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Identification of a chemical substructure that is immobilized to ferrite nanoparticles (FP)
Authors:Nishio Kosuke  Gokon Nobuyuki  Hasegawa Makoto  Ogura Yuji  Ikeda Morihito  Narimatsu Hiroki  Tada Masaru  Yamaguchi Yuki  Sakamoto Satoshi  Abe Masanori  Handa Hiroshi
Institution:Department of Biological Information, Graduate School of Bioscience and Biotechnology, Tokyo Institute of Technology, 4259 Nagatsuta-cho, Midori-ku, Yokohama 226-8501, Japan.
Abstract:Despite the wide utility of ferrite nanoparticles (FP), a methodology to conjugate heterologous molecules to FP is still limited and characterization of small molecule-conjugated FP is not well known. Here, we describe what kinds of proteins and amino acids are selectively immobilized onto FP when FP is synthesized in the presence of these molecules. Two-dimentional gel electrophoresis (2D SDS-PAGE) showed that proteins with low pI value were selectively bound to FP. Quantitative analyses using HPLC suggested that L-aspartic acid (Asp) and L-cysteine (Cys) were bound to FP selectively among natural amino acids examined. Additional analysis of compounds-conjugated FP revealed that selective binding of Asp to FP was attributed with its molecular structure. It was found that the substructure of amino acid-bound to FP specifically was composed of a defined chelation of two carboxyl groups separated by two carbon atoms as deduced from FT-IR measurement. Thus, we concluded that molecules possessing two carboxyl groups separated by two carbons were bound to FP spontaneously and selectively, which might enable the attachment of free functional groups onto the FP surface if their molecules have functional groups other than carboxyl groups. The resulting complex might be applicable as a chemical tag to immobilize various molecules onto FP.
Keywords:Ferrite nanoparticles (FP)  l-Aspartic acid" target="_blank">l-Aspartic acid  Carboxyl group  FT-IR  Chemical substructure
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