Total synthesis of the natural, medium-length, peptaibol pentadecaibin and study of the chemical features responsible for its membrane activity

Laura Morbiato; David S A Haneen; Fernando Formaggio; Marta De Zotti

doi:10.1002/psc.3479

Total synthesis of the natural, medium-length, peptaibol pentadecaibin and study of the chemical features responsible for its membrane activity

J Pept Sci. 2023 Aug;29(8):e3479. doi: 10.1002/psc.3479. Epub 2023 Jan 27.

Authors

Laura Morbiato¹, David S A Haneen², Fernando Formaggio^{1

3}, Marta De Zotti^{1

3}

Affiliations

¹ Department of Chemical Sciences, University of Padova, Padova, Italy.
² Chemistry Department, Faculty of Science, Ain Shams University, Cairo, Abbassia, 11566, Egypt.
³ Padova Unit, CNR Institute of Biomolecular Chemistry, University of Padova, Padova, Italy.

PMID: 36652104
DOI: 10.1002/psc.3479

Abstract

Peptaibols are naturally occurring, antimicrobial peptides endowed with well-defined helical conformations and resistance to proteolysis. Both features stem from the presence in their sequence of several, C^α -tetrasubstituted, α-aminoisobutyric acid (Aib) residues. Peptaibols interact with biological membranes, usually causing their leakage. All of the peptaibol-membrane interaction mechanisms proposed so far begin with peptide aggregation or accumulation. The long-length alamethicin, the most studied peptaibol, acts by forming pores in the membranes. Conversely, the carpet mechanism has been claimed for short-length peptaibols, such as trichogin. The mechanism of medium-length peptaibols is far less studied, and this is partly due to the difficulties of their synthesis. They are believed to perturb membrane permeability in different ways, depending on the membrane properties. The present work focuses on pentadecaibin, a recently discovered, medium-length peptaibol. In contrast to the majority of its family members, its sequence does not comprise hydroxyprolines or prolines, and its helix is not kinked. A reliable and effective synthesis procedure is described that allowed us to produce also two shorter analogs. By a combination of techniques, we were able to establish a 3D-structure-activity relationship. In particular, the membrane activity of pentadecaibin heavily depends on the presence of three consecutive Aib residues that are responsible for the clear, albeit modest, amphiphilic character of its helix. The shortest analog, devoid of two of these three Aib residues, preserves a well-defined helical conformation, but not its amphipathicity, and loses almost completely the ability to cause membrane leakage. We conclude that pentadecaibin amphiphilicity is probably needed for the peptide ability to perturb model membranes.

Keywords: amphiphilicity; helical conformation; peptaibol; peptide-membrane interaction.

MeSH terms

Alamethicin* / analysis
Alamethicin* / chemistry
Alamethicin* / metabolism
Anti-Bacterial Agents / chemistry
Anti-Bacterial Agents / pharmacology
Biological Transport
Cell Membrane / chemistry
Molecular Conformation
Peptaibols* / analysis
Peptaibols* / chemistry
Peptaibols* / metabolism

Substances

Peptaibols
Alamethicin
Anti-Bacterial Agents

Abstract

MeSH terms

Substances

Grants and funding