My life with FMD: Member FMDSA; Fibromuscular Dysplasia Society of America;
What is Fibromuscular Dysplasia? (FMD)
(written by Susan M. Begelman, M.D., updated 8/2/2004)
Please note, the information provided on this page is designed to support, not replace, the relationship that exists between you and your physician.
What is Fibromuscular Dysplasia (FMD)?
What are the signs and/or symptoms of FMD?
What kind of treatment is there for FMD?
What is Fibromuscular Dysplasia (FMD)?
The word “dysplasia” simply means abnormal cellular development or growth. In people with FMD, the dysplasia involves the walls of one or more arteries in the body. Areas of narrowing, called stenosis, may occur as a result of abnormal cell development. If enough narrowing causes a decrease in blood flow through the artery, symptoms may result. Many people with FMFD do not have any symptoms or signs on physical examination and are diagnosed by accident during a radiology scan for another problem.
FMD is most commonly found in the arteries that supply the kidneys with blood (renal arteries). Up to 75% of all patients with FMD will have disease in the renal arteries (Fenves, 1999). The second most common artery affected is the carotid artery, which is found in the neck and supplies the brain with blood. Less commonly, FMD affects the arteries in the abdomen (supplying the liver, spleen and intestines) and extremities (legs and arms). More than one artery may have evidence of FMD in 28% of people with this disease (Luscher, 1986).
Prior to diagnosing a person with FMD, several other diseases should be ruled out. These include: arteriosclerosis, commonly referred to as “hardening of the arteries”, inflammatory vascular diseases (vasculitis) such as Takayasu’s arteritis (abnormally dilated arteries).
The cause of FMD is not yet known, but several theories have been suggested. A number of case reports in the literature have identified the disease in multiple members of the same family including twins. As a result it is felt that there may be a genetic cause. However, a relative may have different artery involvement, different disease severity, or not develop FMD at all. In fact, not all individuals with FMD have a family member who also has the disease.
FMD is also more commonly seen in women than in men resulting in the theory that hormones may play an important role in disease development. This theory is further supported by the fact that most women are premenopausal at the time of diagnosis. However, in small population studies, one’s reproductive history (the number of pregnancies and when they occurred) as well as the use of birth control pills did not correlate with the development of FMD.
Other possible causes of FMD include abnormal development of the arteries that supply the vessel wall with blood resulting in inadequate oxygen supply; the anatomic position of the artery within the body; medications (ergotamine preparations, methysergide); and tobacco use. It is possible that many factors are involved in the development of FMD. This area requires further research.
What are the signs and/or symptoms of FMD?
Many people with this disease do not have symptoms or findings on a physical examination. The signs and/or symptoms that a person with FMD may experience depend on the arteries affected and the degree of narrowing within them. The two most common areas affected by FMD are the renal arteries (arteries carrying blood to the kidneys) and the carotid arteries (arteries carrying blood to the brain). Any pain or clinical sign related to FMD typically comes from the organ that is supplied by that artery. For example, FMD in the kidney arteries may cause high blood pressure. Progression of the disease can also result in ischemic renal atrophy, where some of the kidney’s tissue dies due to lack of oxygen, and in rare circumstances, kidney failure.
Patients with impaired carotid arteries may have nonspecific complaints including dizziness, temporary blurring or loss of vision, tinnitus (ringing or buzzing in the ears), vertigo (feeling as if the room was spinning around you), neck pain, and or chronic headaches. However, a person with severe FMD may have neurologic symptoms involving the facial muscles (drooping of the face, for example), stroke, or transient ischemic attack. People with carotid FMD have a higher risk for intracranial aneurysms (abnormal dilations of the arteries in the brain). An intracranial hemorrhage (bleeding in the brain) may occur if an aneurysm ruptures.
FMD involving the mesenteric arteries (arteries that supply the intestines, liver and spleen with blood) can result in abdominal pain after eating and unintended weight loss. FMD in the arms and legs can cause limb discomfort with use, cold limbs, weakness, numbness, or skin changes in the fingers and toes due to lack of blood flow.
Anyone can have FMD. However, it is much more common in women. Most women are typically diagnosed between the ages of 25-50. However, some forms of this disease are more common in children or teenagers.
It is difficult to determine how common FMD is in the general population. This is due to several reasons. Individuals with mild disease are often asymptomatic and so the disease may go undetected. Most studies examining the prevalence of FMD have looked at specific patient populations in whom individuals may have already suffered from serious consequences of the disease. Incidence rates have been quoted at 0.5-1.1% although this may not be indicative of how many people actually have FMD.
There are a number of methods that can be used to detect FMD. These include CT scan, MRI, Ultrasound, and Angiogram. The experience and expertise available at your medical institution will play an important role in what diagnostic options are available to you.
In the most common forms of FMD, a characteristic “string of beads” appearance is seen in the affected artery. This appearance is due to changes in the cellular tissue of the artery wall that causes the arteries to alternatively become narrow and dilated. A less common, but more aggressive form of FMD may cause areas of vessel narrowing only without the “string of beads” appearance.
What kind of treatment is there for FMD?
There is no cure for FMD. However, in some cases an attempt should be made to improve the flow of blood through the vessel. The kind of treatment used for FMD depends largely upon which arteries are affected, the presence and severity of the symptoms, and if there is progression of the disease. The experience and expertise available at your medical institution will also play an important role in what treatment options are available to you. Currently, there is not a set protocol for treating FMD.
If your health care professionals feel that treatment is warranted, most often percutaneous transluminal angioplasty (PTA) is preferred. PTA is often performed at the same time as an arteriogram. Arteriography is a procedure that is performed by a radiologist, vascular surgeon, or a cardiologist with appropriate training that involves inserting a wire into or near the affected artery and injecting contrast material, a dye that can be detected by an X-ray machine. An x-ray of the affected area is then taken and examined. If an angioplasty is performed, a catheter is extended into the affected artery and a small balloon is inflated that “stretches” open the vessel. A metal stent is typically not required to keep the vessel open.
The individual is usually awake during the procedure although medications may be given to make the patient more comfortable. This outpatient procedure usually lasts from one to two hours with a recovery period of up to six hours (this varies widely). If angioplasty is performed, the procedure and recovery period may be longer. Occasionally traditional surgery is performed.
Most individuals should take an antiplatelet agent daily (i.e., aspirin). All patients who use tobacco should be encouraged to quit. The appropriate treatment will vary with each individual and severity of disease. It should be discussed in depth with a specialist who is very knowledgeable about FMD and its natural history.
FMDSA Frequently Asked Questions were authored by Susan M. Begelman, M.D., Staff Physician, The Cleveland Clinic Foundation. Updated August 2, 2004.
BIBLIOGRAPHY
Begelman, SM and Olin, JW. Fibromuscular Dysplasia, Current Opinion in Rheumatology. (2000) 12:41-47.
Fenves, AZ and Ram, CV. Fibromuscular Dysplasia of the Renal Arteries, Current Hypertension Reports. (1999) 1:546-549.
Lusher, TF, Keller HM, Imhof, HG, Griminger, P, Kuhlmann, U, Largiader, F, Schneider, E, Schneider, J, Vetter, W. Fibromuscular Hyperplasia: Extension of the disease and therapeutic outcome. Results of the University Hospital Zurich Cooperative Study on Fibromuscular Hyperplasia. Nephron. (1986). 44(Suppl 1): 109-114.
Lusher, TF, Lie, JT, Stanson, AW. Houser, OW, Hollier, LH, and Sheps, SG. Arterial Fibromuscular Dysplasia, Mayo Clinic Proceedings. (1987) 62: 931-952.
My Life With Fibromuscular Dysplasia
I was diagnosed with Fibromuscular Dysplasia in 1992 at age 42. I went to an ear/nose/throat specialist for a sinus infection. I complained to the Dr. that I constantly hear my heartbeat pounding in my ear, and my ear feels like it is full of water. The doctor said my symptoms sounded like a case of clogged arteries, which usually affects older people.
The doctor listened to the arteries in my neck and then told me, "I think we have a problem." He then sent me immediately to the hospital across the street for an ultrasound. The ultrasound indicated I had an 80% blockage. I was then referred to a surgeon who said he did not think the results of the ultrasound could not be a true diagnosis. At that time I was slim, my cholesterol level was perfect, my triglycerides and everything was perfect.
I was then scheduled for an arteriogram. (And I was scared to death.) The arteriogram revealed no clogged arteries, but I did have the famous "string of beads" that accompanies FMD. I had FMD in both inner carotid arteries with a 25% stenosis. I wasn’t even told what Fibromuscular Dysplasia was or what to expect from this disease. Everyone just acted so relieved that I didn’t have clogged arteries. They actually told me, "You don’t have clogged arteries after all, you have Fibromuscular Dysplasia" and then they walked out.
I ran into the radiologist later and he briefed me a little and told me this was something I did need to keep checking on because it is a progressive disease. I got a copy of my medical records and started researching. Back in 1992 it was almost impossible to find any information on this disease. Personal Computers were not common like they are now. I went to my local library and contacted National Organization for Rare Disorders but got very little information.
In 1995 I felt the disease had progressed, the sound in my ear was much louder and I had a lot of pressure in my head. I discussed this with my physician and he referred me to a surgeon for another arteriogram. The arteriogram indicated now a 50% stenosis and also an aneurysm behind my right eye.
Now I was referred to a neurosurgeon to repair the aneurysm. I was told all the complications that could happen during brain surgery, including death. The neurosurgeon scheduled my surgery for the following week. He needed time to get a team together including my regular surgical physician. During that week I was trying to adjust and accept what I would be facing. Of course I was scared and concerned. After a few days I came to terms with the upcoming event.
I went to see the staff attorney where I worked and asked her help in making out a will, a living will, and a power of attorney. I was single at the time but had a teenage daughter and a son. The staff attorney commented to me that I certainly was calm and accepting of the situation. I told her I had decided "Whatever happens, the Lord and I can handle it."
The surgery went fine, and I had two clips placed to seal off the aneurysm. I had no complications except double vision for a few months. This was due to swelling of the brain. After 11 days in the hospital and some physical therapy I was released from the hospital. I followed my doctor’s orders to a T and healed rapidly with no complications.
I have had several follow-up arteriograms since then. The last arteriogram was in 2005, indicating a 75% stenosis in the inner carotids and the FMD is now in my renal arteries, vertebral arteries, and legs.
Since the FMD is so widely scattered in my brain, the doctors say surgery is a last resort. I take an aspirin every day, do not eat red meat, watch my cholesterol, and try to avoid stress.
I do suffer from migraines, ocular migraines accompanied by a lot of visual problems and severe pain in the vertebral arteries. I still have the constant heartbeat pounding in my ear and feeling of a lot of pressure in my head. I do have some other health problems also that seem to accompany age.
I am #10 out of 11 children (yes, eleven), and the only one in my family that has been diagnosed with FMD. I hope and pray my son, daughter, and granddaughter never have to face FMD.
Now there is so much information available to help anyone who may be diagnosed with FMD. Thanks to the FMDSA and all their hard work to get this disease recognized by NORD, The American Stroke Organization, other medical organizations, and all the great web links now available.
My motto is "The Best Wealth is Health".
The Best Wealth is Health!
Link to FMDSA http://fmdsa.org/index.html
The FMDSA website is designed to help patients, healthcare workers and physicans find the latest information on Fibromuscular Dysplasia. We have put together resources and diagnostic information on the disease, how you can participate in research, spread awareness, and ways you can help us find a cure.