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Preclinical NCI-MPACT: prospective modeling of the mutation-based NCI-MPACT clinical trial therapeutic strategy in patient-derived xenograft models

  1. Author:
    Evrard,Yvonne
    Alcoser, Sergio Y
    Mullendore,Michael
    Chen,Li
    Lih, Chih-Jian
    Kannan, Vishnuprabha Rahul
    Datta, Vivekananda
    Dutko,Lindsay
    Jiwani,Shahanawaz
    Rubinstein, Lawrence V
    Zhao, Yingdong
    Williams, P Mickey
    Palmisano, Alida
    Kuhlmann, Laura
    Simpson, Mel
    Kummar, Shivaani
    Das,Biswajit
    Karlovich,Chris
    Polley, Eric
    Li, Ming-Chung
    Chen, Alice P
    Hollingshead, Melinda G
    Doroshow, James H

  2. Author Address

    Applied and Developmental Research Directorate (ADRD), Frederick National Laboratory for Cancer Research, Frederick, MD, United States., Division of Cancer Treatment and Diagnosis, National Cancer Institute, Bethesda, MD, United States., Molecular Characterization Laboratory, Frederick National Laboratory for Cancer Research, National Cancer Institute, Frederick, MD, United States., General Dynamics Information Technology (GDIT), Falls Church, VA, United States., Division of Hematology/Medical Oncology, School of Medicine, Oregon Health & Science University, Portland, OR, United States., Department of Public Health Sciences, University of Chicago, Chicago, IL, United States., Center for Cancer Research, National Cancer Institute, Bethesda, MD, United States.,
    1. Year: 2025
    2. Epub Date: 2025 05 19
  2. Journal: Frontiers in Oncology
    1. 15
    2. Pages: 1571635
  4. Type of Article: Article
  5. Article Number: 1571635
  1. Abstract:

    The National Cancer Institute's Molecular Profiling-Based Assignment of Cancer Therapy (NCI-MPACT) randomized phase 2 clinical trial assessed the utility of applying tumor DNA sequencing to treatment selection. Here, we report the results of a companion preclinical study in patient-derived xenograft (PDX) models to evaluate how each tumor responded to each of the treatment regimens studied in the NCI-MPACT trial instead of simply to the specific regimen targeting the study-actionable mutation of interest (aMOI). Fifty-one PDX models (46 with and 5 without NCI-MPACT aMOIs) were tested against both the arm that would have been assigned in the NCI-MPACT trial as well as every other study regimen: (1) veliparib plus temozolomide or (2) adavosertib plus carboplatin (targeting the DNA repair pathway); (3) everolimus (targeting the PI3K pathway); and (4) trametinib (targeting the RAS/RAF/MEK pathway). Durability of response was measured by relative median time to tumor quadrupling event-free survival (EFSx4 = 2), and duration of tumor regression. Eleven of 50 models (22%) treated with veliparib plus temozolomide responded according to one or both metrics, as did 2/47 models (4.2%) treated with adavosertib plus carboplatin, and 2/46 models (4.3%) treated with trametinib; no models responded to erlotinib. Follow-up studies demonstrated that temozolomide drove the activity of the veliparib plus temozolomide combination and drug sensitivity to temozolomide correlated with MGMT deficiency. This prospective preclinical study confirmed the modest response rates in the NCI-MPACT clinical trial. Substantial responses to temozolomide suggest that this drug represents an effective treatment for patients with MGMT deficiency, regardless of cancer type. Copyright © 2025 Evrard, Alcoser, Mullendore, Chen, Lih, Kannan, Datta, Dutko, Jiwani, Rubinstein, Zhao, Williams, Palmisano, Kuhlmann, Simpson, Kummar, Das, Karlovich, Polley, Li, Chen, Hollingshead and Doroshow.

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External Sources

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  2. DOI: 10.3389/fonc.2025.1571635
  3. PMID: 40458731
  4. PMCID: PMC12127203

Library Notes

  1. Fiscal Year: FY2024-2025
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