Article title: Multiple Endocrine Neoplasia Type 1: NIDDK
Main condition: MEN1
Conditions: MEN1, glands, pancreas, pituitary
Endocrine glands are different from other organs in the body because they release hormones into the bloodstream. Hormones are powerful chemicals that travel through the blood, controlling and instructing the functions of various organs. Normally, the hormones released by endocrine glands are carefully balanced to meet the body's needs.
In patients with MEN1, sometimes more than one group of endocrine glands, such as the parathyroid, the pancreas, and the pituitary become overactive at the same time. Most people who develop overactivity of only one endocrine gland do not have MEN1.
The parathyroids are the endocrine glands earliest and most often affected by MEN1. The human body normally has four parathyroid glands, which are located close to the thyroid gland in the front of the neck. The parathyroids release into the bloodstream a chemical called parathyroid hormone, which helps maintain a normal supply of calcium in the blood, bones, and urine.
In MEN1, all four parathyroid glands tend to be overactive. They release too much parathyroid hormone, leading to excess calcium in the blood. High blood calcium, known as hypercalcemia, can exist for many years before it is found by accident or by family screening. Unrecognized hypercalcemia can cause excess calcium to spill into the urine, leading to kidney stones or kidney damage.
Nearly everyone who inherits a susceptibility to MEN1 (a "carrier") will develop overactive parathyroid glands (hyperparathyroidism) by age 50, but the disorder can often be detected before age 20. Hyperparathyroidism may cause no problems for many years or it may cause problems such as tiredness, weakness, muscle or bone pain, constipation, indigestion, kidney stones, or thinning of bones.
Treatment of Hyperparathyroidism.
It is sometimes difficult
to decide whether hyperparathyroidism in MEN1 is severe enough to need
treatment, especially in a person who has no symptoms. The usual treatment
is an operation to remove the three largest parathyroid glands and all but
a small part of the fourth. After parathyroid surgery, regular testing of
blood calcium should continue, since the small piece of remaining
parathyroid tissue can grow larger and cause recurrent
hyperparathyroidism. People whose parathyroid glands have been completely
removed by surgery must take daily supplements of calcium and vitamin D to
prevent hypocalcemia (low blood calcium).
The Pancreas
The pancreas gland, located behind the stomach, releases digestive juices into the intestines and releases key hormones into the bloodstream. Some hormones produced in the islet cells of the pancreas and their effects are:
About one in three patients with MEN1 has gastrin-releasing tumors, called gastrinomas. (The illness associated with these tumors is sometimes called Zollinger-Ellison syndrome.) The ulcers caused by gastrinomas are much more dangerous than typical stomach or intestinal ulcers; left untreated, they can cause rupture of the stomach or intestine and even death.
Treatment of Gastrinomas.
The gastrinomas associated with
MEN1 are difficult to cure by surgery, because it is difficult to find the
multiple small gastrinomas in the pancreas and small intestine. In the
past, the standard treatment for gastrinomas was the surgical removal of
the entire stomach to prevent acid production. The mainstay of treatment
is now very powerful medicines that block stomach acid release, called
acid pump inhibitors. Taken by mouth, these have proven effective in
controlling most cases of Zollinger-Ellison syndrome.
The Pituitary Gland
The pituitary is a small gland inside the head, behind the bridge of the nose. Though small, it produces many important hormones that regulate basic body functions. The major pituitary hormones and their effects are:
Treatment of Prolactinomas.
Most prolactinomas are small, and
treatment may not be needed. If treatment is needed, a very effective type
of medicine known as a dopamine agonist can lower the production of
prolactin and shrink the prolactinoma. Occasionally, prolactinomas do not
respond well to this medication. In such cases, surgery, radiation, or
both may be needed.
Other rare complications arise from pituitary tumors that release high amounts of ACTH, which in turn stimulates the adrenal glands to produce excess cortisol. Pituitary tumors that produce growth hormone cause excessive bone growth or disfigurement.
Another rare complication is an endocrine tumor inside the chest or in the stomach, known as a carcinoid. In general, surgery is the mainstay of treatment for all of these rare types of tumors, except for gastric carcinoids which usually require no treatment.
Another type of benign tumor often seen in people with MEN1 is a plum-sized, fatty tumor called a lipoma, which grows under the skin. Lipomas cause no health problems and can be removed by simple cosmetic surgery if desired. These tumors are also fairly common in the general population.
Benign tumors do not spread to or invade other parts of the body. Cancer cells, by contrast, break away from the primary tumor and spread, or metastasize, to other parts of the body through the bloodstream or lymphatic system.
The pancreatic islet cell tumors associated with MEN1 tend to be numerous and small, but most are benign and do not release active hormones into the blood. Eventually, about half of MEN1 cases will develop a cancerous pancreatic tumor.
Treatment of Pancreatic Endocrine Cancer in MEN1.
Since the
type of pancreatic endocrine cancer associated with MEN1 can be difficult
to recognize, difficult to treat, and very slow to progress, doctors have
different views about the value of surgery in managing these tumors.
One approach is to "watch and wait," using medical, or nonsurgical treatments. According to this school of thought, pancreatic surgery has serious complications, so it should not be attempted unless it will cure a tumor that is secreting too much hormone.
Another school advocates early surgery, perhaps when a tumor grows to a certain size, to remove pancreatic endocrine cancer in MEN1 (even if it does not over secrete a hormone) before it spreads and becomes dangerous. There is no clear evidence, however, that aggressive surgery to prevent pancreatic endocrine cancer from spreading actually leads to longer survival for patients with MEN1.
Doctors agree that excessive release of certain hormones (such as gastrin) from pancreatic endocrine cancer in MEN1 needs to be treated, and medications are often effective in blocking the effects of these hormones. Some tumors, such as insulin-producing tumors of the pancreas, are usually benign and single and are curable by pancreatic surgery. Such surgery needs to be considered carefully in each patient's case.
In addition, the age at which MEN1 can begin to cause endocrine gland overfunction can differ strikingly from one family member to another. One person may have only mild hyperparathyroidism beginning at age 50, while a relative may develop complications from tumors of the parathyroid, pancreas, and pituitary by age 20.
Sometimes a patient with MEN1 knows of no other case of MEN1 among relatives. The commonest explanations are that knowledge about the family is incomplete or that the patient carries a new MEN1 gene mutation.
If you have been diagnosed with MENl, it is important to get periodic checkups because MEN1 can affect different glands, and even after treatment, residual tissue can grow back. Careful monitoring enables your doctor to adjust your treatment as needed and to check for any new disturbances caused by MEN1. Most people with MEN1 will have long and productive lives.
The MEN1 gene was very recently identified. As of 2001, a small number of centers around the world have begun to offer MEN1 gene testing on a research or commercial basis. The likelihood of finding a mutation in an MEN1 family has varied from 60 percent to 94 percent depending on methods. When a mutation is found, further testing in other relatives can become much easier. Many relatives can be tested once and be found without the known MEN1 mutation in their family, and then they can be freed from uncertainty and from any further testing ever for MEN1. When a mutation is not found in a family or isolated case, it does not prove that no MEN1 mutation is present. Depending on the clinical and laboratory information, it may still be very likely that a mutation is present but undetected.
In the meantime, though, screening of close relatives of persons with MEN1, who are at high risk, generally involves testing for hyperparathyroidism, the most common and usually the earliest sign of MEN1. Any doctor can screen for hyperparathyroidism by testing the blood for total calcium and sometimes one or two other substances such as ionized calcium and parathyroid hormone. An abnormal result indicates that the person probably has MEN1, but a normal finding in all cannot rule out the chance that he or she will develop hyperparathyroidism at a later time. Blood testing can usually show signs of early hyperparathyroidism many years before symptoms of hyperparathyroidism occur.
Testing can detect the problems caused by MEN1 tumors many years before their later complications develop. Finding these tumors early enables your doctor to begin preventive treatment, reducing the chances that MEN1 will cause problems later.
Genetic counseling can help individuals and couples through the
decision-making process with family planning. Genetic counselors will
provide information to help with the decision-making process, but they
will not tell individuals or couples what decision to make or how to make
it.
The NIDDK conducts and supports a variety of research in endocrine disorders, including MEN1. NIDDK and other NIH researchers isolated the MEN1 gene in 1997. Researchers have also shown that the MEN1 gene contributes to common endocrine tumors outside of the setting.
The following articles about MEN1 can be found in medical libraries, some college and university libraries, and through interlibrary loan in most public libraries.
Chandrasekharappa, S.C., Guru, S.C., Manickam, P., Olufemi, S., Collins, F.S. Emmert-Buck, M.R., Debelenko, L.V., Zhuang, Z., Lubensky, I.A., Liotta, L.A., Crabtree, J.S., Wang, Y., Roe, B.A., Weisemann, J., Boguski, M.S., Agarwal, S.K., Kester, M.B., Kim, Y.S., Heppner, C., Dong, Q., Spiegel, A.M., Burns, A.L., Marx, S.J., "Positional cloning of the gene for multiple endocrine neoplasia-type 1," Science 276:404-407, 1997.
Marx SJ. Multiple endocrine neoplasia type 1. In: Metabolic Basis of Inherited Diseases, 8th Ed. ed. Scriver CS, et al. McGraw Hill, NY, 2001. pp 943-966.
Schussheim DH, Skarulis MC, Agarwal SK, Simonds WF, Burns AL, Spiegel AM, Marx SJ. MEN1: New clinical and basic findings. Trends Endocrinol Metab 12: 173-178, 2001.
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This e-pub was written by Stephen J. Marx, M.D. and reviewed by Robert T. Jensen, M.D., both of the National Institute of Diabetes and Digestive and Kidney Diseases. It is based in part on the booklet, "Understanding Multiple Endocrine Neoplasia Type 1," published by the NIH Clinical Center's Communications Office.
NIH Publication No. 97-3048
June 1997
E-text last reviewed: August 2001
Reviewer: Stephen J. Marx,
M.D.
NIDDK, NIH
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