The cyclic polymer topology strongly alters the interfacial, physico-chemical properties of polymer brushes, when compared to the linear counterparts. In this study, we especially concentrated on poly-2-ethyl-2-oxazoline (PEOXA) cyclic and linear grafts assembled on titanium oxide surfaces by the "grafting-to" technique. The smaller hydrodynamic radius of ring PEOXAs favors the formation of denser brushes with respect to linear analogs. Denser and more compact cyclic brushes generate a steric barrier that surpasses the typical entropic shield by a linear brush. This phenomenon, translates into an improved resistance towards biological contamination from different protein mixtures. Moreover, the enhancement of steric stabilization coupled to the intrinsic absence of chain ends by cyclic brushes, produce surfaces displaying a super-lubricating character when they are sheared against each other. All these topological effects pave the way for the application of cyclic brushes for surface functionalization, enabling the modulation of physico-chemical properties that could be just marginally tuned by applying linear grafts.
The application of polymer “brushes”, with their unique physicochemical properties, has led to a radical change in the way we functionalize biomaterials or formulate hybrids; however, their attractive traits can be largely surpassed by applying different polymer topologies, beyond the simple linear chain. Cyclic and loop brushes provide enhanced steric stabilization, improved biopassivity, and lubrication compared to their linear analogues. Focusing on poly(2-ethyl-2-oxazoline) (PEOXA), an emerging polymer in nanobiotechnology, we systematically investigate how topology effects determine the structure of PEOXA brushes and to what extent technologically relevant properties such as protein resistance, nanomechanics, and nanotribology can be tuned by varying brush topology. The highly compact structure of cyclic PEOXA brushes confers an augmented entropic barrier to the surface, efficiently hindering unspecific interactions with biomolecules. Moreover, the intrinsic absence of chain ends at the cyclic-brush interface prevents interdigitation when two identical polymer layers are sheared against each other, dramatically reducing friction. Loop PEOXA brushes present structural and interfacial characteristics that are intermediate between those of linear and cyclic brushes, which can be precisely tuned by varying the relative concentration of loops and tails within the assembly. Such topological control allows biopassivity to be progressively increased and friction to be tuned.
Three-dimensional (3D) control over the placement of bioactive cues is fundamental to understand cell guidance and develop engineered tissues. Two-photon patterning (2PP) provides such placement at micro-to millimeter scale, but non-specific interactions between proteins and functionalized extracellular matrices (ECMs) restrict its use. Here we report a 2PP system based on non-fouling hydrophilic photocages and Sortase A-based enzymatic coupling offering unprecedented orthogonality and signal-to-noise ratio in both inert hydrogels and complex mammalian matrices. Improved photocaged peptide synthesis, and protein functionalization protocols with broad applicability are introduced. Importantly, the method enables 2PP in a single step and in the presence of fragile biomolecules and cells. As a corollary, we demonstrate the guidance of axons through 3D-patterned nerve growth factor (NGF) within brain-mimetic ECMs. Our approach allows for the interrogation of the role of complex signaling molecules in 3D matrices, thus helping to better understand biological guidance in tissue development and regeneration.
Bilayer films featuring cyclic, poly(2-alkyl-2-oxazoline) brush interfaces display excellent biopassivity, lubrication and long-term stability in chemically harsh aqueous environments.
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