Abstract
One target of protective immunity against the Plasmodium liver stage in BALB/c mice is represented by the circumsporozoite protein (CSP), and mainly involves its recognition by IFN-γ producing specific CD8+T-cells. In a previous in vitro study we showed that primary hepatocytes from BALB/c mice process Plasmodium berghei (Pb) CSP (PbCSP) and present CSP-derived peptides to specific H-2kd restricted CD8+T-cells with subsequent killing of the presenting cells. We now extend these observations to an in vivo infection model in which infected hepatocytes and antigen specific T-cell clones are transferred into recipient mice inducing protection from sporozoite (SPZ) challenge. In addition, using a similar protocol, we suggest the capacity of hepatocytes in priming of naïve T-cells to provide protection, as further confirmed by induction of protection after depletion of cross-presenting dendritic cells (DCs) by cytochrome c (cyt c) treatment or using traversal deficient parasites. Our results clearly show that hepatocytes present Plasmodium CSP to specific-primed CD8+T-cells, and could also prime naïve T-cells, leading to protection from infection. These results could contribute to a better understanding of liver stage immune response and design of malaria vaccines.
Highlights
Immunization of rodents and humans with radiation- or genetically-attenuated sporozoites (SPZ) (RAS, GAS) confers preerythrocytic stage specific protective immunity to an infectious challenge [1,2]
Peptides Peptides PbCS245–253 (YIPSAEKI) and PbCS253–260 modified with iodo-azidosalicylic acid (IASA) and azidobenzoic acid (ABA) groups, (IASA)-YIPSAEK(ABA)I representing the epitope for C7 clone (H-2Kd-restricted and PbCSP specific CTL) and S14 (H2Kd-restricted and an irrelevant CTL), respectively [3,21], were synthesized by solid-phase F-moc chemistry
TAP 2/2 mice were selected to bypass the possibility that presentation could be performed by professional antigen presenting cells (APCs) through processing of apoptotic, infected hepatocytes or live SPZs possibly externally associated with BALB/c hepatocytes
Summary
Immunization of rodents and humans with radiation- or genetically-attenuated sporozoites (SPZ) (RAS, GAS) confers preerythrocytic stage specific protective immunity to an infectious challenge [1,2]. This protective immunity is mediated in part by CD8+ T-cells specific for the CSP and other not yet identified proteins [2,3,4,5]. The role of hepatocytes as antigen presenting cells (APCs) in the activation of primed T-cells to provide sterile protection seems to be accepted. The role of liver cells and, in particular, hepatocytes in the activation of Plasmodium-specific CD8+ T-cells is not clearly elucidated. While both pathways of antigen presentation co-exist, their role in providing a protective CD8+ T-
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