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Phyllis A. Gimotty

Phyllis A. Gimotty

University of Pennsylvania · Rehabilitation Medicine

Active 1980–2024

h-index79
Citations39.1k
Papers538196 last 5y
Funding$200.4M
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Research topics

  • Oncology
  • Internal medicine
  • Medicine
  • Cancer research
  • Cell biology
  • Chemistry
  • Biology
  • Surgery
  • Biochemistry

Selected publications

  • Stiff matrix induces exosome secretion to promote tumour growth

    Nature Cell Biology · 2023 · 219 citations

    • Cell biology
    • Chemistry
    • Biology
  • Effects of systemic inflammation on relapse in early breast cancer

    npj Breast Cancer · 2021 · 37 citations

    • Medicine
    • Internal medicine
    • Oncology

    Chronic inflammation has been a proposed mechanism of resistance to aromatase inhibitors in breast cancer. Stratifying by HER2 status, a matched case-control study from the Wellness After Breast Cancer-II cohort was performed to assess whether or not elevated serum inflammatory biomarkers (C-Reactive protein [CRP], interleukin-6 [IL-6], and serum amyloid A [SAA]) and/or the presence of a high-risk IL-6 promoter genotype were associated with recurrence of hormone receptor positive (HR+) early breast cancer. Estrogen levels were also measured and correlated with biomarkers and disease outcomes. CRP and SAA were significantly associated with an increased risk of recurrence in the HR+/HER2- group, but not the HR+/HER2+ group. Mean serum estrogen levels were non-significantly elevated in patients who relapsed vs. non-relapsed patients. Surprisingly, high-risk IL-6 promoter polymorphisms were strongly associated with HER2+ breast cancer relapse, which has potential therapeutic implications, as elevated intracellular IL-6 has been associated with trastuzumab resistance in pre-clinical models.

  • Identifying predictors of <scp>HPV</scp> ‐related head and neck squamous cell carcinoma progression and survival through patient‐derived models

    International Journal of Cancer · 2020 · 54 citations

    • Medicine
    • Oncology
    • Internal medicine

    levels found in a PDX from an outlier case with lethal outcome led to detection of similar profiles among recurrent HPV+ HNSCCs. Transcriptional data from the Cancer Genome Atlas was used to demonstrate that the lower E2F target gene expression predicted by reduced E7 levels has potential as a biomarker of disease recurrence risk. Our findings bridge a critical gap in preclinical models for HPV+ HNSCCs and simultaneously reveal novel potential applications of quantifying mutational burden and viral oncogene functions for biomarker development.

Recent grants

Frequent coauthors

  • Meenhard Herlyn

    144 shared
  • E. Tahirović

    Queen Mary University of London

    98 shared
  • Haijun Zhou

    Cornell University

    98 shared
  • Tron Va

    Queen's University

    98 shared
  • Christopher D. Hobday

    Houston Methodist

    98 shared
  • Paulo Nuin

    Ontario Institute for Cancer Research

    98 shared
  • Abi Daoud

    University Hospitals of Cleveland

    98 shared
  • Van Belle

    Methodist Hospital

    98 shared
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