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Isolation and characterization of new human carrier peptides from two important vaccine immunogens
Institution:1. Department of Chemistry “Ugo Schiff”, University of Florence, Sesto Fiorentino, Florence, Italy;2. Harvard Medical School Department of Immunology, Blavatnik Institute, Boston, MA, United States;3. Department of Chemistry and CRC Polymeric Materials (LaMPo), University of Milan, Milano, Italy
Abstract:In the preparation of glycoconjugate vaccines in clinical practice, two highly immunogenic carrier proteins, CRM197 and tetanus toxoid (TT), are predominantly conjugated with the capsular polysaccharides (CPSs) of bacterial pathogens. In addition, TT has long been used as an effective vaccine to prevent tetanus. While these carrier proteins play an important role in immunogenicity and vaccine design alike, their defined human major histocompatibility complex class II (MHCII) T cell epitopes are inadequately characterized. In this current work, we use mass spectrometry to identify the peptides from these carrier proteins that are naturally processed and presented by human B cells via MHCII pathway. The MHCII-presented peptides are screened for their T cell stimulation using primary CD4+ T cells from four healthy adult donors. These combined methods reveal a subset of eleven CD4+ T cell epitopes that proliferate and stimulate human T cells with diverse MHCII allelic repertoire. Six of these peptides stand out as potential immunodominant epitopes by responding in three or more donors. Additionally, we provide evidence of these natural epitopes eliciting more significant T cell responses in donors than previously published TT peptides selected from T cell epitope screening. This study serves toward understanding carrier protein immune responses and thus enables the use of these peptides in developing novel knowledge-based vaccines to combat persisting problems in glycoconjugate vaccine design.
Keywords:Tetanus toxoid  MHC class II  T cell  B cell  Glycoconjugate vaccines  Carrier protein
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