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Analysis of binding properties and specificity through identification of the interface forming residues (IFR) for serine proteases |
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| Authors: | Cristina Ribeiro Roberto C Togawa Izabella AP Neshich Ivan Mazoni Adauto L Mancini Raquel C de Melo Minardi Carlos H da Silveira José G Jardine Marcelo M Santoro Goran Neshich |
| Affiliation: | 1.Department of Biochemistry and Immunology, Institute of Biological Sciences,Federal University of Minas Gerais,Belo Horizonte,Brazil;2.Embrapa Genetic Resources and Biotechnology,Brasilia,Brazil;3.Embrapa Information Technologies,Campinas,Brazil;4.Department of Mathematics and Computer Science - Federal University of Itajubá,Itajubá,Brazil;5.Department of Computer Science, Institute of Exact Sciences,Federal University of Minas Gerais,Belo Horizonte,Brazil |
| Abstract: | BackgroundEnzymes belonging to the same super family of proteins in general operate on variety of substrates and are inhibited by wide selection of inhibitors. In this work our main objective was to expand the scope of studies that consider only the catalytic and binding pocket amino acids while analyzing enzyme specificity and instead, include a wider category which we have named the Interface Forming Residues (IFR). We were motivated to identify those amino acids with decreased accessibility to solvent after docking of different types of inhibitors to sub classes of serine proteases and then create a table (matrix) of all amino acid positions at the interface as well as their respective occupancies. Our goal is to establish a platform for analysis of the relationship between IFR characteristics and binding properties/specificity for bi-molecular complexes. |
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