Materials from peptide assembly: towards the treatment of cancer and transmittable disease.

As the prevalence of cancer and transmittable disease persists, the development of new and more advanced therapies remains a priority in medical research. An emerging platform for the treatment of these illnesses is the use of materials formed via peptide assembly where the bulk material itself acts as the therapeutic. Higher ordered peptide structures with defined chemistry are capable of cellular targeting, recognition, and internalization.

The effect of protein structure on their controlled release from an injectable peptide hydrogel.

Hydrogel materials are promising vehicles for the delivery of protein therapeutics. Proteins can impart physical interactions, both steric and electrostatic in nature, that influence their release from a given gel network. Here, model proteins of varying hydrodynamic diameter and charge are directly encapsulated and their release studied from electropositive fibrillar hydrogels prepared from the self-assembling peptide, MAX8.

Sequence-dependent gelation kinetics of β-hairpin peptide hydrogels.

The gelation kinetics of four β-hairpin oligopeptides that have been designed to exhibit responsive behavior to changes in environmental conditions, such as pH, ionic strength and temperature, are characterized using multiple particle tracking microrheology and circular dichroism (CD) spectroscopy. The peptides, predominantly an alternating sequence of valine and lysine residues, differ by a point substitution of a single amino acid near a type II'β-turn sequence. The rate of gelation becomes faster for point substitutions which reduce the total charge of the peptide.

Fast dynamics of semiflexible chain networks of self-assembled peptides.

We present the first neutron spin echo (NSE) measurements of self-assembling peptide hydrogel networks to study the fibril dynamics on the nanometer and nanosecond length and time scales. MAX1 and MAX8 are synthetic beta-hairpin peptides that undergo triggered self-assembly at the nanoscale to form a physically cross-linked network of fibrils with a defined cross-section. When subjected to physiological pH and ionic strength (pH 7.

Macromolecular diffusion and release from self-assembled beta-hairpin peptide hydrogels.

Self-assembling peptide hydrogels are used to directly encapsulate and controllably release model FITC-dextran macromolecules of varying size and hydrodynamic diameters. MAX1 and MAX8 are two peptide sequences with different charge states that have been designed to intramolecularly fold and self assemble into hydrogels at physiological buffer conditions (pH 7.4, 150 mM NaCl).

Correlations between structure, material properties and bioproperties in self-assembled beta-hairpin peptide hydrogels.

A de novo designed beta-hairpin peptide (MAX8), capable of undergoing intramolecular folding and consequent intermolecular self-assembly into a cytocompatible hydrogel, has been studied. A combination of small angle neutron scattering (SANS) and cryogenic-transmission electron microscopy (cryo-TEM) have been used to quantitatively investigate the MAX8 nanofibrillar hydrogel network morphology. A change in the peptide concentration from 0.

Self-assembling materials for therapeutic delivery.

A growing number of medications must be administered through parenteral delivery, i.e., intravenous, intramuscular, or subcutaneous injection, to ensure effectiveness of the therapeutic.