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Title: 3DM: systematic analysis of heterogeneous superfamily data to discover protein functionalities.
Author(s): Kuipers, R.K.P. (321457056)
Joosten, H.J.
Berkel, W.J. van
Leferink, N.G.
Rooijen, E.
Ittmann, E.
Zimmeren, F. van
Jochens, H.
Bornscheuer, U.
Vriend, G. (069590842)
Santos, V.A. dos
Schaap, P.J.
Publication year: 2010
Document type: Article / Letter to editor
Journal: Proteins
ISSN: 0887-3585
Volume: vol. 78
Issue: iss. 9
Start page: p. 2101
End page: p. 2113
Abstract: Ten years of experience with molecular class-specific information systems (MCSIS) such as with the hand-curated G protein-coupled receptor database (GPCRDB) or the semiautomatically generated nuclear receptor database has made clear that a wide variety of questions can be answered when protein-related data from many different origins can be flexibly combined. MCSISes revolve around a multiple sequence alignment (MSA) that includes "all" available sequences from the entire superfamily, and it has been shown at many occasions that the quality of these alignments is the most crucial aspect of the MCSIS approach. We describe here a system called 3DM that can automatically build an entire MCSIS. 3DM bases the MSA on a multiple structure alignment, which implies that the availability of a large number of superfamily members with a known three-dimensional structure is a requirement for 3DM to succeed well. Thirteen MCSISes were constructed and placed on the Internet for examination. These systems have been instrumental in a large series of research projects related to enzyme activity or the understanding and engineering of specificity, protein stability engineering, DNA-diagnostics, drug design, and so forth.
Subject: Bioinformatics
NCMLS 3A: Genetics and epigenetic pathways of disease
NCMLS 3B: Chemical and physical biology
Organization: CMBI
UMCN Extern
Bioinformatics
Appears in Collections:Academic bibliography

Please use this identifier to cite or link to this item: http://hdl.handle.net/2066/89595

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