Chloroquine particularly accumulates in the pigmented tissue of the eye. Bernstein et al (1963) have shown, that the drug does not concentrate in iris, choroid or pigment epithelium in albino rats. In vitro studies have shown that the drug avidly binds to melanin (Perez et al, 1964), and there is considerable evidence that retinal toxicity is due to accumulation of the drug in the pigmented layers of the eye (Bernstein and Ginsberg, 1964). Why blanching of the hair and eyebrows (Dall and Keane, 1959) often accompanies retinal toxicity remains obscure. Retinal damage is a dosage phenomenon. On average 550 g are required before damage occurs, although patients have been reported who developed chloroquine retinopathy after much smaller doses (Scherbel et al, 1965). The incidence of the complication is difficult to assess from the literature, but varies from 0.1 to 15 per cent (von Sallman and Bernstein, 1963, Henkin and Rothfield, 1963). Presumably this wide divergence in incidence reflects different diagnostic criteria. Nevertheless, the complication is very serious since with few exceptions (Crews 1964) progressive blindness developes despite discontinuing therapy (Hobbs, Sorsby and Freedman, 1959). It is our belief that anti-malarials should be prescribed with the greatest caution, and probably not for longer than a year. Chrys otherapy There seems little doubt that gold salts exert a beneficial effect in rheumatoid arthritis (Fraser, 1945), Empire Rheumatism Council 1960 and 1961, Cooperative Clinics of the American Rheumatism Association, 1973, Sigler et al 1974 and Luukkainen et al, 1977). The study of Luukkainen et al (1977) is of particular interest since it suggests that progression of erosive changes may be delayed, but not, it should be noted, arrested completely. Jessop and Currey (1968) noted no benefit of gold in adjuvant arthritis in rats, although others have observed its benefit in mycoplasma arthritis in mice (Sabin and Warren, 1940). The main indication for gold therapy is failure of the patient to respond to non- steroidal anti-inflammatory drugs. The gold preparation used in the United Kingdom is sodium aurothiomalete (myocrisin). After weekly injections of small doses of 10 mg and 25 mg to avoid allergic reactions the patient is given weekly injections of 50 mg until a total of 500 mg has been given. After this injections can be given every 2 weeks until 1 g has been given. Thereafter monthly injections are given. The problem to-day is when to discontinue therapy, since relapse tends to occur. Toxic reactions are the most worrying aspect of gold therapy and require discontinuing therapy in about one third of patients. Gold is probably the most toxic preparation in the British Pharmacopoeia (Gerwood, 1973) and causes more deaths per prescription than any other drug. The highest incidence of toxicity occurs after 200 to 400 mg, and appears lower after 1 g (Jessop, 1972). Toxicity can be avoided by excluding patients with dermatitis, hepatic and renal disease. Gold dermatitis is often preceeded by pruritus and eosinophilia (Davis et al, 1973). In practice it is difficult often to know whether a rash is due to gold or not, but it is wise to err on the safe side and discontinue therapy if a rash, however mild, occurs. Gold is excreted in the urine and may give rise to renal damage (Strunk and Ziff 1970). Gold inclusions lying between the epithelial cells and the glomerular capillary wall basement membrane are often seen, but their role in causing proteinuria remains uncertain (Strunk and Ziff, 1970). What is certain, however, is that acute tubular necrosis may occur and is invariably fatal. A nephrotic syndrome may occur due to membranous glomerulonephritis (Vaamonde and Hunt, 1970), and surprisingly carries a good prognosis. A trace of proteinuria is not a contraindication for continuing treatment with gold, but a proteinuria of 30 mg per 100 ml or more certainly is (Jessop, 1972). Haematological complications often occur without warning. Eosinophilia if marked and persistent is a definite contraindication to continuing gold therapy. Persistent thrombocytopenia is often fatal, and pancytopenia and neutropenia also carry a high mortality despite D-penicillamine or dimercaptol therapy. Westwick and his 91

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