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Polyurea-urethane Temperature-responsive Hydrogels for Sustained Delivery of Anti-VEGF Therapeutics. | LitMetric

Polyurea-urethane Temperature-responsive Hydrogels for Sustained Delivery of Anti-VEGF Therapeutics.

Chem Asian J

Institute of Materials Research and Engineering (IMRE), Agency for Science, Technology and Research (A*STAR) #08-03, 2 Fusionopolis Way, Singapore, Singapore, 138634, Republic of Singapore.

Published: September 2024

AI Article Synopsis

  • Temperature-responsive hydrogels, known as thermogels, are effective for delivering both small drugs and larger biological therapeutics, with properties influenced by the polymer's hydrophilic-hydrophobic balance and molecular characteristics.
  • A new study focused on enhancing hydrogen bonding by creating amphiphilic polymers with urea linkages, leading to improved hydration and better gel properties, such as phase transition temperature and stiffness.
  • Results indicated that these urea linkages significantly changed the drug release profile of Aflibercept, showcasing the potential to optimize drug delivery outcomes by adjusting hydrogen bonding in polymer structures.

Article Abstract

Temperature-responsive hydrogels, or thermogels, have emerged as a leading platform for sustained delivery of both small molecule drugs and macromolecular biologic therapeutics. Although thermogel properties can be modulated by varying the polymer's hydrophilic-hydrophobic balance, molecular weight and degree of branching, varying the supramolecular donor-acceptor interactions on the polymer remains surprisingly overlooked. Herein, to study the influence of enhanced hydrogen bonding on thermogelation, we synthesized a family of amphiphilic polymers containing urea and urethane linkages using quinuclidine as an organocatalyst. Our findings showed that the presence of strongly hydrogen bonding urea linkages significantly enhanced polymer hydration in water, in turn affecting hierarchical polymer self-assembly and macroscopic gel properties such as sol-gel phase transition temperature and gel stiffness. Additionally, analysis of the sustained release profiles of Aflibercept, an FDA-approved protein biologic for anti-angiogenic treatment, showed that urea bonds on the thermogel were able to significantly alter the drug release mechanism and kinetics compared to usage of polyurethane gels of similar composition and molecular weight. Our findings demonstrate the unrealized possibility of modulating gel properties and outcomes of sustained drug delivery through judicious variation of hydrogen bonding motifs on the polymer structure.

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Source
http://dx.doi.org/10.1002/asia.202400453DOI Listing

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