Temporal stability of naturally acquired immunity to Merozoite Surface Protein-1 in Kenyan Adults

doi:10.1186/1475-2875-8-162

Malaria Journal

Volume 8

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Dent AE
Chelimo K
Sumba PO
Spring MD
Crabb BS
Moormann AM
Tisch DJ
Kazura JW

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Chelimo K
Sumba PO
Spring MD
Crabb BS
Moormann AM
Tisch DJ
Kazura JW
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Research

Temporal stability of naturally acquired immunity to Merozoite Surface Protein-1 in Kenyan Adults

Arlene E Dent¹ , Kiprotich Chelimo² , Peter O Sumba² , Michele D Spring³ , Brendan S Crabb⁴ , Ann M Moormann¹ , Daniel J Tisch¹ and James W Kazura¹

¹Case Western Reserve University, Cleveland, OH, USA

²Kenya Medical Research Institute, Kisumu, Kenya

³Walter Reed Army Institute of Research, Silver Spring, MD, USA

⁴Burnet Institute of Medical Research, Melbourne, Australia

author email corresponding author email

Malaria Journal 2009, 8:162doi:10.1186/1475-2875-8-162


Published:	16 July 2009

Abstract

Background

Naturally acquired immunity to blood-stage Plasmodium falciparum infection develops with age and after repeated infections. In order to identify immune surrogates that can inform vaccine trials conducted in malaria endemic populations and to better understand the basis of naturally acquired immunity it is important to appreciate the temporal stability of cellular and humoral immune responses to malaria antigens.

Methods

Blood samples from 16 adults living in a malaria holoendemic region of western Kenya were obtained at six time points over the course of 9 months. T cell immunity to the 42 kDa C-terminal fragment of Merozoite Surface Protein-1 (MSP-1₄₂) was determined by IFN-γ ELISPOT. Antibodies to the 42 kDa and 19 kDa C-terminal fragments of MSP-1 were determined by serology and by functional assays that measure MSP-1₁₉invasion inhibition antibodies (IIA) to the E-TSR (3D7) allele and growth inhibitory activity (GIA). The haplotype of MSP-1₁₉alleles circulating in the population was determined by PCR. The kappa test of agreement was used to determine stability of immunity over the specified time intervals of 3 weeks, 6 weeks, 6 months, and 9 months.

Results

MSP-1 IgG antibodies determined by serology were most consistent over time, followed by MSP-1 specific T cell IFN-γ responses and GIA. MSP-1₁₉IIA showed the least stability over time. However, the level of MSP-1₁₉specific IIA correlated with relatively higher rainfall and higher prevalence of P. falciparum infection with the MSP-1₁₉E-TSR haplotype.

Conclusion

Variation in the stability of cellular and humoral immune responses to P. falciparum blood stage antigens needs to be considered when interpreting the significance of these measurements as immune endpoints in residents of malaria endemic regions.