Low Prevalence of Antibodies to Preerythrocytic but Not Blood-Stage Plasmodium falciparum Antigens in an Area of Unstable Malaria Transmission Compared to Prevalence in an Area of Stable Malaria Transmission

doi:10.1128/IAI.00591-08

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Infection and Immunity, December 2008, p. 5721-5728, Vol. 76, No. 12
0019-9567/08/$08.00+0 doi:10.1128/IAI.00591-08
Copyright © 2008, American Society for Microbiology. All Rights Reserved.

Low Prevalence of Antibodies to Preerythrocytic but Not Blood-Stage Plasmodium falciparum Antigens in an Area of Unstable Malaria Transmission Compared to Prevalence in an Area of Stable Malaria Transmission

Gregory S. Noland,¹ Brett Hendel-Paterson,¹ Xinan M. Min,¹ Ann M. Moormann,² John M. Vulule,³ David L. Narum,⁴ David E. Lanar,⁵ James W. Kazura,² and Chandy C. John¹^*

University of Minnesota, Minneapolis, Minnesota,¹ Case Western Reserve University, Cleveland, Ohio,² Kenya Medical Research Institute, Kisumu, Kenya,³ National Institutes of Health, Bethesda, Maryland,⁴ Walter Reed Army Institute for Research, Silver Spring, Maryland⁵

Received 13 May 2008/ Returned for modification 26 August 2008/ Accepted 12 September 2008

In areas where levels of transmission of Plasmodium falciparumare high and stable, the age-related acquisition of high-levelimmunoglobulin G (IgG) antibodies to preerythrocytic circumsporozoiteprotein (CSP) and liver-stage antigen 1 (LSA-1) has been associatedwith protection from clinical malaria. In contrast, age-relatedprotection from malaria develops slowly or not at all in residentsof epidemic-prone areas with unstable low levels of malariatransmission. We hypothesized that this suboptimal clinicaland parasitological immunity may in part be due to reduced antibodiesto CSP or LSA-1 and/or vaccine candidate blood-stage antigens.Frequencies and levels of IgG antibodies to CSP, LSA-1, thrombospondin-relatedadhesive protein (TRAP), apical membrane antigen 1 (AMA-1),erythrocyte binding antigen 175 (EBA-175), and merozoite surfaceprotein 1 (MSP-1) were compared in 243 Kenyans living in a highlandarea of unstable transmission and 210 residents of a nearbylowland area of stable transmission. Levels of antibodies toCSP, LSA-1, TRAP, and AMA-1 in the oldest age group (>40years) in the unstable transmission area were lower than orsimilar to those of children 2 to 6 years old in the stabletransmission area. Only 3.3% of individuals in the unstabletransmission area had high levels of IgG (>2 arbitrary units)to both CSP and LSA-1, compared to 43.3% of individuals in thestable transmission area. In contrast, antibody levels to andfrequencies of MSP-1 and EBA-175 were similar in adults in areasof stable and unstable malaria transmission. Suboptimal immunityto malaria in areas of unstable malaria transmission may relatein part to infrequent high-level antibodies to preerythrocyticantigens and AMA-1.

* Corresponding author. Mailing address: University of Minnesota Department of Pediatrics, 717 Delaware St., SE, Room 363, MC1932, Minneapolis, MN 55455. Phone: (612) 625-8383. Fax: (612) 625-2920. E-mail: ccj{at}umn.edu

Published ahead of print on 22 September 2008.

Editor: W. A. Petri, Jr.