| Literature DB >> 26830671 |
James A Church1,2, Lydia Nyamako3, Peter Olupot-Olupot4,5, Kathryn Maitland6,7, Britta C Urban8,9.
Abstract
BACKGROUND: Children with severe malaria are at increased risk of invasive bacterial disease particularly infection with enteric gram-negative organisms. These organisms are likely to originate from the gut, however, how and why they breach the intestinal interface in the context of malaria infection remains unclear. One explanation is that accumulation of infected red blood cells (iRBCs) in the intestinal microvasculature contributes to tissue damage and subsequent microbial translocation which can be addressed through investigation of the impact of cytoadhesion in patients with malaria and intestinal damage.Entities:
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Year: 2016 PMID: 26830671 PMCID: PMC4736236 DOI: 10.1186/s12936-016-1110-3
Source DB: PubMed Journal: Malar J ISSN: 1475-2875 Impact factor: 2.979
Baseline group characteristics
| Children with parasite adhesion data | Children without parasite adhesion data | |
|---|---|---|
| Number of children | 48 | 61 |
| Median age (months) | 25.5 (12–40) | 26 (15–44) |
| Median haemoglobin | 6.5 (4.3–9.5) | 5.9 (3.8–9.3) |
| Severe malaria | 38 (79.2 %) | 49 (80.3 %) |
| Impaired consciousness | 22 (45.8 %) | 25 (37.3 %) |
| Coma | 4 (8.3 %) | 4 (6.5 %) |
| Severe anaemia | 18 (37.5 %) | 27 (44 %) |
| Respiratory distress | 37 (77 %) | 43 (70.5 %) |
| Endotoxemia (EAA ≥ 0.4 U) | 16 (33 %) | 31 (50.8 %) |
| I-FABP ≥183 pg/ml | 10 (20.8 %) | 12 (19.6 %) |
Fig. 1Adhesion of iRBC in children with impaired consciousness or anaemia. Shown are dot plots of the number of iRBCs/mm2 binding to CD36, ICAM-1 or the percentage of iRBCs in rosettes with RBCs in children with (plus) or without (minus) impaired consciousness (prostration or coma) and in children with (plus) or without (minus) anaemia (Hb ≤ 7). Median and interquartile range are indicated, * denotes p value of <0.05 (Mann–Whitney U test)
Fig. 2Adhesion of iRBC in children with endotoxemia or increased plasma concentrations of I-FABP. Shown are dot plots of the number of iRBCs/mm2 binding to CD36, ICAM-1 or the percentage of iRBCs in rosettes with RBCs in children with (plus) or without (minus) endotoxemia and in children with (plus) or without (minus) increased plasma concentrations of I-FABP (I-FABP ≥ 183 ng/ml) indicating acute enterocyte damage. Median ans interquartile range are indicated, * denotes p value of <0.05 (Mann–Whitney U test)
Fig. 3Correlation between iRBC adhesion to ICAM-1 and the plasma concentration of TNF. Shown is a scatter plot of iRBCs/mm2 binding to ICAM1 and the plasma concentration of TNF (pg/ml). Values from children with increased plasma concentration of I-FABP (I-FABP ≥ 183 ng/ml) are indicated by an open circle and values of children with a plasma concentration below pathological levels (I-FABP < 183 ng/ml) are indicated by black circles