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HIDDEN MARKOV MODELS IN COMPUTATIONAL BIOLOGY

HIDDEN MARKOV MODELS IN COMPUTATIONAL BIOLOGY. CS 594: An Introduction to Computational Molecular Biology BY Shalini Venkataraman Vidhya Gunaseelan. DNA. transcription. mRNA. translation. Protein. Relationship Between DNA, RNA And Proteins. CCTGAGCCAACTATTGATGAA.

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HIDDEN MARKOV MODELS IN COMPUTATIONAL BIOLOGY

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  1. HIDDEN MARKOV MODELS IN COMPUTATIONAL BIOLOGY CS 594: An Introduction to Computational Molecular Biology BY Shalini Venkataraman Vidhya Gunaseelan

  2. DNA transcription mRNA translation Protein Relationship Between DNA, RNA And Proteins CCTGAGCCAACTATTGATGAA CCUGAGCCAACUAUUGAUGAA PEPTIDE

  3. Protein Structure Primary Structure of Proteins The primary structure of peptides and proteins refers to the linear number and order of the amino acids present.

  4. Protein Structure Secondary Structure Protein secondary structure refers to regular, repeated patters of folding of the protein backbone. How a protein folds is largely dictated by the primary sequence of amino acids Beta Sheet Alpha Helix

  5. Multiple Alignment Process • Process of aligning three or more sequences with each other • Generalization of the algorithm to align two sequences • Local multiple alignment uses Sum of pairs scoring scheme

  6. HMM Architecture • Markov Chains • What is a Hidden Markov Model(HMM)? • Components of HMM • Problems of HMMs

  7. Markov Chains Rain Sunny Cloudy State transition matrix : The probability of the weather given the previous day's weather. States : Three states - sunny, cloudy, rainy. Initial Distribution : Defining the probability of the system being in each of the states at time 0.

  8. Hidden Markov Models Hidden states : the (TRUE) states of a system that may be described by a Markov process (e.g., the weather). Observable states : the states of the process that are `visible' (e.g., seaweed dampness).

  9. Components Of HMM Output matrix : containing the probability of observing a particular observable state given that the hidden model is in a particular hidden state. Initial Distribution : contains the probability of the (hidden) model being in a particular hidden state at time t = 1. State transition matrix : holding the probability of a hidden state given the previous hidden state.

  10. Example-HMM Transition Prob. Output Prob. Scoring a Sequence with an HMM: The probability of ACCY along this path is .4 * .3 * .46 * .6 * .97 * .5 * .015 * .73 *.01 * 1 = 1.76x10-6.

  11. Problems With HMM Scoring problem: Given an existing HMM and observed sequence , what is the probability that the HMM can generate the sequence

  12. Problems With HMM • Alignment Problem • Given a sequence, what is the optimal state sequence that the HMM would use to generate it

  13. Problems With HMM Training Problem Given a large amount of data how can we estimate the structure and the parameters of the HMM that best accounts for the data

  14. HMMs in Biology • Gene finding and prediction • Protein-Profile Analysis • Secondary Structure prediction • Advantages • Limitations

  15. Finding genes in DNA sequence This is one of the most challenging and interesting problems in computational biology at the moment. With so many genomes being sequenced so rapidly, it remains important to begin by identifying genes computationally.

  16. DNA transcription mRNA translation Protein What is a (protein-coding) gene? CCTGAGCCAACTATTGATGAA CCUGAGCCAACUAUUGAUGAA PEPTIDE

  17. In more detail (color ~state) (Left) (Removed)

  18. Gene Finding HMMs • Our Objective: • To find the coding and non-coding regions of an unlabeled string of DNA nucleotides • Our Motivation: • Assist in the annotation of genomic data produced by genome sequencing methods • Gain insight into the mechanisms involved in transcription, splicing and other processes

  19. Why HMMs • Classification: Classifying observations within a sequence • Order: A DNA sequence is a set of ordered observations • Grammar : Our grammatical structure (and the beginnings of our architecture) is right here: • Success measure: # of complete exons correctly labeled • Training data: Available from various genome annotation projects

  20. HMMs for gene finding • Training- Expectation Maximization (EM) • Parsing – Viterbi algorithm An HMM for unspliced genes. x : non-coding DNA c : coding state

  21. Genefinders- a comparison Sn = Sensitivity Sp = Specificity Ac = Approximate Correlation ME = Missing Exons WE = Wrong Exons GENSCAN Performance Data, http://genes.mit.edu/Accuracy.html

  22. Protein Profile HMMs • Motivation • Given a single amino acid target sequence of unknown structure, we want to infer the structure of the resulting protein. Use Profile Similarity • What is a Profile? • Proteins families of related sequences and structures • Same function • Clear evolutionary relationship • Patterns of conservation, some positions are more conserved than the others

  23. An Overview Aligned Sequences Build a Profile HMM (Training) Database search Query against Profile HMM database (Forward) Multiple alignments (Viterbi)

  24. Building – from an existing alignment ACA - - - ATG TCA ACT ATC ACA C - - AGC AGA - - - ATC ACC G - - ATC insertion Transition probabilities Output Probabilities A HMM model for a DNA motif alignments, The transitions are shown with arrows whose thickness indicate their probability. In each state, the histogram shows the probabilities of the four bases.

  25. Building – Final Topology Deletion states Matching states Insertion states No of matching states = average sequence length in the family PFAM Database- of Protein families (http://pfam.wustl.edu)

  26. Database Searching • Given HMM, M, for a sequence family, find all members of the family in data base. • LL – score LL(x) = log P(x|M) • (LL score is length dependent – must normalize or use Z-score)

  27. Query a new sequence Suppose I have a query protein sequence, and I am interested in which family it belongs to? There can be many paths leading to the generation of this sequence. Need to find all these paths and sum the probabilities. Consensus sequence: P (ACACATC) = 0.8x1 x 0.8x1 x 0.8x0.6 x 0.4x0.6 x 1x1 x 0.8x1 x 0.8 = 4.7 x 10 -2 ACAC - - ATC

  28. Multiple Alignments • Try every possible path through the model that would produce the target sequences • Keep the best one and its probability. • Output : Sequence of match, insert and delete states • Viterbi alg. Dynamic Programming

  29. Building – unaligned sequences • Baum-Welch Expectation-maximization method • Start with a model whose length matches the average length of the sequences and with random output and transition probabilities. • Align all the sequences to the model. • Use the alignment to alter the output and transition probabilities • Repeat. Continue until the model stops changing • By-product: It produced a multiple alignment

  30. PHMM Example An alignment of 30 short amino acid sequences chopped out of a alignment of the SH3 domain. The shaded area are themost conserved and were represented by the main states in the HMM. The unshaded area was represented by an insert state.

  31. Prediction of Protein Secondary structures • Prediction of secondary structures is needed for the prediction of protein function. • Analyze the amino-acid sequences of proteins • Learn secondary structures • helix, sheet and turn • Predict the secondary structures of sequences

  32. Advantages • Characterize an entire family of sequences. • Position-dependent character distributions and position-dependent insertion and deletion gap penalties. • Built on a formal probabilistic basis • Can make libraries of hundreds of profile HMMs and apply them on a large scale (whole genome)

  33. Limitations • Markov Chains • Probabilities of states are supposed to be independent • P(y) must be independent of P(x), and vice versa • This usually isn’t true P(x) P(y) …

  34. Limitations - contd • Standard Machine Learning Problems • Watch out for local maxima • Model may not converge to a truly optimal parameter set for a given training set • Avoid over-fitting • You’re only as good as your training set • More training is not always good

  35. CONCLUSION • For links & slides • www.evl.uic.edu/shalini/hmm/

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