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The role of lipid geometry in designing liposomes for the solubilisation of poorly water soluble drugs. | LitMetric

AI Article Synopsis

  • Liposomes are effective for delivering both water-soluble and low-solubility drugs, serving as solubilising agents and drug targeting agents.
  • Research focused on how bilayer packaging, influenced by alkyl chain length and symmetry, affects drug solubilisation in liposomes.
  • Findings showed that liposomes made from longer chain, saturated lipids enhance drug loading capacity, while the size of the drug, rather than its lipophilicity, significantly impacts how well it can be incorporated into the bilayer.

Article Abstract

Liposomes are well recognised for their ability to improve the delivery of a range of drugs. More commonly they are applied for the delivery of water-soluble drugs, but given their structural attributes, they can also be employed as solubilising agents for low solubility drugs as well as drug targeting agents. To further explore the potential of liposomes as solubilising agents, we have investigated the role of bilayer packaging in promoting drug solubilisation in liposome bilayers. The effect of alkyl chain length and symmetry was investigated to consider if using 'mis-matched' phospholipids could create 'voids' within the bilayers, and enhance bilayer loading capacity. Lipid packing was investigated using Langmuir studies, which demonstrated that increasing the alkyl chain length enhanced lipid packing, with condensed monolayers forming, whilst asymmetric lipids formed less condensed monolayers. However, this more open packing did not translate into improved drug loading, with the longer chain, condensed bilayers formed from long-chain, saturated lipids offering higher drug loading capacity. These studies demonstrate that liposomes formulated from longer chain, saturated lipids offer enhanced solubilisation capacity. However the molecular size, rather than lipophilicity, of the drug to be incorporated was also a key factor dominating bilayer incorporation efficiency.

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Source
http://dx.doi.org/10.1016/j.ijpharm.2012.06.056DOI Listing

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