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dc.contributor.authorRamutton, Thiranut
dc.contributor.authorHendriksen, Ilse CE
dc.contributor.authorMwanga-Amumpaire, Juliet
dc.contributor.authorMtove, George
dc.contributor.authorOlaosebikan, Rasaq
dc.contributor.authorTshefu, Antoinette K
dc.contributor.authorOnyamboko, Marie A
dc.contributor.authorKarema, Corine
dc.contributor.authorMaitland, Kathryn
dc.contributor.authorGomes, Ermelinda
dc.contributor.authorGesase, Samwel
dc.contributor.authorReyburn, Hugh
dc.contributor.authorSilamut, Kamolrat
dc.contributor.authorChotivanich, Kesinee
dc.contributor.authorPromnares, Kamoltip
dc.contributor.authorFanello, Caterina I
dc.contributor.authorSeidlein, Lorenz von
dc.contributor.authorDay, Nicholas PJ
dc.contributor.authorWhite, Nicholas J
dc.contributor.authorDondorp, Arjen M
dc.contributor.authorImwong, Mallika
dc.contributor.authorWoodrow, Charles J
dc.date.accessioned2024-06-06T09:28:58Z
dc.date.available2024-06-06T09:28:58Z
dc.date.issued2012
dc.identifier.citationRamutton, T., Hendriksen, I. C., Mwanga-Amumpaire, J., Mtove, G., Olaosebikan, R., Tshefu, A. K., ... & Woodrow, C. J. (2012). Sequence variation does not confound the measurement of plasma PfHRP2 concentration in African children presenting with severe malaria. Malaria journal, 11, 1-7.en_US
dc.identifier.urihttp://ir.must.ac.ug/xmlui/handle/123456789/3713
dc.description.abstractBackground: Plasmodium falciparum histidine-rich protein PFHRP2 measurement is used widely for diagnosis, and more recently for severity assessment in falciparum malaria. The Pfhrp2 gene is highly polymorphic, with deletion of the entire gene reported in both laboratory and field isolates. These issues potentially confound the interpretation of PFHRP2 measurements. Methods: Studies designed to detect deletion of Pfhrp2 and its paralog Pfhrp3 were undertaken with samples from patients in seven countries contributing to the largest hospital-based severe malaria trial (AQUAMAT). The quantitative relationship between sequence polymorphism and PFHRP2 plasma concentration was examined in samples from selected sites in Mozambique and Tanzania. Results: There was no evidence for deletion of either Pfhrp2 or Pfhrp3 in the 77 samples with lowest PFHRP2 plasma concentrations across the seven countries. Pfhrp2 sequence diversity was very high with no haplotypes shared among 66 samples sequenced. There was no correlation between Pfhrp2 sequence length or repeat type and PFHRP2 plasma concentration. Conclusions: These findings indicate that sequence polymorphism is not a significant cause of variation in PFHRP2 concentration in plasma samples from African children. This justifies the further development of plasma PFHRP2 concentration as a method for assessing African children who may have severe falciparum malaria. The data also add to the existing evidence base supporting the use of rapid diagnostic tests based on PFHRP2 detection.en_US
dc.description.sponsorshipWellcome Trust of Gareat Britain.en_US
dc.language.isoen_USen_US
dc.publisherMalaria journalen_US
dc.subjectMalariaen_US
dc.subjectFalciparumen_US
dc.subjectSevereen_US
dc.subjectAfricaen_US
dc.subjectHistidine-rich proteinen_US
dc.subjectTandem repeaten_US
dc.titleSequence variation does not confound the measurement of plasma PfHRP2 concentration in African children presenting with severe malariaen_US
dc.typeArticleen_US


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