AI Article Synopsis

  • Humoral immune responses are crucial for immunity against malaria, and understanding impairments in these responses can aid in vaccine development.
  • The study compared immune responses to 483 malaria antigens between adults in two regions with differing malaria transmission levels, finding significant differences in reactivity in those with higher transmission.
  • Using protein microarrays, researchers identified several reactive antigens and noted that reductions in CD4(+) T-cell counts did not greatly affect malaria-specific immunity, indicating potential vaccine targets.

Article Abstract

Introduction: Humoral immune responses play a pivotal role in naturally acquired immunity to malaria. Understanding which humoral responses are impaired among individuals at higher risk for malaria may improve our understanding of malaria immune control and contribute to vaccine development.

Methods: We compared humoral responses with 483 Plasmodium falciparum antigens between adults in, Kisumu (high, year-long malaria transmission leading to partial immunity), and adults in Kisii (low, seasonal malaria transmission). Then within each site, we compared malaria-specific humoral responses between those at higher risk for malaria (CD4(+) ≤500) and those at lower risk for malaria (CD4(+) >500). A protein microarray chip containing 483 P. falciparum antigens and 71 HIV antigens was used. Benjamini-Hochberg adjustments were made to control for multiple comparisons.

Results: Fifty-seven antigens including CSP, MSP1, LSA1 and AMA1 were identified as significantly more reactive in Kisumu than in Kisii. Ten of these antigens had been identified as protective in an earlier study. CD4(+) T-cell count did not significantly impact humoral responses.

Conclusion: Protein microarrays are a useful method to screen multiple humoral responses simultaneously. This study provides useful clues for potential vaccine candidates. Modest decreases in CD4 counts may not significantly impact malaria-specific humoral immunity.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3406934PMC
http://dx.doi.org/10.1002/prca.201100021DOI Listing

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