Bacteria
provide a well-known playground for scientists and the evolution of these
earliest life forms has shed important perspective on potential therapies for
some of the most common, deadly diseases.
Researchers at Case Western Reserve University
School of Medicine have now discovered that, the gas nitric oxide (NO),
produced in all cells of the human body for natural purposes, plays a
fundamental regulatory role in controlling bacterial function, via a signaling
mechanism called S-nitrosylation (SNO), which binds NO to protein molecules. In
addition, the researchers discovered a novel set of 150 genes that regulate SNO
production and disruption of these genes created bacterial cell damage
resembling the cell damage seen in many common human diseases. Collectively
these data point to new classes of antibiotics and several new disease
treatments.
The findings, which appear in the April 27 issue of
the journal Science, are significant in that they establish a parallel between
how bacteria and human cells behave, and, they shed new light on how diseases
that entail the same mechanism found in the bacteria may be treated.
According to the traditional Primordial Soup Theory,
the earliest forms of life, including bacteria, utilize nitrate (the
fertilizer) as an energy source. Its byproduct, NO, previously thought to play
no significant role, is now revealed to be important for bacterial function, as
it is in humans. This discovery suggests that for billions of years, NO has
served as a fundamental signaling mechanism; and important related functions
have been conserved in the evolution of bacteria to man.
"The mechanism, which was known to exist in
human cells, but not previously thought to occur in bacteria, controls cell
function and operates very broadly," says Jonathan Stamler, MD, director,
Institute for Transformative Molecular Medicine and the Robert S. and Sylvia K.
Reitman Family Foundation Distinguished Chair in Cardiovascular Innovation,
Case Western Reserve School of Medicine and University Hospitals Case Medical
Center, and director, Harrington Discovery Institute, University Hospitals Case
Medical Center.
"Because the SNO mechanism can malfunction in
ways that are characteristic of many diseases, what we learn from this research
is immediately applicable to the development of new antibiotics and promises
new insights and treatments to common diseases, including Alzheimer's,
Parkinson's, heart disease, and cancer. It's not often that researchers get a
big picture view of a fundamental process important to most cellular
functions."
In humans, faulty NO processing contributes to many
diseases, including cancer, Alzheimer's disease, Parkinson's disease, heart
failure, and asthma. SNOs then build up on proteins creating specific
signatures of disease. Similarly in the bacteria, the researchers found the
absence of certain genes from the newly discovered set, contributed to a
build-up of SNO on cell proteins. Knowing for the first time what genes are
critically related to SNO build-up gives valuable insight into these disease
processes. In addition, the turning on or off of the genes is a new opportunity
to counter disease.
"The system we have today to control human cell
function in the heart and brain evolved a billion years ago to work in
bacteria. So a process that operates in bacteria is also the cause of many
diseases. This offers the obvious opportunity to create new antibiotics but
also therapeutic hope for multiple diseases."
The mechanism at the heart of the research is
S-nitrosylation (SNO), a cellular process in which a nitric oxide (NO)-based
molecule binds with a protein to activate cell signaling and fuel specific or
more general cell activity.
In the event such protein modifications go awry,
forming too few or too many NO attachments, disease can result. Understanding
SNO binding within bacteria provides a basis for developing new drugs to
disable the errant protein attachments that may contribute to disease, Dr.
Stamler says. Also, drugs that disrupt the SNO controlling proteins represent
novel potential antibiotics.
What keeps nitrosylation under control in bacteria,
the researchers discovered, is a group of 150 genes that is regulated by the
transcription factor or protein OxyR. The genes controlled by OxyR prevent
aberrant NO protein attachments from taking place and keep them from
interfering with normal cell function. Specifically, the genes dictate how
bacteria that breathe on an ancient substance called nitrate, which they use in
place of oxygen, handle nitrosative stress, a condition that results when NO
molecules bind uncontrollably with protein molecules, changing their shape and
function.
Prior to this research, OxyR was thought to operate
only when oxygen was present. In fact, OxyR is a "master regulator"
of protein S-nitrosylation that works to alleviate nitrosative stress, the new
Science study shows. Relief of nitrosative stress is being sought by many
companies and investigators to treat neurologic diseases, heart disease, and
cancer.
Nitrosative stress is the primordial equivalent of
oxidative stress, the harmful free radical injury caused by breathing in
oxygen, which damages cells and contributes to aging and disease. The 150 genes
identified by the Case Western Reserve researchers help manage the protein
modifications that occur in bacteria as they breathe, and help eliminate NO
when necessary, to avert potential cell damage or death. Without these genes,
the bacteria cells would likely succumb to nitrosative stress.
Because nitrosative stress is characteristic of many
diseases, including cancer and sepsis, what researchers learn about this state
in bacteria can provide new perspective on these diseases and how to treat
them, Dr. Stamler says. "We may be seeing disease evolution in its
earliest form."
The new research builds upon Dr. Stamler's ongoing
efforts to identify diseases in which protein modifications go awry, to provide
a basis for the development of disease-specific drug therapies. He and his team
are actively working to determine what the 150 genes identified in this
research do, to isolate the genes that pertain to human diseases and spot
opportunities to develop therapies to correct genetic malfunctions. Progress
has already been made.
ScienceDaily
No comments:
Post a Comment