Understanding the Biophysical Interaction of LTX-315 with Tumoral Model Membranes

Host defense peptides are found primarily as natural antimicrobial agents among all lifeforms. These peptides and their synthetic derivatives have been extensively studied for their potential use as therapeutic agents. The most accepted mechanism of action of these peptides is related to a nonspecific mechanism associated with their interaction with the negatively charged groups present in membranes, inducing bilayer destabilization and cell death through several routes. Among the most recently reported peptides, LTX-315 has emerged as an important oncolytic peptide that is currently in several clinical trials against different cancer types. However, there is a lack of biophysical studies regarding LTX-315 and its interaction with membranes. This research focuses primarily on the understanding of the molecular bases of LTX-315 ' s interaction with eukaryotic lipids, based on two artificial systems representative of non-tumoral and tumoral membranes. Additionally, the interaction with individual lipids was studied by differential scanning calorimetry and Fourier-transformed infrared spectroscopy. The results showed a strong interaction of LTX-315 with the negatively charged phosphatidylserine. The results are important for understanding and facilitating the design and development of improved peptides with anticancer activity.

Automated summary

Host defense peptides are natural antimicrobial agents that have potential therapeutic use. LTX-315, a recently reported peptide, has shown promising oncolytic activity, but its interaction with membranes has not been well studied. This research investigated the interaction of LTX-315 with eukaryotic lipids using artificial systems, and found a strong interaction with phosphatidylserine. These findings contribute to the understanding and development of improved anticancer peptides.