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OSTEOARTHRITIS
What is osteoarthritis?
Osteoarthritis is the collective name for a family of bone diseases
involving the degeneration of cartilage and abnormal growth of
new bone and connective tissue. In late stage cases, abnormal
bone growth causes visible bumps and ridges around the joints.
Osteoarthritis can affect most joints, including the spine, but is
more common in the knees, hips, feet and hands. Nodal
osteoarthritis, affecting the finger joints, which occurs
predominantly in middle-aged women, is clinically distinct from,
for example, osteoarthritis of the knees, which is often related to
obesity and shows a more even sex distribution. Symptoms
depend on the joints affected, but include pain, stiffness and
loss of function. Pain can become severe in the later stages of
osteoarthritis, when replacement of the joint affected may be
necessary. In 2005, there were 62,677 hip replacements and
62,818 knee replacements carried out in England and Wales.
Who does osteoarthritis affect and what does it cost?
By the age of 65, 80 per cent of people show evidence of
osteoarthritis in X-rays, although only about 25 per cent have
symptoms. Estimates have put the number of people suffering from
osteoarthritis in the United Kingdom at 8.5 million, with more than
2 million visiting their GP each year because of osteoarthritis. The
prevalence of osteoarthritis increases markedly with age in both
men and women.
The total cost of arthritis (of which osteoarthritis makes up the
largest component) to the NHS and social services has been
estimated at £5.5 billion in 2000. Of this, the cost of operations to
replace hip and knee joints was £405 million, other hospital costs
were £259 million, GP consultations cost £307 million, and the cost of medications was £341 million. In addition, 206 million
working days were lost in that year due to arthritis, corresponding
to a loss of production of over £18 billion.
Present treatments and shortcomings
Current treatments for osteoarthritis are solely concerned with
managing symptoms such as pain; there is no medication that has
been proven to prevent the disease or modify its course. Exercises
to build muscle are useful in people who are still active, simple
painkillers or non-steroidal anti-inflammatory drugs (NSAIDs) are
prescribed for pain control, and corticosteroid injections into the
joint can help in acute cases. In addition, various preparations are
available for injection into the knee joint to improve the condition
of the joints, but this does not alter the course of disease.
NSAIDs inhibit an enzyme called cyclo-oxygenase (COX), blocking
the formation of inflammatory prostaglandins. COX exists in two
forms: COX-1 and COX-2. Prostaglandins produced by COX-2 are
inflammatory and damage the gut, leading to gastric ulcers and
bleeding, but those from COX-1 have a protective effect. Of the
older NSAIDs, some inhibit COX-2 more than COX-1 but are not
entirely selective. Two of these are meloxicam (Mobic, Boehringer
Ingelheim) and nabumetone (Relifex, Meda). Both have a lower
risk of ulcers than NSAIDS that mainly inhibit COX-1, such as
indomethacin, sulindac, aspirin and piroxicam.
COX-2 selective NSAIDs have been developed and introduced, but
some have had to be withdrawn, following the finding of a raised
incidence of heart problems. There is evidence that the risk of such
side-effects differs from one selective COX-2 inhibitor to another and three remain available for pain relief in osteoarthritis. These
are: celecoxib (Celebrex, Pfizer), etoricoxib (Arcoxia, Merck Sharp
& Dohme), and lumiracoxib (Prexige, Novartis). Some of the older
and widely used NSAIDs, ibuprofen and diclofenac, have also
been associated with heart problems. While the risk of such
side-effects remains small in all of these cases, the physician and
patient must make any decision on the long-term use of high doses
of painkillers on the basis of weighing up both risks and benefits.
NEW
SINCE 2000 |
| 2000 - |
Celecoxib (Celebrex, Pfizer) |
| 2002 - |
Etoricoxib (Arcoxia, Merck
Sharp & Dohme) |
2005 - |
Lumiracoxib (Prexige,
Novartis) |
What's in the development pipeline?
Additional pain-killers, including selective inhibitors of COX-2,
are being studied for use in osteoarthritis and Daiichi-Sankyo has
CS-706 in Phase 2 trial. NicOx is developing a version of
naproxen (HCT 3012, naproxcinod), which has reached Phase 3
trial in osteoarthritis of the knee. This compound is expected not
to show the blood pressure-raising effect of NSAIDs that may be
responsible for the increased risk of heart problems. Pfizer also has
a compound (CJ-23423) in phase 2 trial for osteoarthritis.
Meanwhile, CombinatoRx Inc has reported positive results with a
Phase 2 study of its CRx-102 for pain reduction in osteoarthritis of
the hand.
New treatment approaches are also being studied by various
companies. Sanofi-aventis has HOE 140 (icatibant) in Phase 2 trial
and an oral form of calcitonin (SMC 021) being studied by
Novartis and an anti-inflammatory compound (SC-84250) from
Pfizer have reached the same stage. At Phase 1, Schwarz Pharma
(UCB) is developing lacosamide and Wyeth (AGG-523, PLA-695)
and Merck Sharp & Dohme (MK0822) also have compounds in
development.
The possibility of modifying disease progress is also being
investigated. Risedronate (Actonel, Procter & Gamble), a
compound in the bisphosphonate group, slows bone destruction
in osteoporosis and, as tiny fractures of bone at the joint surface
have been suggested as a possible underlying cause of
osteoarthritis, it might slow disease progress in osteoarthritis
too. Although a reduction in pain was not found, risedronate did
reduce the level of a marker of bone turnover that is associated
with the progression of osteoarthritis. Also, GlaxoSmithKline is
investigating an inhibitor (GSK 462795, relacatib) of an enzyme
that may affect bone destruction, and this is at Phase 1.
FOR FURTHER INFORMATION CONTACT:
ARTHRITIS CARE
18 Stephenson Way
London, NW1 2HD
Phone: 0808 800 4050 (Helpline)
Website: www.arthritiscare.org.uk
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