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Published byKatrina Griffith Modified over 8 years ago
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Aligning Kinases Applying MSA Analysis to the CDK family
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Building A Multiple Sequence Alignment
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chite ---ADKPKRPLSAYMLWLNSARESIKRENPDFK-VTEVAKKGGELWRGLKD wheat --DPNKPKRAPSAFFVFMGEFREEFKQKNPKNKSVAAVGKAAGERWKSLSE trybr KKDSNAPKRAMTSFMFFSSDFRS----KHSDLS-IVEMSKAAGAAWKELGP mouse -----KPKRPRSAYNIYVSESFQ----EAKDDS-AQGKLKLVNEAWKNLSP ***. :::.:... :.. *. *: * chite AATAKQNYIRALQEYERNGG- wheat ANKLKGEYNKAIAAYNKGESA trybr AEKDKERYKREM--------- mouse AKDDRIRYDNEMKSWEEQMAE * :.*. : Extrapolation Motifs/Patterns Phylogeny Profiles Struc. Prediction Multiple Alignments Are CENTRAL to MOST Bioinformatics Techniques. Potential Uses of A Multiple Sequence Alignment?
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1 Organizing a Family Gathering The CDK example
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Choosing the Right Sequences SwisProt Litterature Other Databases
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Organizing the Data SRS Public Data IGS Data Aventis CDK Genecard Manual Automatic
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Accessing the Data: The Fischer Server Fischer will Contain – A collection of Flat files – A secure SRS server – File Formats The server is a Technology Pipeline – Can be adapted in real time – Can be Transfered
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Our CDK Data CDKs and CDK-like – Protein Information Functional Features Structural Information – Genomic Information Genes Variant SNPs
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Our MSA dataset 29 amino acid sequences (CDKS and Aurora families, stemming from primary transcripts) – 2 isoforms of a cdk member 4 PDB structures : – 1MUO (AUR A) – 1BLX (CDK 6 ) – 1b38 (CDK 2) – 1H4L (CDK 5) Use of T-coffee release 1.78 with integration of the structure informations contained in pdb files
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2 Aligning The Sequences
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Building A Multiple Sequence Alignment ClustalW T-Coffee Muscle Hand Editing Combination Comparison
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Using Structural Information 3D-Coffee Struct Vs Struct Seq Vs Struct Thread Superpose Seq Vs Seq Local Global
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Method
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Accessing the Methods: Fischer Public 3D-Coffee server – igs-server.cnrs-mrs.fr/TCoffee/ Fischer – Latest version of T-Coffee – Customised parameters – Coktails of MSA methods
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3 Dressing Up a Multiple Sequence Alignment
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Feature Dressing -25 Binding site -20 Phospho -40 nsSNP -50 Splice Site … Escript
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Feature Dressing
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4 How Good Is The Alignment ????
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T-Coffee CORE Evaluation
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CORE index Specificity ( ) and Sensitivity ( )
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Feature Based Evaluation
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Features mapping on multiple alignment T-coffee ATP binding site Glycine loop ATP binding site Glycine loop Non-synonymous SNP ClustalW
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Structure Based Evaluation APDB
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Include Sequences with Known Structures – Do Not use Structural Information Score 1 – Use Structural Information:Score 2 If Score1 ~ Score 2 – Structural Information does not help much – The alignment is of reasonnable quality
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Evaluating a Multiple Sequence Alignment T-Coffee CORE index Feature Based Library APDB
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Maninupulating and Comparing Alignments Reformating/Processing – seq_reformat – extract_from_pdb Coloring – seq_reformat – ESCript Comparing – aln_compare
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5 Thinking Large ????
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T-Coffee_dpa T-Coffee is limited to a small number of sequences T-coffee_dpa: Double Progressive Algo – Able to handle large datasets – 1000 sequences and more – Able to use structural information
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Using A Multiple Sequence Alignment
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1 Exploring The Alignment
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Cdk's signature Cdk's T-loop (orange) and aurora's Activating loop Substrat recognition motif
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2 Using The Alignment Does my Sequence Make Sense
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Identifying Abnormalities within an MSA Insertion within the Nuc Binding Site…
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Identifying Abnormalities within an MSA
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Activation loop (orange)
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Identifying Abnormalities within an MSA Retinoblastoma
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2 Using The Alignment Analysing the Structure with The Alignment
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The Evoltionnary Trace
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3 Using The Alignment Spotting differences
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What makes a CDK not and AurorA
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4 Clustering and Correlating
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Function Trees Vs Lead Trees 1-Select Functionnaly Important Positions 2-Make a tree based on these positions 3-Compare the tree with the lead tree PROBLEMS: – Choose on the right positions – Describe the Leads with the right determinants
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