4.6 Article

QSalignWeb: A Server to Predict and Analyze Protein Quaternary Structure

期刊

出版社

FRONTIERS MEDIA SA
DOI: 10.3389/fmolb.2021.787510

关键词

web server; protein evolution; protein quaternary structure; protein structure alignment; physiological interface; crystal contact; protein superposition; protein interactions

资金

  1. European Research Council (ERC) under the European Union's Horizon 2020 research and innovation program [819318]
  2. Israel Science Foundation [1452/18]
  3. Estelle Funk Foundation
  4. Estate of Fannie Sherr
  5. Estate of Albert Delighter
  6. Merle S. Cahn Foundation
  7. Arnold Bortman Family Foundation
  8. Estate of Elizabeth Wachsman
  9. European Research Council (ERC) [819318] Funding Source: European Research Council (ERC)

向作者/读者索取更多资源

The QSalign web server allows users to submit homo-oligomeric structures and predict their physiological relevance by searching for homologs based on sequence similarity and PFAM domain architecture. Representative QSs in the protein family of the query are also provided for further analysis and homology modeling.
The identification of physiologically relevant quaternary structures (QSs) in crystal lattices is challenging. To predict the physiological relevance of a particular QS, QSalign searches for homologous structures in which subunits interact in the same geometry. This approach proved accurate but was limited to structures already present in the Protein Data Bank (PDB). Here, we introduce a webserver (www.QSalign.org)& nbsp;allowing users to submit homo-oligomeric structures of their choice to the QSalign pipeline. Given a user-uploaded structure, the sequence is extracted and used to search homologs based on sequence similarity and PFAM domain architecture. If structural conservation is detected between a homolog and the user-uploaded QS, physiological relevance is inferred. The web server also generates alternative QSs with PISA and processes them the same way as the query submitted to widen the predictions. The result page also shows representative QSs in the protein family of the query, which is informative if no QS conservation was detected or if the protein appears monomeric. These representative QSs can also serve as a starting point for homology modeling.

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