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Active RESEARCH GRANT UKRI Gateway to Research

The essential link between DNA repair and cell wall synthesis in bacteria

£5.09M GBP

Funder Biotechnology and Biological Sciences Research Council
Recipient Organization Newcastle University
Country United Kingdom
Start Date Dec 01, 2023
End Date Nov 30, 2026
Duration 1,095 days
Number of Grantees 1
Roles Principal Investigator
Data Source UKRI Gateway to Research
Grant ID BB/Y002644/1
Grant Description

Bacteria are too small to be seen without a microscope, but they are abundant and ubiquitous and, their influence on our life is enormous. Humans share our body with a large number and a very diverse number of species of bacteria that thrive in/on different parts of our body. While some of the bacteria are beneficial for the environment and for our health, some cause diseases, from small wound infections, to diarrhoea to lethal diseases such as sepsis and pneumonia.

Being one of the earliest life forms on earth, bacteria are robust and have evolved to be able to survive and propagate in different environments. The cell wall that is located outside of the bacterial cell membrane protects bacteria from adverse environmental conditions and also prevents the cell from bursting due to its high internal pressure. When bacteria propagate, the stress-bearing cell wall needs to expand in such a way that the new cell wall material is synthesised and woven into the existing wall without weakening or damaging the wall in the process.

Compromising the integrity of the cell wall will lead to cell death by lysis. Many of our best antibiotics, e.g., penicillin, kill bacteria by inhibiting cell wall synthesis.

In addition to a strong yet dynamic cell wall, to produce fit and healthy progeny the cell also needs to duplicate its chromosome without mistakes and then partition the two sister chromosomes to the appropriate positions in the cell before cell division. It is essential that all mistakes and any damage that occurs during the process of duplication are repaired so that the chromosomes inherited by the daughter cells are intact.

Therefore, maintaining the integrity of the chromosome and maintaining the integrity of the cell wall are both essential for bacteria. However, they are considered independent processes and are not known to be connected.

Recently we were surprised and excited to discover some potential links between these two seemingly unrelated processes: 1) Mutants of the cell wall synthesis gene ponA, which is known to have 'thinner' cells, exhibit chromosome defects; 2) In many bacteria the ponA gene is located on the chromosome in a 'cluster' with a chromosome repair gene called recU. Normally genes forming a cluster have related functions, and a cell wall synthesis gene being so tightly associated with a DNA repair gene, in so many bacteria, suggests a functional link between these two genes. 3) Removal of either ponA or recU does not affect the viability of the cell, but removing both genes is lethal.

This is puzzling but interesting as it again indicates that chromosome repair and cell wall synthesis are somehow connected. 4) Many bacteria have a second cluster of genes that contain a gene involved in chromosome repair (for a different type of damage) and genes involved in cell wall metabolism. This suggests that chromosome repair and cell wall synthesis may have multiple links.

This proposal aims to investigate and understand the potential links between chromosome repair and cell wall synthesis. We want to know how the links are mediated, the impacts of cell width and impaired cell wall synthesis on chromosome repair and distribution, and how DNA damage affects the cell wall. A molecular understanding of the chromosome - cell wall links will help us identify new targets for antibiotics, and develop new antimicrobial strategies to optimise the use of the existing antibiotics and combat antibiotics resistance.

All Grantees

Newcastle University

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