My lab uses X-ray crystallography to better understand the relationship between proteins and ligands. Tiny differences in the structure of a molecule can radically change the interaction between a protein and ligand and we are only begining to understand how many factors play a role in this interaction. By manipulating the individual components of a compound it is possible to create a chemical that binds to the protein better than the natural substrate, and prevent the natural reaction from occurring. This is the basis for rational drug design. Our efforts have lead us to collaborations with other labs and scientists in many disciplines as our approach to directed compound design has applications not only in basic research but also in pesticide development, health research and clinical research.
- Musa, T. L., Ioerger, T. R., & Sacchettini, J. C. (2009). THE TUBERCULOSIS STRUCTURAL GENOMICS CONSORTIUM: A STRUCTURAL GENOMICS APPROACH TO DRUG DISCOVERY. Advances in protein chemistry and structural biology. STRUCTURAL GENOMICS, PART C. (pp. 41-76).
- Lücke, C., Fushman, D., Ludwig, C., Hamilton, J. A., Sacchettini, J. C., & Rüterjans, H. (1999). A comparative study of the backbone dynamics of two closely related lipid binding proteins: Bovine heart fatty acid binding protein and porcine ileal lipid binding protein. Lipid Binding Proteins within Molecular and Cellular Biochemistry. (pp. 109-121). Springer Us.
- Scapin, G., Young, A., Kromminga, A., Veerkamp, J. H., Gordon, J. I., & Sacchettini, J. C. (1993). High resolution X-ray studies of mammalian intestinal and muscle fatty acid-binding proteins provide an opportunity for defining the chemical nature of fatty acid: protein interactions. Cellular Fatty Acid-Binding Proteins II. (pp. 3-13). Springer Us.
- Cistola, D. P., Sacchettini, J. C., & Gordon, J. I. (1990). 13C NMR studies of fatty acid-protein interactions: comparison of homologous fatty acid-binding proteins produced in the intestinal epithelium. Cellular Fatty Acid-binding Proteins. (pp. 101-110). Springer Us.
- Sacchettini, J. C., Banaszak, L. J., & Gordon, J. I. (1990). Expression of rat intestinal fatty acid binding protein in E. coli and its subsequent structural analysis: a model system for studying the molecular details of fatty acid-protein interaction. Cellular Fatty Acid-binding Proteins. (pp. 81-93). Springer Us.
- Purkey, H. E., Lashuel, H. A., Peterson, S. A., Baures, P. W., Klabunde, T., Sacchettini, J. C., & Kelly, J. W. (1998). Inhibiting transthyretin amyloid formation with small molecules.. ACS Photonics. 216, U219-U219.
- Lieberman, J. M., Marks, W. H., Cohn, S., Jaicks, R., Woode, L., Sacchettini, J., ... Burns, G. (1998). Organ Failure, Infection, and the Systemic Inflammatory Response Syndrome Are Associated with Elevated Levels of Urinary Intestinal Fatty Acid Binding Protein. J Trauma Acute Care Surg. 45(5), 900-906..
- Sacchettini, J. C. (1997). Combatting drug resistant tuberculosis.. ACS Photonics. 214, 7-CARB.
- Zhang, F. L., Lucke, C., Baier, L. J., Sacchettini, J. C., & Hamilton, J. A. (1997). Comparison of T54 allele with normal A54 allele of human intestinal fatty acid binding protein.. Biophys J. 72(2), MP294-MP294.
- Xu, Y., Eads, J., Sacchettini, J. C., & Grubmeyer, C. (1996). Catalytic base in hypoxanthine-guanine phosphoribosyltransferase (HGPRTase).. ACS Photonics. 212, 45-BIOL.
- Xu, Y., Eads, J., Sacchettini, J. C., & Grubmeyer, C. (1996). Catalytic base in hypoxanthine-guanine phosphoribosyltransferase (HGPRTase).. BIOCHEMISTRY. 35(28), 45-45.
- Zhang, F. L., Lucke, C., Baier, L. J., Sacchettini, J. C., & Hamilton, J. A. (1996). Multidimensional NMR studies of the structure of human intestinal fatty acid binding protein (I-FABP). Biophys J. 70(2), SU388-SU388.
- BAIER, L. J., & SACCHETTINI, J. C. (1995). AN AMINO-ACID SUBSTITUTION IN THE HUMAN INTESTINAL FATTY-ACID-BINDING PROTEIN ALTERS THE RATE OF TRANSPORT OF FATTY-ACIDS ACROSS INTESTINE-LIKE CELLS. DIABETES. 44, A41-A41.
- MIKAMI, B., HEHRE, E. J., DEGANO, M., & SACCHETTINI, J. C. (1994). CRYSTALLOGRAPHIC ELUCIDATION OF THE ACTIVE-SITE STRUCTURE OF BETA-AMYLASE. ACS Photonics. 207, 95-CARB.
- LOPEZ, M. M., SACCHETTINI, J. C., & FREIRE, E. (1994). THERMODYNAMIC CHARACTERIZATION OF THE STRUCTURAL STABILITY OF A PREDOMINANTLY BETA-STRUCTURE PROTEIN - RAT INTESTINAL FATTY-ACID-BINDING PROTEIN (I-FABP). Biophys J. 66(2), A180-A180.
- Reddy, M., Sacchettini, J. C., Zhou, N. E., & Mccutchen, B. F. (2019). Compositions and methods for inhibition of mycobacteria.
- Sacchettini, J. C., Miller, M. W., Wallis, D., Zhou, N. E., & Fossum, T. W. (2019). Compositions and methods for drug sensitization of parasites.
- Sacchettini, J., Zhou, N., Baker, D., Maxwell, S., & Wallis, D. (2018). Compositions and methods for drug-sensitization or inhibition of a cancer cell.
- Rao, J., Cirillo, J., Xie, H., & Sacchettini, J. (2017). ?-lactamase substrates and methods of their use for the diagnosis of tuberculosis.
- Rao, J., Cirillo, J. D., Xie, H., & Sacchettini, J. C. (2017). β-lactamase substrates and methods of their use for the diagnosis of tuberculosis.
- Harshbarger, Wayne (2015-05). X-Ray Crystal Structure of Human 20s Proteasome in Complex with Carfilzomib. (Doctoral Dissertation)
- Jung, Hunmin (2014-12). Development of Potent and Selective Inhibitors of Mycobacterium Tuberculosis, Plasmodium Falciparum and Staphylococcus Aureus Dihydrofolate Reductase. (Doctoral Dissertation)
- Joseph, Sonia (2014-08). The Biochemical Investigation and Isolation of Small Molecule Inhibitors for Two Essential Proteins of Mycobacterium tuberculosis H37Rv: IspD and Wag31. (Master's Thesis)
- Lalgondar, Mallikarjun (2014-05). Structural Studies and Evaluation of Inhibitors of Mycobacterium tuberculosis H37Rv Shikimate Dehydrogenase (MtSDH). (Master's Thesis)