The Coding and Noncoding Architecture of the Caulobacter crescentus Genome
Creators
- 1. Stanford University
- 2. University of California, San Francisco
- 3. University of Chicago
Description
Caulobacter crescentus undergoes an asymmetric cell division controlled by a genetic circuit that cycles in space and time. We provide a universal strategy for defining the coding potential of bacterial genomes by applying ribosome profiling, RNA-seq, global 5′-RACE, and liquid chromatography coupled with tandem mass spectrometry (LC-MS) data to the 4-megabase C. crescentus genome. We mapped transcript units at single base-pair resolution using RNA-seq together with global 5′-RACE. Additionally, using ribosome profiling and LC-MS, we mapped translation start sites and coding regions with near complete coverage. We found most start codons lacked corresponding Shine-Dalgarno sites although ribosomes were observed to pause at internal Shine-Dalgarno sites within the coding DNA sequence (CDS). These data suggest a more prevalent use of the Shine-Dalgarno sequence for ribosome pausing rather than translation initiation in C. crescentus. Overall 19% of the transcribed and translated genomic elements were newly identified or significantly improved by this approach, providing a valuable genomic resource to elucidate the complete C. crescentus genetic circuitry that controls asymmetric cell division.
Files
journal.pgen.1004463.pdf
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Additional details
Identifiers
- DOI
- 10.1371/journal.pgen.1004463
- Other
- oai:uchicago.tind.io:10394
Funding
- National Institutes of Health
- postdoctoral fellowship
- National Institutes of Health
- R01 GM51426
- National Institutes of Health
- R01 GM32506
- Stanford University
- graduate fellowship
- Helen Hay Whitney Foundation
- National Institutes of Health
- Pathway to Independence Award
- Gordon and Betty Moore Foundation
- GBMF 2550.03
- Life Sciences Research Foundation
- Jane Coffin Childs Memorial Fund
- Fellowship
- National Institutes of Health
- training grant
- Howard Hughes Medical Institute