Abstract

The goal of this proposal is to give a genetic, thermodynamic and structural description of how one protein fold (and function) changes into another. This is based on our ability to: 1) Create highly homologous proteins with different folds (heteromorphic pairs); 2) Engineer dual functional capacity within each member of the heteromorphic pair such that one binding function is manifest in one fold and cryptic in the other fold; 3) Use the thermodynamic linkage between folding and binding to determine folding propensity; 4) Use NMR to determine structures of heteromorphic pairs. Our ability to parse the fold-specific folding code from the overall stability code allows us to study a code for conformational switching between two folds. ? ? The specific goals are as follows: 1. Determine an efficient evolutionary path from one fold and function to another; 2. Establish the minimum sequence gap separating two functional folds; 3. Generate heteromorphic pairs of maximum identity for structural and thermodynamic study. We will study how small sets of amino acids determine two different native folds. This will be done by completely examining the functional sequence space separating the two folds, measuring the effects of small numbers of mutations on folding propensity, and determining structures to assess how a limited set of interactions can determine fold. Understanding how a small set of mutations can cause a switch between two stable, monomeric folds and two different functions will have profound implications on our understanding of protein folding, bioinformatics and the natural evolution of new folds and functions.
The aim of this proposal is to better understand how amino acid sequence specifies unique tertiary folds by reducing the folding problem to those amino acids that contain the most information toward specifying one fold versus another. This work has direct implications for understanding the protein folding code and the evolution of new folds and will greatly benefit the fields of protein engineering, protein structure prediction, and de novo protein design. Advances in these areas will be needed in the continuing development of new biomedically useful therapeutics to improve human health. ? ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
2R01GM062154-05A1
Application #
7387991
Study Section
Macromolecular Structure and Function B Study Section (MSFB)
Program Officer
Smith, Ward
Project Start
2002-03-01
Project End
2012-08-31
Budget Start
2008-09-01
Budget End
2009-08-31
Support Year
5
Fiscal Year
2008
Total Cost
$277,334
Indirect Cost

  Institution

Name
University of MD Biotechnology Institute
Department
Type
Organized Research Units
DUNS #
603819210
City
Baltimore
State
MD
Country
United States
Zip Code
21202

  Publications

Kulkarni, Prakash; Solomon, Tsega L; He, Yanan et al. (2018) Structural metamorphism and polymorphism in proteins on the brink of thermodynamic stability. Protein Sci 27:1557-1567
Jolly, Mohit Kumar; Kulkarni, Prakash; Weninger, Keith et al. (2018) Phenotypic Plasticity, Bet-Hedging, and Androgen Independence in Prostate Cancer: Role of Non-Genetic Heterogeneity. Front Oncol 8:50
Lin, Xingcheng; Roy, Susmita; Jolly, Mohit Kumar et al. (2018) PAGE4 and Conformational Switching: Insights from Molecular Dynamics Simulations and Implications for Prostate Cancer. J Mol Biol 430:2422-2438
Kulkarni, Prakash; Jolly, Mohit Kumar; Jia, Dongya et al. (2017) Phosphorylation-induced conformational dynamics in an intrinsically disordered protein and potential role in phenotypic heterogeneity. Proc Natl Acad Sci U S A 114:E2644-E2653
He, Yanan; Chen, Yihong; Mooney, Steven M et al. (2015) Phosphorylation-induced Conformational Ensemble Switching in an Intrinsically Disordered Cancer/Testis Antigen. J Biol Chem 290:25090-102
Porter, Lauren L; He, Yanan; Chen, Yihong et al. (2015) Subdomain interactions foster the design of two protein pairs with ?80% sequence identity but different folds. Biophys J 108:154-62
Bryan, Philip N; Orban, John (2013) Implications of protein fold switching. Curr Opin Struct Biol 23:314-6
He, Yanan; Chen, Yihong; Alexander, Patrick A et al. (2012) Mutational tipping points for switching protein folds and functions. Structure 20:283-91
Morrone, Angela; McCully, Michelle E; Bryan, Philip N et al. (2011) The denatured state dictates the topology of two proteins with almost identical sequence but different native structure and function. J Biol Chem 286:3863-72
Shen, Yang; Bryan, Philip N; He, Yanan et al. (2010) De novo structure generation using chemical shifts for proteins with high-sequence identity but different folds. Protein Sci 19:349-56

Showing the most recent 10 out of 25 publications