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Secondary Structure Tuning of a Pseudoprotein Between β-Meander and α-Helical Forms in the Solid-State.

Vignesh AthiyarathMithun C MadhusudhananSooraj KunnikuruvanKana M Sureshan
Published in: Angewandte Chemie (International ed. in English) (2021)
Tuning the secondary structure of a protein or polymer in the solid-state is challenging. Here we report the topochemical synthesis of a pseudoprotein and its secondary structure tuning in the solid-state. We designed the dipeptide monomer N3 -Leu-Ala-NH-CH2 -C≡CH (1) for topochemical azide-alkyne cycloaddition (TAAC) polymerization. Dipeptide 1 adopts an anti-parallel β-sheet-like stacked arrangement in its crystals. Upon heating, the dipeptide undergoes quantitative TAAC polymerization in a crystal-to-crystal fashion yielding large polymers. The reaction occurs between the adjacent monomers in the H-bonded anti-parallel stack, yielding pseudoprotein having a β-meander structure. When dissolved in methanol, this pseudoprotein changes its secondary structure from β-meander to α-helical form and it retains the new secondary structure upon desolvation. This work demonstrates a novel paradigm for tuning the secondary structure of a polymer in the solid-state.
Keyphrases
  • solid state
  • room temperature
  • high resolution
  • mass spectrometry
  • small molecule
  • amino acid
  • protein protein