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Edward E. Morrisey

Edward E. Morrisey

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University of Pennsylvania · Rehabilitation Medicine

Active 1995–2024

h-index108
Citations43.8k
Papers397116 last 5y
Funding$70.1M1 active
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Research topics

  • Biology
  • Genetics
  • Virology
  • Cell biology
  • Pharmacology
  • Computational biology
  • Immunology
  • Medicine
  • Biochemistry

Selected publications

  • Drug repurposing screens reveal cell-type-specific entry pathways and FDA-approved drugs active against SARS-Cov-2

    Cell Reports · 2021 · 250 citations

    • Pharmacology
    • Virology
    • Biology

    There is an urgent need for antivirals to treat the newly emerged severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2). To identify new candidates, we screen a repurposing library of ∼3,000 drugs. Screening in Vero cells finds few antivirals, while screening in human Huh7.5 cells validates 23 diverse antiviral drugs. Extending our studies to lung epithelial cells, we find that there are major differences in drug sensitivity and entry pathways used by SARS-CoV-2 in these cells. Entry in lung epithelial Calu-3 cells is pH independent and requires TMPRSS2, while entry in Vero and Huh7.5 cells requires low pH and triggering by acid-dependent endosomal proteases. Moreover, we find nine drugs are antiviral in respiratory cells, seven of which have been used in humans, and three are US Food and Drug Administration (FDA) approved, including cyclosporine. We find that the antiviral activity of cyclosporine is targeting Cyclophilin rather than calcineurin, revealing essential host targets that have the potential for rapid clinical implementation.

  • SARS-CoV-2 induces double-stranded RNA-mediated innate immune responses in respiratory epithelial-derived cells and cardiomyocytes

    Proceedings of the National Academy of Sciences · 2021 · 248 citations

    • Biology
    • Virology
    • Cell biology

    cells implicates OAS-RNase L in restricting SARS-CoV-2. Finally, while SARS-CoV-2 fails to antagonize these host defense pathways, which contrasts with other coronaviruses, the IFN signaling response is generally weak. These host-virus interactions may contribute to the unique pathogenesis of SARS-CoV-2.

  • The in vivo genetic program of murine primordial lung epithelial progenitors

    Nature Communications · 2020 · 68 citations

    • Biology
    • Cell biology
    • Computational biology

    Abstract Multipotent Nkx2-1-positive lung epithelial primordial progenitors of the foregut endoderm are thought to be the developmental precursors to all adult lung epithelial lineages. However, little is known about the global transcriptomic programs or gene networks that regulate these gateway progenitors in vivo. Here we use bulk RNA-sequencing to describe the unique genetic program of in vivo murine lung primordial progenitors and computationally identify signaling pathways, such as Wnt and Tgf-β superfamily pathways, that are involved in their cell-fate determination from pre-specified embryonic foregut. We integrate this information in computational models to generate in vitro engineered lung primordial progenitors from mouse pluripotent stem cells, improving the fidelity of the resulting cells through unbiased, easy-to-interpret similarity scores and modulation of cell culture conditions, including substratum elastic modulus and extracellular matrix composition. The methodology proposed here can have wide applicability to the in vitro derivation of bona fide tissue progenitors of all germ layers.

Recent grants

Frequent coauthors

  • Yuzhen Zhang

    State Key Laboratory of Cardiovascular Disease

    200 shared
  • Ying Tian

    193 shared
  • Michael P. Morley

    University of Pennsylvania

    187 shared
  • Lin Zhang

    179 shared
  • Xiaoli Chen

    Chinese Academy of Sciences

    179 shared
  • Paul Chan

    Wan Fang Hospital

    179 shared
  • Xiangjian Zheng

    177 shared
  • Zuoren Yu

    Shanghai East Hospital

    177 shared

Education

  • Ph.D., Biochemistry

    Northwestern University

    1994
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