The American Journal of Tropical Medicine and Hygiene | 2019
Plasmodium malariae—Repeat Light Microscopy when Molecular Testing is Not Available
Abstract
A 31-year-old previously healthy male required hospital admission after returning from rural Cameroon 10 weeks prior with severe myalgia, chills, 72 hours cyclical fever to 103.1 F, and tachycardia for 2 weeks. He endorsed adherence to atovoquone/proguanil chemoprophylaxis and recalled no exposure to lake or stream water. He was ill appearing, but without focal abnormalities. Laboratory findings were significant for leukopenia 2,900 cells/uL, thrombocytopenia 82,000 cells/uL, aspartate aminotranferase 316 units/L, and alanine aminotransferase 400 units/L. Initial three light microscopy (LM) and rapid diagnostic test (RDT) with BinaxNOW (Alere, Inc., Waltham, MA) were negative. However, continued investigation eventually revealed Plasmodium malariae on the fourth LM in its pathognomonic “rosette” schizont (Figure 1) and “band”–developing gametocyte (Figure 2). The patient was treated effectively with artemether/lumefantrine. Plasmodium malariae infections were once considered a rare and mild illness largely because of poor sensitivity on RDT and LM. However, recent improvement in polymerase chain reaction (PCR) technique increased the identification of P. malariae that might have been misdiagnosed as fever of unknown origin. Although there were reports of late onset and recrudescent fever despite adherent chemoprophylaxis, subsequent treatment has been paradoxically successful with thesamemedication. BecauseofP.malariae’s longsenescent periods, recrudescent ability, and low parasite burden, clinicians musthavehighclinicalsuspicionandconsider repeatingLMwhen resource is limited or using PCR for diagnosis.