Fibrin matrices: The versatile therapeutic delivery systems.

Int J Biol Macromol

Interdisciplinary Biotechnology Unit, Aligarh Muslim University, Aligarh 202002, India. Electronic address:

Published: November 2015

AI Article Synopsis

  • Fibrin sealants, traditionally used by surgeons to control bleeding, are now being explored for innovative drug delivery, especially for antibiotics.
  • Fibrinogen, derived from blood plasma, is converted into fibrin, which can be shaped into various forms like films, beads, and nanoparticles for therapeutic applications.
  • Techniques like binding drugs to the fibrin matrix and using liposomes can help control the release rates of these therapeutics, enhancing their effectiveness in medical treatments.

Article Abstract

Fibrin sealants, that have been employed for over a century by surgeons to stop post surgery bleeding, are finding novel applications in the controlled delivery of antibiotics and several other therapeutics. Fibrinogen can be easily purified from blood plasma and converted by thrombolysis to fibrin that undergoes spontaneous aggregation to form insoluble clot. During the gelling, fibrin can be formulated into films, clots, threads, microbeads, nanoconstructs and nanoparticles. Whole plasma clots in the form of beads and microparticles can also be prepared by activating endogenous thrombin, for possible drug delivery. Fibrin formulations offer remarkable scope for controlling the porosity as well as in vivo degradability and hence the release of the associated therapeutics. Binding/covalent-linking of therapeutics to the fibrin matrix, crosslinking of the matrix with bifunctional reagents and coentrapment of protease inhibitors have been successful in regulating both in vitro and in vivo release of the therapeutics. The release rates can also be remarkably lowered by preentrapment of therapeutics in insoluble particles like liposomes or by anchoring them to the matrix via molecules that bind them as well as fibrin.

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Source
http://dx.doi.org/10.1016/j.ijbiomac.2015.07.054DOI Listing

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