Scientists at The Scripps Research Institute have unraveled a complex
chemical pathway that enables bacteria to form clusters called biofilms.
Such improved understanding might eventually aid the development of new
treatments targeting biofilms, which are involved in a wide variety of
human infections and help bacteria resist antibiotics.
int on April 26, 2012, by the journal Molecular Cell, explains how nitric oxide, a signaling molecule involved in the immune system, leads to biofilm formation.
"It is estimated that about 80 percent of human pathogens form
biofilms during some part of their life cycle," said Scripps Research
president and CEO Michael Marletta, PhD, who led the work. "In this
study, we have detailed for the first time the signaling pathway from
nitric oxide to the sensor through cellular regulators and on to the
biological output, biofilm formation."
"There's a lot of interest right now in finding ways to influence
biofilm formation in bacteria," said lead author Lars Plate, a graduate
student in Marletta's team, which recently moved to Scripps Research
from the University of California, Berkeley. "Figuring out the signaling
pathway is a prerequisite for that."
Biofilm formation is a critical phenomenon that occurs when bacterial
cells adhere to each other and to surfaces, at times as part of their
growth stage and at other times to gird against attack. In such
aggregations, cells on the outside of a biofilm might still be
susceptible to natural or pharmaceutical antibiotics, but the interior
cells are relatively protected. This can make them difficult to kill
using conventional treatments.
Biofilms can form on surgical instruments such as heart valves or
catheters, leading to potentially deadly infections. Likewise,
difficult-to-eliminate biofilms also play key roles in a host of
conditions from gum disease to cholera, and from cystic fibrosis to
Legionnaires' disease.
For years, the Marletta lab and other groups have been studying how
nitric oxide regulates everything from blood vessel dilation to nerve
signals in humans and other vertebrates. Past research had also revealed
that nitric oxide is involved in influencing bacterial biofilm
formation.
Nitric oxide in sufficient quantity is toxic to bacteria, so it's
logical that nitric oxide would trigger bacteria to enter the safety
huddle of a biofilm. But nobody knew precisely how.
In the new study, the scientists set out to find what happens after
the nitric oxide trigger is pulled. "The whole project was really a
detective story in a way," said Plate.
In vertebrates, nitric oxide can bind to something called the
Heme-Nitric Oxide/Oxygen (H-NOX) binding domain on a specific enzyme,
activating that enzyme and beginning the chemical cascades that lead to
physiological functions such as blood vessel dilation.
Many bacteria also have H-NOX domains, including key pathogens, so
this seemed the best starting point for the investigation. From there,
the team turned to genomic data.
Genes for proteins that interact are often found adjacent to one
another. Based on this fact, the researchers were able to infer a
connection between the bacterial H-NOX domain and an enzyme called
histidine kinase, which transfers phosphate chemical groups to other
molecules in signaling pathways. The question was where the phosphates
were going.
To learn more, the researchers used a technique called
phosphotransfer profiling. This involved activating the histidine kinase
and then allowing them to react separately with about 20 potential
targets. Those targets that the histidine kinase rapidly transferred
phosphates to had to be part of the signaling pathway. "It's a neat
method that we used to get an answer that was in fact very surprising,"
said Plate.
The experiments revealed that the histidine kinase phosphorylated
three proteins called response regulators that work together to control
biofilm formation for the project's primary study species, the bacterium
Shewanella oneidensis, which is found in lake sediments.
Further work showed that each regulator plays a complementary role,
making for an unusually complex system. One regulator activates gene
expression, another controls the activity of an enzyme producing cyclic
diguanosine monophosphate, an important bacterial messenger molecule
that is critical in biofilm formation, and the third tunes the degree of
activity of the second.
Since other bacterial species use the same chemical pathway uncovered
in this study, the findings pave the way to further explore the
potential for pharmaceutical application. As one example, researchers
might be able to block biofilm formation with chemicals that interrupt
the activity of one of the components of this nitric oxide cascade.
Marletta's group has already explored nitric oxide's role in
controlling Legionnaires' disease and, among other goals, will focus now
on understanding biofilm formation in the bacterium that causes
cholera.
This research was supported by the National Institutes of Health and a
Chang-Lin Tien Graduate Fellowship in the Environmental Sciences.
Journal Reference:
- Lars Plate, Michael A. Marletta. Nitric Oxide Modulates Bacterial Biofilm Formation through a Multicomponent Cyclic-di-GMP Signaling Network. Molecular Cell, 2012; DOI: 10.1016/j.molcel.2012.03.023
Courtesy: ScienceDaily
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