ABSTRACT
The co-occurrence of malaria and schistosomiasis is common in tropical regions
of the world. Malaria induces a strong Th1 response while schistosomiasis skews
the response to a Th2. Several studies demonstrate a non consistent effect of
schistosomiasis infection on progression of malaria. On one hand, schistosomiasis
infections protect against cerebral malaria while on the other hand, they are
associated with increased malaria severity. This study examined the role of
Schistosoma mansoni eggs on Plasmodium berghei malaria progression in
BALB/c mice. The objectives were to determine the changes in Th1, Th2
cytokines and IgG levels which are markers associated with malaria and
schistosomiasis protection and also determine if S. mansoni eggs lead to
protection from P. berghei malaria. Two groups of mice were used: the
experimental group and the control group. The experimental group was injected
with a triple dose of S. mansoni eggs at ten day interval before being challenged
with P. berghei. The control group was infected with P. berghei only. Five mice
from both groups were euthanized at each time point (day 3, 6, 9 and 12 post
challenge with P. berghei) and the spleen and serum collected. Five mice from
each group were monitored throughout the experiment. Parasitaemia was
monitored daily using Giemsa stained blood smears. The results showed that the
experimental mice exhibited lower levels of P. berghei parasitaemia (15.52%) as
compared to the controls (23.06%). However the difference was not significant
(p>0.05). IgG levels were found to be higher in the experimental mice compared
to controls due to stimulation by soluble egg antigen (SEA). The differences in
IgG levels between the two study groups was not significant (p>0.05). The levels
of IFN- γ and IL-4 were higher in the experimental mice than the control group
though the difference was not significant (p=0.213). The levels of IgG and IL-4 in
experimental mice could be responsible for the delay in death reported in these
mice and enhanced survivorship. In conclusion, S. mansoni eggs did not induce
significant differences in cytokine and IgG levels; nevertheless they contributed to
delaying death in the experimental mice by two days by enhancing levels of IgG
and IL-4. These findings provide a pointer for further research in this field using
higher animal model such as the non human primates for a better understanding of
the immunomodulatory role of schistosoma eggs on progression of malaria.
DONALD, N (2021). The Role Of Schistosoma Mansoni Eggs In Immune Protection Against Plasmodium Berghei Infected Mice. Afribary. Retrieved from https://afribary.com/works/the-role-of-schistosoma-mansoni-eggs-in-immune-protection-against-plasmodium-berghei-infected-mice
DONALD, NYANGAHU "The Role Of Schistosoma Mansoni Eggs In Immune Protection Against Plasmodium Berghei Infected Mice" Afribary. Afribary, 27 May. 2021, https://afribary.com/works/the-role-of-schistosoma-mansoni-eggs-in-immune-protection-against-plasmodium-berghei-infected-mice. Accessed 23 Dec. 2024.
DONALD, NYANGAHU . "The Role Of Schistosoma Mansoni Eggs In Immune Protection Against Plasmodium Berghei Infected Mice". Afribary, Afribary, 27 May. 2021. Web. 23 Dec. 2024. < https://afribary.com/works/the-role-of-schistosoma-mansoni-eggs-in-immune-protection-against-plasmodium-berghei-infected-mice >.
DONALD, NYANGAHU . "The Role Of Schistosoma Mansoni Eggs In Immune Protection Against Plasmodium Berghei Infected Mice" Afribary (2021). Accessed December 23, 2024. https://afribary.com/works/the-role-of-schistosoma-mansoni-eggs-in-immune-protection-against-plasmodium-berghei-infected-mice