Specific Binding of Streptavidin onto the Nonbiofouling Titanium/Titanium Oxide Surface through Surface-Initiated, Atom Transfer Radical Polymerization and Bioconjugation of Biotin

• Published in: Macromolecular research Vol. 17; no. 3; pp. 174 - 180
• Main Authors: Kang, Sung Min, Lee, Bong Soo, Kim, Wan-Joong, Choi, Insung S., Kil, Munjae, Jung, Hyuk-jun, Oh, Eugene
• Format: Journal Article
• Language: English
• Published: Berlin/Heidelberg 한국고분자학회 01.03.2009; Springer-Verlag
• Subjects: Characterization and Evaluation of Materials; Chemistry; Chemistry and Materials Science; Complex Fluids and Microfluidics; Nanochemistry; Nanotechnology; Physical Chemistry; Polymer Sciences; Soft and Granular Matter; 고분자공학; biological applications of polymers; atom transfer radical polymerization; Titanium/titanium oxide; titanium/titanium oxide
• ISSN: 1598-5032; 2092-7673
• DOI: 10.1007/BF03218675

Chemical modification of titanium/titanium oxide (Ti/TiO 2 ) substrates has recently gained a great deal of attention because of the applications of Ti/TiO 2 -based materials to biomedical areas. The reported modification methods generally involve passive coating of Ti/TiO 2 substrates with protein-resistant materials, and poly(ethylene glycol) (PEG) has proven advantageous for bestowing a nonbiofouling property on the surface of Ti/TiO 2 . However, the wider applications of Ti/TiO 2 -based materials to biomedical areas will require the introduction of biologically active moieties onto Ti/TiO 2 , in addition to nonbiofouling property. In this work, we therefore utilized surface-initiated polymerization to coat the Ti/TiO 2 substrates with polymers presenting the nonbiofouling PEG moiety and subsequently conjugated biologically active compounds to the PEG-presenting, polymeric films. Specifically, a Ti/TiO 2 surface was chemically modified to present an initiator for atom transfer radical polymerization, and poly(ethylene glycol) methacrylate (PEGMA) was polymerized from the surface. After activation of hydroxyl groups of poly(PEGMA) (pPEGMA) with N,N ′-disuccinimidyl carbonate, biotin, a model compound, was conjugated to the pPEGMA films. The reactions were confirmed by infrared spectroscopy, X-ray photoelectron spectroscopy, contact angle goniometry, and ellipsometry. The biospecific binding of target proteins was also utilized to generate micropatterns of proteins on the Ti/TiO 2 surface.