Shuaishuai Yuan

Fabricating a Cycloolefin Polymer Immunoassay Platform with a Dual-Function Polymer Brush via a Surface-Initiated Photoiniferter-Mediated Polymerization Strategy

The development of technologies for a biomedical detection platform is critical to meet the global challenges of various disease diagnoses. In this study, an inert cycloolefin polymer (COP) support was modified with two-layer polymer brushes possessing dual functions, i.e., a low fouling poly[poly(ethylene glycol) methacrylate] [p(PEGMA)] bottom layer and a poly(acrylic acid) (PAA) upper layer for antibody loading, via a surface-initiated photoiniferter-mediated polymerization strategy for fluorescence-based immunoassay. It was demonstrated through a confocal laser scanner that, for the as-prepared COP-g-PEG-b-PAA-IgG supports, nonspecific protein adsorption was suppressed, and the resistance to nonspecific protein interference on antigen recognition was significantly improved, relative to the COP-g-PAA-IgG references. This strategy for surface modification of a polymeric platform is also applicable to the fabrication of other biosensors.

Nuclease-Functionalized Poly(Styrene-b-isobutylene-b-styrene) Surface with Anti-Infection and Tissue Integration Bifunctions

Hydrophobic thermoplastic elastomers, e.g., poly(styrene-b-isobutylene-b-styrene) (SIBS), have found various in vivo biomedical applications. It has long been recognized that biomaterials can be adversely affected by bacterial contamination and clinical infection. However, inhibiting bacterial colonization while simultaneously preserving or enhancing tissue-cell/material interactions is a great challenge. Herein, SIBS substrates were functionalized with nucleases under mild conditions, through polycarboxylate grafts as intermediate. It was demonstrated that the nuclease-modified SIBS could effectively prevent bacterial adhesion and biofilm formation. Cell adhesion assays confirmed that nuclease coatings generally had no negative effects on L929 cell adhesion, compared with the virgin SIBS reference. Therefore, the as-reported nuclease coating may present a promising approach to inhibit bacterial infection, while preserving tissue-cell integration on polymeric biomaterials.

Facile Fabrication of Lubricant-Infused Wrinkling Surface for Preventing Thrombus Formation and Infection

Despite the advanced modern biotechniques, thrombosis and bacterial infection of biomedical devices remain common complications that are associated with morbidity and mortality. Most antifouling surfaces are in solid form and cannot simultaneously fulfill the requirements for antithrombosis and antibacterial efficacy. In this work, we present a facile strategy to fabricate a slippery surface. This surface is created by combining photografting polymerization with osmotically driven wrinkling that can generate a coarse morphology, and followed by infusing with fluorocarbon liquid. The lubricant-infused wrinkling slippery surface can greatly prevent protein attachment, reduce platelet adhesion, and suppress thrombus formation in vitro. Furthermore, E. coli and S. aureus attachment on the slippery surfaces is reduced by ∼98.8% and ∼96.9% after 24 h incubation, relative to poly(styrene-b-isobutylene-b-styrene) (SIBS) references. This slippery surface is biocompatible and has no toxicity to L929 cells. This surface-coating strategy that effectively reduces thrombosis and the incidence of infection will greatly decrease healthcare costs.

Liquid-Infused Poly(styrene-b-isobutylene-b-styrene) Microfiber Coating Prevents Bacterial Attachment and Thrombosis

Infection and thrombosis associated with medical implants cause significant morbidity and mortality worldwide. As we know, current technologies to prevent infection and thrombosis may cause severe side effects. To overcome these complications without using antimicrobial and anticoagulant drugs, we attempt to prepare a liquid-infused poly(styrene-b-isobutylene-b-styrene) (SIBS) microfiber coating, which can be directly coated onto medical devices. Notably, the SIBS microfiber was fabricated through solution blow spinning. Compared to electrospinning, the solution blow spinning method is faster and less expensive, and it is easy to spray fibers onto different targets. The lubricating liquids then wick into and strongly adhere the microfiber coating. These slippery coatings can effectively suppress blood cell adhesion, reduce hemolysis, and inhibit blood coagulation in vitro. In addition, Pseudomonas aeruginosa (P. aeruginosa) on the lubricant infused coatings slides readily, and no visible residue is left after tilting. We furthermore confirm that the lubricants have no effects on bacterial growth. The slippery coatings are also not cytotoxic to L929 cells. This liquid-infused SIBS microfiber coating could reduce the infection and thrombosis of medical devices, thus benefiting human health.

Enhanced biocompatibility of biostable poly(styrene-b-isobutylene-b-styrene) elastomer via poly(dopamine)-assisted chitosan/hyaluronic acid immobilization

The biostable poly(styrene-b-isobutylene-b-styrene) (SIBS) elastomers are well-known for their large-scale in vivo application as drug-eluting coatings in coronary stents. In this study, the SIBS elastomers were modified with a poly(dopamine) (PDA) adherent layer, followed by integrating both chitosan (CS) and hyaluronic acid (HA) onto their surfaces. The as-prepared samples (SIBS-CS-g-HA) presented excellent cytocompatibility because CS facilitates cell attachment and HA enhances cell proliferation. The initial adhesion test of E. coli on SIBS-CS-g-HA showed effective antiadhesive properties. The in vitro antibacterial test confirmed that SIBS-CS-g-HA has good antibacterial activity.

Infection-resistant styrenic thermoplastic elastomers that can switch from bactericidal capability to anti-adhesion

Styrenic thermoplastic elastomers (STPEs), particularly for poly(styrene-b-isobutylene-b-styrene) (SIBS), have aroused great interest in the indwelling and implant applications. However, the biomaterial-associated infection is a great challenge for these hydrophobic elastomers. Here, benzyl chloride (BnCl) groups are initially introduced into the SIBS backbone via Friedel-Crafts chemistry, followed by reaction with methyl 3-(dimethylamino) propionate (MAP) to obtain a cationic carboxybetaine ester-modified elastomer. The as-prepared elastomer is able to kill bacteria efficiently, while upon the hydrolysis of carboxybetaine esters into zwitterionic groups, the resultant surface has antifouling performances against proteins, platelets, erythrocytes, and bacteria. This STPE that switches from bactericidal efficacy during storage to the antifouling property in service has great potential in biomedical applications, and is generally applicable to the other styrene-based polymers.

Surface functionalization of styrenic block copolymer elastomeric biomaterials with hyaluronic acid via a “grafting to” strategy

As a biostable elastomer, the hydrophobicity of styrenic block copolymer (SBC) intensely limits its biomedical applications. In order to overcome such shortcoming, the SBC films were grafted with hyaluronic acid (HA) using a coupling agent. The surface chemistry of the modified films was examined by ATR-FTIR and XPS techniques, and the surface morphology was visually described by AFM. The biological performances of the HA-modified films were evaluated by a series of experiments, such as protein adsorption, platelet adhesion, and in vitro cytocompatibility. It was found that the HA-modified samples showed a low adhesiveness to fibroblast at the initial stage; however, it stimulated the growth of fibroblast. The L929 fibroblast growth presented a strong dependence on the molecular weight (MW) of HA. The samples modified with 17kDa HA exhibited the worst wettability and platelet adhesion, while providing the best results of supporting fibroblast proliferation.

A hierarchical polymer brush coating with dual-function antibacterial capability

Bacterial infections are problematic in many healthcare-associated devices. Antibacterial surfaces integrating the strength of bacteria repellent and bactericidal functions exhibit an encouraging efficacy in tackling this problem. Herein, a hierarchical dual-function antibacterial polymer brush coating that integrates an antifouling bottom layer with a bactericidal top layer is facilely constructed via living photograft polymerization. Excellent resistance to bacterial attachment is correlated with the antifouling components, and good bactericidal activity is afforded by the bactericidal components, and therefore the hierarchical coating shows an excellent long-term antibacterial capability. In addition, due to the presence of the hydrophilic background layer, the hierarchical surface has the greatly improved biocompatibility, as shown by the suppression of platelet adhesion and activation, the inhibition of erythrocyte adhesion and damage, and low toxicity against mammalian cells. The hierarchical polymer brush system provides the basis for the development of long-term antibacterial and biocompatible surfaces.

Surface modification of cycloolefin polymer via surface-initiated photoiniferter-mediated polymerization for suppressing bioadhesion

Inert cycloolefin polymers (COPs), which possess excellent optical properties, are a series of ideal materials for fabricating cheap disposable biosensor platforms. However, their antibioadhesion properties are expected to be improved prior to their application as biosensor supports. In this study, for the first time the COP supports were modified with well-controlled neutral, anionic and cationic polymer brushes via surface-initiated photoiniferter-mediated polymerization. This graft polymerization was confirmed by infrared spectroscopy, and X-ray photoelectron spectroscopy. The antibioadhesion properties of the modified supports were evaluated through a series of biological experiments. It was found that among these modified samples, the anionic poly(2-carboxyethyl acrylate)-modified COP supports presented the best antibioadhesion performances, i.e., suppressing protein adsorption, platelet adhesion and red blood cell attachment.