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Clustal Ω for Protein Multiple Sequence Alignment

Clustal Ω for Protein Multiple Sequence Alignment. Des Higgins (Conway Institute, University College Dublin, Ireland), “ Clustal Omega for Protein Multiple Sequence Alignment,” presentation at ISMB/ECCB 2011.

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Clustal Ω for Protein Multiple Sequence Alignment

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  1. ClustalΩ for Protein Multiple Sequence Alignment Des Higgins (Conway Institute, University College Dublin, Ireland), “Clustal Omega for Protein Multiple Sequence Alignment,” presentation at ISMB/ECCB 2011. Sievers et al., “Fast, scalable generation of high quality protein multiple sequence alignments using Clustal Omega,” unpublished manuscript, 2011. Presented by Hershel Safer in Ron Shamir’s group meeting on 17.8.2011. 17 August 2011

  2. Outline Background on multiple sequence alignment (MSA) Considerations for a new MSA tool ClustalΩ Benchmarking: Methods and issues Benchmarking results References 17 August 2011

  3. Example of MSA: Globins From Higgins 2011 17 August 2011

  4. Example continued: Red columns are alpha helices From Higgins 2011 17 August 2011

  5. Approaches to finding MSAs • Exact solution using dynamic programming: Finding “optimal” MSA for N sequences of length L takes time O(LN) • Progressive alignment: Greedy heuristic that mimics evolution. • Start by creating guide tree that specifies “evolutionary closeness.” Complexity is O(N2) for fixed L. • Build increasingly large sub-alignments in the order specified by the guide tree. Complexity is O(N). • Works for up to a few thousand sequences 17 August 2011

  6. Example of progressive alignment From Higgins 2011 17 August 2011

  7. Example of progressive alignment, cont’d. From Higgins 2011 17 August 2011

  8. Example of progressive alignment, cont’d. From Higgins 2011 17 August 2011

  9. Features of progressive alignment • Advantages • Fast • Gives pretty good results on large problems • Provides good basis for manual tweaking • Disadvantages • Hard to know if a solution is good – no objective function • Errors are not corrected. Once two sequences are aligned, they keep the same relative alignment (e.g., later indels apply identically to both sequences). 17 August 2011

  10. Consistency criterion Addresses problem of errors introduced by early mis-alignments Use library of pairwise alignments that is created for building the guide tree For each pair of aligned residues in the library, check their alignment in other pairwise alignments. Scores for progressive alignment are modified to reflect consistency across the entire library of pairwise comparisons. Helps avoid early mis-alignment. Complexity: worst case O(N3L2), in practice O(N3L). 17 August 2011

  11. Two kinds of popular MSA tools • Fast (<10,000 sequences) • Clustal W • MAFFT (with --partree, can handle >>10,000 sequences) • Muscle • Kalign • Accurate but slow (<100s of sequences) • T-Coffee • ProbCons • MSAProbs 17 August 2011

  12. Outline Background on multiple sequence alignment (MSA) Considerations for a new MSA tool ClustalΩ Benchmarking: Methods and issues Benchmarking results References 17 August 2011

  13. Why a new MSA tool? • Starting to see uses for MSAs with hundreds of thousands of sequences • Metagenomics • Next-generation sequencing 17 August 2011

  14. Goals for a new MSA tool Want a tool that scales well (time and space) to hundreds of thousands of sequences and still gives accurate results Scalability: Up to several hours to align hundreds of thousands of sequences on a desktop computer Accuracy: Similar to Clustal W 17 August 2011

  15. Outline Background on multiple sequence alignment (MSA) Considerations for a new MSA tool ClustalΩ Benchmarking: Methods and issues Benchmarking results References 17 August 2011

  16. ClustalΩ: Possibly the last MSA tool you will need • Building guide tree: Use mBed to cluster in time O(N log(N)) • Progressive alignment: Use HHalign to sequentially align pairs of profile HMMs • Take advantage of existing alignments • External profile alignment: Use an existing profile HMM of sequences homologous to input set to help align input set • Iterate guide tree construction and/or progressive alignment • Add sequences to existing alignments without starting from scratch 17 August 2011

  17. Building guide tree using mBed • Reduces quadratic time/space of clustering and guide-tree construction to O(N log(N)) • Cluster sequences • Select log2(N) seed sequences • Compute distance from each sequence to all seeds, using k-tuple distance measure (k=2) for unaligned sequences. • Cluster sequences using k-means • Build guide tree • Construct UPGMA sub-tree separately for each cluster (use UPGMA code from Muscle) • Link sub-trees using distances between clusters 17 August 2011

  18. Progressive alignment using HHalign HHalign is a method for pairwise alignment of profile HMMs It was designed to search HMM databases to identify remote homologs (sequence identity <20%) In ClustalΩ, sequences and sub-alignments are converted to profile HMMs. Transition, insertion, and deletion probabilities are computed, and pseudo-counts are added as needed. HHalign is used to align sub-alignments, in the order defined by the guide tree. 17 August 2011

  19. External profile alignment (EPA) Take advantage of existing HMMs to guide pairwise alignment in early stages – avoid seemingly good alignments that are bad in the context of the entire MSA If the kinds of sequences are known, can often find a relevant HMM in Pfam. Contribution of external profile decreases as sub-alignments get larger, as larger sub-alignments contain the information that would come from the external profile. Overhead: Can triple the alignment time 17 August 2011

  20. EPA performance 17 August 2011

  21. Iteration instead of EPA Can bootstrap profile information if external profile is not available or not desired MSA of original sequences can be converted to HMM and used as in EPA MSA can also be used to rebuild guide tree Can iterate this process Can decouple iteration of guide-tree construction and HMM construction – can freeze one and just iterate the other, or iterate both 17 August 2011

  22. Iteration performance 17 August 2011

  23. Availability of ClustalΩ Download a copy (Unix/Linux, Windows, Mac) EBI website Galaxy analysis system (coming soon?) 17 August 2011

  24. Outline Background on multiple sequence alignment (MSA) Considerations for a new MSA tool ClustalΩ Benchmarking: Methods and issues Benchmarking results References 17 August 2011

  25. Benchmark databases for MSA • BAliBASE • Collection of manually refined MSAs based on 3D structural superposition • Annotated core blocks: highly conserved regions that can be reliably aligned • Occasionally updated to represent kinds of complex sequences encountered in real problems, as kinds of alignments attempted change. • Divided into reference sets that represent different kinds of alignment challenges • Other MSA benchmark DBs: Prefab, Homstrad, Oxbench, SABmark, IRMbase 17 August 2011

  26. ClustalΩ benchmarking approach • Compared to 11 other MSA programs • Score is fraction of columns identical in generated and reference alignments • Used 3 benchmark databases • BAliBASE: Consider only core regions of alignments • Prefab • HomFam: Created for this work to test scalability to many sequences. Combined Homstrad families with corresponding Pfam families. Only tested with “fast” tools. 17 August 2011

  27. Problems with benchmarking databases DBs include questionable alignments DBs have biased coverage of fold families and kinds of proteins Test results may be biased if similar methods used to construct DB and in MSA tool (e.g., pairwise alignment method) Focus on core blocks over-estimates accuracy because these regions are more easily aligned Including gaps is problematic: Gap position is not considered, and a misplaced gap can improve the accuracy score. Amount of sequence divergence in DB alignments: twilight zone (20-35% identity) vs. higher or lower Sum-of-pairs vs. column scores 17 August 2011

  28. Problems with benchmarking databases, cont’d. • How representative is the benchmark? • Method may behave well on benchmark, not in real world • Method may behave well in real world, not on benchmark • Conclusion of Edgars: “protein alignment assessment is more challenging than generally realized, and skepticism is appropriate for claims that method rankings or advances can be reliably measured by current benchmarks.” 17 August 2011

  29. Outline Background on multiple sequence alignment (MSA) Considerations for a new MSA tool ClustalΩ Benchmarking: Methods and issues Benchmarking results References 17 August 2011

  30. BAliBASE benchmark 17 August 2011

  31. Prefab benchmark 17 August 2011

  32. HomFam benchmark 17 August 2011

  33. Scalability of running time 17 August 2011

  34. Outline Background on multiple sequence alignment (MSA) Considerations for a new MSA tool ClustalΩ Benchmarking: Methods and issues Benchmarking results References 17 August 2011

  35. Additional references Notredame et al. (2002), “T-Coffee: A novel method for fast and accurate multiple sequence alignment,” J Mol Biol 302:205. [Introduced notion of consistency] Blackshields et al. (2010), “Sequence embedding for fast construction of guide trees for multiple sequence alignment,” Algorithms for Mol Biol 5:21. [mBed algorithm] Söding (2005), “Protein homology detection by HMM-HMM comparison,” Bioinformatics 21:951. [HHalign algorithm] Thompson et al. (2005), “BAliBASE 3.0: Latest developments of the multiple sequence alignment benchmark,” Proteins 61:127. 17 August 2011

  36. Additional references, cont’d. Mizuguchi et al. (1998), “HOMSTRAD: A database of protein structure alignments for homologous families,” Protein Sci 7:2469. Edgar (2004), “MUSCLE: Multiple sequence alignment with high accuracy and high throughput,” Nucleic Acids Res 32:1792. [Introduced PREFAB benchmarking DB] Edgar (2010), “Quality measures for protein alignment benchmarks,” Nucleic Acids Res 38:2145. Aniba et al. (2010), “Issues in bioinformatics benchmarking: The case study of multiple sequence alignment,” Nucleic Acids Res 38:7353. 17 August 2011

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