie E., primary, Chien, A. Jo, primary, Haddad, Tufia, primary, Forero-Torres, Andres, primary, Wallace, Anne M., primary, Kaplan, Henry, primary, Pusztai, Lajos, primary, Euhus, David, primary, Nanda, Rita, primary, Elias, Anthony D., primary, Clark, Amy S., primary, Godellas, Constantine, primary, Boughey, Judy C., primary, Isaacs, Claudine, primary, Tripathy, Debu, primary, Lu, Janice, primary, Yung, Rachel L., primary, Gallagher, Rosa I., primary, Wulfkuhle, Julia D., primary, Brown-Swigart, Lamorna, primary, Krings, Gregor, primary, Chen, Yunn Yi, primary, Potter, David A., primary, Stringer-Reasor, Erica, primary, Blair, Sarah, primary, Asare, Smita M., primary, Wilson, Amy, primary, Hirst, Gillian L., primary, Singhrao, Ruby, primary, Buxton, Meredith, primary, Clennell, Julia L., primary, Sanil, Ashish, primary, Berry, Scott, primary, Asare, Adam L., primary, Matthews, Jeffrey B., primary, DeMichele, Angela M., primary, Hylton, Nola M., primary, Melisko, Michelle, primary, Perlmutter, Jane, primary, Rugo, Hope S., primary, Symmans, W. Fraser, primary, van't Veer, Laura J., primary, Yee, Douglas, primary, Berry, Donald A., primary, and Esserman, Laura J., primary

Published

2024

18. Supplementary Methods S1 from Neoadjuvant Trebananib plus Paclitaxel-based Chemotherapy for Stage II/III Breast Cancer in the Adaptively Randomized I-SPY2 Trial—Efficacy and Biomarker Discovery

Author

Albain, Kathy S., primary, Yau, Christina, primary, Petricoin, Emanuel F., primary, Wolf, Denise M., primary, Lang, Julie E., primary, Chien, A. Jo, primary, Haddad, Tufia, primary, Forero-Torres, Andres, primary, Wallace, Anne M., primary, Kaplan, Henry, primary, Pusztai, Lajos, primary, Euhus, David, primary, Nanda, Rita, primary, Elias, Anthony D., primary, Clark, Amy S., primary, Godellas, Constantine, primary, Boughey, Judy C., primary, Isaacs, Claudine, primary, Tripathy, Debu, primary, Lu, Janice, primary, Yung, Rachel L., primary, Gallagher, Rosa I., primary, Wulfkuhle, Julia D., primary, Brown-Swigart, Lamorna, primary, Krings, Gregor, primary, Chen, Yunn Yi, primary, Potter, David A., primary, Stringer-Reasor, Erica, primary, Blair, Sarah, primary, Asare, Smita M., primary, Wilson, Amy, primary, Hirst, Gillian L., primary, Singhrao, Ruby, primary, Buxton, Meredith, primary, Clennell, Julia L., primary, Sanil, Ashish, primary, Berry, Scott, primary, Asare, Adam L., primary, Matthews, Jeffrey B., primary, DeMichele, Angela M., primary, Hylton, Nola M., primary, Melisko, Michelle, primary, Perlmutter, Jane, primary, Rugo, Hope S., primary, Symmans, W. Fraser, primary, van't Veer, Laura J., primary, Yee, Douglas, primary, Berry, Donald A., primary, and Esserman, Laura J., primary

Published

2024

19. Race, Gene Expression Signatures, and Clinical Outcomes of Patients With High-Risk Early Breast Cancer

Author

Kyalwazi, Beverly, primary, Yau, Christina, additional, Campbell, Michael J., additional, Yoshimatsu, Toshio F., additional, Chien, A. Jo, additional, Wallace, Anne M., additional, Forero-Torres, Andres, additional, Pusztai, Lajos, additional, Ellis, Erin D., additional, Albain, Kathy S., additional, Blaes, Anne H., additional, Haley, Barbara B., additional, Boughey, Judy C., additional, Elias, Anthony D., additional, Clark, Amy S., additional, Isaacs, Claudine J., additional, Nanda, Rita, additional, Han, Hyo S., additional, Yung, Rachel L., additional, Tripathy, Debasish, additional, Edmiston, Kristen K., additional, Viscusi, Rebecca K., additional, Northfelt, Donald W., additional, Khan, Qamar J., additional, Asare, Smita M., additional, Wilson, Amy, additional, Hirst, Gillian L., additional, Lu, Ruixiao, additional, Symmans, William Fraser, additional, Yee, Douglas, additional, DeMichele, Angela M., additional, van ’t Veer, Laura J., additional, Esserman, Laura J., additional, and Olopade, Olufunmilayo I., additional

Published

2023

20. Author Correction: Surgical Standards for Management of the Axilla in Breast Cancer Clinical Trials with Pathological Complete Response Endpoint

Author

Boughey, Judy C., Alvarado, Michael D., Lancaster, Rachael B., Symmans, W. Fraser, Mukhtar, Rita, Wong, Jasmine M., Ewing, Cheryl A., Potter, David A., Tuttle, Todd M., Hieken, Tina J., Carter, Jodi M., Jakub, James W., Kaplan, Henry G., Buchanan, Claire L., Jaskowiak, Nora T., Sattar, Husain A., Mueller, Jeffrey, Nanda, Rita, Isaacs, Claudine J., Pohlmann, Paula R., Lynce, Filipa, Tousimis, Eleni A., Zeck, Jay C., Lee, M. Catherine, Lang, Julie E., Mhawech-Fauceglia, Paulette, Rao, Roshni, Taback, Bret, Goodellas, Constantine, Chen, Margaret, Kalinsky, Kevin M., Hibshoosh, Hanina, Killelea, Brigid, Sanft, Tara, Hirst, Gillian L., Asare, Smita, Matthews, Jeffrey B., Perlmutter, Jane, Esserman, Laura J., and I-SPY2 Investigators

Published

2019

21. Computational drug repositioning for the identification of new agents to sensitize drug-resistant breast tumors across treatments and receptor subtypes

Author

Yu, Katharine, Basu, Amrita, Yau, Christina, Wolf, Denise M., Goodarzi, Hani, Bandyopadhyay, Sourav, Korkola, James E., Hirst, Gillian L., Asare, Smita, DeMichele, Angela, Hylton, Nola, Yee, Douglas, Esserman, Laura, van ‘t Veer, Laura, and Sirota, Marina

Subjects

Cancer Research, Oncology

Published

2023

22. I-SPY2

Author

Esserman, Laura, primary, Hylton, Nola, additional, Asare, Smita, additional, Yau, Christina, additional, Yee, Doug, additional, DeMichele, Angie, additional, Perlmutter, Jane, additional, Symmans, Fraser, additional, van’t Veer, Laura, additional, Matthews, Jeff, additional, Berry, Donald A., additional, and Barker, Anna, additional

Published

2018

23. Abstract GS5-04: Identification of symptoms that are associated with irAEs in the I-SPY clinical trial

Author

Basu, Amrita, primary, Umashankar, Saumya, additional, Melisko, Michelle, additional, Lu, Ruixiao, additional, Yu, Hongmei, additional, Yau, Christina, additional, Asare, Smita, additional, Pitsouni, Maria, additional, Shatsky, Rebecca A., additional, Isaacs, Claudine, additional, DeMichele, Angela, additional, Hershman, Dawn, additional, Nanda, Rita, additional, Kim, Mi-Ok, additional, Esserman, Laura J., additional, and Rugo, Hope, additional

Published

2023

24. Abstract PD11-01: PD11-01 Evaluation of the PD-1 Inhibitor Cemiplimab in early-stage, high-risk HER2-negative breast cancer: Results from the neoadjuvant I-SPY 2 TRIAL

Author

Stringer-Reasor, Erica, primary, Shatsky, Rebecca A., additional, Chien, Jo, additional, Wallace, Anne, additional, Boughey, Judy C., additional, Albain, Kathy S., additional, Han, Hyo S., additional, Nanda, Rita, additional, Isaacs, Claudine, additional, Kalinsky, Kevin, additional, Mitri, Zahi, additional, Clark, Amy S., additional, Vaklavas, Christos, additional, Thomas, Alexandra, additional, Trivedi, Meghna S., additional, Lu, Janice, additional, Asare, Smita, additional, Lu, Ruixiao, additional, Pitsouni, Maria, additional, Wilson, Amy, additional, Perlmutter, Jane, additional, Rugo, Hope, additional, Schwab, Richard, additional, Symmans, W. Fraser, additional, Hylton, Nola M., additional, Van ’t Veer, Laura, additional, Yee, Douglas, additional, DeMichele, Angela, additional, Berry, Donald, additional, Esserman, Laura J., additional, and Investigators, I-SPY, additional

Published

2023

25. Association of Residual Ductal Carcinoma In Situ With Breast Cancer Recurrence in the Neoadjuvant I-SPY2 Trial

Author

Osdoit, Marie, primary, Yau, Christina, additional, Symmans, W. Fraser, additional, Boughey, Judy C., additional, Ewing, Cheryl A., additional, Balassanian, Ron, additional, Chen, Yunn-Yi, additional, Krings, Gregor, additional, Wallace, Anne M, additional, Zare, Somaye, additional, Fadare, Oluwole, additional, Lancaster, Rachael, additional, Wei, Shi, additional, Godellas, Constantine V., additional, Tang, Ping, additional, Tuttle, Todd M, additional, Klein, Molly, additional, Sahoo, Sunati, additional, Hieken, Tina J., additional, Carter, Jodi M., additional, Chen, Beiyun, additional, Ahrendt, Gretchen, additional, Tchou, Julia, additional, Feldman, Michael, additional, Tousimis, Eleni, additional, Zeck, Jay, additional, Jaskowiak, Nora, additional, Sattar, Husain, additional, Naik, Arpana M., additional, Lee, Marie Catherine, additional, Rosa, Marilin, additional, Khazai, Laila, additional, Rendi, Mara H., additional, Lang, Julie E., additional, Lu, Janice, additional, Tawfik, Ossama, additional, Asare, Smita M., additional, Esserman, Laura J., additional, and Mukhtar, Rita A., additional

Published

2022

26. Abstract LB111: Comparison of the predictive and prognostic significance of circulating tumor DNA in patients with high risk HER2-negative breast cancer receiving neoadjuvant chemotherapy

Author

Magbanua, Mark Jesus Mendoza, primary, Swigart, Lamorna Brown, additional, Renner, Derrick, additional, Shchegrova, Svetlana, additional, Hirst, Gillian L., additional, Yau, Christina, additional, Wolf, Denise M., additional, Wu, Hsin-Ta, additional, Kalashnikova, Ekaterina, additional, Delson, Amy L., additional, Chien, A. Jo, additional, Tripathy, Debu, additional, Asare, Smita, additional, Salari, Raheleh, additional, Rodriguez, Angel, additional, Zimmermann, Bernhard, additional, Sethi, Himanshu, additional, Aleshin, Alexey, additional, Billings, Paul, additional, Nanda, Rita, additional, Rugo, Hope S., additional, Esserman, Laura J., additional, Liu, Minetta C., additional, DeMichele, Angela, additional, and van 't Veer, Laura, additional

Published

2022

27. An ectopically expressed serum miRNA signature is prognostic, diagnostic, and biologically related to liver allograft rejection

Author

Shaked, Abraham, Chang, Bao‐Li, Barnes, Michael R., Sayre, Peter, Li, Yun R., Asare, Smita, DesMarais, Michele, Holmes, Michael V., Guettouche, Toumy, and Keating, Brendan J.

Published

2017

28. Abstract PD8-07: Evaluation of Tucatinib + (Paclitaxel + Pertuzumab + Trastuzumab) followed by AC in high-risk HER2 positive (HER2+) stage II/III breast cancer: Results from the I-SPY 2 TRIAL

Author

Potter, David A, primary, Roesch, Erin, additional, Yau, Christina, additional, Lu, Ruixiao, additional, Wolf, Denise, additional, Samson, Susan, additional, Stafford, Debra, additional, Albain, Kathy S, additional, Isaacs, Claudine, additional, Trivedi, Meghana, additional, Yee, Douglas, additional, Boughey, Judy, additional, Thomas, Alexandra, additional, Chien, A. Jo, additional, Hylton, Nola, additional, Li, Wen, additional, DeMichele, Angela, additional, Perlmutter, Jane, additional, Symmans, W. Fraser, additional, Hershman, Dawn L, additional, Melisko, Michelle, additional, van 't Veer, Laura J, additional, Wilson, Amy, additional, Asare, Smita M, additional, Berry, Donald A, additional, Schwab, Richard, additional, Rugo, Hope S, additional, and Esserman, Laura J, additional

Published

2022

29. Abstract PD10-07: Chemokine12 (CK12) tertiary lymphoid gene expression signature as a predictor of response in 3 immunotherapy arms of the neoadjuvant ISPY 2 TRIAL - pembrolizumab with and without SD101, and durvalumab combined with olaparib - and in 9 other arms of the trial including platinum-based and dual-anti-HER2 therapies

Author

Soliman, Hatem, primary, Wolf, Denise, additional, Chien, Jo, additional, Yau, Christina, additional, Campbell, Michael, additional, Magbanua, Mark, additional, Lu, Ruixiao, additional, O'Grady, Nicholas, additional, Brown-Swigart, Lamorna, additional, Hirst, Gillian, additional, Parker, Beverly, additional, Sit, Laura, additional, Asare, Smita, additional, Yee, Doug, additional, DeMichele, Angie, additional, Nanda, Rita, additional, Pusztai, Lajos, additional, Berry, Don, additional, Esserman, Laura, additional, and Van't Veer, Laura, additional

Published

2022

30. Abstract OT1-10-02: I-SPY2 endocrine optimization protocol (EOP): A pilot neoadjuvant endocrine therapy study with amcenestrant as monotherapy or in combination with abemacicilib or letrozole in molecularly selected HR+/HER2- clinical stage 2/3 breast cancer

Author

Chien, A. Jo, primary, Kalinsky, Kevin M, additional, Molina-Vega, Julissa, additional, Mukhtar, Rita, additional, Giridhar, Karthik, additional, Olopade, Olufunmilayo I, additional, Basu, Amrita, additional, Asare, Smita M, additional, Henderson, Paul, additional, Hirst, Gillian, additional, Lu, Ruixiao, additional, Jones, Ella, additional, Hylton, Nola, additional, Brown-Swigart, Lamorna, additional, van 't Veer, Laura J, additional, Yee, Douglas, additional, Mayer, Ingrid, additional, and Esserman, Laura J, additional

Published

2022

31. Abstract GS4-02: Analysis of clinical outcomes and expression-based immune signatures by race in the I-SPY 2 trial

Author

Kyalwazi, Beverly, primary, Yau, Christina, additional, Olopade, Olufunmilayo, additional, Chien, A. Jo, additional, Wallace, Anne, additional, Forero-Torres, Andres, additional, Pusztai, Lajos, additional, Ellis, Erin, additional, Albain, Kathy, additional, Blaes, Anne, additional, Haley, Barbara, additional, Boughey, Judy, additional, Elias, Anthony, additional, Clark, Amy, additional, Isaacs, Claudine, additional, Nanda, Rita, additional, Han, Hyo, additional, Yung, Rachel, additional, Tripathy, Debu, additional, Edmiston, Kristen, additional, Viscusi, Rebecca, additional, Northfelt, Donald, additional, Khan, Qamar, additional, Sanil, Ashish, additional, Berry, Scott, additional, Asare, Smita, additional, Wilson, Amy, additional, Hirst, Gillian, additional, Hylton, Nola, additional, Melisko, Michelle, additional, Perlmutter, Jane, additional, Rugo, Hope, additional, Symmans, Fraser, additional, van ‘t Veer, Laura, additional, Berry, Donald, additional, and Esserman, Laura, additional

Published

2022

32. Residual cancer burden after neoadjuvant chemotherapy and long-term survival outcomes in breast cancer: a multicentre pooled analysis of 5161 patients

Author

Yau, Christina, primary, Osdoit, Marie, additional, van der Noordaa, Marieke, additional, Shad, Sonal, additional, Wei, Jane, additional, de Croze, Diane, additional, Hamy, Anne-Sophie, additional, Laé, Marick, additional, Reyal, Fabien, additional, Sonke, Gabe S, additional, Steenbruggen, Tessa G, additional, van Seijen, Maartje, additional, Wesseling, Jelle, additional, Martín, Miguel, additional, del Monte-Millán, Maria, additional, López-Tarruella, Sara, additional, Boughey, Judy C, additional, Goetz, Matthew P, additional, Hoskin, Tanya, additional, Gould, Rebekah, additional, Valero, Vicente, additional, Edge, Stephen B, additional, Abraham, Jean E, additional, Bartlett, John M S, additional, Caldas, Carlos, additional, Dunn, Janet, additional, Earl, Helena, additional, Hayward, Larry, additional, Hiller, Louise, additional, Provenzano, Elena, additional, Sammut, Stephen-John, additional, Thomas, Jeremy S, additional, Cameron, David, additional, Graham, Ashley, additional, Hall, Peter, additional, Mackintosh, Lorna, additional, Fan, Fang, additional, Godwin, Andrew K, additional, Schwensen, Kelsey, additional, Sharma, Priyanka, additional, DeMichele, Angela M, additional, Cole, Kimberly, additional, Pusztai, Lajos, additional, Kim, Mi-Ok, additional, van 't Veer, Laura J, additional, Esserman, Laura J, additional, Symmans, W Fraser, additional, Adamson, Kathi, additional, Albain, Kathy S., additional, Asare, Adam L., additional, Asare, Smita M., additional, Balassanian, Ron, additional, Beckwith, Heather, additional, Berry, Scott M., additional, Berry, Donald A., additional, Boughey, Judy C., additional, Buxton, Meredith B., additional, Chen, Yunn-Yi, additional, Chen, Beiyun, additional, Chien, A. Jo, additional, Chui, Stephen Y., additional, Clark, Amy S., additional, Clennell, Julia L., additional, Datnow, Brian, additional, DeMichele, Angela M., additional, Duan, Xiuzhen, additional, Edmiston, Kirsten K., additional, Elias, Anthony D., additional, Ellis, Erin D., additional, Esserman, Laura L., additional, Euhus, David M., additional, Fadare, Oluwole, additional, Feldman, Michael D, additional, Forero-Torres, Andres, additional, Haley, Barbara B., additional, Han, Hyo S., additional, Harada, Shuko, additional, Haugen, Patricia, additional, Helsten, Teresa, additional, Hirst, Gillian L., additional, Hylton, Nola M., additional, Isaacs, Claudine, additional, Kemmer, Kathleen, additional, Khan, Qamar J., additional, Khazai, Laila, additional, Klein, Molly E., additional, Krings, Gregor, additional, Lang, Julie E., additional, LeBeau, Lauren G., additional, Leyland-Jones, Brian, additional, Liu, Minetta C., additional, Lo, Shelly, additional, Lu, Janice, additional, Magliocco, Anthony, additional, Matthews, Jeffrey B., additional, Melisko, Michelle E., additional, Mhawech-Fauceglia, Paulette, additional, Moulder, Stacy L., additional, Murthy, Rashmi K., additional, Nanda, Rita, additional, Northfelt, Donald W., additional, Ocal, Idris T., additional, Olopade, Olufunmilayo, additional, Pambuccian, Stefan, additional, Paoloni, Melissa, additional, Park, John W., additional, Parker, Barbara A., additional, Perlmutter, Jane, additional, Peterson, Garry, additional, Rendi, Mara, additional, Rugo, Hope S., additional, Sahoo, Sunati, additional, Sams, Sharon, additional, Sanil, Ashish, additional, Sattar, Husain, additional, Schwab, Richard B., additional, Singhrao, Ruby, additional, Steeg, Katherine, additional, Stringer-Reasor, Erica, additional, Symmans, W. Fraser, additional, Tawfik, Ossama, additional, Tripathy, Debasish, additional, Troxell, Megan L., additional, van't Veer, Laura J., additional, Venters, Sara J., additional, Vinh, Tuyethoa, additional, Viscusi, Rebecca K., additional, Wallace, Anne M., additional, Wei, Shi, additional, Wilson, Amy, additional, Yau, Christina, additional, Yee, Douglas, additional, and Zeck, Jay C., additional

Published

2022

33. Assessment of Residual Cancer Burden and Event-Free Survival in Neoadjuvant Treatment for High-risk Breast Cancer

Author

Symmans, W. Fraser, primary, Yau, Christina, additional, Chen, Yunn-Yi, additional, Balassanian, Ron, additional, Klein, Molly E., additional, Pusztai, Lajos, additional, Nanda, Rita, additional, Parker, Barbara A., additional, Datnow, Brian, additional, Krings, Gregor, additional, Wei, Shi, additional, Feldman, Michael D., additional, Duan, Xiuzhen, additional, Chen, Beiyun, additional, Sattar, Husain, additional, Khazai, Laila, additional, Zeck, Jay C., additional, Sams, Sharon, additional, Mhawech-Fauceglia, Paulette, additional, Rendi, Mara, additional, Sahoo, Sunati, additional, Ocal, Idris Tolgay, additional, Fan, Fang, additional, LeBeau, Lauren Grasso, additional, Vinh, Tuyethoa, additional, Troxell, Megan L., additional, Chien, A. Jo, additional, Wallace, Anne M., additional, Forero-Torres, Andres, additional, Ellis, Erin, additional, Albain, Kathy S., additional, Murthy, Rashmi K., additional, Boughey, Judy C., additional, Liu, Minetta C., additional, Haley, Barbara B., additional, Elias, Anthony D., additional, Clark, Amy S., additional, Kemmer, Kathleen, additional, Isaacs, Claudine, additional, Lang, Julie E., additional, Han, Hyo S., additional, Edmiston, Kirsten, additional, Viscusi, Rebecca K., additional, Northfelt, Donald W., additional, Khan, Qamar J., additional, Leyland-Jones, Brian, additional, Venters, Sara J., additional, Shad, Sonal, additional, Matthews, Jeffrey B., additional, Asare, Smita M., additional, Buxton, Meredith, additional, Asare, Adam L., additional, Rugo, Hope S., additional, Schwab, Richard B., additional, Helsten, Teresa, additional, Hylton, Nola M., additional, van ’t Veer, Laura, additional, Perlmutter, Jane, additional, DeMichele, Angela M., additional, Yee, Douglas, additional, Berry, Donald A., additional, and Esserman, Laura J., additional

Published

2021

34. Effect of Pembrolizumab Plus Neoadjuvant Chemotherapy on Pathologic Complete Response in Women With Early-Stage Breast Cancer

Author

Nanda, Rita, primary, Liu, Minetta C., additional, Yau, Christina, additional, Shatsky, Rebecca, additional, Pusztai, Lajos, additional, Wallace, Anne, additional, Chien, A. Jo, additional, Forero-Torres, Andres, additional, Ellis, Erin, additional, Han, Heather, additional, Clark, Amy, additional, Albain, Kathy, additional, Boughey, Judy C., additional, Jaskowiak, Nora T., additional, Elias, Anthony, additional, Isaacs, Claudine, additional, Kemmer, Kathleen, additional, Helsten, Teresa, additional, Majure, Melanie, additional, Stringer-Reasor, Erica, additional, Parker, Catherine, additional, Lee, Marie C., additional, Haddad, Tufia, additional, Cohen, Ronald N., additional, Asare, Smita, additional, Wilson, Amy, additional, Hirst, Gillian L., additional, Singhrao, Ruby, additional, Steeg, Katherine, additional, Asare, Adam, additional, Matthews, Jeffrey B., additional, Berry, Scott, additional, Sanil, Ashish, additional, Schwab, Richard, additional, Symmans, W. Fraser, additional, van ‘t Veer, Laura, additional, Yee, Douglas, additional, DeMichele, Angela, additional, Hylton, Nola M., additional, Melisko, Michelle, additional, Perlmutter, Jane, additional, Rugo, Hope S., additional, Berry, Donald A., additional, and Esserman, Laura J., additional

Published

2020

35. Abstract P3-09-02: Evaluation of a novel agent plus standard neoadjuvant therapy in early stage, high-risk HER2 negative breast cancer: Results from the I-SPY 2 TRIAL

Author

Liu, Minetta C., primary, Robinson, Patricia A, additional, Yau, Christina, additional, Wallace, Anne M, additional, Chien, A. Jo, additional, Stringer-Reasor, Erica, additional, Nanda, Rita, additional, Yee, Douglas, additional, Albain, Kathy S, additional, Boughey, Judy C, additional, Han, Heather S, additional, Elias, Anthony D, additional, Kalinsky, Kevin, additional, Clark, Amy S, additional, Kemmer, Kathleen, additional, Isaacs, Claudine, additional, Lang, Julie E, additional, Lu, Janice, additional, Sanft, Tara, additional, DeMichele, Angela, additional, Hylton, Nola M, additional, Melisko, Michelle E, additional, Perlmutter, Jane, additional, Rugo, Hope S, additional, Schwab, Richard, additional, Symmans, W. Fraser, additional, van't Veer, Laura J, additional, Haugen, Patricia K, additional, Wilson, Amy, additional, Singhrao, Ruby, additional, Asare, Smita, additional, Sanil, Ashish, additional, Berry, Donald A, additional, and Esserman, Laura J, additional

Published

2020

36. Abstract PD9-05: Lack of background parenchymal enhancement suppression in breast MRI during neoadjuvant chemotherapy may be associated with inferior treatment response in hormone receptor positive breast cancer

Author

Onishi, Natsuko, primary, Li, Wen, additional, Newitt, David C., additional, Harnish, Roy, additional, Gibbs, Jessica, additional, Jones, Ella F., additional, Nguyen, Alex, additional, Wilmes, Lisa, additional, Joe, Bonnie N., additional, Campbell, Michael J., additional, Basu, Amrita, additional, van’t Veer, Laura J., additional, DiMichele, Angela, additional, Yee, Douglas, additional, Berry, Donald A., additional, Albain, Kathy S., additional, Boughey, Judy C., additional, Chien, A. Jo, additional, Clark, Amy S., additional, Edmiston, Kirsten K., additional, Elias, Anthony D., additional, Ellis, Erin D., additional, Euhus, David M., additional, Han, Heather S., additional, Isaacs, Claudine, additional, Khan, Qamar J., additional, Lang, Julie E., additional, Lu, Janice, additional, Meisel, Jane L., additional, Mitri, Zaha, additional, Nanda, Rita, additional, Northfelt, Donald W., additional, Sanft, Tara, additional, Stringer-Reasor, Erica, additional, Viscusi, Rebecca K., additional, Wallace, Anne M., additional, Yung, Rachel, additional, Melisko, Michelle E., additional, Perlmutter, Jane, additional, Rugo, Hope S., additional, Schwab, Richard, additional, Symmans, W. Fraser, additional, Asare, Smita M., additional, Yau, Julie E., additional, Yau, Christina, additional, Esserman, Laura J., additional, and Hylton, Nola M., additional

Published

2020

37. Abstract P6-02-01: The effect of background parenchymal enhancement on the predictive performance of functional tumor volume measured in MRI

Author

Li, Wen, primary, Onishi, Natsuko, additional, Newitt, David C, additional, Harnish, Roy, additional, Jones, Ella F, additional, Wilmes, Lisa J, additional, Gibbs, Jessica, additional, Price, Elissa, additional, Joe, Bonnie N, additional, Chien, A. Jo, additional, Berry, Donald A, additional, Boughey, Judy C, additional, Albain, Kathy S, additional, Clark, Amy S, additional, Edmiston, Kirsten K, additional, Elias, Anthony D, additional, Ellis, Erin D, additional, Euhus, David M, additional, Han, Heather S, additional, Isaacs, Claudine, additional, Khan, Qamar J, additional, Lang, Julie E, additional, Lu, Janice, additional, Meisel, Jane L, additional, Mitri, Zaha, additional, Nanda, Rita, additional, Northfelt, Donald W, additional, Sanft, Tara, additional, Stringer-Reasor, Erica, additional, Viscusi, Rebecca K, additional, Wallace, Anne M, additional, Yee, Douglas, additional, Yung, Rachel, additional, Melisko, Michelle E, additional, Perlmutter, Jane, additional, Rugo, Hope S, additional, Schwab, Richard, additional, Symmans, W. Fraser, additional, van't Veer, Laura J, additional, Yau, Christina, additional, Asare, Smita M, additional, DeMichele, Angela, additional, Goudreau, Sally, additional, Abe, Hiroyuki, additional, Sheth, Deepa, additional, Wolverton, Dulcy, additional, Fountain, Kelly, additional, Ha, Richard, additional, Wynn, Ralph, additional, Crane, Erin P, additional, Dillis, Charlotte, additional, Kuritza, Theresa, additional, Morley, Kevin, additional, Nelson, Michael, additional, Church, An, additional, Niell, Bethany, additional, Drukteinis, Jennifer, additional, Oh, Karen Y, additional, Jafarian, Neda, additional, Brandt, Kathy, additional, Choudhery, Sadia, additional, Bang, Dae Hee, additional, Mullins, Christiane, additional, Woodard, Stefanie, additional, Zamora, Kathryn W, additional, Ojeda-Fornier, Haydee, additional, Eghedari, Mohammad, additional, Sheth, Pulin, additional, Hovanessian-Larsen, Linda, additional, Rosen, Mark, additional, McDonald, Elizabeth S, additional, Spektor, Michael, additional, Giurescu, Marina, additional, Newell, Mary S, additional, Cohen, Michael A, additional, Berman, Elise, additional, Lehman, Constance, additional, Smith, William, additional, Fitzpatrick, Kim, additional, Borders, Marisa H, additional, Yang, Wei, additional, Dogan, Basak, additional, Esserman, Laura J, additional, and Hylton, Nola M, additional

Published

2020

38. Abstract PD9-04: Breast cancer subtype specific association of pCR with MRI assessed tumor volume progression during NAC in the I-SPY 2 trial

Author

Li, Wen, primary, Onishi, Natsuko, additional, Newitt, David C, additional, Gibbs, Jessica, additional, Wilmes, Lisa J, additional, Jones, Ella F, additional, Joe, Bonnie N, additional, Sit, Laura S, additional, Yau, Christina, additional, Chien, A. Jo, additional, Price, Elissa, additional, Albain, Kathy S, additional, Kuritza, Theresa, additional, Morley, Kevin, additional, Boughey, Judy C, additional, Brandt, Kathy, additional, Choudhery, Sadia, additional, Clark, Amy S, additional, Rosen, Mark, additional, McDonald, Elizabeth S, additional, Elias, Anthony D, additional, Wolverton, Dulcy, additional, Fountain, Kelly, additional, Euhus, David M, additional, Han, Heather S, additional, Niell, Bethany, additional, Drukteinis, Jennifer, additional, Lang, Julie E, additional, Lu, Janice, additional, Meisel, Jane L, additional, Mitri, Zaha, additional, Nanda, Rita, additional, Northfelt, Donald W, additional, Sanft, Tara, additional, Stringer-Reasor, Erica, additional, Viscusi, Rebecca K, additional, Wallace, Anne M, additional, Yee, Douglas, additional, Yung, Rachel, additional, Asare, Smita M, additional, Melisko, Michelle E, additional, Perlmutter, Jane, additional, Rugo, Hope S, additional, Schwab, Richard, additional, Symmans, W. Fraser, additional, van't Veer, Laura J, additional, Berry, Donald A, additional, DeMichele, Angela, additional, Abe, Hiroyuki, additional, Sheth, Deepa, additional, Edmiston, Kirsten K, additional, Ellis, Erin D, additional, Ha, Richard, additional, Wynn, Ralph, additional, Crane, Erin P, additional, Dillis, Charlotte, additional, Nelson, Michael, additional, Church, An, additional, Isaacs, Claudine, additional, Khan, Qamar J, additional, Oh, Karen Y, additional, Jafarian, Neda, additional, Bang, Dae Hee, additional, Mullins, Christiane, additional, Woodard, Stefanie, additional, Zamora, Kathryn W, additional, Ojeda-Fornier, Haydee, additional, Sheth, Pulin, additional, Hovanessian-Larsen, Linda, additional, Eghtedari, Mohammad, additional, Spektor, Michael, additional, Giurescu, Marina, additional, Newell, Mary S, additional, Cohen, Michael A, additional, Berman, Elise, additional, Lehman, Constance, additional, Smith, William, additional, Fitzpatrick, Kim, additional, Borders, Marisa H, additional, Yang, Wei, additional, Dogan, Basak, additional, Goudreau, Sally, additional, Brown, Thelma, additional, Esserman, Laura J, additional, and Hylton, Nola M, additional

Published

2020

39. Abstract P3-11-02: Evaluation of patritumab/paclitaxel/trastuzumab over standard paclitaxel/trastuzumab in early stage, high-risk HER2 positive breast cancer: Results from the neoadjuvant I-SPY 2 trial

Author

Helsten, Teresa L, primary, Lo, Shelly S, additional, Yau, Christina, additional, Kalinsky, Kevin, additional, Elias, Anthony D, additional, Wallace, Anne M, additional, Chien, A. Jo, additional, Lu, Janice, additional, Lang, Julie E, additional, Albain, Kathy S, additional, Stringer-Reasor, Erica, additional, Clark, Amy S, additional, Boughey, Judy C, additional, Ellis, Erin D, additional, Yee, Douglas, additional, DeMichele, Angela, additional, Isaacs, Claudine, additional, Perlmutter, Jane, additional, Rugo, Hope S, additional, Schwab, Richard, additional, Hylton, Nola M., additional, Symmans, W. Fraser, additional, Melisko, Michelle E, additional, van't Veer, Laura J, additional, Wilson, Amy, additional, Singhrao, Ruby, additional, Asare, Smita M, additional, Sanil, Ashish, additional, Berry, Donald A, additional, and Esserman, Laura J, additional

Published

2020

40. Circulating tumor DNA in neoadjuvant treated breast cancer reflects response and survival

Author

Magbanua, Mark Jesus M., primary, Brown-Swigart, Lamorna, additional, Wu, Hsin-Ta, additional, Hirst, Gillian L., additional, Yau, Christina, additional, Wolf, Denise M., additional, Tin, Antony, additional, Salari, Raheleh, additional, Shchegrova, Svetlana, additional, Pawar, Hemant, additional, Delson, Amy L., additional, DeMichele, Angela, additional, Liu, Minetta C., additional, Chien, A. Jo, additional, Asare, Smita, additional, Lin, Cheng-Ho J., additional, Billings, Paul, additional, Aleshin, Alexey, additional, Sethi, Himanshu, additional, Louie, Maggie, additional, Zimmermann, Bernhard, additional, Esserman, Laura J., additional, and van ’t Veer, Laura J., additional

Published

2020

41. Durvalumab With Olaparib and Paclitaxel for High-Risk HER2-Negative Stage II/III Breast Cancer: Results From the Adaptively Randomized I-SPY2 Platform Trial

Author

Pusztai, Lajos, primary, Yau, Christina, additional, Wolf, Denise M., additional, Han, Hyo S., additional, Du, Lili, additional, Wallace, Anne M., additional, Stringer-Reasor, Erica, additional, Boughey, Judy C., additional, Chien, A. Jo, additional, Elias, Anthony D., additional, Beckwith, Heather, additional, Nanda, Rita, additional, Albain, Kathy S., additional, Clark, Amy S., additional, Kemmer, Kathleen, additional, Kalinsky, Kevin M., additional, Isaacs, Claudine, additional, Thomas, Alexandra, additional, Shatsky, Rebecca, additional, Helsten, Teresa L., additional, Forero-Torres, Andres, additional, Liu, Minetta C., additional, Brown-Swigart, Lamorna, additional, Petricoin, Emmanuel F., additional, Wulfkuhle, Julia D., additional, Asare, Smita M., additional, Wilson, Amy, additional, Singhrao, Ruby, additional, Sit, Laura, additional, Hirst, Gillian L., additional, Berry, Scott, additional, Sanil, Ashish, additional, Asare, Adam L., additional, Matthews, Jeffrey B., additional, Perlmutter, Jane, additional, Melisko, Michele, additional, Rugo, Hope S., additional, Schwab, Richard B., additional, Symmans, W. Fraser, additional, Yee, Doug, additional, van't Veer, Laura, additional, Hylton, Nola M., additional, DeMichele, Angela M., additional, Berry, Donald A., additional, and Esserman, Laura J., additional

Published

2020

42. Ancillary study management systems: a review of needs

Author

Nelson Elizabeth K, Piehler Britt, Rauch Adam, Ramsay Sarah, Holman Drienna, Asare Smita, Asare Adam, and Igra Mark

Subjects

Computer applications to medicine. Medical informatics, R858-859.7

Abstract

Abstract Background The valuable clinical data, specimens, and assay results collected during a primary clinical trial or observational study can enable researchers to answer additional, pressing questions with relatively small investments in new measurements. However, management of such follow-on, “ancillary” studies is complex. It requires coordinating across institutions, sites, repositories, and approval boards, as well as distributing, integrating, and analyzing diverse data types. General-purpose software systems that simplify the management of ancillary studies have not yet been explored in the research literature. Methods We have identified requirements for ancillary study management primarily as part of our ongoing work with a number of large research consortia. These organizations include the Center for HIV/AIDS Vaccine Immunology (CHAVI), the Immune Tolerance Network (ITN), the HIV Vaccine Trials Network (HVTN), the U.S. Military HIV Research Program (MHRP), and the Network for Pancreatic Organ Donors with Diabetes (nPOD). We also consulted with researchers at a range of other disease research organizations regarding their workflows and data management strategies. Lastly, to enhance breadth, we reviewed process documents for ancillary study management from other organizations. Results By exploring characteristics of ancillary studies, we identify differentiating requirements and scenarios for ancillary study management systems (ASMSs). Distinguishing characteristics of ancillary studies may include the collection of additional measurements (particularly new analyses of existing specimens); the initiation of studies by investigators unaffiliated with the original study; cross-protocol data pooling and analysis; pre-existing participant consent; and pre-existing data context and provenance. For an ASMS to address these characteristics, it would need to address both operational requirements (e.g., allocating existing specimens) and data management requirements (e.g., securely distributing and integrating primary and ancillary data). Conclusions The scenarios and requirements we describe can help guide the development of systems that make conducting ancillary studies easier, less expensive, and less error-prone. Given the relatively consistent characteristics and challenges of ancillary study management, general-purpose ASMSs are likely to be useful to a wide range of organizations. Using the requirements identified in this paper, we are currently developing an open-source, general-purpose ASMS based on LabKey Server (http://www.labkey.org) in collaboration with CHAVI, the ITN and nPOD.

Published

2013

43. Abstract CT136: Evaluation of talazoparib in combination with irinotecan in early stage, high-risk HER2 negative breast cancer: Results from the I-SPY 2 TRIAL

Author

Schwab, Richard, primary, Clark, Amy S., additional, Yau, Christina, additional, Hylton, Nola, additional, Li, Wen, additional, Wolfe, Denise, additional, Chien, A Jo, additional, Wallace, Anne M., additional, Forero-Torres, Andres, additional, Stringer-Reasor, Erica, additional, Nanda, Rita, additional, Jaskowiak, Nora, additional, Boughey, Judy, additional, Haddad, Tufia, additional, Han, Heather S., additional, Lee, Catherine, additional, Albain, Kathy, additional, Isaacs, Claudine, additional, Elias, Anthony D., additional, Ellis, Erin D., additional, Shah, Payal, additional, Lang, Julie E., additional, Lu, Janice, additional, Tripathy, Debasish, additional, Kemmer, Kathleen, additional, Yee, Douglas, additional, Haley, Barbara, additional, Majure, Melanie, additional, Roesch, Erin, additional, Vaklavas, Christos, additional, Ewing, Cheryl, additional, Helsten, Teresa, additional, Symmans, W Fraser, additional, Perlmutter, Jane, additional, Rugo, Hope S., additional, Melisko, Michelle, additional, Wilson, Amy, additional, Singhrao, Ruby, additional, Veer, Laura van 't, additional, DeMichele, Angela, additional, Asare, Smita, additional, Berry, Don, additional, and Esserman, Laura J., additional

Published

2019

44. Abstract 2611: Evaluation of ANG/TIE/hypoxia pathway genes and signatures as predictors of response to trebananib (AMG 386) in the neoadjuvant I-SPY 2 TRIAL for Stage II-III high-risk breast cancer

Author

Wolf, Denise M., primary, Yau, Christina, additional, Brown-Swigart, Lamorna, additional, Hirst, Gillian, additional, Investigators, I-SPY 2 TRIAL, additional, Asare, Smita, additional, Schwab, Richard, additional, Berry, Don, additional, Esserman, Laura, additional, Albain, Kathy S., additional, Leland-Jones, Brian, additional, and Veer, Laura van 't, additional

Published

2018

45. Pembrolizumab plus standard neoadjuvant therapy for high-risk breast cancer (BC): Results from I-SPY 2.

Author

Nanda, Rita, primary, Liu, Minetta C., additional, Yau, Christina, additional, Asare, Smita, additional, Hylton, Nola, additional, Veer, Laura Van't, additional, Perlmutter, Jane, additional, Wallace, Anne M., additional, Chien, Amy Jo, additional, Forero-Torres, Andres, additional, Ellis, Erin, additional, Han, Heather, additional, Sanders Clark, Amy, additional, Albain, Kathy S., additional, Caroline Boughey, Judy, additional, Elias, Anthony D., additional, Berry, Donald A., additional, Yee, Douglas, additional, DeMichele, Angela, additional, and Esserman, Laura, additional

Published

2017

46. Association of Event-Free and Distant Recurrence–Free Survival With Individual-Level Pathologic Complete Response in Neoadjuvant Treatment of Stages 2 and 3 Breast Cancer: Three-Year Follow-up Analysis for the I-SPY2 Adaptively Randomized Clinical Trial

Author

Yee, Douglas, DeMichele, Angela M., Yau, Christina, Isaacs, Claudine, Symmans, W. Fraser, Albain, Kathy S., Chen, Yunn-Yi, Krings, Gregor, Wei, Shi, Harada, Shuko, Datnow, Brian, Fadare, Oluwole, Klein, Molly, Pambuccian, Stefan, Chen, Beiyun, Adamson, Kathi, Sams, Sharon, Mhawech-Fauceglia, Paulette, Magliocco, Anthony, Feldman, Mike, Rendi, Mara, Sattar, Husain, Zeck, Jay, Ocal, Idris T., Tawfik, Ossama, LeBeau, Lauren Grasso, Sahoo, Sunati, Vinh, Tuyethoa, Chien, A. Jo, Forero-Torres, Andres, Stringer-Reasor, Erica, Wallace, Anne M., Pusztai, Lajos, Boughey, Judy C., Ellis, Erin D., Elias, Anthony D., Lu, Janice, Lang, Julie E., Han, Hyo S., Clark, Amy S., Nanda, Rita, Northfelt, Donald W., Khan, Qamar J., Viscusi, Rebecca K., Euhus, David M., Edmiston, Kirsten K., Chui, Stephen Y., Kemmer, Kathleen, Park, John W., Liu, Minetta C., Olopade, Olufunmilayo, Leyland-Jones, Brian, Tripathy, Debasish, Moulder, Stacy L., Rugo, Hope S., Schwab, Richard, Lo, Shelly, Helsten, Teresa, Beckwith, Heather, Haugen, Patricia, Hylton, Nola M., van’t Veer, Laura J., Perlmutter, Jane, Melisko, Michelle E., Wilson, Amy, Peterson, Garry, Asare, Adam L., Buxton, Meredith B., Paoloni, Melissa, Clennell, Julia L., Hirst, Gillian L., Singhrao, Ruby, Steeg, Katherine, Matthews, Jeffrey B., Asare, Smita M., Sanil, Ashish, Berry, Scott M., Esserman, Laura J., and Berry, Donald A.

Abstract

IMPORTANCE: Pathologic complete response (pCR) is a known prognostic biomarker for long-term outcomes. The I-SPY2 trial evaluated if the strength of this clinical association persists in the context of a phase 2 neoadjuvant platform trial. OBJECTIVE: To evaluate the association of pCR with event-free survival (EFS) and pCR with distant recurrence–free survival (DRFS) in subpopulations of women with high-risk operable breast cancer treated with standard therapy or one of several novel agents. DESIGN, SETTING, AND PARTICIPANTS: Multicenter platform trial of women with operable clinical stage 2 or 3 breast cancer with no prior surgery or systemic therapy for breast cancer; primary tumors were 2.5 cm or larger. Women with tumors that were ERBB2 negative/hormone receptor (HR) positive with low 70-gene assay score were excluded. Participants were adaptively randomized to one of several different investigational regimens or control therapy within molecular subtypes from March 2010 through 2016. The analysis included participants with follow-up data available as of February 26, 2019. INTERVENTIONS: Standard-of-care neoadjuvant therapy consisting of taxane treatment with or without (as control) one of several investigational agents or combinations followed by doxorubicin and cyclophosphamide. MAIN OUTCOMES AND MEASURES: Pathologic complete response and 3-year EFS and DRFS. RESULTS: Of the 950 participants (median [range] age, 49 [23-77] years), 330 (34.7%) achieved pCR. Three-year EFS and DRFS for patients who achieved pCR were both 95%. Hazard ratios for pCR vs non-pCR were 0.19 for EFS (95% CI, 0.12-0.31) and 0.21 for DRFS (95% CI, 0.13-0.34) and were similar across molecular subtypes, varying from 0.14 to 0.18 for EFS and 0.10 to 0.20 for DRFS. CONCLUSIONS AND RELEVANCE: The 3-year outcomes from the I-SPY2 trial show that, regardless of subtype and/or treatment regimen, including 9 novel therapeutic combinations, achieving pCR after neoadjuvant therapy implies approximately an 80% reduction in recurrence rate. The goal of the I-SPY2 trial is to rapidly identify investigational therapies that may improve pCR when validated in a phase 3 confirmatory trial. Whether pCR is a validated surrogate in the sense that a therapy that improves pCR rate can be assumed to also improve long-term outcome requires further study. TRIAL REGISTRATION: ClinicalTrials.gov Identifier: NCT01042379

Published

2020

47. An ectopically expressed serum miRNA signature is prognostic, diagnostic, and biologically related to liver allograft rejection

Author

Shaked, Abraham, primary, Chang, Bao‐Li, additional, Barnes, Michael R., additional, Sayre, Peter, additional, Li, Yun R., additional, Asare, Smita, additional, DesMarais, Michele, additional, Holmes, Michael V., additional, Guettouche, Toumy, additional, and Keating, Brendan J., additional

Published

2016

48. Banking RNA for Biomarker Discovery: Assessing RNA Quality and Yield for Long Term Use

Author

Philogene, Mary Carmelle, primary, Ali, Hodan, additional, Bourcier, Katarzyna, additional, Asare, Adam, additional, Lim, Noha, additional, Asare, Smita, additional, and Phippard, Deborah, additional

Published

2010

49. Nutritional Intervention to Prevent (NIP) Type 1 Diabetes A Pilot Trial.

Author

Chase, H. Peter, Lescheck, Ellen, Rafkin-Mervis, Lisa, Krause-Steinrauf, Heidi, Chritton, Sonia, Asare, Smita M., Adams, Sara, Skyler, Jay S., and Clare-Salzler, Michael

Abstract

The objective of this study was to describe a pilot trial of using an omega-3 fatty acid (docosahexaenoic acid [DHA]) to prevent islet cell autoimmunity in infants with an increased risk for developing type 1 diabetes (T1D). Infants from pregnant mothers who either have T1D (or the father or a previous child has T1D) and who entered the study in the third trimester or infants younger than age 5 months having a first-degree family member with T1D were eligible for the study. Infants from either group also had to have an increased genetic (HLA) risk for T1D (or multiple first-degree relatives with T1D) to be eligible. The study is a multicenter, 2-arm, randomized, double-masked clinical trial that will last 4 years (1 year of recruitment and 3 years of treatment). Treatment with DHA (or control) began in the last trimester of pregnancy or in the first 5 months after birth. Inflammatory mediators, including cytokines, chemokines, eicosanoids, and C-reactive protein, are being measured along with fatty acids in maternal and infant blood. Ninety-eight infants were enrolled (41 during pregnancy and 57 in the 5 months after birth). HLA results of the 97 eligible infants (1 infant had a protective 0602 allele and was thus ineligible) showed that 90 have DR3 and/or DR4. Seven infants were enrolled without DR3/4 but who instead had multiple first-degree relatives with T1D. Compliance has been excellent, and no families have discontinued participation. Intervention trials in this high-risk group are feasible but require significant effort to identify potential participants. [ABSTRACT FROM PUBLISHER]

Published

2009

50. Nutritional Intervention to Prevent (NIP) Type 1 Diabetes.

Author

Chase, H. Peter, Asare, Smita, Greenbaum, Carla, Lachin, John, Leschek, Ellen, Krause-Steinrauf, Heidi, Rafkin-Mervis, Lisa, and Clare-Salzler, Michael

Subjects

*NUTRITION, *DIABETES prevention, *DIABETES in children, *THERAPEUTICS, *FEASIBILITY studies, *INFANTS, *DOCOSAHEXAENOIC acid, *AUTOANTIBODIES

Abstract

Evidence for the initiation of type 1 diabetes (T1D) early in life comes from studies demonstrating 80% of children who develop this disease before the age of 12 years manifest autoantibodies prior to age 3 years. T1D prevention therefore may be most successful when treatments are begun at an early age. However, such interventions must be safe and not interfere with the growth and development of infants. A pilot feasibility trial to prevent the initiation of islet inflammation in high-risk infants has been initiated by Type 1 Diabetes TrialNet in which 90 infants from 10 clinical sites will receive docosahexaenoic acid (DHA), an omega 3 fatty acid, or a placebo. In human studies, supplementation with DHA effectively reduced inflammatory responses, e.g., IL-1b (beta) and IL-12, and blocked Th1 responses, thus targeting key immuno-pathogenie events that may block or reduce early β (beta) cell destruction. In the current study, DHA (or placebo) is either given to pregnant mothers in their third trimester of pregnancy (Group A) or administered to infants within the first 6 months after birth (Group B). In order to continue (Group A) or enter (Group B) the one year pilot trial, infants must have a family history of T1D and must express high-risk HLA alleles. The goals of the trial are; i) enroll 90 subjects in 12 months, ii) demonstrate 90/95% compliance in visits/taking supplement, iii) demonstrate DHA supplementation increases RBC DHA levels by greater than or equal to 20%, iv) demonstrate DHA supplementation reduces inflammatory cytokine production, e.g. IL-1β (beta), by greater than or equal to 20%, and v) demonstrate DHA supplementation does not interfere with immunity. Upon reaching these goals a full trial would ensue where infants will receive DHA supplements until age 3 years. Annual follow-up will occur until age 6 years with contact to age 9 years. The study endpoint will be the development of 2 persistent biochemical islet autoantibodies. AIDA-Funded Research [ABSTRACT FROM AUTHOR]

Published

2007