T cells control the generation of nanomolar-affinity anti-glycan antibodies.

نویسندگان

  • Zinaida Polonskaya
  • Shenglou Deng
  • Anita Sarkar
  • Lisa Kain
  • Marta Comellas-Aragones
  • Craig S McKay
  • Katarzyna Kaczanowska
  • Marie Holt
  • Ryan McBride
  • Valle Palomo
  • Kevin M Self
  • Seth Taylor
  • Adriana Irimia
  • Sanjay R Mehta
  • Jennifer M Dan
  • Matthew Brigger
  • Shane Crotty
  • Stephen P Schoenberger
  • James C Paulson
  • Ian A Wilson
  • Paul B Savage
  • M G Finn
  • Luc Teyton
چکیده

Vaccines targeting glycan structures at the surface of pathogenic microbes must overcome the inherent T cell-independent nature of immune responses against glycans. Carbohydrate conjugate vaccines achieve this by coupling bacterial polysaccharides to a carrier protein that recruits heterologous CD4 T cells to help B cell maturation. Yet they most often produce low- to medium-affinity immune responses of limited duration in immunologically fit individuals and disappointing results in the elderly and immunocompromised patients. Here, we hypothesized that these limitations result from suboptimal T cell help. To produce the next generation of more efficacious conjugate vaccines, we have explored a synthetic design aimed at focusing both B cell and T cell recognition to a single short glycan displayed at the surface of a virus-like particle. We tested and established the proof of concept of this approach for 2 serotypes of Streptococcus pneumoniae. In both cases, these vaccines elicited serotype-specific, protective, and long-lasting IgG antibodies of nanomolar affinity against the target glycans in mice. We further identified a requirement for CD4 T cells in the anti-glycan antibody response. Our findings establish the design principles for improved glycan conjugate vaccines. We surmise that the same approach can be used for any microbial glycan of interest.

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عنوان ژورنال:
  • The Journal of clinical investigation

دوره 127 4  شماره 

صفحات  -

تاریخ انتشار 2017