President and Chief Executive Officer, Professor
Ph.D., Australian National University, 1979

Cancer; cell cycle; DNA replication; chromatin assembly; biochemistry; yeast genetics

email This e-mail address is being protected from spambots. You need JavaScript enabled to view it , phone (516) 367-8383, fax (516) 367-8879

Two important stages of cell division are the accurate duplication of genetic information contained within chromosomal DNA and the segregation of the replicated DNA during mitosis. We investigate the mechanism and control of DNA replication in human cells and the yeast Saccharomyces cerevisiae. Previous studies resulted in the identification of many of the cellular proteins that function at the DNA replication fork during the S-phase of the cell division cycle, including proteins that facilitate chromatin assembly dependent upon DNA replication. These latter proteins propagate epigenetically determined states of gene expression and the inheritance of chromatin structures. We continue to study the epigenetic inheritance of chromatin structures in eukaryotes.

The main thrust of our current research is to investigate the mechanism and cell cycle regulation of the initiation of chromosome DNA replication. A key protein that binds to origins of DNA replication, called the Origin Recognition Complex (ORC), initiates the entire process of making chromosomes competent for duplication. ORC binds origins of DNA replication and to other initiation proteins such as Cdc6p and Cdt1 to recruit the MCM helicase. Later steps in the process of initiation are controlled by cyclin- and Dbf4-dependent protein kinases. ORC subunits are also involved in the function of centromeres and in controlling the inheritance of centrosomes, the organelles that facilitate spindle formation during mitosis. Finally, ORC plays a major role in the spatial control of DNA replication in the nucleus and the timing of when different regions of chromosomes are copied in S phase.

Selected Publications

Li, H. and Stillman, B. 2012. The origin recognition complex: a biochemical and structural view. Subcell. Biochem. 62: 37–58.

Mazurek, A., Luo, W., Krasnitz, A., Hicks, J., Scott, Powers, S. and Stillman, B. 2012. DDX5 regulates DNA replication and is essential for cell proliferation in a subset of breast cancer cells. Cancer Discov. 2: 812–819. 

Hossain, M. and Stillman, B. 2012. Meier-Gorlin Syndrome mutations disrupt an Orc1 CDK inhibitory domain and cause centrosome re-duplication. Genes Dev. 26: 1797–1810. 

Nakano, S., Stillman, B. and Horvitz, H. R. 2011. Replication-coupled chromatin assembly generates a neuronal bilateral asymmetry in C. elegans. Cell 147: 1525–1536. 

Sheu, Y-J. and Stillman, B. 2010. The Dbf4-Cdc7 kinase promotes S phase by alleviating an inhibitory activity in Mcm4. Nature 463: 113­–117.