Selected article for: "cell receptor and Env protein"

Author: Lee, Jeong Hyun; Hu, Joyce K.; Georgeson, Erik; Nakao, Catherine; Groschel, Bettina; Dileepan, Thamotharampillai; Jenkins, Marc K.; Seumois, Gregory; Vijayanand, Pandurangan; Schief, William R.; Crotty, Shane
Title: Modulating the quantity of HIV Env-specific CD4 T cell help promotes rare B cell responses in germinal centers
  • Cord-id: tni20p0t
  • Document date: 2020_12_23
  • ID: tni20p0t
    Snippet: Immunodominance to nonneutralizing epitopes is a roadblock in designing vaccines against several diseases of high interest. One hypothetical possibility is that limited CD4 T cell help to B cells in a normal germinal center (GC) response results in selective recruitment of abundant, immunodominant B cells. This is a central issue in HIV envelope glycoprotein (Env) vaccine designs, because precursors to broadly neutralizing epitopes are rare. Here, we sought to elucidate whether modulating the qu
    Document: Immunodominance to nonneutralizing epitopes is a roadblock in designing vaccines against several diseases of high interest. One hypothetical possibility is that limited CD4 T cell help to B cells in a normal germinal center (GC) response results in selective recruitment of abundant, immunodominant B cells. This is a central issue in HIV envelope glycoprotein (Env) vaccine designs, because precursors to broadly neutralizing epitopes are rare. Here, we sought to elucidate whether modulating the quantity of T cell help can influence recruitment and competition of broadly neutralizing antibody precursor B cells at a physiological precursor frequency in response to Env trimer immunization. To do so, two new Env-specific CD4 transgenic (Tg) T cell receptor (TCR) mouse lines were generated, carrying TCR pairs derived from Env-protein immunization. Our results suggest that CD4 T cell help quantitatively regulates early recruitment of rare B cells to GCs.

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