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Novel polymeric micelles for drug delivery: Material characterization and formulation screening. | LitMetric

AI Article Synopsis

  • A growing number of poorly water-soluble new chemical entities are being discovered in drug development, prompting the use of polymeric micelles made from block copolymers for better delivery of these lipophilic drugs.
  • Researchers established a screening method to synthesize seven different block copolymers (BP001 to BP007), varying in composition, surface properties, and lipophilicity, and characterized them using H(1)-NMR and SEC methods.
  • The study found that micelles, primarily composed of BP006 and BP007, had a suitable size and strong drug-polymer interactions, leading to enhanced performance and controlled release of dexamethasone, with a half-life of 11 hours in human plasma.

Article Abstract

A rising number of new chemical entities that exhibit only poor aqueous solubility are identified in drug discovery processes. Polymeric micelles composed of block copolymers (BP) facilitate the delivery of such lipophilic molecules in drug therapy. Consequently, a rational screening and selection procedure for novel BP was established. Further, the interplay of polymer structure, micelle formation and drug binding was studied. Therefore seven polymers (BP001 to BP007) were synthesized from different monomer compositions resulting in nanocarriers varying in surface decoration and lipophilicity. These polymers were characterized by H(1)-NMR and SEC. The molecular weight was ranging between 13 and 37kDa. The critical micelle concentration and micellar integrity in presence of human plasma were determined. Micelles were loaded with dexamethasone and characterized with regards to their size, morphology and surface charge. Polymeric micelles with a size of 49.21-236.37nm were obtained. A half-life of 11h was determined for five of the copolymers in presence of human plasma. Two nanocarrier formulations (BP006 and BP007) were exhibiting optimal micellar integrity in vitro and a modified release profile under biorelevant conditions. Strongest drug-polymer interaction was observed for nanocarrier compositions providing benzyl and carboxylic groups and were composed of BP006 and BP007.

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Source
http://dx.doi.org/10.1016/j.ijpharm.2016.05.029DOI Listing

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