Research in the Department of Biochemistry

Research Groups

Introduction

Blundell
Brindle
Broadhurst
Brown
Carrington
Dupree
Evan Head of Dept.
Farndale
Gay
Grace
Griffin
Hendrich
Hesketh
Higgins
Hollfelder
Hong
Howe
Hyvonen
Jackson S
Jackson T
Jackson R
Laue
Leadlay
Lester
Lilley
Lipkow

Livesey
Luisi
Lummis
Mata
McCafferty
Metcalfe
Mishima
Miska
Monie
Mott
Murzina
Nietlispach
Owen
Oliver
Packman
Pellegrini
Robinson
Salmond
Scadden
Silva
Smith A
Smith C
Standart
Thomas
Timmers
Tolkovsky
Welch
Zhang

Past members

Crystallographic and Functional Studies of Regulatory Assemblies and Molecular Machines

Research Grouping: Structural and molecular cell biology

Our aim is to understand how fundamental cellular processes are controlled through molecular interactions in multi-component assemblies.

The expression of genetic information can be regulated by controlling the life time of mRNA to fine tune an organism's response to developmental or environmental stimuli. In the bacterium, E. coli, this is regulated by an multi-enzyme assembly called the RNA degradosome. We are exploring the structure and function of the RNA degradosome assembly. The structure of the catalytic domain in complex with RNA substrate is shown in the figure below.

We are studying thiamine-dependent, multi-enzyme assemblies from central metabolism. We have also undertaken a collaborative study of bacterial systems which transport proteins and antibiotics outside of the cell. A structural view of this system will help us to understand the molecular bases of virulence and drug resistance in the Gram-negative family of bacteria.

We directly visualise the individual components and their complexes at an atomic level using X-ray diffraction to reveal the intricate and subtle structures which underlie these complexes. We also use a number of other techniques such as non-dissociating mass spectrometry, neutron and X-ray solution scattering, and calorimetry to analyse macromolecular complexes.

While RNase E forms a tetramer composed of a dimer of dimers, the selective advantage of this quaternary organization is not well understood. The large conformational changes we observe suggest that a highly flexible quaternary organization may play a role in the degradation of structured RNAs. Depicted here is a speculative model of the RNase E tetramer degrading a structured fragment of RNA that serves to illustrate the conformational changes. In the upper left is a view of a single dimer in which one of the S1/5’-sensing domain (blue) has closed down upon an RNA substrate and holds it adjacent to a catalytic cleavage site on a DNase I domain. The complementary protomer within the dimer does not possess a substrate RNA and is in the open configuration. In the lower right, a second dimer plays a supporting role in the degradation of the RNA, interacting with the substrate via a S1 domain to further stabilize the complex. Figure prepared using PDB files 2BX2, 2VMK, and 2A64.

Larger version of this figure

Lab members
Kasia Bandyra, Vivian Chan, Dijun Du, Vasiliki Fadouloglou, Maja Gorna, Steven Hardwick, Hong-Ting Lin, Xue Pei, Zbyszek Pietras, Yi-Chun Tsai

References

Frank, R.A.W., Titman, C., Pratap, V., Luisi, B.F. and Perham, R.N. (2004) A molecular switch and proton-wire synchronize the active-sites in thiamine-dependent enzymes. Science 306, 872-876
Callaghan, A.J., Marcaida, M.J., Stead, J.A., McDowall, K.J., Scott, W.G. and Luisi, B.F. (2005) The structure of E. coli RNase E catalytic domain and implications for RNA turnover. Nature 437 1187-1191.
Frank, R.A.W., Kay, C.W.M., Hirst, J. and Luisi, B.F. (2008) Off-pathway, oxygen-dependent thiamine radical in the Krebs cycle. J. Amer. Chem. Soc 130, 1662-1668.
Bavro, V.N., Pietras, Z., Furnham, N., Perez-Cano, L., Fernandez-Recio, J., Pei, X.Y., Misra, R. and Luisi, B.F. (2008) Channel-opening and assembly in a bacterial drug efflux machine. Molecular Cell 30, 114-121.



© 2005 Department of Biochemistry, University of Cambridge Information provided by Len Packman 7 October, 2009

	Dr Ben Luisi