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Persistent antigen exposure via the eryptotic pathway drives terminal T cell dysfunction

Sci Immunol. 2021-02; 
Elyse A Watkins, Jennifer T Antane, Jaeda L Roberts, Kristen M Lorentz, Sarah Zuerndorfer, Anya C Dunaif, Lucas J Bailey, Andrew C Tremain, Mindy Nguyen, Roberto C De Loera, Rachel P Wallace, Rachel K Weathered, Stephan Kontos, Jeffrey A Hubbell
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Custom Vector Construction … For Fab payload sequences, such as OVA, DNA was purchased from Genscript and cloned into the HEK vectors at the C terminus of the heavy chain. Amino acid sequence of A8B1 heavy and light chains, as well as antigens, can be found in table S3. … Get A Quote

摘要

Although most current treatments for autoimmunity involve broad immunosuppression, recent efforts have aimed to suppress T cells in an antigen-specific manner to minimize risk of infection. One such effort is through targeting antigen to the apoptotic pathway to increase presentation of the antigen of interest in a tolerogenic context. Erythrocytes present a rational candidate to target because of their high rate of eryptosis, which facilitates continual uptake by antigen-presenting cells in the spleen. Here, we develop an approach that binds antigens to erythrocytes to induce sustained T cell dysfunction. Transcriptomic and phenotypic analyses revealed signatures of self-tolerance and exhaustion, including up-... More

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