Acute phase proteins as markers of systemic illness in acute diarrhoea

Fifty-seven Tanzanian children, 6-25 months, hospitalized with acute diarrh oea were grouped according to whether there was clinical evidence-of system ic infection (Sr) (n=35) or not (n=22). Serum acute phase proteins were mea sured in samples taken within 48 h of admission. Means for C-reactive prote in (CRP) and serum amyloid A (SAA) were significantly higher in children wi th SI compared to those without (geometric means (95% CI); CRP, mg/l: 22.1 (13.6-35.5) vs 7.4 (4.4-12.4); SAA, mg/l: 12.2 (6.8-22.1) vs 4.9 (2.5-9.7)) . Levels of al-acid glycoprotein were similar in both groups (1.16 g/l (0.9 5-1.43) vs 1.04 (0.83-1.29), respectively). CRP greater than or equal to 30 mg/l had a positive predictive value of 95%, and specificity of 96% for co rrectly identifying SI, but a low sensitivity (51%) and negative predictive value (55%). Clinical outcome of diarrhoea was worse in children with SI: more needed intravenous fluids (23% vs 5%), the duration of diarrhoea was l onger (59.4 vs 34.2 h) and mortality was higher (6% vs 0%). APPs were not f ound to be useful markers of systemic illness in acute diarrhoea in this po pulation.