Giri Narasimhan - users.cs.fiu.edugiri/teach/qbic/Su10/Lec7.pdf · BSC 4934: QʼBIC Capstone...
Transcript of Giri Narasimhan - users.cs.fiu.edugiri/teach/qbic/Su10/Lec7.pdf · BSC 4934: QʼBIC Capstone...
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BSC 4934: QʼBIC Capstone Workshop"
Giri Narasimhan ECS 254A; Phone: x3748
[email protected] http://www.cs.fiu.edu/~giri/teach/BSC4934_Su10.html
July 2010
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Protein Structures" Sequences of amino acid residues
20 different amino acids
Primary Quaternary Tertiary Secondary
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Proteins" Primary structure is the sequence of
amino acid residues of the protein, e.g., Flavodoxin: AKIGLFYGTQTGVTQTIAESIQQEFGGESIVDLNDIANADA…
Different regions of the sequence form local regular secondary structures, such as " Alpha helix, beta strands, etc.
AKIGLFYGTQTGVTQTIAESIQQEFGGESIVDLNDIANADA…
Secondary
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More on Secondary Structures"
α-helix " Main chain with peptide bonds " Side chains project outward from helix " Stability provided by H-bonds between CO and
NH groups of residues 4 locations away. β-strand
" Stability provided by H-bonds with one or more β-strands, forming β-sheets. Needs a β-turn.
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Proteins" Tertiary structures are formed by packing
secondary structural elements into a globular structure.
Myoglobin Lambda Cro
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Quaternary Structures in Proteins"
Quaternary"
• The final structure may contain more than one “chain” arranged in a quaternary structure. "
Insulin Hexamer"
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More quaternary structures"
Muscle creatine kinase"(Homodimer)"
Bovine deoxyhemoglobin"(Heterotetramer)"
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Molecular Representations"
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Amino Acid Types"
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All 3 figures are cartoons of an amino acid residue."
Structure of a single amino acid"
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Chains of amino acids"
Amino acids vs Amino acid residues!
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Angles φ and ψ in the polypeptide chain"
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Ramachandran Plot"
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Amino Acid Structures from Klug & Cummings
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Amino Acid Structures from Klug & Cummings
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Amino Acid Structures from Klug & Cummings
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Amino Acid Structures from Klug & Cummings
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Alpha Helix"
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Beta Strands and Sheets"
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Supersecondary structures"
βαβ repeat
Gamma β"crystallin
Greek Key
βαβ-meander
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Modular Nature of Proteins"
Proteins are collections of “modular” domains. For example,
F2 E E
E F2
F2
K K
K Catalytic Domain
Catalytic Domain
PLAT
Coagulation Factor XII
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Modular Nature of Protein Structures"
Example: Diphtheria Toxin
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Domain Architecture Tools"
CDART " Protein AAH24495; Domain Architecture;
" It’s domain relatives;
" Multiple alignment for 2nd domain
SMART
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Active Sites"
Active sites in proteins are usually hydrophobic pockets/crevices/troughs that involve sidechain atoms.
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Active Sites"
Left PDB 3RTD (streptavidin) and the first site located by the MOE Site Finder. Middle 3RTD with complexed ligand (biotin). Right Biotin ligand overlaid with calculated alpha spheres of the first site.
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Secondary Structure Prediction Software"
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PDB: Protein Data Bank" Database of protein tertiary and quaternary
structures and protein complexes. http://www.rcsb.org/pdb/
Over 29,000 structures as of Feb 1, 2005. Structures determined by
" NMR Spectroscopy " X-ray crystallography " Computational prediction methods
Sample PDB file: Click here [▪]
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Protein Folding"
How to find minimum energy configuration?
Unfolded
Molten Globule State
Folded Native State
Rapid (< 1s)
Slow (1 – 1000 s)
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Protein Structures" Most proteins have a hydrophobic core. Within the core, specific interactions take place
between amino acid side chains. Can an amino acid be replaced by some other amino
acid? " Limited by space and available contacts with nearby
amino acids Outside the core, proteins are composed of loops
and structural elements in contact with water, solvent, other proteins and other structures.
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Viewing Protein Structures" SPDBV RASMOL CHIME
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Secondary Structure Prediction Software"
Recent Ones:"GOR V"PREDATOR"Zpred"PROF"NNSSP"PHD"PSIPRED"Jnet"
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Chou & Fasman Propensities"
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GOR IV prediction for 1bbc"
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PDB: Protein Data Bank" Database of protein tertiary and quaternary
structures and protein complexes. http://www.rcsb.org/pdb/
Over 29,000 structures as of Feb 1, 2005. Structures determined by
" NMR Spectroscopy " X-ray crystallography " Computational prediction methods
Sample PDB file: Click here [▪]
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PDB Search Results"
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Protein Folding"
How to find minimum energy configuration?
Unfolded
Molten Globule State
Folded Native State
Rapid (< 1s)
Slow (1 – 1000 s)
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Protein Folding"
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Energy Landscape"
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Protein Structures" Most proteins have a hydrophobic core. Within the core, specific interactions take place
between amino acid side chains. Can an amino acid be replaced by some other amino
acid? " Limited by space and available contacts with nearby
amino acids Outside the core, proteins are composed of loops
and structural elements in contact with water, solvent, other proteins and other structures.
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Viewing Protein Structures" SPDBV RASMOL CHIME
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Structural Alignment" What is structural alignment of proteins?
" 3-d superimposition of the atoms as “best as possible”, i.e., to minimize RMSD (root mean square deviation).
" Can be done using VAST and SARF
Structural similarity is common, even among proteins that do not share sequence similarity or evolutionary relationship.
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Other databases & tools" MMDB contains groups of structurally related proteins SARF structurally similar proteins using secondary structure elements VAST Structure Neighbors SSAP uses double dynamic programming to structurally align proteins
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Protein Structure Prediction" Holy Grail of bioinformatics Protein Structure Initiative to determine a set of protein
structures that span protein structure space sufficiently well. WHY? " Number of folds in natural proteins is limited. Thus a newly
discovered proteins should be within modeling distance of some protein in set.
CASP: Critical Assessment of techniques for structure prediction " To stimulate work in this difficult field
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PSP Methods" homology-based modeling methods based on fold recognition
" Threading methods ab initio methods
" From first principles " With the help of databases
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ROSETTA" Best method for PSP As proteins fold, a large number of partially folded, low-
energy conformations are formed, and that local structures combine to form more global structures with minimum energy.
Build a database of known structures (I-sites) of short sequences (3-15 residues).
Monte Carlo simulation assembling possible substructures and computing energy
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Modeling Servers" SwissMODEL 3DJigsaw CPHModel ESyPred3D Geno3D SDSC1 Rosetta MolIDE SCWRL PSIPred MODELLER LOOPY
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Gel Electrophoresis for Protein!
Protein is also charged Has to be denatured - WHY Gel: SDS-Polyacrylamide gels Add sample to well Apply voltage Size determines speed Add dye to assess the speed Stain to see the protein bands
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Q'BIC Bioinformatics 49
Protein Gel!
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2D-Gels!
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2D Gel Electrophoresis!
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Mass Spectrometry
Mass measurements By Time-of-Flight Pulses of light from laser ionizes protein that is absorbed on metal target. Electric field accelerates molecules in sample towards detector. The time to the detector is inversely proportional to the mass of the molecule. Simple conversion to mass gives the molecular weights of proteins and peptides.
Using Peptide Masses to Identify Proteins: One powerful use of mass spectrometers is to identify a protein from its peptide mass fingerprint. A peptide mass fingerprint is a compilation of the molecular weights of peptides generated by a specific protease. The molecular weights of the parent protein prior to protease treatment and the subsequent proteolytic fragments are used to search genome databases for any similarly sized protein with identical or similar peptide mass maps. The increasing availability of genome sequences combined with this approach has almost eliminated the need to chemically sequence a protein to determine its amino acid sequence.
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Mass Spectrometry!
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Protein Sequence!
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20 amino acids How is it ordered? Basis: Edman Degradation (Pehr Edman)
Limited ~30 residues React with Phenylisothiocyanate Cleave and chromatography
First separate the proteins – Use 2D gels Then digest to get pieces Then sequence the smaller pieces Tedious Mass spectrometry