Brandon L. Seal scite author profile

A rapidly forming polymer matrix with affinity-based controlled release properties was developed based upon interactions between heparin-binding peptides and heparin. Dynamic mechanical testing of 10% (w/v) compositions consisting of a 3:1 molar ratio of poly(ethylene glycol)-co-peptide (approximately 18,000 g/mol) to heparin (approximately 18,000 g/mol) revealed a viscoelastic profile similar to that of concentrated, large molecular weight polymer solutions and melts. In addition, the biopolymer mixtures recovered quickly following thermal denaturation and mechanical insult. These gel-like materials were able to sequester exogenous heparin-binding peptides and could release these peptides over several days at rates dependent on relative heparin affinity. The initial release rates ranged from 3.3% per hour for a peptide with low heparin affinity to 0.025% per hour for a peptide with strong heparin affinity. By altering the affinity of peptides to heparin, a series of peptides can be developed to yield a range of release profiles useful for controlled in vivo delivery of therapeutics.

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Hemocompatible Poly(NIPAm-MBA-AMPS) Colloidal Nanoparticles as Carriers of Anti-inflammatory Cell Penetrating Peptides

Bartlett

Medow

Panitch

et al. 2012

Biomacromolecules

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Anionic copolymer systems containing sulfated monomers have great potential for delivery of cationic therapeutics, but N-isopropylacrylamide (NIPAm) 2-acrylamido-2-methyl-1-propanesulfonic acid (AMPS) copolymer nanoparticles have seen limited characterization to date with regard to physical properties relevant to loading and release of therapeutics. Characterization of polymeric nanoparticles incorporating AMPS showed an increased size and decreased thermodynamic swelling ratios of AMPS containing particles as compared to NIPAm nanoparticles lacking AMPS. Particles with increasing AMPS addition showed an increased propensity for uniformity, intraparticle colloidal stability, and drug loading capacity. Peptide encapsulated in particles was shielded from peptide degradation in serum. Particles were shown not impede blood coagulation or to cause hemolysis. This study has demonstrated that AMPS incorporation into traditional NIPAm nanoparticles presents a tunable parameter for changing particle LCST, size, swelling ratio, ζ potential, and cationic peptide loading potential. This one-pot synthesis results in a thermosensitive anionic nanoparticle system that is a potentially useful platform to deliver cationic cell penetrating peptides.

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Viscoelastic Behavior of Environmentally Sensitive Biomimetic Polymer Matrices

Seal

Panitch

2006

Macromolecules

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By incorporating polysaccharide-peptide interactions into poly(ethylene glycol) hydrogels, we created a unique polymer matrix exhibiting characteristics imparted by both covalent and physical cross-links. Dynamic mechanical testing revealed that the properties of this system were sensitive to temperature changes and thermally reversible. At lower temperatures and higher frequencies, the elastic response was dominated by physical cross-links created by associations between heparin and heparin binding peptides; the matrices were stabilized by covalent cross-links at higher temperatures. Furthermore, the strength of the physical cross-links depended on the relative affinity between heparin and heparin binding peptides. This system could serve as a model to investigate how the presence of both physical and covalent cross-links influences the viscoelastic behavior of biomimetic polymeric materials.

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Tuning Cell Adhesion by Incorporation of Charged Silicate Nanoparticles as Cross‐Linkers to Polyethylene Oxide

Schexnailder

Gaharwar

Bartlett

et al. 2010

Macromolecular Bioscience

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Controlling cell adhesion on a biomaterial surface is associated with the long-term efficacy of an implanted material. Here we connect the material properties of nanocomposite films made from PEO physically cross-linked with layered silicate nanoparticles (Laponite) to cellular adhesion. Fibroblast cells do not adhere to pure PEO, but they attach to silicate containing nanocomposites. Under aqueous conditions, the films swell and the degree of swelling depends on the nanocomposite composition and film structure. Higher PEO compositions do not support cell proliferation due to little exposed silicate surfaces. Higher silicate compositions do allow significant cell proliferation and spreading. These bio-nanocomposites have potential for the development of biomedical materials that can control cellular adhesion.

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Brandon L. Seal

Polymeric biomaterials for tissue and organ regeneration

Physical Polymer Matrices Based on Affinity Interactions between Peptides and Polysaccharides

Hemocompatible Poly(NIPAm-MBA-AMPS) Colloidal Nanoparticles as Carriers of Anti-inflammatory Cell Penetrating Peptides

Viscoelastic Behavior of Environmentally Sensitive Biomimetic Polymer Matrices

Tuning Cell Adhesion by Incorporation of Charged Silicate Nanoparticles as Cross‐Linkers to Polyethylene Oxide

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