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Drugs Helping People with Parkinson's Disease
by Evelyn Zamula
Walter is approaching 80, but his smooth, unlined face looks years younger.
When he sits quietly in his chair, no one can tell he has Parkinson's
disease. He has never had tremor, the trembling of the hand or foot that
plagues the majority of people with this chronic neurological ailment.
But watch him try to get out of the chair. He grips the wooden arms, moves to
the edge of the seat, and rocks back and forth a number of times to gain
momentum. Using all his strength, he pushes down on his hands to propel
himself upright. For a long time he stands as if rooted to the spot. Then he
hurries forward, shoulders bent, walking in short, shuffling steps, looking
every one of his 80 years.
For the most part, Walter (who asked that his last name not be used) has
coped remarkably well with his illness, which began when he was 65. Until a
few months ago, he drove his car around the rural area where he lives, doing
his little errands. But lately he appears to be going downhill rapidly
despite carefully regulated medication. Doing fine tasks with his hands, such
as buttoning his shirt and handling eating utensils, has become more and more
difficult, which depresses him. Slight drooling has also become a problem.
But what bothers him most is that he has begun to hallucinate, a side effect
of one of the drugs he is taking. He stands at the window and peers into the
woods, seeing strange creatures that are not there, but appear only too real
to him. His daughter reports that this retired policeman, once strong and
confident, becomes anxious when left alone. Since it's not possible for her
to be with him all the time, she is thinking, finally, of a nursing home.
Unlike Walter, Virginia "Jinny" Krohnfeldt's first symptom was a tremor that
affected her writing hand. Her symptoms showed up much earlier, too, when she
was in her mid-40s, 13 years ago. Presently a realtor in the Washington,
D.C., area, Krohnfeldt had to resign her high level government job because it
became difficult for her to sign checks, an essential part of her duties.
Like Walter, Krohnfeldt also stoops and shuffles, symptoms that make her
appear to many people as if she is a drug abuser. Once reluctant to tell
people she had Parkinson's disease, Krohnfeldt is now outspoken about her
condition: "Better to say you have Parkinson's than have people think you're
on drugs."
Diagnosing the Disease
The chief or major signs of Parkinson's disease are slowness of movement
(bradykinesia), tremor, and muscle stiffness or rigidity.
In addition to these, Parkinson patients may have minor signs, including a
mask-like face (which accounts for Walter's deceptively youthful look),
drooling, stooped posture, "freezing" (feet unable to move), difficulty
swallowing, mumbly speech, sleep disturbances, a tendency to fall forward
(propulsion) or backward (retropulsion), infrequent blinking, and bowel and
bladder problems. Diagnosis is based on the presence of two major signs, or
one major sign and at least two minor signs. Often, the disease progresses so
slowly that it may take years before a doctor can make a firm diagnosis.
To rule out other brain disorders, doctors may also order tests, such as a
computerized axial tomography ("CAT") scan, which produces images of "slices"
of the brain, or an electroencephalogram (EEG), which measures electrical
activity in the brain. These tests are usually normal in patients with
Parkinson's disease.
Dopamine Key
Parkinson's disease results from a depletion of the chemical dopamine in the
brain. Dopamine is produced and stored in a small, pigmented group of nerve
cells in the upper brainstem called the substantia nigra. Long, thin fibers
connect these pigmented cells to nerve cells in the corpus striatum, a part
of the brain that controls movement, balance, walking, and posture. Dopamine
aids the transmission of messages between the pigmented nerve cells and the
striatal nerve cells.
If, for any reason, the substantia nigra's nerve cells are injured or
destroyed, the corpus striatum does not receive enough dopamine to correctly
program movement, and parkinsonian symptoms develop. Symptoms may not show up
until more than 50 percent of the dark nerve cells are destroyed and the
striatal dopamine content is reduced by 80 percent or more, a process that
can take many years. During the course of the disease, the substantia nigra
continues to degenerate.
Treatment with Levodopa
In 1817, the British physician James Parkinson described as the "shaking
palsy" the disease that now bears his name. He had little at his disposal to
relieve the disease's disturbing symptoms. Medical men of his time were great
believers in keeping the bowels open and bloodletting; Dr. Parkinson approved
of the former for palsy patients, but not the latter.
Until levodopa (or L-DOPA) was introduced in the 1960s, doctors relied mostly
on botanical preparations, such as tincture of belladonna, to treat the
disease. Then Arvid Carlsson, a Swedish professor, found in 1957 that the
effects of reserpine, a drug that caused parkinsonism in laboratory animals,
could be reversed by injections of levodopa. He proved that dopamine levels
in the brain were reduced by reserpine and restored to normal by levodopa,
and suggested that levodopa be tried in treating Parkinson's disease.
Doctors prescribed the drug timidly at first--either given by mouth or
injected into a vein--fearing serious adverse reactions. The results were
disappointing. But George Cotzias, M.D., of the Brookhaven National
Laboratories, Upton, N.Y., daringly prescribed doses a thousand times greater
than had ever been used. His patients improved dramatically. When Leonard L.,
a postencephalitic Parkinson patient (and hero of the movie "Awakenings,"
based on the book by Oliver Sacks, M.D.), heard about the drug, he spelled
out on his letterboard, "Dopamine is Resurrectamine. Cotzias is the Chemical
Messiah."
FDA approved levodopa in 1970. But there were problems. Curiously, levodopa
can cross the blood-brain barrier--where it is converted in the brain to
dopamine--but dopamine itself cannot. When taken orally, an enzyme in the
blood and tissues converts levodopa to dopamine so rapidly that only a small
part of a levodopa dose enters the brain unchanged. Consequently, large
amounts of levodopa are needed to relieve neurological symptoms and replace
the lost dopamine, causing unbearable nausea and other side effects.
Researchers found that when carbidopa was added to levodopa, it blocked the
enzyme responsible for the breakdown of levodopa in the body, and allowed
more levodopa to get to the brain. Carbidopa makes it possible to use about
75 percent less levodopa, thereby reducing nausea and vomiting. This
combination of levodopa and carbidopa is marketed as Sinemet.
Another problem with levodopa medications is that some patients develop
complications with long-term use. This has made some doctors reluctant to
prescribe them until symptoms interfere with the quality of life. (Recent
studies have shown that it may make no difference to the eventual outcome
when levodopa drugs are started, because no anti-parkinsonian agent can slow
the natural progression of the underlying disease.) After about four or five
years, sometimes sooner, the patient begins to respond less satisfactorily to
levodopa. Dyskinesias, or involuntary movements (such as lip smacking or
tongue thrusting), may develop. Reducing the dose helps reduce the
dyskinesias, but results in a worsening of Parkinson symptoms.
Some Parkinson disease patients may have "on-off" effects, which means that
their movements fluctuate from normal to abnormal in a random fashion, or as
a "wearing off," when symptoms return as the blood level of levodopa
decreases. The controlled-release form of Sinemet, Sinemet CR, which was
approved for use by FDA in 1991, was formulated to help keep blood levels of
levodopa more constant throughout the day, possibly preventing these
fluctuations.
Modernizing Old Therapies
Anticholinergic drugs have been used to treat Parkinson's disease for almost
a century. (Those old botanical preparations had anticholinergic properties.)
Used along with levodopa, modern anticholinergic drugs are useful in reducing
tremor. As decreased amounts of dopamine are produced in the brain, an
imbalance with the neurotransmitter acetylcholine occurs, making symptoms
worse. Anticholinergics work by partially blocking the action of
acetylcholine. Examples of anticholinergic medications used to treat
Parkinson's disease are Artane (trihexyphenidyl), Akineton (biperiden),
Kemadrin (procyclidine), Pagitane (cycrimine), and Cogentin (benztropine).
Although used primarily in treating asthma and allergies, antihistamines are
also effective against tremor because of their anticholinergic properties.
Most frequently used antihistamines for this purpose are Benadryl
(diphenhydramine) and Phenoxene (chlorphenoxamine).
Like antihistamines, Symmetrel (amantadine), an antiviral drug, was
serendipitously discovered to benefit patients with Parkinson's disease.
Prescribed for a woman to prevent flu, Symmetrel relieved some of her
Parkinson symptoms and made her generally feel better. It is helpful both in
the early and late stages. In addition to its anticholinergic properties,
Symmetrel promotes the release of dopamine in the brain.
Other drugs, called dopamine agonists (activators), bypass the degenerating
nerve cells in the substantia nigra and directly stimulate the striatal
dopamine receptors. Though dopamine receptors are selective about which
chemical messengers they'll receive, they can respond to synthetic compounds
that aren't dopamine, but act like dopamine in the brain. Dopamine agonists
can be used alone, but are more effective when used with Sinemet. They are
usually added to the treatment when the patient is encountering too many side
effects, such as dyskinesias, with Sinemet. Dopamine agonists available in
the United States are Parlodel (bromocriptine) and Permax (pergolide). They
don't necessarily have the same effects in all patients, so if one drug loses
its efficacy or causes too many side effects, the physician may prescribe the
other drug.
MAO-B inhibitors block the MAO-B enzyme in the brain that helps break down
and metabolize dopamine. When the enzyme's action is slowed down, more
dopamine may be available to relieve symptoms and improve motor performance,
allowing Parkinson patients to move about more freely. Eldepryl (deprenyl) is
the only MAO-B inhibitor to be approved for use in treating Parkinson's
disease in this country. It is useful for patients with advanced disease who
are having problems with Sinemet. In a large clinical trial in 1989, Eldepryl
showed a possible neuroprotective effect by prolonging the time before the
patient needed levodopa treatment.
Many Parkinson's disease patients suffer from profound depression, as well as
insomnia. Doctors may prescribe tricyclic antidepressants (such as Elavil,
Endep and Tofranil) that have both anticholinergic and sedative properties.
Medications that relieve symptoms of depression, such as Prozac and Desyrel,
are also used.
Many doctors say that levodopa preparations will probably continue to be the
most useful drugs in treating Parkinson's disease for a long time.
Researchers are studying newer drugs that will enhance levodopa's
effectiveness by slowing down the rate at which the body breaks it down. They
have also found that medications approved for other uses (such as Clozaril)
can reduce side effects. Other substances (such as Eldepryl and vitamins C
and E) are under study to see if they can reduce the rate of disease
progression.
It's unlikely that results will be available soon enough to benefit Walter,
who now lives in a nursing home in the small Midwestern town where he grew up
and served on the police force. In general, he is doing fairly well, but no
sooner is his medication adjusted to get rid of one troublesome side effect
than a different one appears in its place. The usual infirmities of old age
have added to his problems.
Krohnfeldt's symptoms are under control, except that her hand still trembles
and she is suffering from dyskinesia--her right foot sometimes moves
spastically back and forth and she is unable to stop it. But Krohnfeldt
retains her good spirits. "I've always said it's my cross to bear. If I can
stick with it, I'll hang in there. It's better than a lot of other diseases I
wouldn't care to have. I started an exercise program about six weeks ago and
it's doing me a world of good. I play golf occasionally and work out for two
hours a day three times a week, and I feel just great. I get a lot of support
from my family. My kids are behind me and that helps." n
Evelyn Zamula is a freelance writer who lives in Potomac, Md.
Trying to Find the Cause
Parkinson's disease affects slightly more men than women and more whites than
blacks in the United States. About three-quarters of all patients develop the
disease between 50 and 65, though one person in seven develops it earlier, in
the 30s or 40s. An estimated 1.5 million Americans have the disorder,
according to the Parkinson's Disease Foundation.
The question of whether the disease has a genetic factor has been debated for
years. Studies of both identical and fraternal twins, in which one twin had
Parkinson's disease, showed that the unaffected twin had about the same
frequency of the disorder as found in the general population.
"There is no definitive data to support whether Parkinson's is or is not
hereditary," says Thomas Chase, M.D., chief, experimental therapeutics
branch, National Institute of Neurological Disorders and Stroke, Bethesda,
Md. "The mainstream thinking is that most Parkinson disease cases look as
though they do not have any hereditary component whatsoever, on the face of
it. The twin studies support that view ....
"But one can't be absolutely sure that there is no hereditary component in
ordinary [idiopathic] Parkinson's disease, because there are two or three
families around the world where Parkinson's is clearly hereditary."
A recent study of two large families from the same small town in southern
Italy revealed that 41 family members in four generations, including members
who emigrated to the United States, have had a particularly serious form of
the disease. Genealogical studies of the two families showed a common
ancestor dating to the early 1700s.
"Fortunately, these cases are exceedingly rare," says Chase. "So when a
patient asks if Parkinson's can be inherited, the answer is the chance is one
in a million."
Other experts debate whether Parkinson's disease has an environmental cause.
The occurrence of the condition in couples married for many years, presumably
eating the same diet in the same environment--in many cases in
institutions--is exceptionally low. However, one researcher found that
residents of three adjacent kibbutzim (community settlements) in Israel have
five times the incidence of Parkinson's disease found in neighboring areas.
Until recently, all three kibbutzim used drinking water from the same well,
possibly contaminated by a nearby junkyard with rusting automobiles and
tractor parts. Other researchers have also noted a higher risk of Parkinson's
disease among rural populations who use well water.
Some, such as Donald M. Calne, D.M., University of British Columbia, argue
that Parkinson's disease is not a specific disease entity, but rather a
syndrome that may have either a genetic or environmental cause, depending on
the particular case. Professor C.D. Marsden of the National Hospital for
Nervous Diseases, London, U.K., writes in The Lancet (April 21, 1990): "A
more complex theory is that the development of Parkinson's disease may be due
to a combination of exposure to an environmental toxin with an inherited
inability to adequately dispose of such a toxin."
The possibility that a virus or other infectious agent is responsible has
been proposed, but sophisticated techniques have so far been unsuccessful in
finding any such agent.
About 85 percent of patients who develop tremor, rigidity, slowness of
movement, and minor signs have ordinary (or idiopathic--of no known cause)
Parkinson's disease. Other patients with the same symptoms for which the
cause is known have symptomatic or secondary parkinsonism. Parkinsonism can
be induced by a variety of causes. One type is caused by drugs that block the
dopamine receptors in the brain. The chief offenders are the antipsychotic
drugs, such as Haldol, Thorazine, Loxitane, Stelazine, Mellaril, Prolixin,
Compazine, Orap, and others of this class. Fortunately, these symptoms
disappear when the drugs are withdrawn or the dose is lowered.
(Benzodiazepine, or minor, tranquilizers such as Valium and Librium do not
cause parkinsonism.)
The drug reserpine is prescribed in low doses to combat high blood pressure;
in high doses, however, reserpine depletes dopamine in the brain and causes
parkinsonism. Its effects are also reversible when use is discontinued.
Other chemicals are also implicated. In 1977, a young chemist in California
synthesized a street narcotic that was contaminated with a byproduct known as
MPTP. After several injections, he developed a tremor and was unable to move
or speak. When he died in 1978 of a drug overdose, the autopsy showed
irreversible damage to the brain's dopamine-producing systems.
In a study conducted in the province of Quebec, Canada, researchers found a
strong correlation between the use of herbicides chemically related to MPTP,
such as paraquat, and the development of Parkinson's disease. In one area
where these types of herbicides were heavily used, the incidence of
parkinsonism was seven times higher than in neighboring areas with low
herbicide use.
Certain occupations are associated with the destruction of the
dopamine-producing cells of the brain. Mechanics exposed to carbon monoxide,
welders and miners exposed to manganese, and people in contact with mercury
or carbon disulfide in rubber manufacture, for example, may have symptoms
resembling those of parkinsonism.
Brain tumors, head injuries, strokes, tuberculosis, syphilis, subdural
hematoma, degenerative diseases such as Alzheimer's, hereditary diseases
(Huntington's chorea and Wilson's disease), or any other condition that
damages the cells of the substantia nigra, may cause some degree of
parkinsonism, but these cases are rare. n
--E.Z.
Some Drugs Used to Treat Parkinson's Disease
Drug
Use
Main Side Effects
Anticholinergics
relieves rigidity,
dry mouth, blurred
Artane
tremor and drooling
vision, mental changes,
Akineton
difficulty in voiding,
Cogentin
constipation
Kemadrin
Pagitane
Antidepressants with
relieves depression
same as anticholinergics
anticholinergic activity
and sleep (may also
Elavil
relieve anxiety)
Endep
Tofranil
Antidepressants without
relieves depression
mental changes
anticholinergic activity
(may also decrease anxiety
Desyrel
and improve sleep)
Prozac
Antihistamines reduces tremor and drowsiness
Benedryl can be sedating
Phenoxine
Anti-psychotomimetics may lessen mental changes
Mellaril hallucinations and
Clozaril delusions
Antiviral improves all mottling of skin,
Symmetrel symptoms swelling of feet,
confusion,
hallucinations
Dopa decarboxylase improves all involuntary
inhibitor combined symptoms movements, mental
with levodopa changes, dizziness
Sinemet
Sinemet (controlled-
release)
Dopamine agonists improves all nausea, dizziness
Parlodel symptoms on standing, mental
Permax changes
MAO-B Inhibitor may slow progression dizziness, nausea,
Eldepryl of the disease and insomnia
increases the effectiveness
of levodopa