Meiler Lab

Protein de-novo Folding

Methods Development
Contact Prediction BCL Align Sequence Alignment and Fold Recognition Sparse EPR Data guided Protein Structure Elucidation Jufo9D Secondary Structure and TM Span Prediction Protein Structure Prediction using Fold Templates BCL::Cluster: Clustering biological molecules with PyMOL visualization Gradient Minimization for Structure Refinement RosettaTMH
Applications
Modeling of Protein IIIA Structure Determination of DsbB using Paramagnetic Restraints Structure determination of KCNE3 using paramagnetic restraints

Protein Structure Prediction from Sparse Data

Methods Development
Protein Structure Prediction Cryo-EM Fit Cryo-EM Guided Protein Fold Elucidation Membrane Protein Structure Prediction using Sparse NMR Restraints RosettaEPR BCL::EMFitMinimize Protein Structure Prediction using SAXS Data
Applications
Modeling Rhodopsin Interaction with G-Protein and Arrestin Mechanism of Activation of the heterotrimeric G protein alpha subunit

Cheminformatics

Methods Development
Chemical Shift Prediction PharmMap Method Development for QSAR Ligand-based Virtual Screening Development of RosettaQSAR Knowledge-Based Small Molecule Conformational Sampling Novel HTS Datasets composed to benchmark ligand-based QSAR Modeling
Applications
mGluR5 Related Neurological Diseases Allosteric Modulators of Neuropeptide Y Receptors Malaria - Inhibition of beta-Hematin Crystallization in Plasmodium falciparum Rapid in silico target identification for anti-malarials

Protein-Protein Interactions

Applications
Structural Characterization of HoxA11 HIV Antibody/Antigens Interactions Antibiotics- Protein/Peptide Interfaces Antibody/Antigens Interaction

Ligand Docking

Methods Development
Rosetta Drug Design Rosetta Design Modeling Partial Covalent Interactions in Protein Ligand Interfaces RosettaLigandEnsemble Drug Design through Foldit Video Game
Applications
Structural Determinants of Antidepressant Drugs GPCR Model Building, Refinement, and Ligand Docking HIV-1 Protease Inhibitor Docking Protein-Ligand Interaction as Cancer Therapeutics

Protein Design

Applications
Evolution of TIM Barrels Chemical Basis of Ligand-Macromolecule Recognition

Protein-Ligand Interaction as Cancer Therapeutics

The cell cycle is controlled by a number of proteins in signaling pathways. One such protein is the KRAS protein which links extra-cellular signals with cell growth and proliferation via signal transduction involving activation and deactivation cycle. This activation-deactivation cycle involves nucleotide exchange process that converts inactive GDP bound form to active GTP bound form. Point mutations of Ras (k-Ras) generate constitutively active protein which leads to tumor genesis. Constitutively active Ras is also involved in re-insurgence after cancer therapy. Therefore there is a great deal of interest in search of inhibitors of nucleotide exchange process as potential anticancer drugs.
We are doing a virtual screen of Ligand Library with proteins of interest for identifying potential Cancer Therapeutics.

Alumni Project Members: Sandeep Kothiwale , Edward W. Lowe Jr

Center for Structural Biology
465 21st Ave South, BIOSCI/MRBIII
Vanderbilt University, Nashville, TN