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Visualizing Protein Structures Genetic information, stored in DNA, is conveyed as proteins Genetic information, stored in DNA, is conveyed as proteins The immediate product of translation is the primary protein structure General Amino Acid Structure H H2N α C R COOH List of Amino Acids and Their Abbreviations Nonpolar (hydrophobic) amino acid glycine alanine valine leucine isoleucine methionine phenylalanine tryptophan proline 3 letter code Gly Ala Val Leu Ile Met Phe Trp Pro 1 letter code G A V L I M F W P Polar (hydrophilic) serine threonine cysteine tyrosine asparagine glutamine Ser Thr Cys Tyr Asn Gln S T C Y N Q Electrically Charged (negative and hydrophilic) aspartic acid glutamic acid Asp Glu D E Electrically Charged (positive and hydrophilic) lysine Lys K arginine Arg R histidine His H Others X = unknown * = STOP General Amino Acid Structure H H2N α C R COOH Peptide Bond Formation Peptides have rotatable bonds of defined lengths Note- all proteins have polarity- N termini; C termini The ‘protein-folding problem’. • Proteins -- hundreds of thousands of different ones -- are the biochemical molecules that make up cells, organs and organisms. Proteins put themselves together, in a process termed "folding." How they do that is called "the proteinfolding problem," and it may be the most important unanswered question in the life sciences. WHY?? The primary sequence dictates the secondary and tertiary structure of the protein Protein Structure Two questions • Can you change the 3 (tertiary) o sequence without changing the 1 (primary) sequence? o • Can you change the 1o (primary) o sequence without changing the 3 (tertiary) sequence? What is known about protein folding? • Secondary Structures are dominated by: • 1) a-helix • 2) b-sheet a-helical structure is a very regular structure (3.6 amino acids/turn) b-sheet: anti-parallel b-sheet: parallel Hydrogen Bonding And Secondary Structure alpha-helix beta-sheet Hydrogen Bonding • One of the most important stabilizing forces in protein structure! • Both a-helix and b-sheet are dependent on H-bonding. Protein Folding is progressive? 1° - first 2°- second 3° - third Formation of tertiary structure The tertiary structure (or conformation) is the way alpha -helixes and beta -pleated sheets fold in respect to each other. Amino acids which are very distant in the primary structure might be close in the tertiary one because of the folding of the chain. Structure Stabilizing Interactions (Factors governing 3° structure) • Noncovalent – Van der Waals forces (transient, weak electrical attraction of one atom for another) – Hydrophobic (clustering of nonpolar groups) – Hydrogen bonding – Salt bridges • Covalent – Disulfide bonds Hydrophobic and Hydrophilic Interactions: • Hydrophilic amino acids are those whose sidechains offer hydrogen bonding partners to the surrounding water molecules. • Hydrophobic amino acids: • Hydrophilic amino acids: • Tend to internalize in water. • Tend to externalize in water. • Tend to externalize in a membrane • Tend to internalize in a membrane Disulfide Bridge Disulfide Bridge – Linking Distant Amino Acids Structure Stabilizing Interactions (Factors governing 3° structure) • Noncovalent – Van der Waals forces (transient, weak electrical attraction of one atom for another) – Hydrophobic (clustering of nonpolar groups) – Hydrogen bonding – Salt bridges • Covalent – Disulfide bonds • Protein G Structure Tutorial • The transformation happens quickly and spontaneously. It takes only a fraction of a second for a floppy chain of beads to fold into the shape it will keep for the rest of its working life. • How does that happen? How do the linear -- and, in some sense, one-dimensional -structures of proteins carry the information that tells them to take on permanent threedimensional shapes? Is it possible to study a protein chain and predict the folded shape it will take? • That is the protein-folding problem. DNA sequencing information predictions of the primary amino acid sequence. Needed- Software that will convert o the 1 sequence to its corresponding o 3 sequence. Needed- Software that will describe a o 1 sequence that will generate a o particular 3 sequence. Structure classification: • Finding proteins that have similar chemical architectures. This involves developing a representation of how units of secondary structure come together to form ‘domains’*. • *compact regions of structure within the large protein structure. • The Protein Data Bank The End • WHY IS PROTEIN FOLDING SO DIFFICULT TO UNDERSTAND? • It's amazing that not only do proteins selfassemble -- fold -- but they do so amazingly quickly: some as fast as a millionth of a second. While this time is very fast on a person's timescale, it's remarkably long for computers to simulate. In fact there is a 1000 X gap between the simulation timescales (nanoseconds) and the times at which the fastest proteins fold (microseconds). A Glimpse of the Holy Grail? • The prediction of the native conformation of a protein of known amino acid sequence is one of the great open questions in molecular biology and one of the most demanding challenges in the new field of bioinformatics. Using fast programs and lots of supercomputer time, Duan and Kollman (1) report that they have successfully folded a reasonably sized (36-residue) protein fragment by molecular dynamics simulation into a structure that resembles the native state. At last it seems that the folding of a protein by detailed computer simulation is not as impossible as most workers in the field believe. Proteins from Scratch: • Not long ago, it seemed inconceivable that proteins could be designed from scratch. Because each protein sequence has an astronomical number of potential conformations, it appeared that only an experimentalist with the evolutionary life span of Mother Nature could design a sequence capable of folding into a single, well-defined three-dimensional structure. But now, on page 82 of this issue, Dahiyat and Mayo (1) describe a new approach that makes de novo protein design as easy as running a computer program. Well almost. Progress in the ‘protein-folding problem’? • When proteins fold, they don’t try ever possible 3D conformation. Protein folding is an orderly process (i.e. there are molecular shortcuts involved). Success in protein-folding? Given the primary sequence of a protein, the success rate in predicting the proper 3D structure of a protein shows strong correlation, to the % of the protein that showed similarity to proteins of known structure. The primary sequence dictates the secondary and tertiary structure of the protein