Gene/Protein
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Pivot Concepts:
Gene/Protein
Disease
Symptom
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Target Concepts:
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Query: UMLS:C0024530 (
malaria
)
44,886
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
The immunogenicity of the synthetic
malaria
vaccine SPf66 has been recently improved by the application of new adjuvants as QS-21 saponin or poly-D,L-lactide-co-glycolide (PLGA) polymers. The search for less invasive administration routes made us test the immunogenicity of SPf66-loaded microparticles by the nasal route in Balb/c mice. We report here that the intranasal administration of the adequate PLGA vaccine formulations greatly improves and maintains higher antibody levels compared to the conventional alum adjuvant and to the administration of the particles by other routes (subcutaneous, oral). Systemic immune responses were characterized as mixed Th1/Th2-type: IFN-gamma and IgG2a isotype were found as signs of Th1 activation, whilst
IgE
and IgG1 secretions indicate Th2 response. Since both types of response have been associated to protective immunity in
malaria
, we postulate that this new approach supposes an advantage over the traditional adjuvants and routes.
...
PMID:Potent, long lasting systemic antibody levels and mixed Th1/Th2 immune response after nasal immunization with malaria antigen loaded PLGA microparticles. 1506 65
Helminths are the most prevalent parasitic infections and
malaria
is the deadliest parasitic disease. Helminths have been reported to be protective against the severe forms of
malaria
but they were also possibly linked to increased
malaria
-incidence and gametocyte carriage. Connecting the dots between observations suggests that statistical regularities throughout the evolution of worms and
malaria
parasites in the same hosts, may have led to the emergence of non-zero interactions as observed in iterated prisoners dilemma games. Thus by protecting the host, helminths protect themselves and their reproductive potential, but also favor the dissemination and reproduction of Plasmodium falciparum. The proximate causes of this evolutionarily stable strategy might be mediated by
IgE
and the CD23/NO pathway, the protective role of IL10 in helminth-infected patients, and possibly the hematological consequences of worms. The chronic activation of the CD23/NO pathway might be instrumental in downregulating the expression of cytoadherence receptors thus reducing sequestration of parasitized red blood cells in the deep organs. Mild anemia in helminth-infected patients might favor gametocytogenesis and send attractive cues to the vector. This framework leads to numerous testable hypotheses and could explain certain singularities regarding the double edged role of
IgE
and NO. Among these hypotheses, there are 2 practical ones: the impact of helminths on
malaria
vaccine candidates, and the theoretical risk of increasing the severity of
malaria
after anthelmintics. The capacity for increased
IgE
responses could thus have been vital in our ancestor's wormy and malarious past. Allergies may be what remains of it in the modern world.
...
PMID:Interactions between worm infections and malaria. 1514 5
Previous studies identified an allelic variant of the IL4 promoter region (IL4-589T) that appears to enhance the transcriptional activity of IL4, and is associated with increased
IgE
levels. Total serum
IgE
levels are elevated in
malaria
endemic regions, and higher in children with severe
malaria
. Here, we investigated the relationship of the IL4-589C/T polymorphism with severity of the disease in a case-control study of severe
malaria
in Burkina Faso, West Africa. No association between the IL4-589T and severe
malaria
was observed. No difference in Plasmodium falciparum-specific
IgE
was detected between severe and uncomplicated
malaria
patients. Among children with severe
malaria
, total
IgE
levels were significantly elevated in those carrying the IL4-589T allele (P = 0.018). In children with uncomplicated
malaria
, no significant difference was found. These results raise the possibility that there is a relationship between susceptibility to severe
malaria
,
IgE
production and genetic variation in the IL4 region, which merits further investigation in other epidemiological settings.
...
PMID:IL4-589C/T polymorphism and IgE levels in severe malaria. 1517 47
Immunological characteristics were assessed for prospective risk of clinical
malaria
in a longitudinally followed population in a holoendemic area of Tanzania. Baseline characteristics including crude Plasmodium falciparum extract-specific
IgE
and IgG; total
IgE
; and parasitological indices, e.g. number of P. falciparum clones, were investigated among 700 asymptomatic individuals. Cox regression analysis estimated the risk of succumbing to a new clinical episode during a 40 weeks follow up. High anti-P. falciparum
IgE
levels were associated with reduced risk of acute
malaria
in all age groups independently of total
IgE
levels. Statistically significant reduced odds ratio of 0.26 (95% CI, 0.09-0.72, P=0.010) and 0.44 (95% CI, 0.19-0.99, P=0.047) for the two highest fifths, respectively was observed after adjustment for age, sex, total
IgE
, numbers of parasite clones per infection and HIV-1 seropositivity. In contrast, high levels of
malaria
specific IgG or total
IgE
were not associated with reduced risk to succumb to a new clinical episode. A protective effect of asymptomatic multiclonal P. falciparum infections was also confirmed. For the first time, anti-malarial
IgE
levels in asymptomatic individuals in endemic area are found to be associated with reduced risk for subsequent
malaria
disease. Specific
IgE
antibodies may play role in maintaining anti-malarial immunity, or indicate other aspects of immune function relevant for protection against
malaria
.
...
PMID:Elevated anti-malarial IgE in asymptomatic individuals is associated with reduced risk for subsequent clinical malaria. 1521 32
The epidemiological coexistence of schistosomiasis and
malaria
is frequently observed in developing countries. Co-infection with
malaria
in children could influence the development of acquired immunity associated with the resistance or the pathology of schistosomiasis. In the present study, performed during May to June 1996 in Senegal, the humoral immune response to Schistosoma haematobium 28 kDa glutathione S-transferase (Sh28GST) vaccinal antigen and to soluble egg antigens (SEA) has been evaluated in individuals infected by S. haematobium. Specific immunoglobulin G3 (IgG3) and
IgE
responses were significantly higher in co-infected children with Plasmodium falciparum compared with children infected with S. haematobium only. In addition, circulating levels of interferon-gamma (IFN-gamma), interleukin-10 (IL-10), and soluble tumor necrosis factor receptor II (sTNF-RII), 3 parameters associated with schistosomiasis morbidity, were significantly increased in co-infected children. Taken together, this study indicated that
malaria
co-infection can both influence the acquired specific immune response to schistosome antigens and unbalance the regulation of inflammatory factors closely involved in schistosomiasis pathology.
...
PMID:Malaria co-infection in children influences antibody response to schistosome antigens and inflammatory markers associated with morbidity. 1522 60
Cytoadherence of parasitized red blood cells (PRBCs) to postcapillary venules and cytokine production are clearly involved in the pathogenesis of cerebral
malaria
. Nitric oxide and TNF-alpha have been proposed as major effector molecules both in protective and physiopathological processes during
malaria
infections. Nitric oxide production has been shown to be induced by engagement of CD23 antigen. This study aimed to investigate the potential role of the CD23/nitric oxide pathway in the control of the cytoadherence of PRBCs on human endothelial cells. We demonstrate that normal human lung endothelial cells (HLECs) are able to express the low affinity receptor for
IgE
(Fc in RII/CD23), following cell incubation with interleukin 4 or PRBCs. Ligation of the CD23 antigen by a specific anti-CD23 monoclonal antibody at the cell surface of HLECs was found to induce iNOS mRNA and protein expression, NO release and P. falciparum killing. In addition, the specific CD23-engagement on these cells also induced a significant decrease in ICAM-1 expression, an adhesion molecule implicated in PRBCs cytoadherence. These data not only described for the first time the expression of a CD23 antigen at the cell surface of endothelial cells but also suggest a possible new regulatory mechanisms via the CD23/NO pathway during
malaria
infection.
...
PMID:Induction of the CD23/nitric oxide pathway in endothelial cells downregulates ICAM-1 expression and decreases cytoadherence of Plasmodium falciparum-infected erythrocytes. 1527 65
Immunoglobulin E has been associated with severe
malaria
suggesting a regulatory role for interleukin (IL)-4 and/or
IgE
in the pathogenesis of severe
malaria
. We have investigated possible associations between polymorphisms in the IL-4 repeat region (intron 3) and promoter regions (IL-4 +33CT and - 590CT) in Ghanaian children with severe
malaria
. There was a significantly higher frequency of IL-4 intron-3 B1B1 genotype in the cerebral
malaria
group [P < 0.0001, odds ratio (OR) = 8.7]. The genotype and allele frequencies of the IL-4 -590 and +33 polymorphisms did not differ between the four study groups. Carriers of IL-4 +33T/-590T with cerebral
malaria
had elevated total
IgE
compared to non-carriers (P = 0.03). Our data suggest that IL-4 and/or
IgE
play a regulatory role in the pathogenesis of severe or complicated
malaria
.
...
PMID:Allelic polymorphisms in the repeat and promoter regions of the interleukin-4 gene and malaria severity in Ghanaian children. 1537 17
The Fulani are known to be less susceptible to Plasmodium falciparum malaria infections and to have lower parasitaemia despite living under similar
malaria
transmission intensity compared with other ethnic tribes. The aim of the present study was to examine whether the Fulani were more polarised towards Th2 as reflected by higher numbers of
malaria
-specific IL-4- and IL-10-producing cells and lower numbers of IFN-gamma- and IL-12-producing cells as compared to their neighbour ethnic tribe, the Dogon of Mali. Total
IgE
and both anti-
malaria
IgE
and IgG antibodies were measured by ELISA and the numbers of IL-4-, IFN-gamma-, IL-10- and IL-12-producing cells were enumerated using enzyme-linked ImmunoSpot assay (ELISPOT). Numbers of parasite clones were detected by polymerase chain reaction (PCR). The study was performed outside the transmission period and all individuals included were asymptomatic. The results revealed that the Fulani were less parasitised, had fewer circulating parasite clones in their blood, had significantly higher anti-
malaria
IgG and
IgE
antibodies and higher proportions of
malaria
-specific IL-4- and IFN-gamma-producing cells compared to the Dogon. The higher antigen-specific production of IL-4 among the Fulani was statistically significant both before and after adjustment for level of spontaneous cytokine production, while greater IFN-gamma production only attained statistical significance after adjustment for spontaneous levels. Taken together, the association of higher anti-malarial
IgE
and IgG antibodies and increased numbers of specific IL-4- and IFN-gamma-producing cells compared to the ethnic sympatric tribe, the Dogon, may assist in explaining the lower susceptibility to
malaria
observed in the Fulani.
...
PMID:Different antibody- and cytokine-mediated responses to Plasmodium falciparum parasite in two sympatric ethnic tribes living in Mali. 1571 67
We compared
malaria
indicators among sympatric groups to study human heterogeneities in the response to Plasmodium falciparum malaria infection. Four cross-sectional surveys and two longitudinal surveys in two sympatric ethnic groups (Dogon and Fulani) in Mali were carried out from 1998 to 2000. Spleen and parasite rates were evaluated during the cross-sectional surveys and disease incidence was assessed during longitudinal surveys. In spite of similar sociocultural factors and entomologic inoculation rates between ethnic groups, the Fulani had a significantly higher spleen enlargement rate, lower parasite rate, and were less affected by the disease than the Dogon group, whose frequency of hemoglobin C was higher than that recorded among the Fulani group. The Fulani group had significantly higher levels of IgG and
IgE
against crude
malaria
antigen than the Dogon group, suggesting a role of anti-
malaria
antibodies in the immune protection seen in this group.
...
PMID:Difference in susceptibility to malaria between two sympatric ethnic groups in Mali. 1577 14
We have shown previously that numerous
IgE
(+) macrophage-like cells are present in the villous stroma of full term placenta and that there was no difference in the amount of
IgE
(+) cells between allergic and non-allergic mothers. The presence of such an abundant number of
IgE
(+) cells in the placenta in allergic as well as non-allergic women suggests that the
IgE
is of some importance for a successful pregnancy outcome. Here we have investigated the
IgE
-pattern in 59 placentas from second and third trimesters from Sweden with different degrees of chorioamnionitis and 27 full term placentas from Ghana with and without
malaria
parasites. The immunohistochemical staining pattern for
IgE
looked similar to our previous study, with the
IgE
located on Hofbauer-like cells. We could not find any difference in the amount or distribution of
IgE
(+) cells between
malaria
-infected and non-infected placentas, nor between different degrees of chorioamnionitis. The
IgE
score in the placenta did not correlate with the levels of
IgE
in maternal serum or plasma. However, the
IgE
score was significantly higher in second- compared to third-trimester placentas (P = 0.03). This might reflect a maturation time-point in the fetus and in the intrauterine environment during the second trimester, or it might be associated with the increased number of intrauterine fetal deaths in the second trimester.
...
PMID:Presence of IgE cells in human placenta is independent of malaria infection or chorioamnionitis. 1663 92
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