Abstract

In just the last few years, fluorescent light microscopy has shown that in bacteria, many proteins are dynamically regulated in both time and space, certain chromosomal loci are strictly positioned, and numerous cytoskeletal filaments exist. Thus instead of being simple """"""""bags"""""""" of enzymes, even prokaryotic cells have substantial internal organization that enables their life cycle. The molecular basis of this organization is still unclear, but two key functions of""""""""the bacterial cytoskeleton have been hypothesized: determination of cell shape and segregation of chromosomes during cell division. In support of these hypotheses, several shape-altering mutations have been found in proteins which form cytoskeletal filaments just inside the cytoplasmic membrane, including MreB, Mbl, CreS, and FtsZ. In addition, it is now clear that at least some bacterial plasmids are segregated by prokaryotic actin homologs that form filamentous mitotic machineries, and specific molecular models have been proposed. A growing body of evidence suggests that prokaryotic chromosomes are also actively segregated and positioned by protein filaments. Concurrent to these discoveries, electron cryotomography has emerged as a powerfulnew tool to visualize the three- dimensional structure of intact, small cells to """"""""molecular resolution"""""""" (~4-8 nm) in a life-like state. Capitalizing on the recent installation of a one-of-a-kind, state-of-the-art electron cryomicroscope at the California Institute of Technology, we have, for the first time just last year, visualized bacterial cytoskeletal filaments directly within intact cells. Here we propose to extend these results and test the hypotheses above by determining the structure of the bacterial cytoskeleton in several model species throughout their life cycles by electron cryotomography. We believe the most exciting result will be direct visualization of mitotic machineries involved in bacterial chromosome segregation. Because this work will exploit prototype new instrumentation, a significant component of the effort will be technology development. This will include optimizing and refining strategies for collecting dual-axis tilt-series of frozen-hydrated cells as well as development of software to optimally merge the images into a three-dimensional reconstruction.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI067548-03
Application #
7325689
Study Section
Microscopic Imaging Study Section (MI)
Program Officer
Korpela, Jukka K
Project Start
2005-12-15
Project End
2010-11-30
Budget Start
2007-12-01
Budget End
2008-11-30
Support Year
3
Fiscal Year
2008
Total Cost
$326,377
Indirect Cost

  Institution

Name
California Institute of Technology
Department
Type
Schools of Arts and Sciences
DUNS #
009584210
City
Pasadena
State
CA
Country
United States
Zip Code
91125

  Publications

Swulius, Matthew T; Chen, Songye; Jane Ding, H et al. (2011) Long helical filaments are not seen encircling cells in electron cryotomograms of rod-shaped bacteria. Biochem Biophys Res Commun 407:650-5
Shetty, Ameesha; Chen, Shicheng; Tocheva, Elitza I et al. (2011) Nanopods: a new bacterial structure and mechanism for deployment of outer membrane vesicles. PLoS One 6:e20725
Briegel, Ariane; Chen, Songye; Koster, Abraham J et al. (2010) Correlated light and electron cryo-microscopy. Methods Enzymol 481:317-41
Leong, Peter A; Yu, Xuekui; Zhou, Z Hong et al. (2010) Correcting for the ewald sphere in high-resolution single-particle reconstructions. Methods Enzymol 482:369-80
Chen, Songye; McDowall, Alasdair; Dobro, Megan J et al. (2010) Electron cryotomography of bacterial cells. J Vis Exp :
Cabeen, Matthew T; Murolo, Michelle A; Briegel, Ariane et al. (2010) Mutations in the Lipopolysaccharide biosynthesis pathway interfere with crescentin-mediated cell curvature in Caulobacter crescentus. J Bacteriol 192:3368-78
Ingerson-Mahar, Michael; Briegel, Ariane; Werner, John N et al. (2010) The metabolic enzyme CTP synthase forms cytoskeletal filaments. Nat Cell Biol 12:739-46
Möll, Andrea; Schlimpert, Susan; Briegel, Ariane et al. (2010) DipM, a new factor required for peptidoglycan remodelling during cell division in Caulobacter crescentus. Mol Microbiol 77:90-107
Kuhn, Juliane; Briegel, Ariane; Morschel, Erhard et al. (2010) Bactofilins, a ubiquitous class of cytoskeletal proteins mediating polar localization of a cell wall synthase in Caulobacter crescentus. EMBO J 29:327-39
Iancu, Cristina V; Morris, Dylan M; Dou, Zhicheng et al. (2010) Organization, structure, and assembly of alpha-carboxysomes determined by electron cryotomography of intact cells. J Mol Biol 396:105-17

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