Modulating adaptive immune responses to peptide self-assemblies

Jai S. Rudra, Tao Sun, Katelyn C. Bird, Melvin D. Daniels, Joshua Z. Gasiorowski, Anita S. Chong, Joel H. Collier

Research output: Contribution to journalArticlepeer-review

237 Scopus citations


Self-assembling peptides and peptide derivatives have received significant interest for several biomedical applications, including tissue engineering, wound healing, cell delivery, drug delivery, and vaccines. This class of materials has exhibited significant variability in immunogenicity, with many peptides eliciting no detectable antibody responses but others eliciting very strong responses without any supplemental adjuvants. Presently, strategies for either avoiding strong antibody responses or specifically inducing them are not well-developed, even though they are critical for the use of these materials both within tissue engineering and within immunotherapies. Here, we investigated the molecular determinants and immunological mechanisms leading to the significant immunogenicity of the self-assembling peptide OVA-Q11, which has been shown previously to elicit strong antibody responses in mice. We show that these responses can last for at least a year. Using adoptive transfer experiments and T cell knockout models, we found that these strong antibody responses were T cell-dependent, suggesting a route for avoiding or ensuring immunogenicity. Indeed, by deleting amino acid regions in the peptide recognized by T cells, immunogenicity could be significantly diminished. Immunogenicity could also be attenuated by mutating key residues in the self-assembling domain, thus preventing fibrillization. A second self-assembling peptide, KFE8, was also nonimmunogenic, but nanofibers of OVA-KFE8 elicited strong antibody responses similar to OVA-Q11, indicating that the adjuvant action was not dependent on the specific self-assembling peptide sequence. These findings will facilitate the design of self-assembled peptide biomaterials, both for applications where immunogenicity is undesirable and where it is advantageous.

Original languageEnglish
Pages (from-to)1557-1564
Number of pages8
JournalACS nano
Issue number2
StatePublished - Feb 28 2012


  • biomaterial
  • scaffold
  • self-assembly
  • tissue engineering
  • vaccine


Dive into the research topics of 'Modulating adaptive immune responses to peptide self-assemblies'. Together they form a unique fingerprint.

Cite this