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Wednesday, August 20, 2008
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Acromegaly
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Acromegaly
is a hormonal disorder that results when the pituitary gland
produces excess growth hormone (GH). It most commonly affects
middle-aged adults and can result in serious illness and
premature death. Once recognized, acromegaly is treatable
in most patients, but because of its slow and often insidious
onset, it frequently is not diagnosed correctly.
The name acromegaly
comes from the Greek words for "extremities" and "enlargement"
and reflects one of its most common symptoms, the abnormal
growth of the hands and feet. Soft tissue swelling of
the hands and feet is often an early feature, with patients
noticing a change in ring or shoe size. Gradually, bony
changes alter the patient's facial features: the brow
and lower jaw protrude, the nasal bone enlarges, and spacing
of the teeth increases.
Overgrowth
of bone and cartilage often leads to arthritis. When tissue
thickens, it may trap nerves, causing carpal tunnel syndrome,
characterized by numbness and weakness of the hands. Other
symptoms of acromegaly include thick, coarse, oily skin;
skin tags; enlarged lips, nose and tongue; deepening of
the voice due to enlarged sinuses and vocal cords; snoring
due to upper airway obstruction; excessive sweating and
skin odor; fatigue and weakness; headaches; impaired vision;
abnormalities of the menstrual cycle and sometimes breast
discharge in women; and impotence in men. There may be
enlargement of body organs, including the liver, spleen,
kidneys and heart.
The most serious
health consequences of acromegaly are diabetes mellitus,
hypertension, and increased risk of cardiovascular disease.
Patients with acromegaly are also at increased risk for
polyps of the colon that can develop into cancer.
When GH-producing
tumors occur in childhood, the disease that results is
called gigantism rather than acromegaly. Fusion of the
growth plates of the long bones occurs after puberty so
that development of excessive GH production in adults
does not result in increased height. Prolonged exposure
to excess GH before fusion of the growth plates causes
increased growth of the long bones and increased height.
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Acromegaly
is caused by prolonged overproduction of GH by the pituitary
gland. The pituitary is a small gland at the base of the
brain that produces several important hormones to control
body functions such as growth and development, reproduction,
and metabolism. GH is part of a cascade of hormones that,
as the name implies, regulates the physical growth of the
body. This cascade begins in a part of the brain called
the hypothalamus, which makes hormones that regulate the
pituitary. One of these, growth hormone-releasing hormone
(GHRH), stimulates the pituitary gland to produce GH. Another
hypothalamic hormone, somatostatin, inhibits GH production
and release. Secretion of GH by the pituitary into the bloodstream
causes the production of another hormone, called insulin-like
growth factor 1 (IGF-1), in the liver. IGF-1 is the factor
that actually causes the growth of bones and other tissues
of the body. IGF-1, in turn, signals the pituitary to reduce
GH production. GHRH, somatostatin, GH, and IGF-1 levels
in the body are tightly regulated by each other and by sleep,
exercise, stress, food intake and blood sugar levels. If
the pituitary continues to make GH independent of the normal
regulatory mechanisms, the level of IGF-1 continues to rise,
leading to bone growth and organ enlargement. The excess
GH also causes changes in sugar and lipid metabolism and
can cause diabetes.
Pituitary
Tumors
In over 90
percent of acromegaly patients, the overproduction of
GH is caused by a benign tumor of the pituitary gland,
called an adenoma. These tumors produce excess GH and,
as they expand, compress surrounding brain tissues, such
as the optic nerves. This expansion causes the headaches
and visual disturbances that are often symptoms of acromegaly.
In addition, compression of the surrounding normal pituitary
tissue can alter production of other hormones, leading
to changes in menstruation and breast discharge in women
and impotence in men.
There is a
marked variation in rates of GH production and the aggressiveness
of the tumor. Some adenomas grow slowly and symptoms of
GH excess are often not noticed for many years. Other
adenomas grow rapidly and invade surrounding brain areas
or the sinuses, which are located near the pituitary.
In general, younger patients tend to have more aggressive
tumors.
Most pituitary
tumors arise spontaneously and are not genetically inherited.
Many pituitary tumors arise from a genetic alteration
in a single pituitary cell which leads to increased cell
division and tumor formation. This genetic change, or
mutation, is not present at birth, but is acquired during
life. The mutation occurs in a gene that regulates the
transmission of chemical signals within pituitary cells;
it permanently switches on the signal that tells the cell
to divide and secrete GH. The events within the cell that
cause disordered pituitary cell growth and GH oversecretion
currently are the subject of intensive research.
Non-pituitary
Tumors
In a few patients,
acromegaly is caused not by pituitary tumors but by tumors
of the pancreas, lungs, and adrenal glands. These tumors
also lead to an excess of GH, either because they produce
GH themselves or, more frequently, because they produce
GHRH, the hormone that stimulates the pituitary to make
GH. In these patients, the excess GHRH can be measured
in the blood and establishes that the cause of the acromegaly
is not due to a pituitary defect. When these non-pituitary
tumors are surgically removed, GH levels fall and the
symptoms of acromegaly improve.
In patients
with GHRH-producing, non-pituitary tumors, the pituitary
still may be enlarged and may be mistaken for a tumor.
Therefore, it is important that physicians carefully analyze
all "pituitary tumors" removed from patients with acromegaly
in order not to overlook the possibility that a tumor
elsewhere in the body is causing the disorder.
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Small
pituitary adenomas are common. During autopsies, they are
found in up to 25 percent of the U.S. population. However,
these tumors rarely cause symptoms or produce excessive
GH or other pituitary hormones. Scientists estimate that
about 3 out of every million people develop acromegaly each
year and that 40 to 60 out of every million people suffer
from the disease at any time. However, because the clinical
diagnosis of acromegaly often is missed, these numbers probably
underestimate the frequency of the disease.
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If
a doctor suspects acromegaly, he or she can measure the
GH level in the blood after a patient has fasted overnight
to determine if it is elevated. However, a single measurement
of an elevated blood GH level is not enough to diagnose
acromegaly, because GH is secreted by the pituitary in spurts
and its concentration in the blood can vary widely from
minute to minute. At a given moment, a patient with acromegaly
may have a normal GH level, whereas a GH level in a healthy
person may be five times higher.
Because of
these problems, more accurate information can be obtained
when GH is measured under conditions in which GH secretion
is normally suppressed. Physicians often use the oral
glucose tolerance test to diagnose acromegaly, because
ingestion of 75 g of the sugar glucose lowers blood GH
levels less than 2 ng/ml in healthy people. In patients
with GH overproduction, this reduction does not occur.
The glucose tolerance test is the most reliable method
of confirming a diagnosis of acromegaly.
Physicians
also can measure IGF-1 levels in patients with suspected
acromegaly. As mentioned earlier, elevated GH levels increase
IGF-1 blood levels. Because IGF-1 levels are much more
stable over the course of the day, they are often a more
practical and reliable measure than GH levels. Elevated
IGF-1 levels almost always indicate acromegaly. However,
a pregnant woman's IGF-1 levels are two to three times
higher than normal. In addition, physicians must be aware
that IGF-1 levels decline in aging people and may be abnormally
low in patients with poorly controlled diabetes mellitus.
After acromegaly
has been diagnosed by measuring GH or IGF-1, imaging techniques,
such as computed tomography (CT) scans or magnetic resonance
imaging (MRI) scans of the pituitary are used to locate
the tumor that causes the GH overproduction. Both techniques
are excellent tools to visualize a tumor without surgery.
If scans fail to detect a pituitary tumor, the physician
should look for non-pituitary tumors in the chest, abdomen,
or pelvis as the cause for excess GH. The presence of
such tumors usually can be diagnosed by measuring GHRH
in the blood and by a CT scan of possible tumor sites.
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The
goals of treatment are to reduce GH production to normal
levels, to relieve the pressure that the growing pituitary
tumor exerts on the surrounding brain areas, to preserve
normal pituitary function, and to reverse or ameliorate
the symptoms of acromegaly. Currently, treatment options
include surgical removal of the tumor, drug therapy, and
radiation therapy of the pituitary.
Surgery
Surgery is
a rapid and effective treatment. The surgeon reaches the
pituitary through an incision in the nose and, with special
tools, removes the tumor tissue in a procedure called
transsphenoidal surgery. This procedure promptly relieves
the pressure on the surrounding brain regions and leads
to a lowering of GH levels. If the surgery is successful,
facial appearance and soft tissue swelling improve within
a few days. Surgery is most successful in patients with
blood GH levels below 40 ng/ml before the operation and
with pituitary tumors no larger than 10 mm in diameter.
Success depends on the skill and experience of the surgeon.
The success rate also depends on what level of GH is defined
as a cure. The best measure of surgical success is normalization
of GH and IGF-1 levels. Ideally, GH should be less than
2 ng/ml after an oral glucose load. A review of GH levels
in 1,360 patients worldwide immediately after surgery
revealed that 60 percent had random GH levels below 5
ng/ml. Complications of surgery may include cerebrospinal
fluid leaks, meningitis, or damage to the surrounding
normal pituitary tissue, requiring lifelong pituitary
hormone replacement.
Even when surgery
is successful and hormone levels return to normal, patients
must be carefully monitored for years for possible recurrence.
More commonly, hormone levels may improve, but not return
completely to normal. These patients may then require
additional treatment, usually with medications.
Drug Therapy
Two medications
currently are used to treat acromegaly. These drugs reduce
both GH secretion and tumor size. Medical therapy is sometimes
used to shrink large tumors before surgery. Bromocriptine
(Parlodel®) in divided doses of about 20 mg daily reduces
GH secretion from some pituitary tumors. Side effects
include gastrointestinal upset, nausea, vomiting, light-headedness
when standing, and nasal congestion. These side effects
can be reduced or eliminated if medication is started
at a very low dose at bedtime, taken with food, and gradually
increased to the full therapeutic dose.
Because bromocriptine
can be taken orally, it is an attractive choice as primary
drug or in combination with other treatments. However,
bromocriptine lowers GH and IGF-1 levels and reduces tumor
size in less than half of patients with acromegaly. Some
patients report improvement in their symptoms although
their GH and IGF-1 levels still are elevated.
The second
medication used to treat acromegaly is octreotide (Sandostatin®).
Octreotide is a synthetic form of a brain hormone, somatostatin,
that stops GH production. This drug must be injected under
the skin every 8 hours for effective treatment. Most patients
with acromegaly respond to this medication. In many patients,
GH levels fall within one hour and headaches improve within
minutes after the injection. Several studies have shown
that octreotide is effective for long-term treatment.
Octreotide also has been used successfully to treat patients
with acromegaly caused by non-pituitary tumors.
Because octreotide
inhibits gastrointestinal and pancreatic function, long-term
use causes digestive problems such as loose stools, nausea,
and gas in one third of patients. In addition, approximately
25 percent of patients develop gallstones, which are usually
asymptomatic. In rare cases, octreotide treatment can
cause diabetes. On the other hand, scientists have found
that in some acromegaly patients who already have diabetes,
octreotide can reduce the need for insulin and improve
blood sugar control.
Radiation
Therapy
Radiation therapy
has been used both as a primary treatment and combined
with surgery or drugs. It is usually reserved for patients
who have tumor remaining after surgery. These patients
often also receive medication to lower GH levels. Radiation
therapy is given in divided doses over four to six weeks.
This treatment lowers GH levels by about 50 percent over
2 to 5 years. Patients monitored for more than 5 years
show significant further improvement. Radiation therapy
causes a gradual loss of production of other pituitary
hormones with time. Loss of vision and brain injury, which
have been reported, are very rare complications of radiation
treatments.
No single treatment
is effective for all patients. Treatment should be individualized
depending on patient characteristics, such as age and
tumor size. If the tumor has not yet invaded surrounding
brain tissues, removal of the pituitary adenoma by an
experienced neurosurgeon is usually the first choice.
After surgery, a patient must be monitored for a long
time for increasing GH levels. If surgery does not normalize
hormone levels or a relapse occurs, a doctor will usually
begin additional drug therapy. The first choice should
be bromocriptine because it is easy to administer; octreotide
is the second alternative. With both medications, long-term
therapy is necessary because their withdrawal can lead
to rising GH levels and tumor re-expansion. Radiation
therapy is generally used for patients whose tumors are
not completely removed by surgery; for patients who are
not good candidates for surgery because of other health
problems; and for patients who do not respond adequately
to surgery and medication.
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Benefits
versus risks of medical therapy for acromegaly. Acromegaly
Therapy Consensus Development Panel. American Journal
of Medicine 97(5):468-473, 1994.
Eastman RC,
Gorden P, Glatstein E, Roth J. Radiation Therapy of Acromegaly.
Endocrinology and Metabolism Clinics of North America
21(3):693-711, 1992.
Ezzat S, Forster
MJ, Berchtold P, Redelmeier DA, Boerlin V, Harris AG.
Acgromegaly. Clinical and Biochemical Features in 500
Patients. Medicine (Baltimore) 73(5):233-240, 1994.
Ezzat S. Living
with acromegaly. Endocrinology and Metabolism Clinics
of North America 21:753-760, 1992.
Jaffe CA; Barkan
AL. Acromegaly. Recognition and treatment. Drugs
47(3):425-45, 1994.
Jaffe CA, Barkan
AL. Treatment of acromegaly with dopamine agonists. Endocrinology
and Metabolism Clinics of North America 21:713-735,
1992.
Krishna AY;
Phillips LS. Management of acromegaly: a review. American
Journal of Medical Science 308(6):370-375, 1994.
Melmed S. Acromegaly.
New England Journal of Medicine 322:966-977, 1990.
Molitch ME.
Clinical manifestations of acromegaly. Endocrinology
and Metabolism Clinics of North America 21(3):597-614,
1992.
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Pituitary
Tumor Network Association
16350 Ventura Blvd., #231
Encino, CA 91436
(805) 499-9973
Fax: (805) 499-1523
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NIH
Publication No. 95-3924
February 1995
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