Multivesicular Liposomes for the Sustained Release of Angiotensin I-Converting Enzyme (ACE) Inhibitory Peptides from Peanuts: Design, Characterization, and In Vitro Evaluation

Molecules. 2019 May 5;24(9):1746. doi: 10.3390/molecules24091746.

Abstract

The multivesicular liposome (MVL) provides a potential delivery approach to avoid the destruction of the structure of drugs by digestive enzymes of the oral cavity and gastrointestinal system. It also serves as a sustained-release drug delivery system. In this study, we aimed to incorporate a water-soluble substance into MVLs to enhance sustained release, prevent the destruction of drugs, and to expound the function of different components and their mechanism. MVLs were prepared using the spherical packing model. The morphology, structure, size distribution, and zeta potential of MVLs were examined using an optical microscope (OM), confocal microscopy (CLSM), transmission electron cryomicroscope (cryo-EM) micrograph, a Master Sizer 2000, and a zeta sizer, respectively. The digestion experiment was conducted using a bionic mouse digestive system model in vitro. An in vitro release and releasing mechanism were investigated using a dialysis method. The average particle size, polydispersity index, zeta potential, and encapsulation efficiency are 47.6 nm, 1.880, -70.5 ± 2.88 mV, and 82.00 ± 0.25%, respectively. The studies on the controlled release in vitro shows that MVLs have excellent controlled release and outstanding thermal stability. The angiotensin I-converting enzyme (ACE) inhibitory activity of ACE-inhibitory peptide (AP)-MVLs decreased only 2.84% after oral administration, and ACE inhibitory activity decreased by 5.03% after passing through the stomach. Therefore, it could serve as a promising sustained-release drug delivery system.

Keywords: ACE; controlled-release; digestive stability; multivesicular liposomes; peanut peptide.

MeSH terms

  • Administration, Oral
  • Angiotensin-Converting Enzyme Inhibitors / chemistry
  • Angiotensin-Converting Enzyme Inhibitors / pharmacology*
  • Animals
  • Arachis / metabolism*
  • Delayed-Action Preparations
  • Digestive System / chemistry*
  • Drug Compounding
  • Drug Stability
  • Humans
  • Liposomes
  • Mice
  • Models, Biological
  • Particle Size
  • Peptides / chemistry
  • Peptides / pharmacology*
  • Peptidyl-Dipeptidase A
  • Solubility

Substances

  • Angiotensin-Converting Enzyme Inhibitors
  • Delayed-Action Preparations
  • Liposomes
  • Peptides
  • Peptidyl-Dipeptidase A