Towards Clinical Applications of Anti-endotoxin Antibodies;  A Re-appraisal of the Disconnect

Hurley, James C.

doi:10.3390/toxins5122589

Cited by 25 publications

(24 citation statements)

References 173 publications

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“…The effectiveness of heat treatment was confirmed by inclusion of a control sample of plasma spiked with a 0·2 EU mL −1 final concentration of endotoxin standard. Because previous literature on endotoxaemia in HAT have presented endotoxin concentrations as lipopolysaccharide (LPS) equivalents, endotoxin concentrations were expressed as pg mL −1 LPS using the conversion 1 EU mL −1 = 100 pg mL −1 (Hurley, 2013). …”

Section: Methodsmentioning

confidence: 99%

The relationship of endotoxaemia to peripheral and central nervous system inflammatory responses in Human African Trypanosomiasis

et al. 2016

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SUMMARYEndotoxaemia has been described in cases of Human African trypanosomiasis (HAT), but it is unclear if this phenomenon influences inflammatory pathology either in the periphery or central nervous system (CNS). We studied endotoxin concentrations in the plasma and cerebrospinal fluid (CSF) of Trypanosoma brucei rhodesiense patients using the chromogenic Limulus Amoebocyte lysate assay. The relationship of endotoxin concentration to the presentation of gross signs of inflammation and the inflammatory/counter-inflammatory cytokine profile of the relevant compartments were analysed. We demonstrate that HAT patients exhibit parasitaemia-independent plasma endotoxaemia, and that this is associated with splenomegaly and lymphadenopathy. Endotoxin concentrations normalize rapidly after treatment. There was no evidence of endotoxin release in the CNS. A rapid normalization of endotoxin levels after treatment and lack of association with parasitaemia suggest that gut leakage is the main source of endotoxin in the circulation. Low CSF endotoxin concentrations and a lack of any association with neuroinflammatory markers or neurological sequelae suggest that endotoxin does not play a role in the pathogenesis of the disease in the CNS.

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Section: Methodsmentioning

confidence: 99%

The relationship of endotoxaemia to peripheral and central nervous system inflammatory responses in Human African Trypanosomiasis

et al. 2016

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“…In comparative studies with this model, a relatively avirulent strain of E. coli versus P. aeruginosa (48), Staphylococcus aureus (66), or a more virulent strain of E. coli (65) showed similar quantitative levels of bacteremia, whereas the associated hemodynamic changes and shortened survival times were in each case more severe than those observed in association with the avirulent E. coli strain, as would be expected (48,65,66). Surprisingly, despite these expected differences, in each study the levels of endotoxemia were 3-fold (65) to 10-fold (48) lower or even undetectable (46) versus the levels seen after challenge with the avirulent E. coli strain. Interestingly, endotoxins extracted and purified from the virulent and avirulent E. coli strains were equal with respect to potency and endotoxin amount per bacterium; hence, the lack of an association between endotoxemia and disease severity in this experimental model could not be explained on this basis (65).…”

Section: Figmentioning

confidence: 66%

“…Third, paradoxical observations among animal models of sepsis indicate that the concordance of endotoxemia with GN bacteremia and also with outcome is expected to differ for different GN bacteremia types (48). The detection of endotoxemia is of interest in relation to ongoing efforts to develop rapid detection methods for GN bacteremia and the possible application of emerging endotoxemia therapies (46). Finally, newer statistical methods have enabled a reappraisal over a broad range of assay breakpoints (49).…”

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confidence: 99%

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Endotoxemia as a Diagnostic Tool for Patients with Suspected Bacteremia Caused by Gram-Negative Organisms: a Meta-Analysis of 4 Decades of Studies

et al. 2015

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The clinical significance of endotoxin detection in blood has been evaluated for a broad range of patient groups in over 40 studies published over 4 decades. The influences of Gram-negative (GN) bacteremia species type and patient inclusion criteria on endotoxemia detection rates in published studies remain unclear. Studies were identified after a literature search and manual reviews of article bibliographies, together with a direct approach to authors of potentially eligible studies for data clarifications. The concordance between GN bacteremia and endotoxemia expressed as the summary diagnostic odds ratios (DORs) was derived for three GN bacteremia categories across eligible studies by using a hierarchical summary receiver operating characteristic (HSROC) method. Forty-two studies met broad inclusion criteria, with between 2 and 173 GN bacteremias in each study. Among all 42 studies, the DORs (95% confidence interval) were 3.2 (1.7 to 6.0) and 5.8 (2.4 to 13.7) in association with GN bacteremias with Escherichia coli and those with Pseudomonas aeruginosa, respectively. Among 12 studies of patients with sepsis, the proportion of endotoxemia positivity (95% confidence interval) among patients with P. aeruginosa bacteremia (69% [57 to 79%]; P ‫؍‬ 0.004) or with Proteus bacteremia (76% [51 to 91%]; P ‫؍‬ 0.04) was significantly higher than that among patients without GN bacteremia (49% [33 to 64%]), but this was not so for patients bacteremic with E. coli (57% [40 to 73%]; P ‫؍‬ 0.55). Among studies of the sepsis patient group, the concordance of endotoxemia with GN bacteremia was surprisingly weak, especially for E. coli GN bacteremia. The Limulus amebocyte lysis (LAL) assay, which utilizes extracts of blood cells (amebocytes) of the Limulus polyphemus horseshoe crab, is a highly sensitive and specific test available for the detection of endotoxin (lipopolysaccharide [LPS]) (1). This assay is a reliable method for the detection of infection with Gramnegative (GN) bacteria in body fluids other than blood (1). However, the clinical significance of endotoxin detection in blood as both a diagnostic and a prognostic test is unclear, despite over 100 studies published over 4 decades for a broad range of patient groups (2-45). The interpretation of the literature is confounded by a 100-fold increase in assay sensitivity (3) and substantial differences in patient inclusion criteria among the studies in the literature over this period.Moreover, in the evaluations of endotoxemia therapies over this time period, there has been a substantial and unexplained disconnect between the results of animal models of sepsis and the results of subsequent clinical trials of the same therapies (46).Five factors have prompted a reappraisal of this question of the clinical significance of endotoxin detection. First, new studies and new data from older studies relating to endotoxemia detection have appeared and need to be incorporated (5-7, 15, 24, 32, 37, 43, 44). Second, the relevance of recently defined structural differences in lipid A,...

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“…In a randomized study of antiendotoxin antibody (HA-1A) conducted in children with meningococcal septicemia, no significant reduction in mortality was observed in children treated with HA-1A compared with placebo [27]. Subsequent studies in adults with gram-negative septicemia also showed no benefit of therapy with HA-1A [28]. In a randomized controlled trial of recombinant bactericidal permeability-increasing protein (rBPI 21 ), which binds and neutralizes endotoxin and blocks the inflammatory cascade, patients treated with rBPI 21 suffered fewer amputations, fewer blood product transfusions, and improved functional outcomes compared with those treated with placebo [29].…”

Section: Adjunctive Therapiesmentioning

confidence: 99%

Treatment of Meningococcal Disease

Nadel

2016

Journal of Adolescent Health

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Meningococcal disease is a life-threatening infection that may progress rapidly, even after appropriate treatment has commenced. Early suspicion of the diagnosis is vital so that parenteral antibiotic treatment can be administered as soon as possible to reduce the complications of infection. The outcome of meningococcal disease is critically dependent on prompt recognition of two important complications: shock and raised intracranial pressure. Rapid recognition of disease and of these complications, together with appropriate management is crucial to the outcome of affected patients. This article summarizes the clinical features of invasive meningococcal disease, diagnostic tools, treatment modalities, and common post-infection sequelae.

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Towards Clinical Applications of Anti-endotoxin Antibodies; A Re-appraisal of the Disconnect

Cited by 25 publications

References 173 publications

The relationship of endotoxaemia to peripheral and central nervous system inflammatory responses in Human African Trypanosomiasis

The relationship of endotoxaemia to peripheral and central nervous system inflammatory responses in Human African Trypanosomiasis

Endotoxemia as a Diagnostic Tool for Patients with Suspected Bacteremia Caused by Gram-Negative Organisms: a Meta-Analysis of 4 Decades of Studies

Treatment of Meningococcal Disease

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