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Practical algorithms in Sequence Alignment Sushmita Roy BMI/CS 576 Sep 16 th, 2014.

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Presentation on theme: "Practical algorithms in Sequence Alignment Sushmita Roy BMI/CS 576 Sep 16 th, 2014."— Presentation transcript:

1 Practical algorithms in Sequence Alignment Sushmita Roy BMI/CS 576 www.biostat.wisc.edu/bmi576/ sroy@biostat.wisc.edu Sep 16 th, 2014

2 Key concepts Assessing the significance of an alignment – Extreme value distribution gives an analytical form to compute the significance of a score Heuristic algorithms – BLAST algorithm

3 Readings from book Chapter 2 – Section 2.5 – Section 2.7

4 RECAP: Four issues in sequence alignment Type Algorithm Score Significance

5 Classical approach to assessing the significance of score Develop a “background” distribution of alignment score Assess the probability of observing our score S from this background distribution

6 Thought experiment for generating the background distribution Suppose we assume Sequence lengths m and n A particular substitution matrix and amino-acid frequencies And we consider generating random sequences of lengths m and n and finding the best alignment of these sequences This will give us a distribution over alignment scores for random pairs of sequences

7 The extreme value distribution Because we are picking the best alignments, we want to know the distribution of max scores for alignments against a random set of sequences looks like The background distribution is given by an extreme value distribution (EVD) We need to assess the probability of observing a score of S or higher by random chance, that is, we need the form of the CDF: P(x>S)

8 Assessing significance of sequence score alignments It can be shown that the mean of optimal scores is – K, λ estimated from the substitution matrix Probability of observing a score greater than S Substituting U into the equation

9 Need to speed up sequence alignment Consider the task of searching the RefSeq collection of sequences against a query sequence: – most recent release of DB contains 32,504,738 proteins – Entails 33,000,000*(300*300) matrix operations (assuming query sequence is of length 300 and avg. sequence length is 300) O(mn) too slow for large databases with high query traffic We will look at a heuristic algorithm to speed up the search process

10 Heuristic alignment Heuristic algorithm: a problem-solving method which isn’t guaranteed to find the optimal solution, but which is efficient and finds good solutions Heuristic methods do fast approximation to dynamic programming – FASTA [Pearson & Lipman, 1988] – BLAST [Altschul et al., 1990; Altschul et al., Nucleic Acids Research 1997]

11 BLAST: Basic Local Alignment Search Tool Altshul et al 1990 – Cited >48,000 times! Key heuristics in BLAST – A good alignment is made up short stretches of matches: seeds – Extend seeds to make longer alignments Key tradeoff made: sensitivity vs. speed Used EVD theory for random sequence score Works for both protein sequence and DNA sequence – Only scores differ

12 BLAST continued Two parameters control how BLAST searches the database – w: This specifies the length of words to seed the alignment – T: The smallest threshold of word pair match to be considered in the alignment

13 Key steps of the BLAST algorithm For each query sequence 1.Compile a list of high-scoring words of score at least T First generate words in the query sequence Then find words that match query sequence words with score at least T Thus allows for inexact matches 2.Scan the database for hits of these words Relies on indexing performed as pre-processing 3.Extend hits

14 Determining query words Given: query sequence: QLNFSAGW word length w = 2 (default for protein usually w = 3) word score threshold T = 9 Step 1: determine all words of length w in query sequence QL LN NF FS SA AG GW

15 Determining query words Step 2: Determine all words that score at least T when compared to a word in the query sequence QLQL=9 LNLN=10 NFNF=12, NY=9 … SAnone... words from query sequence words with T≥9 Additional words potentially in database Aminoacid substitution matrix

16 Scanning the database Search database for all occurrences of query words Approach: – index database sequences into table of words (pre-compute this) – index query words into table (at query time) NP NS NT NW NY QLNFSAGW MFNYT, STNYD… NPGAT, TSQRPNP… query sequence database sequences

17 Extending a word hit to a larger alignment is straightforward Terminate extension when the score of the current alignment falls a certain distance below the best score found for shorter extensions Extending a hit Query sequence: Q L N F S A DB sequence: R L N Y S W Score: 1 4 5 3 4 -3 Total: 1+4+5+3+4=17

18 How to choose w and T? Tradeoff between running time and sensitivity Sensitivity T – small T: greater sensitivity, more hits to expand – large T: lower sensitivity, fewer hits to expand w – Larger w : fewer query word seeds, lower time for extending, but more possible words (20 w for AAs)

19 Updates to BLAST Two hit method – Lower the threshold but require two words to be on the same diagonal and be no more than A characters apart Ability to handle gaps Ability to handle position-specific score matrix created from alignments generated from iteration i for iteration i+1 Altshul et al 1997

20 Two-hit method Figure from Altshul et al 1997 + Hits wit T>=13 (15 hits). Hits with T>=11 (22 hits) Only these two are considered as they satisfy the two-hit method

21 Summary of BLAST T: Don’t consider seeds with score < T Don’t extend hits when score falls below a specified threshold Pre-processing of database or query helps to improve the running time

22 FASTA Starts with exact seed matches instead of inexact matches that satisfy a threshold Extends seeds (similar to BLAST) Join high scoring seeds allowing for gaps Re-align high scoring matches using dynamic programming

23 Different versions of BLAST programs ProgramQueryDatabase BLASTPProtein BLASTNDNA BLASTX Translated DNA Protein TBLASTNProteinTranslated DNA TBLASTX Translated DNA

24 Sequence databases Web portals/Knowledge bases – NCBI: http://www.ncbi.nih.govhttp://www.ncbi.nih.gov – EBI: http://www.ebi.ac.ukhttp://www.ebi.ac.uk – Sanger: http://www.sanger.ac.ukhttp://www.sanger.ac.uk – Each of these centers link to hundreds of databases Nucleotide sequences – Genbank – EMBL-EBI Nucleotide Sequence Database – Comprise ~8% of the total database (Nucleic Acid Research 2006 Database edition) Protein sequences – UniProtKB

25 Using BLAST http://blast.ncbi.nlm.nih.gov/Blast.cgi Will blast a DNA sequence against NCBI nucleotide database We will select – http://www.ncbi.nlm.nih.gov/nuccore/NG_000007.3?from =70545&to=72150&report=fasta http://www.ncbi.nlm.nih.gov/nuccore/NG_000007.3?from =70545&to=72150&report=fasta

26 Using BLAST Choose the database Enter the query sequence

27 Using BLAST The sequence corresponds to the human HBB (hemoglobin) gene. But we will select the mouse DB Use Megablast (large word size)

28 Interpreting results Assesses significance of a score. Related to P-value, but gives the expected number of alignments of this score value or higher.


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