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Modulation of Phospholipase A 2 Membrane Activity by Anti-inflammatory Drugs.

Angela M Jaramillo-GranadaJinhui LiAneliza Flores VillarrealOmar LozanoJesus Carlos Ruiz-SuárezViviana Monje-GalvanFrancisco J Sierra-Valdez
Published in: Langmuir : the ACS journal of surfaces and colloids (2024)
The phospholipase A 2 (PLA 2 ) superfamily consists of lipolytic enzymes that hydrolyze specific cell membrane phospholipids and have long been considered a central hub of biosynthetic pathways, where their lipid metabolites exert a variety of physiological roles. A misregulated PLA 2 activity is associated with mainly inflammatory-derived pathologies and thus has shown relevant therapeutic potential. Many natural and synthetic anti-inflammatory drugs (AIDs) have been proposed as direct modulators of PLA 2 activity. However, despite the specific chemical properties that these drugs share in common, little is known about the indirect modulation able to finely tune membrane structural changes at the precise lipid-binding site. Here, we use a novel experimental strategy based on differential scanning calorimetry to systematically study the structural properties of lipid membrane systems during PLA 2 cleavage and under the influence of several AIDs. For a better understanding of the AIDs-membrane interaction, we present a comprehensive and comparative set of molecular dynamics (MD) simulations. Our thermodynamic results clearly demonstrate that PLA 2 cleavage is hindered by those AIDs that significantly reduce the lipid membrane cooperativity, while the rest of the AIDs oppositely tend to catalyze PLA 2 activity to different extents. On the other hand, our MD simulations support experimental results by providing atomistic details on the binding, insertion, and dynamics of each AID on a pure lipid system; the drug efficacy to impact membrane cooperativity is related to the lipid order perturbation. This work suggests a membrane-based mechanism of action for diverse AIDs against PLA 2 activity and provides relevant clues that must be considered in its modulation.
Keyphrases
  • molecular dynamics
  • fatty acid
  • antiretroviral therapy
  • anti inflammatory drugs
  • density functional theory
  • emergency department
  • molecular dynamics simulations
  • transcription factor