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Residue Sequence and Structure in the Re evaluation the Categorization of HIV Progression in Subjects Based on CD4 T cell Decline Rates Angela Garibaldi & Ryan Willhite Loyola Marymount University BIOL 398-01 March 23, 2010 Outline • Review of previous experiment using CD4 decline rates • Structure based hypothesis • Methods and programs used • Results • Comparison to More Recent Studies • References Recap of past experiment • Evaluated the categorization of progressors based on CD4 decline rates • Analyzed two moderate progressors (6,7) with rates comparable to non-progressor 13 and rapid progressor 10. • Based on divergence and diversity subject 6 did not act as non-progressor • Subject 7 acted like a rapid progressor. Hypothesis • Subject 7 will be more similar to Methods • Create phylogenetic trees based on amino acid sequence • Use ProtPram to analyze residue composition in subjects 6,7,5,10 • Select 7 and 10 for time point analysis – First clone for selected visits used • Use Cn3d to analyze differences in 3d structure Phylogenetics based on amino acid sequence 10 vs 5 10 vs 7 5 vs 7 Subject 6 v 13 Subjects 6 v 7 Subjects 13 v 5 Subjects 6 v 5 Overall residue composition •All clones available were used in this analysis per individual •Rapid Progressor Subject 10 is the only one with Asn as its most prevalent residue ProtParam Physico-chemical properties of a protein using ExPASy server Subject 5 Properties Subject 6 Subject 7 Subject 10 Residue composition over time Residue composition over time • All clones from selected visits were used. • Subject 10, Rapid Progressor shows Asn as its prevalent residue over time. • Subject 7, Moderate Progressor begins with Asn as prevalent residue • Subject 10 showed sudden jump in Arg %. This may be an artifact. Conclusion • The highest percent of amino acids found in the moderates 5,6, and 7 is (Ile) • The highest percent of amino acids found in the rapid 10 to compare is (Asn) • Looking at these compositions along with protein structure seems to be a more efficient way of categorizing progression • The difference in amino acid composition suggests a role in type of progression A more recent study • Structure of HIV-1 gp120 with gp41interactive region reveals layered envelope architecture and basis of conformational mobility gp120, gp41-interactive region structure •7-stranded β-sandwich,invariant in conformation •highly glycosylated gp120 outer domain. layers act as a shape-changing spacer, facilitating movement between outer domain and gp41-associated β-sandwich • provide for conformational diversity used in immune evasion. • A “layered” gp120 References • Structure of HIV-1 gp120 with gp41interactive region reveals layered envelope architecture and basis of conformational mobility