AutoStructure Theory: Difference between revisions

AutoStructure ^[1] is an automated NOESY assignment engine, which uses a distinct bottom-up topology-constrained approach for iterative NOE interpretation and structure determination. AutoStructure first builds an initial chain fold based on intraresidue and sequential NOESY data, together with characteristic NOE patterns of secondary structures, including helical medium-range NOE interactions and interstrand b-sheet NOE interactions, and unambiguous long-range NOE interactions, based on chemical shift matching and NOESY spectral symmetry considerations. NOESY cross peaks that cannot be uniquely assigned using these methods are not used in the initial structure calculations. Once initial structures are generated and validated, additional NOESY cross peaks are iteratively assigned using the intermediate 3D structures and contact maps, together with knowledge of high-order topology constraints of alpha-helix and beta-sheet packing geometries. This protocol, in principle, resembles the method that an expert would utilize in manually solving a protein structure by NMR.

The input data for AutoStructure are: (i) resonance assignment table, (ii) 2D, 3D, and/or 4D NOESY peak lists, (iii) list of scalar coupling, RDC and slow amide exchange data. AutoStructure generates distance constraint lists and utilizes the programs DYANA/CYANA, Xplor for 3D structure generation on a Linux-based computer cluster. Fig. 1 shows AutoStructure results for three different human protein NMR test data sets: FGF-2, IL-13 and MMP-1, ranging in size from 113 to 169 amino-acid residues. The mean coordinate differences between structures determined by AutoStructure and by manual analysis (0.5 to 0.8 Å for backbone atoms of ordered residues) demonstrate good accuracy of these automated methods.

AutoStructure's ‘bottom up’ strategy is quite different from the “top down” strategies used by the alternative programs CANDID and ARIA, which rely on “ambiguous constraints”.  For NOESY spectra with poor signal-to-noise ratios, such automatically assigned ‘ambiguous constraint” sets may not include any true NOESY assignments, and result in small distortions of the protein structure which maybe avoided by the “bottom up” approach of AutoStructure  CANDID/CYANA also uses a ‘network anchoring” approach similar to, but less comprehensive than, the topology-constrained approach used by AutoStructure. For these reasons, some users may prefer to use both AutoStructure and CANDID/CYANA or ARIA in parallel to assess potential errors in automated NOESY cross peak assignments

ADDIN EN.CITE <EndNote><Cite><Author>Liu</Author><Year>2005</Year><RecNum>193</RecNum><record><rec-number>193</rec-number><foreign-keys><key app="EN" db-id="fe29atzr4stwaueev2lxf2fgp5xx5pavz2a5">193</key></foreign-keys><ref-type name="Journal Article">17</ref-type><contributors><authors><author>Liu, G.</author><author>Shen, Y.</author><author>Atreya, H. S.</author><author>Parish, D.</author><author>Shao, Y.</author><author>Sukumaran, D. K.</author><author>Xiao, R.</author><author>Yee, A.</author><author>Lemak, A.</author><author>Bhattacharya, A.</author><author>Acton, T. A.</author><author>Arrowsmith, C. H.</author><author>Montelione, G. T.</author><author>Szyperski, T.</author></authors></contributors><auth-address>Department of Chemistry, University at Buffalo, State University of New York, Buffalo, NY 14260, USA.</auth-address><titles><title>NMR data collection and analysis protocol for high-throughput protein structure determination</title><secondary-title>Proc Natl Acad Sci U S A</secondary-title></titles><periodical><full-title>Proc Natl Acad Sci U S A</full-title></periodical><pages>10487-92</pages><volume>102</volume><number>30</number><keywords><keyword>Comparative Study</keyword><keyword>Data Collection/methods</keyword><keyword>Fourier Analysis</keyword><keyword>*Models, Molecular</keyword><keyword>Nuclear Magnetic Resonance, Biomolecular/*methods</keyword><keyword>Protein Conformation</keyword><keyword>Proteins/*chemistry</keyword><keyword>Research Support, N.I.H., Extramural</keyword><keyword>Research Support, Non-U.S. Gov&apos;t</keyword><keyword>Research Support, U.S. Gov&apos;t, Non-P.H.S.</keyword><keyword>Research Support, U.S. Gov&apos;t, P.H.S.</keyword></keywords><dates><year>2005</year><pub-dates><date>Jul 26</date></pub-dates></dates><accession-num>16027363</accession-num><urls><related-urls><url>http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&amp;db=PubMed&amp;dopt=Citation&amp;list_uids=16027363 </url></related-urls></urls></record></Cite></EndNote><![endif]-->.