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Nova · Professor Researcher · re-ranking top 20…
M. Jordan Love

M. Jordan Love

· Affiliated Faculty and Carol R. Angle Academic Curator, The Fralin Museum of ArtVerified

University of Virginia · Art History

Active 1956–2024

h-index103
Citations53.9k
Papers520197 last 5y
Funding
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Research topics

  • Immunology
  • Medicine
  • Biology
  • Virology
  • Computational biology
  • Environmental health
  • Pathology
  • Genetics
  • Internal medicine

Selected publications

  • Multimodal profiling of lung granulomas in macaques reveals cellular correlates of tuberculosis control

    Immunity · 2022 · 277 citations

    • Biology
    • Immunology
    • Pathology

    Mycobacterium tuberculosis lung infection results in a complex multicellular structure: the granuloma. In some granulomas, immune activity promotes bacterial clearance, but in others, bacteria persist and grow. We identified correlates of bacterial control in cynomolgus macaque lung granulomas by co-registering longitudinal positron emission tomography and computed tomography imaging, single-cell RNA sequencing, and measures of bacterial clearance. Bacterial persistence occurred in granulomas enriched for mast, endothelial, fibroblast, and plasma cells, signaling amongst themselves via type 2 immunity and wound-healing pathways. Granulomas that drove bacterial control were characterized by cellular ecosystems enriched for type 1-type 17, stem-like, and cytotoxic T cells engaged in pro-inflammatory signaling networks involving diverse cell populations. Granulomas that arose later in infection displayed functional characteristics of restrictive granulomas and were more capable of killing Mtb. Our results define the complex multicellular ecosystems underlying (lack of) granuloma resolution and highlight host immune targets that can be leveraged to develop new vaccine and therapeutic strategies for TB.

  • Engineered SARS-CoV-2 receptor binding domain improves manufacturability in yeast and immunogenicity in mice

    Proceedings of the National Academy of Sciences · 2021 · 100 citations

    Senior authorCorresponding
    • Virology
    • Biology
    • Immunology

    Global containment of COVID-19 still requires accessible and affordable vaccines for low- and middle-income countries (LMICs). Recently approved vaccines provide needed interventions, albeit at prices that may limit their global access. Subunit vaccines based on recombinant proteins are suited for large-volume microbial manufacturing to yield billions of doses annually, minimizing their manufacturing cost. These types of vaccines are well-established, proven interventions with multiple safe and efficacious commercial examples. Many vaccine candidates of this type for SARS-CoV-2 rely on sequences containing the receptor-binding domain (RBD), which mediates viral entry to cells via ACE2. Here we report an engineered sequence variant of RBD that exhibits high-yield manufacturability, high-affinity binding to ACE2, and enhanced immunogenicity after a single dose in mice compared to the Wuhan-Hu-1 variant used in current vaccines. Antibodies raised against the engineered protein exhibited heterotypic binding to the RBD from two recently reported SARS-CoV-2 variants of concern (501Y.V1/V2). Presentation of the engineered RBD on a designed virus-like particle (VLP) also reduced weight loss in hamsters upon viral challenge.

Frequent coauthors

  • Anne S. Hellkamp

    Clinical Research Institute

    197 shared
  • Gervasio A. Lamas

    197 shared
  • Kerry L. Lee

    Clinical Research Institute

    197 shared
  • Roger A. Marinchak

    Lankenau Heart Institute

    196 shared
  • Alexander Paraschos

    Urology Team

    196 shared
  • Raymond Yee

    London Health Sciences Centre

    196 shared
  • Taya V. Glotzer

    Hackensack University Medical Center

    196 shared
  • James E. Cook

    West Virginia University Institute of Technology

    196 shared
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