This renewal proposal describes plans to continue a vigorous chemistry-biology interface (CBI) predoctoral training program that is designed to train scientists in key aspects of fundamental organic and biological chemistry as well as in scientific disciplines at the interface of chemistry and biology. The program, now in its ninth year, further advances the interdisciplinary training of our most motivated and well qualified students by focusing their graduate academic work around a core curriculum in areas spanning both chemical and biological disciplines. Each trainee may carry out his or her doctoral thesis research in one or more of the laboratories of the twenty two faculty trainers affiliated with the following nine participating units: Chemistry and Chemical Biology, Neurobiology and Behavior, Molecular Biology and Genetics, Biomedical Sciences, Chemical and Biomolecular Engineering, Microbiology and Immunology, Plant Pathology, Plant Biology and Nutritional Sciences. All participating faculty have strong research programs either in chemistry with strong biological connections or in biology with strong chemical connections and are well-funded. Their overall research interests are broadly distributed over chemistry (synthetic organic, bioorganic, biophysical, polymer, x-ray crystallography and proteomics) and biology (protein structure and function, enzymology, immunology, signal transduction, chemotaxis, host/pathogen interactions and genetics). CBI trainees attend seminars in their core disciplines (usually weekly) in their respective units, participate together with faculty in a special monthly CBI seminar program, and organize monthly CBI """"""""literature lunches"""""""". Two additional features distinguish the Cornell CBI program. First, trainees invite, organize, and host special CBI seminar speakers each semester. Secondly, trainees are required to participate in internships in biotech, life science, or pharmaceutical companies, through which they gain exposure to, and experience in, interdisciplinary biomedical research.
| Spraker, Joseph E; Wiemann, Philipp; Baccile, Joshua A et al. (2018) Conserved Responses in a War of Small Molecules between a Plant-Pathogenic Bacterium and Fungi. MBio 9: |
| Parvez, Saba; Long, Marcus J C; Poganik, Jesse R et al. (2018) Redox Signaling by Reactive Electrophiles and Oxidants. Chem Rev 118:8798-8888 |
| Khalid, Saima; Baccile, Joshua A; Spraker, Joseph E et al. (2018) NRPS-Derived Isoquinolines and Lipopetides Mediate Antagonism between Plant Pathogenic Fungi and Bacteria. ACS Chem Biol 13:171-179 |
| O'Neill, Erinn M; Mucyn, Tatiana S; Patteson, Jon B et al. (2018) Phevamine A, a small molecule that suppresses plant immune responses. Proc Natl Acad Sci U S A 115:E9514-E9522 |
| Long, Marcus J C; Urul, Daniel A; Chawla, Shivansh et al. (2018) Precision Electrophile Tagging in Caenorhabditis elegans. Biochemistry 57:216-220 |
| Falcke, Jan M; Bose, Neelanjan; Artyukhin, Alexander B et al. (2018) Linking Genomic and Metabolomic Natural Variation Uncovers Nematode Pheromone Biosynthesis. Cell Chem Biol 25:787-796.e12 |
| Poganik, Jesse R; Aye, Yimon (2018) Weighing up the Selenocysteome Uncovers New Sec-rets. Cell Chem Biol 25:1315-1317 |
| O'Donnell, John P; Byrnes, Laura J; Cooley, Richard B et al. (2018) A hereditary spastic paraplegia-associated atlastin variant exhibits defective allosteric coupling in the catalytic core. J Biol Chem 293:687-700 |
| Lim, Fang Yun; Won, Tae Hyung; Raffa, Nicholas et al. (2018) Fungal Isocyanide Synthases and Xanthocillin Biosynthesis in Aspergillus fumigatus. MBio 9: |
| O'Donnell, John P; Cooley, Richard B; Kelly, Carolyn M et al. (2017) Timing and Reset Mechanism of GTP Hydrolysis-Driven Conformational Changes of Atlastin. Structure 25:997-1010.e4 |
Showing the most recent 10 out of 118 publications
