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Gregory T Marczynski

Academic title(s): 

Associate Professor, Department of Microbiology and Immunology

Ìý

Gregory T Marczynski
Contact Information
Address: 

Duff Medical Building
3775 University St., Room 403
Montreal, QC H3A 2B4
Ìý

Phone: 
514-398-3917
514-398-4526
Fax number: 
514-398-7052
Email address: 
greg.marczynski [at] mcgill.ca
Division: 
Faculty Members
Branch: 
Microbiology
Location: 
Lyman Duff Medical Building
Graduate supervision: 

ACCEPTING GRADUATE STUDENTS

Current research: 

Cell cycle and developmental control of chromosomal replication.ÌýWe wish to understand how chromosome replication is coordinated with cellular growth and development so that replication occurs during the appropriate period of the cell cycle, and in the appropriate cell-type during cellular differentiation. The bacteriumÌýCaulobacter crescentusÌýexemplifies this fundamental control problem, because its cellular differentiation is an obligate part of its cell division cycle, and chromosome replication does not initiate until the "swarmer" cell-type differentiates into the "stalked" cell-type. In bothÌýC. crescentusÌýandÌýE. coli, chromosome replication begins at a unique place, the origin of replication. However, despite the detailed knowledge of the biochemical interactions that take place at theÌýE. coliÌýorigin, very little is actually known about the molecular mechanisms that couple replication to the cell cycle in this or any other bacterium. Presumably, special proteins monitor growth and relay the appropriate signals to the replication proteins at the origin of replication.Ìý

InÌýC. crescentus,Ìýwhere the cell cycle is more amenable to analysis, we propose that a key signaling protein (CtrA) couples replication with the cell cycle. This hypothesis is based on the CtrA protein's homology with a class of phosphorelay proteins (the OmprR response regulators) whose biochemical activities are altered by special phosphokinase proteins, and our recent results demonstrating that CtrA protein has five binding sites inside theÌýC. crescentusÌýorigin of replication (Cori). Interestingly, Cori CtrA binding sites overlap an essential Ï㽶ÊÓƵ polymerase promoter and an essential DnaA protein binding site, implying that CtrA may directly interact with these proteins that are thought to be the earliest acting proteins at theÌýE. coliÌýorigin of replication. Despite the ubiquity of phosphorelay proteins, and the universal requirement for replication control, CtrA is the first candidate response regulator with a direct role in replication control.Ìý

We are currently testing the hypothesis that CtrA is a major regulator of chromosome replication by employing several molecular genetic and biochemical approaches, and we are particularly interested in understanding how CtrA interacts with other proteins such as Ï㽶ÊÓƵ polymerase and DnaA. Since the basic problem is one of reprogramming the chromosomes so that one chromosome is active and the other one is inactive in the appropriate cell-type, we are also studying proteins that modify DNA structure. In particular, we are studying a unique DNA methylation protein (that is also regulated by CtrA), and a new class of proteins that condense and decondense chromatin.

Selected publications: 

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