shown by Huskisson et al (1974) and others to be effective, but its place in the treatment of patients with rheumatoid arthritis has still to be determined. Azapropazone has a pyrazolidine ring like phenylbutazone, but in azapropazone the ring is coupled with a 1, 2, 4, benzo- triazine ring. So far azapropazone has caused dyspepsia and an occasional skin rash, but not any of the serious complica- tions associated with phenylbutazone. Azapropazone is effective in rheumatoid arthritis, and probably will find a useful place in management (Brooks and Buchanan, 1976). Feprazone has a terpene group condensed together with a pyrazolidine ring. It was developed with the intention of combining the ulcer-healing properties of the terpenes with the anti-inflammatory effects of the pyrazolidines. The drug appears to have an anti-inflammatory effect comparable with other non-steroidal anti-inflammatory analgesics as indomethacin (Rooney et al, 1974) . Dyspepsia has been found trouble- some and 5 per cent of patients develop rashes. Tolmetin is a pyrrole derivative with some structural similarities to indomethacin. The drug has been found to be effective, but further studies will be required before its place in the management of rheumatoid arthritis is established. Alclofenac is a substituted aryl acetic acid. A considerable amount of work has been done on this drug's ability to displace a natural anti-inflammatory substance from the protein-binding site (Aylward et al, 1975) . However, this has by no means been proved. Alclofenac will also uncouple oxidative phosphorylation, inhibit prostaglandin synthetase, and interfere with the release of ADP from platelets. It has been suggested that alclofenac will fundamentally alter the disease process, but again this has not been proved. Drug rashes are common occuring in 10 per cent of patients, and vasculitis has been reported. Sulindac is a new, non-steroidal anti- inflammatory, analgesic, antipyretic agent produced by Merck, Sharp and Dohme. Chemically it rejoices in the formula; (Z) - 5 - fluoro - 2 - methyí - 1 (p-methylsulfinyl) pheiiyl) methylene - IH - indene - 3 - acetic acid. The drug has been proven of cUnical value in rheumatoid arthritis (Huskisson and Franchimont, 1976, Reynolds et al, 1977) and appears to be weU tolerated. Sulindac has now been extensively studied in a variety of rheumatic disorders including osteoarthritis, ankylosing spondylitis, painful shoulder syndromes and aeute gout, where it has been proven beneficial. We have also recently been able to show that the drug has definite anti-inflammatory properties in man, as evidenced by shrinkage of digital joint circumference and reduction in radioactive technetium uptake in the joints in rheumatoid arthritis. So far no serious side effects have been reported, and the major problem is that of otner non-steroidal antiinflammatory drugs, namely dyspepsia. The Anti - Malarials The 4-aminoquinalone antimalarial drugs have been used in the treatment of rheumatoid arthritis for nearly quarter of a century. The major problem associated with their use is the development of serious retinal damage. Many rheuma- tologists indeed now consider that this compUcation outweighs the clinical benefit derived from their administration. Evidence that antimalarial drugs are beneficial in rheumatoid arthritis rests essentially on two studies in which the drug was compared with placebo for a year or more (Popert et al, 1961, Hamilton and Scott, 1962). The drugs most commonly prescribed are hydroxy- chloroquine sulphate in a dose of 200 mg twice daily and chloroquine sulphate 250 mg once daily. Improvement occurs slowly, maximum benefit not occuring for three to six months. Antimalarials should not be prescribed in patients with psoriasis because of the danger of developing exfoliative dermatitis (Baker, 1966) and they should not be given to children, who may develop cardio-respiratory arrest even after as Httle as 1 g (Markowitz and McGinley, 1964). Pregnancy is a definite contraindication. Rarelj' leucopenia and peripheral neuropathy may occur wit chronic administration of anti-malarials. Surprisingly patients, who develop side effects to chloroquine, such as vomiting, diarrhoea and skin rashes, may tolerate hydr oxychlor oquine. 90

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