Literature DB >> 10526352

An iterative structure-assisted approach to sequence alignment and comparative modeling.

D F Burke1, C M Deane, H A Nagarajaram, N Campillo, M Martin-Martinez, J Mendes, F Molina, J Perry, B V Reddy, C M Soares, R E Steward, M Williams, M A Carrondo, T L Blundell, K Mizuguchi.   

Abstract

Correct alignment of the sequence of a target protein with those of homologues of known three-dimensional structure is a key step in comparative modeling. Usually an iterative approach that takes account of the local and overall structural features is required. We describe such an approach that exploits databases of structural alignments of homologous proteins (HOMSTRAD, http:/(/)www-cryst.bioc.cam.ac.uk/ approximately homstrad) and protein superfamilies (CAMPASS, http:/(/)www-cryst.bioc.cam.ac.uk/ approximately campass), in which structure-based alignments are analyzed and formatted with the program JOY (http:/(/)www-cryst.bioc.cam.ac.uk/ approximately joy) to reveal conserved local structural features. The databases facilitate the recognition of a family or superfamily, they assist in the selection of useful parent structures, they are helpful in alignment of the target sequences with the parent set, and are useful for deriving relationships that can be used in validating models. In the iterative approach, a model is constructed on the basis of the proposed sequence alignment and this is then reexpressed in the JOY format and realigned with the parent set. This is repeated until the model and sequence alignment is optimized. We examine the case for comparison and use of multiple structures of family members, rather than a single parent structure. We use the targets attempted by our group in CASP3 to assess the value of such procedures.

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Year:  1999        PMID: 10526352     DOI: 10.1002/(sici)1097-0134(1999)37:3+<55::aid-prot8>3.3.co;2-2

Source DB:  PubMed          Journal:  Proteins        ISSN: 0887-3585


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