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MNW2 course Introduction to Bioinformatics

MNW2 course Introduction to Bioinformatics. Lecture 22: Markov models Centre for Integrative Bioinformatics FEW/FALW heringa@cs.vu.nl. Problem in biology. Data and patterns are often not clear cut

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MNW2 course Introduction to Bioinformatics

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  1. MNW2 courseIntroduction to Bioinformatics Lecture 22: Markov models Centre for Integrative Bioinformatics FEW/FALW heringa@cs.vu.nl

  2. Problem in biology • Data and patterns are often not clear cut • When we want to make a method to recognise a pattern (e.g. a sequence motif), we have to learn from the data (e.g. maybe there are other differences between sequences that have the pattern and those that do not) • This leads to Data mining and Machine learning

  3. A widely used machine learning approach: Markov models • Contents: • Markov chain models (1st order, higher order and • inhomogeneous models; parameter estimation; classification) • • Interpolated Markov models (and back-off models) • • Hidden Markov models (forward, backward and Baum- • Welch algorithms; model topologies; applications to gene • finding and protein family modeling

  4. Markov Chain Models • a Markov chain model is defined by: • a set of states • some states emit symbols • other states (e.g. the begin state) are silent • a set of transitions with associated probabilities • the transitions emanating from a given state define a distribution over the possible next states

  5. Markov Chain Models • given some sequence x of length L, we can ask how probable the sequence is given our model • for any probabilistic model of sequences, we can write this probability as • key property of a (1st order) Markov chain: the probability of each Xi depends only on Xi-1

  6. Markov Chain Models Pr(cggt) = Pr(c)Pr(g|c)Pr(g|g)Pr(t|g)

  7. Markov Chain Models • Can also have an end state, allowing the model to represent: • Sequences of different lengths • Preferences for sequences ending with particular symbols

  8. Markov Chain Models The transition parameters can be denoted by where Similarly we can denote the probability of a sequence x as Where aBxi represents the transition from the begin state

  9. Example Application • CpG islands • CGdinucleotides are rarer in eukaryotic genomes than expected given the independent probabilities of C, G • but the regions upstream of genes are richer in CG dinucleotides than elsewhere – CpG islands • useful evidence for finding genes • Could predict CpG islands with Markov chains • one to represent CpG islands • one to represent the rest of the genome Example includes using Maximum likelihood and Bayes’ statistical data and feeding it to a HM model

  10. Estimating the Model Parameters • Given some data (e.g. a set of sequences from CpG islands), how can we determine the probability parameters of our model? • One approach: maximum likelihood estimation • given a set of data D • set the parameters  to maximize Pr(D | ) • i.e. make the data D look likely under the model

  11. Maximum Likelihood Estimation • Suppose we want to estimate the parameters Pr(a), Pr(c), Pr(g), Pr(t) • And we’re given the sequences: accgcgctta gcttagtgac tagccgttac • Then the maximum likelihood estimates are: Pr(a) = 6/30 = 0.2 Pr(g) = 7/30 = 0.233 Pr(c) = 9/30 = 0.3 Pr(t) = 8/30 = 0.267

  12. These data are derived from genome sequences

  13. Higher Order Markov Chains • An nth order Markov chain over some alphabet is equivalent to a first order Markov chain over the alphabet of n-tuples • Example: a 2nd order Markov model for DNA can be treated as a 1st order Markov model over alphabet: AA, AC, AG, AT, CA, CC, CG, CT, GA, GC, GG, GT, TA, TC, TG, and TT (i.e. all possible dipeptides)

  14. A Fifth Order Markov Chain

  15. Inhomogenous Markov Chains • In the Markov chain models we have considered so far, the probabilities do not depend on where we are in a given sequence • In an inhomogeneous Markov model, we can have different distributions at different positions in the sequence • Consider modeling codons in protein coding regions

  16. Inhomogenous Markov Chains

  17. A Fifth Order InhomogenousMarkov Chain

  18. Selecting the Order of aMarkov Chain Model • Higher order models remember more “history” • Additional history can have predictive value • Example: – predict the next word in this sentence fragment “…finish __” (up, it, first, last, …?) – now predict it given more history • “Fast guys finish __”

  19. Selecting the Order of aMarkov Chain Model • However, the number of parameters we need to estimate grows exponentially with the order – for modeling DNA we need parameters for an nth order model, with n  5 normally • The higher the order, the less reliable we can expect our parameter estimates to be – estimating the parameters of a 2nd order homogenous Markov chain from the complete genome of E. Coli, we would see each word > 72,000 times on average – estimating the parameters of an 8th order chain, we would see each word ~ 5 times on average

  20. Interpolated Markov Models • The IMM idea: manage this trade-off by interpolating among models of various orders • Simple linear interpolation:

  21. Interpolated Markov Models • We can make the weights depend on the history – for a given order, we may have significantly more data to estimate some words than others • General linear interpolation

  22. Gene Finding: Search by Content • Encoding a protein affects the statistical properties of a DNA sequence – some amino acids are used more frequently than others (Leu more popular than Trp) – different numbers of codons for different amino acids (Leu has 6, Trp has 1) – for a given amino acid, usually one codon is used more frequently than others • This is termed codon preference • Codon preferences vary by species

  23. Codon Preference in E. Coli AA codon /1000 ---------------------- Gly GGG 1.89 Gly GGA 0.44 Gly GGU 52.99 Gly GGC 34.55 Glu GAG 15.68 Glu GAA 57.20 Asp GAU 21.63 Asp GAC 43.26

  24. Search by Content •Common way to search by content – build Markov models of coding & noncoding regions – apply models to ORFs (Open Reading Frames) or fixed- sized windows of sequence • GeneMark [Borodovsky et al.] – popular system for identifying genes in bacterial genomes – uses 5th order inhomogenous Markov chain models

  25. The GLIMMER System • Salzberg et al., 1998 • System for identifying genes in bacterial genomes • Uses 8th order, inhomogeneous, interpolated Markov chain models

  26. IMMs in GLIMMER • How does GLIMMER determine the values? • First, let us express the IMM probability calculation recursively:

  27. IMMs in GLIMMER • If we haven’t seen xi-1… xi-nmorethan 400 times, then compare the counts for the following: • Use a statistical test ( 2) to get a value d indicating our confidence that the distributions represented by the two sets of counts are different

  28. IMMs in GLIMMER 2 score when comparing nth-order with n-1th-order Markov model (preceding slide)

  29. The GLIMMER method • 8th order IMM vs. 5th order Markov model • Trained on 1168 genes (ORFs really) • Tested on 1717 annotated (more or less known) genes

  30. Hidden Markov models (HMMs) Given say a T in our input sequence, which state emitted it?

  31. Hidden Markov models (HMMs) • Hidden State • We will distinguish between the observed parts of a problem and the hidden parts • • In the Markov models we have considered previously, it is clear which state accounts for each part of the observed sequence • In the model above (preceding slide), there are multiple states that could account for each part of the observed sequence • – this is the hidden part of the problem • – states are decoupled from sequence symbols

  32. HMM-based homology searching HMM for ungapped alignment… Transition probabilities and Emission probabilities Gapped HMMs also have insertion and deletion states (next slide)

  33. d1 d2 d3 d4 I0 I1 I2 I3 I4 m0 m1 m2 m3 m4 m5 End Start Profile HMM: m=match state, I-insert state, d=delete state; go from left to right. I and m states output amino acids; d states are ‘silent”. Model for alignment with insertions and deletions

  34. HMM-based homology searching • Most widely used HMM-based profile searching tools currently are SAM-T99 (Karplus et al., 1998) and HMMER2 (Eddy, 1998) • formal probabilistic basis and consistent theory behind gap and insertion scores • HMMs good for profile searches, bad for alignment (due to parametrisation of the models) • HMMs are slow

  35. Homology-derived Secondary Structure of Proteins (HSSP) Sander & Schneider, 1991 It’s all about trying to push “don’t know region” down…

  36. The Parameters of an HMM

  37. HMM for Eukaryotic Gene Finding Figure from A. Krogh, An Introduction to Hidden Markov Models for Biological Sequences

  38. A Simple HMM

  39. Three Important Questions • How likely is a given sequence? the Forward algorithm • What is the most probable “path” for generating a given sequence? the Viterbi algorithm • • How can we learn the HMM parameters given a set of sequences? the Forward-Backward (Baum-Welch) algorithm

  40. How Likely is a Given Sequence? • The probability that the path is taken and the sequence is generated: • (assuming begin/end are the only silent states on path)

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