Arthritis & Rheumatism

There are over 100 types of arthritis and rheumatic diseases including osteoarthritis, rheumatoid arthritis, and fibromyalgia. This site provides the latest arthritic and rheumatic information including the treatment options available.



Arthritis is a common disease that affects millions of people worldwide. This can be felt in the person's joints, skin and organs inside the body. Should the person feel anything wrong, it is advisable to go straight to the doctor. Doctors have discovered that there are over 100 types of arthritis. Given the number, the doctor will not be able to know which one is affecting the person without an examination.

There are 2 common forms of arthritis. The first is rheumatoid arthritis which is considered a chronic disease. There is inflammation in the joints caused by cartilage damage. Anyone who has this will suffer long term joint damage that will lead to chronic pain and disability. Pain is usually felt when waking up in the morning and will gradually disappear during the day.

Rheumatoid arthritis is a problem that will not go away. This happens in three stages. The first is swelling. The second is the rapid division and growth of cells. The third is when these cells release enzymes that will eat the bone causing the joint to lose shape until the person will not be able to move it anymore.

Since this is systemic disease, it can spread and affect other organs in the body. The best way to prevent is from happening is detecting it early to prevent the person from being disabled. This can be treated with proper medication and therapy. There many drugs available that the patient can use. Some drugs offer pain relief to reduce the inflammation. Others can just do one function.

The second is called osteoarthritis. This happens more often than rheumatoid arthritis but unlike the first, there is no inflammation present. The cartilage in the joint is damaged and will eventually degenerate. Pain will slightly be felt when the person gets up but this will hurt later on during the day. Osteoarthritis can either be primary or secondary. When it is primary, it is often associated with age. It is similar to a car where the parts have to be replaced due to wear and tear. Doctors consider this to be normal as people grow older.

The secondary type is often associated with something else that has caused this to happen. Some of these factors are an injury that took place, heredity, obesity and bone density. Osteoarthritis can be treated with medication, exercise, weight control, joint protection, physical and occupational therapy. This is done to relieve the pain and slow the progression of the disease. Both of these are caused by different things. The common thing between these 2 types is that joint pain can happen anywhere in the body.

Given the many medications available to treat this disease, the patient has to be aware of the side effects of each before choosing which one to use. The doctor should explain these to the person in order to make the right decision.



Tuesday, November 13, 2007

I Take Methotrexate For Rheumatoid Arthritis And I’m Concerned About The Side Effects

Since the early 1980’s methotrexate has assumed the position of “gold standard” as a disease modifying anti-rheumatic drug (DMARD) for rheumatoid arthritis (RA). It is effective, relatively safe, and also relatively inexpensive. In the past methotrexate was used either as a single agent or in combination with other DMARDS such as hydroxychloroquine (Plaquenil) or sulfasalazine (Azulfidine). With the advent of the newer biologic drugs, methotrexate is most often used in combination with these biologics for patients with active RA.

Methotrexate works by blocking an enzyme called dihydrofolate reductase. The end result of this action is a reduction in purines and pyrimidines, inhibition of T-cell activation, and reduction of inflammation through the release of a substance called adenosine. Therefore, methotrexate has both anti-inflammatory properties as well as disease-modifying properties. Generally, methotrexate is well tolerated and safe; however, it is discontinued as a result of side effects not infrequently. Most of the side effects related to the low doses used in rheumatoid arthritis are preventable and reversible. Because of the mechanism of action through the antagonism of folate metabolism, there are toxicities that are sometimes seen.

The most common are mouth ulcers, soreness in the mouth, drop in white blood cell counts, drop in platelet counts, and anemia. These side effects can usually be prevented by giving a patient supplemental folic acid. In our clinic we give patients anywhere from one to three mgs per day. One tactic that seems to help with some of the side effects is to split dose the methotrexate- ie., have the patient divide up their dose so that they are taking their tablets over a 24 hour period of time once a week instead of all at gulp.

Patients who develop gastrointestinal upset with tablets occasionally do better with subcutaneous methotrexate. There are also side effects that are not dependent on folate metabolism. These include fatigue, rheumatoid nodule formation, liver damage, and lung damage. Lung damage can be due to fibrosis which can occur over time or there can be an acute syndrome consisting of pneumonitis (lung inflammation), accompanied by fevers, chills, shortness of breath, and respiratory failure. Rare instances of kidney damage have occurred. A much more common scenario though occurs when patients with poorly functioning kidneys are given methotrexate and develop methotrexate toxicity as a result of accumulation of the drug.

There is some data that implicates adenosine as being responsible for some of these side effects. Since methotrexate increases adenosine levels, this is an intriguing possibility. This is being evaluated particularly in a liver disease model. Methotrexate and ethyl alcohol both appear to increase adenosine output from liver cells. In animal models, this paves the way for liver fibrosis. When compounds that block adenosine are given, the liver fibrosis doesn’t occur. The trend now is to use somewhat lower doses of methotrexate and institute biologic drugs earlier. This may also help offset methotrexate toxicity since toxicity to a certain extent is dose dependent. Monitoring for methotrexate toxicity through the use of monthly laboratory testing of blood count and liver function tests, as well as clinical evaluation goes a long way towards preventing many of the potential problems associated with this drug.

Author :Nathan Wei, MD FACP FACR is a rheumatologist and Director of the Arthritis and Osteoporosis Center of Maryland. He is a Clinical Assistant Professor of Medicine at the University of Maryland School of Medicine.

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