Summary Malaria in malaria‐naïve adults is associated with an inflammatory response characterized by expression of specific activation markers on innate immune cells. Here, we investigate activation and adhesion marker expression, and cytokine production in monocytes from children presenting with cerebral malaria ( CM , n = 36), severe malarial anaemia ( SMA , n = 42) or uncomplicated malaria ( UM , n = 66), and healthy aparasitemic children ( n = 52) in Blantyre, Malawi. In all malaria groups, but particularly in the two severe malaria groups, monocyte expression of CD 11b, CD 11c, CD 18, HLA ‐ DR and CD 86, and percentages of TNF ‐α‐ and IL ‐6‐producing monocytes were lower than in healthy controls, while expression of CD 11a, TLR 2 and TLR 4 was lower in children with severe malaria compared with controls. These levels mostly normalized during convalescence, but percentages of cytokine‐producing monocytes remained suppressed in children with SMA . In all malaria groups, especially the SMA group, a greater proportion of monocytes were loaded with haemozoin than among controls. In a P. falciparum hyperendemic area, monocytes in children with acute symptomatic malaria have reduced expression of adhesion molecules and activation markers and reduced inflammatory cytokine production. This immune suppression could be due to accumulation of haemozoin and/or previous exposure to P. falciparum .
【저자키워드】 Monocytes, Integrins, toll‐like receptors and cytokines,