Themed collection Peptide Materials

This review describes recent progress in the area of molecular simulations of peptide assemblies, including peptide-amphiphiles, and drug-amphiphiles.

Living systems contain remarkable functional capability built within sophisticated self-organizing frameworks.

Self-assembling peptide and peptide conjugates have attracted great attention due to their biocompatibility, biodegradability and biofunctionality. This review covers self-assembly of amphiphilic peptides and peptide mimetic materials, as well as their potential applications.

Three peptides that are compositionally identical but sequentially distinct have been designed to study the impact of morphology and hydrophobicity on heme coordination and function.

Collagen mimetic peptides bind to a variety of fiber-forming proteins through complementary hydrophobic interactions, resulting in discs-on-a-string nanostructures and bundling of fibers.

An immunoreceptor tyrosine-based inhibitory motif (ITIM), LYYYYL, as well as its enantiomeric or retro-inverso peptide, self-assembles in water upon enzymatic dephosphorylation, thus illustrating a new approach to design bioinspired soft materials from an important pool of functional peptides.

The display of functional proteins on self-assembled peptide nanofibrils is accomplished by noncovalent attachment using a split-protein strategy.

The synthesis and self-assembly of amphiphilic copolypeptides containing a recombinant elastin-like polypeptide block used as a macroinitiator for the ROP of γ-BLG NCA are presented.

Tailored physical interactions were utilized to tune hierarchical organization and mechanical response in peptide-polymer hybrids.

Complex coacervation is a widely utilized technique for effecting phase separation, though predictive understanding of molecular-level details remains underdeveloped.

Self-assembly of ultra short peptide into proteolytically stable drug carriers.

Coarse grained molecular dynamic simulations demonstrate that interactions between species in dynamic peptide libraries can cause a disrupting self-assembly effect that affects the possible discovery of new materials.

Hydrophobic dipeptide molecules can be used to create interfacial films covering bubbles and droplets made from a range of oils.

This work is showing the ability to control the kinetics of peptide assembly while leaving both the designed α-helical and tetrameric helical bundle intact.

Fmoc-L-DOPA-D-Oxd-OH was prepared starting from commercially available L-DOPA. Its gelation ability was tested by comparison with Fmoc-L-Tyr-D-Oxd-OH and Fmoc-L-Phe-D-Oxd-OH using ten different triggers.

Coarse-grained molecular simulations reveal the influence of pH and flow on the self-assembly of DFAG-OPV3-GAFD optoelectronic peptides.

Silica-specific motifs templated into fibre-forming peptides effectively silicify protein fibres.

Multi-responsive polypeptide-based hydrogels exhibited thermo-, mechano-, and enzyme-responsive properties, enabling performance as a delivery system for encapsulation and release of naproxen.

Through balancing the relative repulsive and attractive intermolecular forces, self-assembling peptide amphiphiles with different sizes but similar pH- and concentration-dependent self-assembly behaviour are created.

A β-annulus-coiled-coil-B peptide self-assembled into an artificial viral capsid and then the addition of a complementary coiled-coil-A peptide showed the formation of capsids with coiled-coil spikes on the surface.

Carbohydrate structures of peptide–carbohydrate conjugates have a noticeable effect on the morphology of self-assembled structures.