Nature Communications (Nov 2024)

Exploration of the hierarchical assembly space of collagen-like peptides beyond the triple helix

  • Le Tracy Yu,
  • Mark A. B. Kreutzberger,
  • Thi H. Bui,
  • Maria C. Hancu,
  • Adam C. Farsheed,
  • Edward H. Egelman,
  • Jeffrey D. Hartgerink

DOI
https://doi.org/10.1038/s41467-024-54560-z
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 11

Abstract

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Abstract The de novo design of self-assembling peptides has garnered significant attention in scientific research. While alpha-helical assemblies have been extensively studied, exploration of polyproline type II helices, such as those found in collagen, remains relatively limited. In this study, we focus on understanding the sequence-structure relationship in hierarchical assemblies of collagen-like peptides, using defense collagen Surfactant Protein A as a model. By dissecting the sequence derived from Surfactant Protein A and synthesizing short collagen-like peptides, we successfully construct a discrete bundle of hollow triple helices. Amino acid substitution studies pinpoint hydrophobic and charged residues that are critical for oligomer formation. These insights guide the de novo design of collagen-like peptides, resulting in the formation of diverse quaternary structures, including discrete and heterogenous bundled oligomers, two-dimensional nanosheets, and pH-responsive nanoribbons. Our study represents a significant advancement in the understanding and harnessing of collagen higher-order assemblies beyond the triple helix.