Cytokine Levels and T cell Apoptosis Associated With Cerebral Malaria Immunopathology During Plasmodium berghei Anka Infection In A Mouse Model
Abstract
During the course of malaria infection, a range of pro- and anti-inflammatory cytokines are
produced by the host immune system. Successful recovery from malaria involves striking a
balance between these counteracting cytokines. The cytokine imbalance contributes to
pathological features but their exact levels have not been elucidated. The present study aimed at
investigating the role played by circulating cytokines in pathophysiology of cerebral malaria.
Using an experimental cerebral malaria (ECM) model, the profile of five serum cytokines was
determined by employing Cytometric Bead Assay. Seventy-two BALB/c mice (7-9 week/old)
were intraperitoneally inoculated with approximately 1 x 105 parasitisized red blood cells at day
0 and randomized into six groups (six mice/group). Another set of noninfected mice was included
to serve as control. The mice were sacrificed at day 4, 6, 8, 11 and 20 pi. The possible role of
cytokines in inducing T-cell apoptosis associated with CM was investigated using the whole
genomic DNA extracted from splenic and brain lymphocytes. Significantly higher systemic levels
(P<0.05,) of IFN-γ (mean ±S.D 210.6±133, 169.8±80.5, 203.6±91.6, 22.0±3.5 pg/ml), were
observed between day 8 and 20 p.i while TNF-α levels were significant at days 4, 8 11, 14 and 20
respectively (M ±S.D 2.9 ± 0.2, 33.9±17.5, 95.5 ±17.0, 22.1±3.6 pg/ml) in BALB/c mice that
survived until day 20 pi with a higher parasitemia (up to 52.6%±0.8). Significant concentrations
(P< 0.05), of IL-4 (M ±S.D 14.6±2.5, 10.6±1.9, 9.6±1.3 pg/ml) were observed between day 4 and
8 respectively but afterwards its levels remained low throughout the course of infection. IL-5 levels
(M xix ±S.D 4.1±0.7, 3.4±1.6) had significant differences at day 11 and 20 pi. The study found
IL-4 to be elevated between days 11 and 20 respectively with no significant differences (P>0.05)
being reported. T-cell pathology was revealed by fragmentation of whole genomic DNA during
the infection which coincided with elevated systemic pro-inflammatory (IFN-γ and TNF-α at day
six) responses which further accelerated the severity of CM. The study demonstrated a parallel
link between T-cell pathology and elevated levels of Th1 cytokines concentrations in the brain and
the spleen. This study revealed that elevated levels of proinflammatory cytokines induce
inflammation and cellular apoptosis inhibiting parasite clearance. Thus, interventions to regulate
the Th1 cytokine responses may be beneficial in the prevention of severe CM. Further work is
needed on IL-2 IL-10 and IL-12 cytokines that could be involved in the pathology