Pretreatment of mice with lipopolysaccharide (LPS) or IL-1β exerts dose-dependent opposite effects on Shiga toxin-2 lethality

Palermo, Marina S.; Alves-Rosa, Fernanda; Rubel, Carolina; Fernández, Gabriela; Fernández-Alonso, G.; Alberto, Fabiana; Rivas, Marta; Isturiz, Martı́n A.

doi:10.1046/j.1365-2249.2000.01103.x

Cited by 60 publications

(72 citation statements)

References 39 publications

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“…Survival rates of BALB/c mice from Shiga toxin 2 were enhanced by 18-h pretreatment of either LPS or dexamethasone whereas only 1 h of LPS pretreatment decreased survival rates. This protection afforded by the 18 h LPS pretreatment condition was shown to be due to the increased endogenous corticosterone production secondary to LPS-induced IL-1 activation of the HPA axis (Palermo et al 2000). In these studies, the role of endogenous glucocorticoids in protection against Shiga toxin lethality was further supported by the decreased survival of adrenalectomized animals or those treated with the GR antagonist RU486.…”

Section: Bacterial Toxinsmentioning

confidence: 90%

Role of the hypothalamic-pituitary-adrenal axis, glucocorticoids and glucocorticoid receptors in toxic sequelae of exposure to bacterial and viral products

Webster

Sternberg

2004

Journal of Endocrinology

164

124

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The hypothalamic-pituitary-adrenal (HPA) axis is activated during many bacterial and viral infections, resulting in an increase in circulating glucocorticoid levels. This HPA axis activation and glucocorticoid response are critical for the survival of the host, as demonstrated by the fact that removal of the HPA axis (by adrenalectomy or hypophysectomy) or glucocorticoid receptor (GR) blockade enhances the severity of the infection and in some cases enhances the mortality rate. Replacement with a synthetic glucocorticoid reverses these effects by reducing the severity of the infection and provides protection against lethal effects. In addition, some bacteria and viral infections have been shown to affect the GR directly. These have been described and the implications of such an effect discussed.

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Section: Bacterial Toxinsmentioning

confidence: 90%

Role of the hypothalamic-pituitary-adrenal axis, glucocorticoids and glucocorticoid receptors in toxic sequelae of exposure to bacterial and viral products

Webster

Sternberg

2004

Journal of Endocrinology

164

124

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“…It has previously been shown that Stx2 causes renal failure in mice (3,33,47). Having demonstrated that Stx2 does not directly affect the murine renal glomerular filtration barrier cells in vitro, we sought to determine the Stx2 target cells in the mouse kidney.…”

Section: Murine Glomerular Cells Do Not Express Gbmentioning

confidence: 99%

Shiga Toxin 2 Targets the Murine Renal Collecting Duct Epithelium

et al. 2009

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Hemolytic-uremic syndrome (HUS) caused by Shiga toxin-producingEscherichia coli infection is a leading cause of pediatric acute renal failure. Bacterial toxins produced in the gut enter the circulation and cause a systemic toxemia and targeted cell damage. It had been previously shown that injection of Shiga toxin 2 (Stx2) and lipopolysaccharide (LPS) caused signs and symptoms of HUS in mice, but the mechanism leading to renal failure remained uncharacterized. The current study elucidated that murine cells of the glomerular filtration barrier were unresponsive to Stx2 because they lacked the receptor glycosphingolipid globotriaosylceramide (Gb 3 ) in vitro and in vivo. In contrast to the analogous human cells, Stx2 did not alter inflammatory kinase activity, cytokine release, or cell viability of the murine glomerular cells. However, murine renal cortical and medullary tubular cells expressed Gb 3 and responded to Stx2 by undergoing apoptosis. Stx2-induced loss of functioning collecting ducts in vivo caused production of increased dilute urine, resulted in dehydration, and contributed to renal failure. Stx2-mediated renal dysfunction was ameliorated by administration of the nonselective caspase inhibitor Q-VD-OPH in vivo. Stx2 therefore targets the murine collecting duct, and this Stx2-induced injury can be blocked by inhibitors of apoptosis in vivo.

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“…These studies indicate a synergistic effect of Stx and LPS in vivo, as has also been shown in vitro using endothelial cells (68). Other reports observed that pretreatment with LPS could either increase or decrease Stx2-induced lethality, depending on the dose and timing of injection and that the effects could be modulated by TNF-␣ or IL-1␤ (97). A recent publication (98) showed that antibodies to LPS block adherence of STEC to human intestinal epithelial cells in vitro, although the biologic significance of this finding has not been evaluated in vivo.…”

Section: Stec Virulence Factorsmentioning

confidence: 99%