MONDAY, June 30 (HealthDay News) -- Caffeine just might prevent
multiple sclerosis, a new animal study suggests.
Giving mice the equivalent of 6 to 8 cups of coffee a day
prevented mice from getting the animal model equivalent of MS, said
Dr. Linda Thompson, of the Oklahoma Medical Research Foundation,
and a member of the team reporting the finding in this week's issue
of the
Proceedings of the National Academy of Sciences.
Multiple sclerosis, an autoimmune disease, affects about 400,000
Americans, according to the National Multiple Sclerosis Society.
The T-cells from the body's immune system attack the myelin, the
fatty sheath that normally protects the nerve fibers in the central
nervous system. This, in turn, produces scar tissue and triggers
the symptoms of MS, which can include numbness, weakness, lack of
muscle coordination and problems with bladder control, speech and
vision.
Here's why the coffee warded off MS, Thompson explained: It
prevented the molecule adenosine, one of the four building blocks
of DNA, from binding to the adenosine receptor at the cellular
level. When adenosine cannot bind to receptors at the cellular
level, this in turn prevents T-cells from reaching the central
nervous system and setting off the events that lead to the animal
version of MS.
"From a scientific point of view, the bottom line is, adenosine
in this mouse model is needed for the disease-causing T-cells to
get into the central nervous system," Thompson said. "That was the
big, unexpected finding."
The discovery shows how important the adenosine molecule is in
allowing immune cells to infiltrate the central nervous system. In
the animals, the T-cells were activated, but they couldn't get into
the central nervous system, because the caffeine was bound to the
adenosine receptors.
Dr. John Richert, executive vice president of research and
clinical programs for the National Multiple Sclerosis Society, said
the new finding is "potentially big news many years down the
road."
But he cautioned that the research is in the early stages, and
the whole process needs to be studied in humans.
Thompson agreed.
"First, we have to learn if adenosine plays the same role in
people," she said. "In humans, it is not known if adenosine
regulates the entry of T-cells into the central nervous
system."
If the same findings bear out in humans, she said, the hope is
to develop a drug that would degrade adenosine, prevent it from
being formed, or prevent T-cells from getting into the central
nervous system. She noted that the discovery holds promise for
other autoimmune diseases, including lupus and rheumatoid
arthritis.
The challenge, she said, is that adenosine receptors "are
everywhere in the body." So, the drug would have to be specific
enough to only act on the adenosine receptors that control access
of the T-cells to the central nervous system.
Even so, Richert said, "it's a potential therapeutic target that
needs to be explored."
More information
To learn more about multiple sclerosis, visit the
National Multiple Sclerosis Society.
