By identifying risk factors for autoimmune
disease,
researchers hope to predict and even prevent its onset.
by Dan Stimson
Wendy Brown feels good, but shes worried it wont last. Two years
ago, Brown felt herself losing strength. She had trouble lifting things
and getting up from a seated position, and when she pushed herself,
her muscles groaned in pain. Those problems came to a head in July
2001, when she traveled from her home in Palm Coast, Fla., for a family
vacation in Hungry Horse, Mont. a small mountain town.
One day, at a picturesque spot in the town, Browns relatives piled
into an old stagecoach for a family photo.
"My mother was 60 and she just climbed right in, but I didnt
have the strength to pull myself up. Thats when I knew something
was definitely wrong," says Brown, who was 31 at the time. Within
two months of returning from the trip, she needed a wheelchair to
get around.
Doctors told her she had polymyositis (PM), an autoimmune disease that weakens the torso, upper arms and thighs. Autoimmune diseases
occur when the immune system attacks the bodys own tissues, and in
PM, that attack is directed against muscle.
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Wendy
Brown (lower center) was the only family member who couldnt
climb aboard this stagecoach in 2001. She has polymyositis. |
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PM, like many other autoimmune diseases, usually requires lifelong
treatment with drugs that suppress the immune system. But remarkably,
after just 15 months on prednisone (a powerful immunosuppressant),
Browns PM went into remission. Shes been without symptoms and without
need for treatment since January, and she hopes to stay that way.
But no one knows whether Brown is in the clear, because no one knows
what causes PM or most other autoimmune diseases.
The need for answers is urgent, for Brown and millions of others.
Although PM is rare, as a group, autoimmune diseases affect between
5 percent and 8 percent of the U.S. population. More common diseases
in that group include rheumatoid arthritis and type 1 diabetes. Less
common, lesser-known ones include PM and other neuromuscular diseases
covered by MDA: dermatomyositis (DM), inclusion-body myositis (IBM),
myasthenia gravis (MG), Lambert-Eaton myasthenic syndrome (LEMS) and,
often, the thyroid-related muscle disorders. (See chart.)
Although each of these diseases is different on the surface, researchers
are learning that they share common risk factors. By identifying those
risk factors, they hope one day to predict who will get an autoimmune
disease and who stands the best chance of permanent remission (which,
so far, has proved rare).
Nature vs. Nurture
One clue to the shared origins of different autoimmune diseases has
come from studies of families.
Autoimmune diseases arent inherited along predictable lines as are,
for example, the muscular dystrophies. However, the genes that determine
how the immune system is likely to behave are thought to affect the
chance of developing an autoimmune disease.
"Its common to see certain families where there are multiple
members with different autoimmune diseases," says Frederick Miller,
a rheumatologist (specialist in inflammatory diseases of the muscles
and joints) and an expert on autoimmune diseases at the National Institute
of Environmental Health Sciences (NIEHS), a branch of the National
Institutes of Health in Bethesda, Md.
"Weve done a study in patients with PM or DM, and found that
first-degree family members [parents, children and siblings] had an
increased risk of having an autoimmune disease but it was unlikely
to be myositis," he says. The relatives were more likely to have
more common autoimmune diseases, such as arthritis or diabetes.
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Normal
Immune System
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1. A bacterium invades the body, displaying proteins
on its surface. The immune system sees these as antigens,
requiring defensive action.
2. An antigen-presenting cell (APC) of the immune system
engulfs the bacterium.
3. The bacterium begins to break up inside the APC,
and its antigens, nestled inside a major histocompatibility
complex (MHC), are displayed on the cells surface like a
flag.
4. T-cells "see" the displayed antigen and
begin secreting cytokines, which help antigen-presenting cells
destroy the bacteria theyve engulfed. They also send signals
to B-cells, instructing them to start making antibodies to
the displayed antigens.
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The exact risk for people who have relatives with autoimmune diseases
isnt clear, but (unsurprisingly) the closer the relative, the higher
the risk. Miller estimates that for identical twins who share 100
percent of their genes when one has an autoimmune disease, the other
has a 20 percent to 40 percent chance of getting the same disease.
Clearly, genes play a role in autoimmune disease, and the same genes
probably are involved in different autoimmune diseases. But other
factors are at work, too.
"The concept is that autoimmune diseases share a number of common
genetic risk factors," Miller says. "Those factors might
get you into the theater of autoimmune disease, and then other genes
and environmental factors may usher you to your particular seat in
that theater."
For example, subtle variations in genes that control the functions
of the immune system might cause susceptibility to an autoimmune disease,
and a "hit" from the environment such as an infection
might provide the final trigger.
Friendly Fire
To understand how the immune system goes astray in autoimmune disease,
its important to know a few things about its normal activity.
When infectious diseases attack our bodies, our immune systems defend
us by mustering a cellular army, in which the essential soldiers are T-cells and B-cells. Collectively known as lymphocytes,
both cell types are born in the bone marrow, but T-cells mature in
the thymus, a gland located just below the throat.
Both cell types travel through the bloodstream, watching for viruses,
bacteria and other disease-causing "germs," but they attack
by different means. T-cells act as the mobile infantry and communications
network for the army, and B-cells provide the long-range artillery.
T-cells use a protein on their surface, called the T-cell receptor,
to latch onto foreign antigens, which are (usually) proteins
or sugars that belong to the invading germ. Attachment of the receptor
to the antigen stimulates the T-cell to attack by releasing cytokines distress signals that call B-cells and other immune cells to the
fray. Once they get the signal from T-cells, B-cells begin releasing antibodies, proteins that stick to the antigen and either mark
its bearer for destruction or attract additional troops.
In autoimmune diseases, "The main problem is either antibodies
or T-cells that are directed against a self-antigen [a protein that
belongs to cells in the body]," says Premkumar Christadoss, an
immunologist and MDA grantee who studies MG at the University of Texas
in Galveston. "During this process, cytokines are released, and
they further contribute to the problem," he says.
This isnt a matter of good immune cells turning bad. Our immune
systems dont come equipped with T-cells or B-cells designed to recognize
specific antigens. Instead, they make a greater diversity of immune
cells than we really need: Random gene rearrangements inside B-cells
and T-cells create billions of distinct antibodies and T-cell receptors
with the potential to match an equal number of antigens.
Cells that encounter and recognize foreign antigens multiply rapidly,
mount an attack, and retain a "memory" of the encounter.
Cells that react to self-antigens normally kill themselves or become
inactive but sometimes they survive and cause trouble.
The self-antigen or antigens are known in some, but not all, autoimmune
diseases. (See chart.)
For example, MG occurs when the immune system targets proteins essential
to the connection between nerve cells and muscle cells. Normally,
the nerve cell releases a chemical called acetylcholine (ACh),
which stimulates muscle contraction by attaching to a docking site
on the muscle cell, called the ACh receptor. Some 85 percent
of people with MG have antibodies to the ACh receptor detectable in
their blood, and a small fraction have antibodies to MuSK a protein
that helps organize ACh receptors on the muscle cell surface. (For
more about MG, see "Managing
Myasthenia," May-June 2003.)
Genetic Clues
Many genes carry the instructions for making T-cell receptors, antibodies
and other components of the immune system, and all of them have the
potential to influence who gets autoimmune diseases. But the genes
behind a set of proteins called the major histocompatibility complex
(MHC) appear to be especially important.
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Molecular
mimicry is the theory that some foreign antigens might have
a similar appearance to self-antigens. T-cells or B-cells that
attack the foreign antigen might be provoked by the self-antigen,
too. |
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T-cells actually cant "see" antigens without help from
these proteins, which exist in two flavors. MHC type 1 is found on
the surface of most cells in the body, and MHC type 2 is found only
on the surface of antigen-presenting cells.
When a cell gets infected with a virus, it sheds the infectious bugs
antigens and directs them to T-cells using MHC type 1. The MHC holds
out the antigen like a hand waving a red flag, waiting for a T-cell
to respond. This is a signal that says, "Kill me before I spread
the infection!"
Antigen-presenting cells actually ingest foreign antigens, such as
those from bacteria, and spit them out into MHC type 2 a signal
that puts T-cells on the alert and causes them to release cytokines.
MHC proteins themselves are important antigens sometimes called human leukocyte antigens (HLA) because the genes responsible
for making them vary in their exact "code" from one person
to the next. MHC differences mark our cells as our own (creating the
possibility of rejection during an organ transplant), ensure that
were not all wiped out by a single nasty germ, and apparently leave
some of us vulnerable to autoimmune disease.
Some MHCs, Christadoss explains, probably have a peculiar way of
displaying antigens that makes them more likely to trigger reactions
to self-antigens. One MHC variant, called HLA-DR3, "imparts
susceptibility to a lot of autoimmune diseases," including PM,
DM and MG, he says.
Several other genes also appear to influence susceptibility to autoimmune
disease. For example, certain variants of the gene encoding cytotoxic-T-lymphocyte-associated
protein 4 (CTLA-4) have been associated with type 1 diabetes and
thyroid disease. CTLA-4 sits on the surface of T-cells, and normally
decreases their responses to antigens.
Infections, Injuries and Interlopers
When someone has a genetic makeup compatible with autoimmune disease,
whats the environmental trigger that pushes him or her over the edge?
Unfortunately, researchers dont have a specific answer in most cases,
but they have a few theories that apply to all autoimmune diseases.
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Ann
Reed |
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One theory is molecular mimicry. This is the idea that, to
T-cells and B-cells, certain viral or bacterial antigens might appear
similar to self-antigens. Once the cells react to the foreign antigen,
they might indiscriminately attack the self-antigen, too. Theres
especially good evidence for this phenomenon in Guillain-Barré
syndrome, a nerve disease caused by antibodies that cross-react to
certain sugars found on nerve cells and on the bacterium Campylobacter
jejuni.
Another idea concerns hidden antigens antigens found only
in tissues that are under limited surveillance by the immune system,
such as the eyes and brain or the inside of a muscle cell.
"An injury or infection [of those tissues] could release a hidden
antigen, and the immune system having never seen it before might
react to it, thinking its a foreign antigen," Christadoss explains.
Although cancer isnt a part of most autoimmune diseases, it might
trigger some, such as LEMS, by presenting previously hidden antigens
to the immune system. LEMS is caused by antibodies to a protein thats
normally found only in nerve cells. Some 60 percent of LEMS cases
are associated with small-cell lung cancer, and in those cases, the
cancerous lung cells produce the nerve cell protein. Successful treatment
of the cancer usually leads to full recovery from LEMS.
A relatively new theory suggests that mixing of maternal and fetal
cells during pregnancy might trigger some autoimmune diseases.
Ann Reed, a pediatric immunologist and MDA grantee at the Mayo Clinic
in Rochester, Minn., has found evidence for this phenomenon called microchimerism in juvenile DM. (In Greek mythology, a chimera
is a monster made of different animal body parts; in medicine, chimerism
refers to the mixture of donor and recipient cells that persists after
a bone marrow transplant.)
In work supported by MDA, Reed says, "We started looking at
children with DM and found that theyre more likely to have maternal
cells present in their blood than are controls [siblings or unrelated
children who dont have DM]." She believes the maternal cells
might be immature lymphocytes that have lain dormant for some time,
but eventually react to the childs tissue.
The reaction can occur in the opposite direction as well. Fetal cells
can persist in a womans blood for up to 30 years after a pregnancy,
and researchers have found that the cells are more likely to persist
in women with the autoimmune disease scleroderma than in controls.
Reed is planning a new study to look for persistence of fetal cells
in women with adult-onset DM.
Digging Deeper
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Frederick
Miller |
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Miller, who heads the newly established Environmental Autoimmunity
Group at NIEHS, has begun one of the largest clinical studies ever
to examine the combined roles of genetic and environmental risk factors
in autoimmune disease.
Hes seeking 400 pairs of twins, or siblings who are close in age,
one of whom has rheumatoid arthritis, lupus erythematosus, systemic
sclerosis, or myositis (PM, DM or IBM) while the other doesnt have
an autoimmune disease.
Hell analyze blood samples for variations in the MHC and other genes,
evidence of microchimerism, and exposure to various infections and
chemicals. Hell also collect information using a questionnaire that
asks about medical history and stressful life events. (For more information,
see the "Clinical Trials" section of MDAs Web site at www.mda.org/research/ctrials.aspx.
Travel to NIEHS isnt necessary to participate in the study.)
Millers research began in April and is expected to last five years.
He says the study is designed to ask, "Why did one sibling develop
the disease while the other one didnt?"
The answer, he believes, "will not only help us predict the
course of autoimmune diseases, but also help us prevent them by screening
individuals at risk. Thats the ultimate goal, which I suspect is
a ways off."
He adds, "A better understanding of mechanisms of the disease
could also lead to better treatments." Indeed, recent insights
into the causes of autoimmune disease have already led to lab experiments
and clinical trials aimed at more effective treatments with fewer
side effects. (See "Better Treatments Through
Better Targets." )
Wendy Brown and her sister Fran (who doesnt have an autoimmune disease)
have already given blood samples and filled out questionnaires for
Millers study.
"Im participating to help find out why people get [these diseases]
and to help find a cure, whether its in my lifetime or somebody elses,"
Brown says. "I wouldnt want anybody else to go through what
I did."
Better Treatments
Through Better Targets
Using immunosuppressant drugs to treat autoimmune
diseases is like using a sledgehammer when a carefully aimed
rubber mallet might do the trick.
The drugs, now commonly used in diseases such
as DM, PM and MG, offer a lifesaving treatment, but their broadly
dampening effects on immune cells leave the body vulnerable
to infection. They also can hinder the function of other cell
types, causing undesirable and occasionally serious side effects.
For example, prednisone can cause weight gain,
cataracts and osteoporosis (bone loss), while methotrexate,
a common treatment for PM and DM, can damage the lungs, kidneys
or liver if its not used carefully.
As scientists learn more about the mechanisms
behind autoimmune diseases, theyre beginning to investigate
new drugs that specifically target troublemaking immune cells
or chemicals, while sparing the rest of the body.
Many of these drugs are actually monoclonal
antibodies (mabs) that are custom-made to stick to the cell
or chemical and block its effects. (Monoclonal means that the
antibodies were all derived from the same type, or "clone,"
of B-cells.)
Taking Out TNF
One target of these new-generation drugs is tumor necrosis factor (TNF), a cytokine (protein released
from immune cells) named for its ability to kill tumor cells
that display abnormal antigens. TNF also helps mobilize immune
cells and can thus stimulate autoimmune reactions. The protein
appears to skyrocket in several autoimmune diseases, including
rheumatoid arthritis and myositis.
Pharmaceutical companies began developing drugs
to inhibit TNF in the early 1990s, and two TNF blockers are
now on the market for rheumatoid arthritis: infliximab (Remicade)
is an antibody against TNF, and etanercept (Enbrel) is a free-floating
version of the TNF receptor, TNFs docking site on immune cells.
It acts as a decoy, keeping TNF away from the cells.
Both drugs are under investigation for myositis
Enbrel against DM at the MDA clinic at St. Josephs Hospital
in Phoenix, and Remicade against DM and PM at the National Institute
of Arthritis, Musculoskeletal and Skin Diseases (NIAMS) in Bethesda,
Md.
Meanwhile, MDA grantee Premkumar Christadoss
is collaborating with Matthew Meriggioli, director of the section
on neuromuscular disease at Rush University in Chicago, to test
the mechanisms of etanercepts action in a small number of MG
patients.
"If this pilot study looks promising, we
hope to proceed with a larger trial," Meriggioli says.
"I believe I have seen evidence for improvement in most
patients, but I have not formally analyzed the data yet."
Cutting Off Complement
Another promising target is complement a system of more than 20 proteins in the blood. The complement
proteins spring into action when they "see" a cell
marked by antibodies, assembling into a killing machine that
punches a hole in the cells surface. This reaction appears
to spin out of control in some autoimmune diseases, especially
DM.
In a small clinical trial completed in 2001,
a complement inhibitor called eculizumab appeared to
improve the skin rash, but not the muscle weakness, associated
with DM. The maker of eculizumab, Alexion Pharmaceuticals, hasnt
announced any follow-up trials, but has acquired an "orphan
drug" designation, which gives it government incentives
to pursue development of the drug for DM.
Meanwhile, Christadoss believes that "eliminating
part of the complement pathway might be a way to treat MG."
In laboratory experiments, hes found that mice with genetic
deficiencies in the complement system are resistant to developing
MG. |
Autoimmune Diseases Covered
by MDAs Program
Disease |
Symptoms |
Target Tissue |
Antigen |
Myasthenia gravis |
Weakness and fatigue, esp. in the face and
neck |
Muscle |
ACh receptor, MuSK,? (unknown)
|
Lambert-Eaton myasthenic syndrome |
Weakness, esp. in the legs and arms |
Nerve cell endings |
? |
Polymyositis |
Generalized weakness |
Muscle |
? |
Dermatomyositis |
Generalized weakness and skin rash |
Blood vessels that supply muscle and skin |
? |
Inclusion-body myositis* |
Weakness and wasting, esp. in the thighs
and hands |
Muscle |
? |
Hyperthyroid myopathy |
Weakness and wasting, esp. in the shoulders |
Thyroid gland (becomes overactive) |
Thyrotropin receptor |
Hypothyroid myopathy |
Weakness and wasting, esp. in the hips |
Thyroid gland (becomes underactive) |
Thyroglobulin |
*Scientists disagree on whether this is an autoimmune disease.
