Barbara Conradt

Associate Professor of Genetics

Regulation of Programmed Cell Death in C. elegans

Programmed cell death, or apoptosis, is the physiological process through which multicellular organisms eliminate superfluous or potentially harmful cells from their body. Deregulated programmed cell death can lead to various types of diseases in humans, including cancer, autoimmune diseases and neurodegenerative diseases, which demonstrates how important this process is for human health. Studies on the molecular mechanisms that regulate and execute programmed cell death will help us understand the function of this process in cellular homeostasis and its role in various pathological processes.

Most of our current knowledge of programmed cell death is based on genetic and molecular analyses of the nematode Caenorhabditis elegans, an organism that is especially amenable to studies on programmed cell death. These studies revealed that the central cellular machinery employed by organisms as diverse as C. elegans and humans to eliminate cells in a 'programmed' manner has been conserved. Using C. elegans as a tool, the goal of our current research is to identify pathways and mechanisms that regulate this central cell-death machinery. In specific, using genetic and molecular approaches, we are studying how the activity of BH3-only proteins (BH3, Bcl-2 Homology region 3), key activators of programmed cell death, are regulated during C. elegans development. Results from these studies will contribute to our knowledge of the molecular mechanisms of programmed cell death not only in C. elegans but in higher organisms as well.

Publications

• Schertel, C. and Conradt, B. 2007. C. elegans orthologues of components of the Rb tumor suppressor complex have distinct pro-apoptotic functions. Development (in press).
• Rolland, S. and Conradt, B. 2006. The role of mitochondria in apoptosis induction in Caenorhabditis elegans: more than just innocent bystanders? Cell Death Differ 13:1281-1286.
• Grote, P. and Conradt, B. 2006. The PLZF-like protein TRA-4 co-operates with the Gli-like transcription factor TRA-1 to promote female development in C. elegans. Dev Cell 11:561-573.
• Conradt, B. 2006. Cell biology: Mitochondria shape up. Nature 443:646-647.
• Jagasia, R., Grote, P., Westermann, B., Conradt, B. 2005. DRP-1-mediated mitochondrial fragmentation during EGL-1-induced cell death in C. elegans. Nature, 433: 754-760.
• Jäger, S., Schwartz, H. T., Horvitz, H. R. and Conradt, B. 2004. The C. elegans F-box protein SEL-10 promotes female development and may act by targeting the proteins FEM-1 and FEM-3 for degradation by the proteasome. PNAS, 101:12549-12554.
• Hoeppner, D. J., Spector, M.S., Ratcliff, T.M., Kinchen, J. M., Granat, S., Lin, S.-C., Bhusri, S. S., Conradt, B., Herman, M. A., and Hengartner, M. O. 2004. eor-1 and eor-2 are required for cell-specific apoptotic death in C. elegans. Dev Biol, 274:125-138.
• Thellmann, M., Hatzold, J. and Conradt, B. 2003. The Snail-like CES-1 protein of C. elegans can block the expression of the BH3-only cell-death activator gene egl-1 by antagonizing the function of bHLH proteins. Development, 130:4057-4071.
• Conradt, B.. 2002. With a little help from your friends: cells don't die alone. Nature Cell Biol, 4: E139-143.
• Conradt, B.. 2001. Cell engulfment, no sooner ced than done. Dev Cell, 1:445-447.
• Chen F., Hersh, B. M., Conradt, B., Zhou Z., Riemer, D., Gruenbaum, Y. and H. R. Horvitz. 2000. CED-4 Translocation to Nuclear Membranes during C. elegans Programmed Cell Death. Science, 287:1485-1489.
• B. Conradt and H. R. Horvitz. 1999. The TRA-1 Sex Determination Protein of C. elegans Regulates Sexually Dimorphic Cell Deaths by Repressing the egl-1 Cell Death Activator Gene. Cell, 98:317-327.
• B. Conradt and H. R. Horvitz. 1998. The C. elegans Protein EGL-1 is Required for Programmed Cell Death and Interacts with the Bcl-2-like Protein CED-9. Cell, 93:519-529.