Giant MagnetoResistive (GMR) Sensors for Measuring Influenza Vaccine
- Funded by National Institutes of Health (NIH)
- Total publications:0 publications
Grant number: 3R01AI125197-05S1
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Key facts
Disease
COVID-19Start & end year
20202021Known Financial Commitments (USD)
$158,000Funder
National Institutes of Health (NIH)Principal Investigator
Paul Joseph Utz, Shan X WangResearch Location
United States of AmericaLead Research Institution
Stanford UniversityResearch Priority Alignment
N/A
Research Category
Pathogen: natural history, transmission and diagnostics
Research Subcategory
Pathogen morphology, shedding & natural history
Special Interest Tags
N/A
Study Type
Unspecified
Clinical Trial Details
N/A
Broad Policy Alignment
Pending
Age Group
Unspecified
Vulnerable Population
Unspecified
Occupations of Interest
Unspecified
Abstract
7. Project Summary/Abstract The overarching goal of this New Aim 4 is to test the hypothesis that SARS-CoV-2 (CoV-2) causes autoimmune disease (AI) in a subset of infected patients. Our preliminary studies on 336 COVID-19 samples from 282 COVID19 patients (four COVID-19 cohorts in three geographically distinct regions) have identified autoantibodies and clinical evidence of AI. To test the hypothesis that autoantibodies develop following CoV-2 infection, we will use autoantigen arrays to identify proteins targeted by autoantibodies, some of which may cause pathogenic inflammatory responses that could mediate lung, skin, and other tissue injury, dysregulated coagulation, endothelial dysfunction, and vasculopathy. We will then test the hypothesis that autoantibodies develop through different mechanisms including molecular mimicry and generation of receptor-blocking anti-cytokine antibodies (ACA) in response to "cytokine storm". We hypothesize that infection with CoV-2 induces 2 different outcomes: (i) the desired outcome - protective responses that neutralize CoV-2; or (ii) pathogenic responses that lead to symptomatic autoimmunity or autoinflammatory disease. Aim 4.1 will test the hypothesis that CoV-2 causes development of autoantibodies and classifiable autoimmune diseases by leveraging our custom "COVID-19 Autoantigen Array" comprising common autoantigens from diseases that affect the lung, endothelium and skin. Aim 4.2 will characterize serum antibodies specific for proteins from CoV-2 and other coronaviruses, and correlate with autoantibodies in Aim 1, by using our "COVID-19 Viral Array" capable of simultaneously quantitating antibodies against many different wild-type and mutant viral proteins and peptides. Viral responses will be correlated with clinical outcomes including development of autoantibodies, and progression to clinical autoimmunity. Aim 4.3 will test the hypothesis that CoV-2 causes autoimmunity through mechanisms including cross-reactivity (molecular mimicry) and cytokine storm which generates receptor-blocking ACA. We will use a variety of lab-based techniques to explore these mechanisms, including purification of antigen-specific IgG from serum, co-immunoprecipitation, and cross-binding assays. Together, the proposed experiments will begin to quantify the impact of CoV-2 on AI, identify which antigens and specific AI are associated with CoV-2, and contribute to our mechanistic understanding of COVID-19 pathogenesis, setting the stage for large-scale epidemiology studies to determine the extent of autoimmunity that results from CoV-2 infection, as well as longterm impacts on the health care system and economy.