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| Status |
Public on Mar 29, 2020 |
| Title |
Integrative and quantitative analysis reveals proper CtrA-dependent cell cycle regulation in the absence of the DivJ/PleC asymmetry module in the stalked budding bacterium Hyphomonas neptunium |
| Organism |
Hyphomonas neptunium |
| Experiment type |
Genome binding/occupancy profiling by high throughput sequencing
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| Summary |
Alphaproteobacteria stand out for their complex cell cycles, which are often regulated by the DivJ/PleC-DivK-DivL-CckA-ChpT-CtrA pathway. DivJ and PleC set up the polarity of the cell, thereby eventually leading to differential activation of the DNA-binding response regulator CtrA in the two nascent daughter cells. CtrA regulates replication and transcription of many genes, thereby ensuring that processes such as motility and cell division take place at the appropriate cell cycle stage. The cell cycle of the stalked budding alphaproteobacterium Hyphomonas neptunium culminates in an asymmetric cell division at the stalk-bud junction. Here, we investigate the role of the pathway from DivJ and PleC down to CtrA in this recently established model organism. Even though DivJ and PleC are localized to opposite poles, suggesting they are involved in polarity establishment inH. neptunium, DivJ, PleC and the other components of the upstream pathway (DivK and PleD) are not essential for cell cycle regulation. In contrast, the downstream part of the pathway starting from DivL is essential and involved in the regulation of important functions such as replication inhibition, cell division and motility, as shown by the identification of the (direct) regulon of CtrA. The overlap between the regulons of DivJ and PleC, DivK and CtrA is only partial, demonstrating that additional factors feeding into the pathway must be present in H. neptunium. Furthermore, unlike in other alphaproteobacteria, the regulation of CtrA throughout the cell cycle does not take place at the level of CtrA abundance in H. neptunium. All in all, the DivL-CckA-ChpT-CtrA pathway plays an essential role in the regulation of the complicated cell cycle ofH. neptunium, but several proteins feeding into CtrA remain undiscovered. The in-depth analysis of CtrA regulation in this stalked budding organism leads to hypotheses that might also hold in well-established model organisms such as Caulobacter crescentus.
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| Overall design |
Examination of CtrA and GcrA whole genome binding/occupency (ChIP-Seq) in WT Hyphomonas neptunium LE670 (ATCC15444).
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| Contributor(s) |
Leicht O, van Teeseling MC, Panis G, Reif CC, Wendt H, Viollier PH, Thanbichler M |
| Citation(s) |
32324740 |
| |
| Submission date |
Jan 11, 2019 |
| Last update date |
May 01, 2023 |
| Contact name |
Patrick H. Viollier |
| E-mail(s) |
[email protected]
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| Organization name |
University of Geneva, Faculty of Medicine / CMU
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| Department |
Dept. Microbiology and Molecular Medicine
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| Street address |
Rue Michel Servet 1
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| City |
Geneva 4 |
| ZIP/Postal code |
1211 |
| Country |
Switzerland |
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| Platforms (1) |
| GPL26030 |
Illumina HiSeq 2000 (Hyphomonas neptunium) |
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| Samples (4)
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| GSM3559993 |
ChIP-Seq_CtrA_H.neptuniumLE670_(GHA-428) |
| GSM3559994 |
ChIP-Seq_CtrA(Totalinput)_H.neptuniumLE670_(GHA-430) |
| GSM3559995 |
ChIP-Seq_GcrA_H.neptuniumLE670_(GHA-465) |
| GSM3559996 |
ChIP-Seq_GcrA(Totalinput)_H.neptuniumLE670_(GHA-466) |
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| This SubSeries is part of SuperSeries: |
| GSE134367 |
Integrative and quantitative view of the CtrA regulatory network in a stalked budding bacterium |
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| Relations |
| BioProject |
PRJNA514449 |
| SRA |
SRP178472 |
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