Increased thromboxane biosynthesis in childhood hemolytic uremic syndrome

Tönshoff, Burkhard; Momper, Rita; Kühl, Peter; Schweer, Horst; Schärer, K; Seyberth, Hannsjörg W.

doi:10.1038/ki.1990.96

Cited by 29 publications

(13 citation statements)

References 43 publications

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“…7 outlines a general mechanism by which platelets may become activated as a consequence of Stx2 and LPS stimulation of endothelial cells, leading to platelet aggregation and platelet-monocyte interactions. These events are proposed to contribute to the known thrombotic complications and pathogenesis of HUS (8,39,41,60,66,81). We demonstrated (Fig.…”

Section: Discussionmentioning

confidence: 50%

Shiga Toxin 2 and Lipopolysaccharide Induce Human Microvascular Endothelial Cells To Release Chemokines and Factors That Stimulate Platelet Function

Guessous¹,

Marcinkiewicz²,

Polanowska-Grabowska³

et al. 2005

Infect Immun

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Shiga toxins (Stxs) produced by Shigella dysenteriae type 1 and enterohemorrhagic Escherichia coli are the most common cause of hemolytic-uremic syndrome (HUS). It is well established that vascular endothelial cells, mainly those located in the renal microvasculature, are targets for Stxs. The aim of the present research was to evaluate whether E. coli-derived Shiga toxin 2 (Stx2) incubated with human microvascular endothelial cells (HMEC-1) induces release of chemokines and other factors that might stimulate platelet function. HMEC-1 were exposed for 24 h in vitro to Stx2, lipopolysaccharide (LPS), or the Stx2-LPS combination, and chemokine production was assessed by immunoassay. More interleukin-8 was released than stromal cell-derived factor 1␣ (SDF-1␣) or SDF-1␤ and RANTES. The Stx2-LPS combination potentiated chemokine release, but Stx2 alone caused more release of SDF-1␣ at 24 h than LPS or Stx2-LPS did. In the presence of low ADP levels, HMEC-1 supernatants activated platelet function assessed by classical aggregometry, single-particle counting, granule secretion, P-selectin exposure, and the formation of platelet-monocyte aggregates. Supernatants from HMEC-1 exposed only to Stx2 exhibited enhanced exposure of platelet P-selectin and platelet-THP-1 cell interactions. Blockade of platelet cyclooxygenase by indomethacin prevented functional activation. The chemokine RANTES enhanced platelet aggregation induced by SDF-1␣, macrophage-derived chemokine, or thymus and activationregulated chemokine in the presence of very low ADP levels. These data support the hypothesis that microvascular endothelial cells exposed to E. coli O157:H7-derived Stx2 and LPS release chemokines and other factors, which when combined with low levels of primary agonists, such as ADP, cause platelet activation and promote the renal thrombosis associated with HUS.

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Section: Discussionmentioning

confidence: 50%

Shiga Toxin 2 and Lipopolysaccharide Induce Human Microvascular Endothelial Cells To Release Chemokines and Factors That Stimulate Platelet Function

Guessous¹,

Marcinkiewicz²,

Polanowska-Grabowska³

et al. 2005

Infect Immun

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“…Deficiency may be caused by low production secondary to damaged endothelium, or by high consumption, and may promote platelet aggregation. Thromboxane is a potent vasoconstrictor that is significantly elevated during acute HUS (176).…”

Section: Prothrombotic Statementioning

confidence: 99%

Pathogenesis of Shiga Toxin-Associated Hemolytic Uremic Syndrome

2001

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“…In contrast, the present study demonstrates that the in vivo PGI z biosynthesis is increased in the acute phase of SHP. A similar discrepancy between in vivo and ex vivo PGI z production has also been observed in hemolyticuremic syndrome (14) and may be explained by the fact that 140 TONSHOFF ET AL. measurement of ex vivo POI2 stimulating activity, in contra st to POI 2-m etabolite excretion rates, does not reflect the actual biologically effective activity of POh in vivo.…”

Section: Discussionmentioning

confidence: 84%

“…As in healthy controls (6) and in conditions with increased platelet-vessel wall interaction (14,15), the end ogenous urinary l l-dehydro-TxB 2 excretion rates exceeded tho se of endogenous urina ry 2,3-dinor-TxB2 in the patients with SHP indicating that l l -deh ydro-Txli -is the more abundant urin ary TxA2 metabolite. The combined anal ysis of both the 2,3-dinor and the ll-dehydro metabolites permits us to rule out that incre ased excretion of one metabolite reflects ju st a shift in the metabolic disposit ion of TxA2 and not a true inc reased TxA2 biosynthe sis.…”

Section: Discussionmentioning

confidence: 99%

“…Increased TxA 2 and POI 2 formation have been reported in other diseases with increased platelet vessel wall interaction such as severe atherosclerosis (15), unstable coronary heart disease (29), a nd systemic sclerosis with Raynaud's phenomenon (30) as models of chronic degenerative vasculopath y and in hemolyticuremic syndrome (14) as a model of acute toxic vasculopathy. The similarity of these findings suggests that although dama ge to the vascular endothelium may result from a variety of insults the response of the vascular endothelium is rather uniform.…”

Section: Discussionmentioning

confidence: 99%

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Increased Biosynthesis of Vasoactive Prostanoids in Schönlein-Henoch Purpura

et al. 1992

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A8STRACT. Schonlein-Henoch purpura (SHP) is an acute immune-mediated vasculitis characterized by infiltration of polymorphonuclear leukocytes into the vessel wall causing damage to the vascular endothelium by the release of proteolytic enzymes. The local inflammatory and thrombotic process may be regulated by increased biosynthesis of vasoacti ve prostanoids. We investigated the biosynthesis of thromboxane A z (TxA z ), a potent vasoconstrictor and platelet agonist, prostacyclin (PGI z ), a vasodilator and platelet antagonist, and prostaglandin E z , a mediator of inflammation, in 14 children with SHP by physicochemical analysis of index metabolites in plasma and urine. TxA z and PGI2 biosynthesis in the systemic circulation was significantly elevated in the acute phase of the disease and correlated with the degree of clinical symptom s. Recurrent episodes of the disea se were associated with phasic increa ses of plasma and urinary TxA z and PGI z metabolites. Renal TxA 2 formation was highest in two patients presenting with the nephrotic syndrome and extracapillary glomerulonephritis. Pro staglandin E z biosynthesis in the systemic circulation was increased in the acute phase of the disea se. The enhanced TxAz formation is consistent with phasic platelet activation in SHP. The increased PGIz biosynthesis reflects endothelial cell damage and may be a response of vascular endothelium to modulate plateletvessel wall and leukocyte-vessel wall interactions. Increa sed prostaglandin E, formation, which probably derives from acti vated polymorphonuclear leukoc ytes and macrophages, is thought to be related to the inflammatory process in SHP. (Pediatr Res 32: 137-140, 1992 ) Abbreviations SHP, Schonlein-Henoch purpura SHP is the most com mon form of vasculitis in child ren (1). The vasculitis is initiated by the subendothelial deposition of IgA/IgG im m une complexes in small blood vessels (2). Complement activation induces infiltratio n of polym orph onuclear leukocytes, which by th e release of prot eolytic enzym es cause damage to th e vessel wall with secondary th rombosis and hem orrhage (3). Th e altered integrity of the vascular endothelium is likely to involve changes in prostanoid biosynthesis at the platelet vascular interface. Tx A 2 , the major cyclooxygenase product of ara chidonic acid in platelets, is a pot ent platelet aggregator and vasocon strictor (4). Th e potential pathophy siologic role of TxA 2 in acute immune-mediated vasculitic disorders has not yet been elucidated.In the present study, we investigated TxA z biosynthesis in childr en with SHP pros pectively during the disease process. To avoid sam pling and analytical probl em s, T xA z biosynthesis was examined by a highly specific and sensitive method, which measures two m ajor urinary enzymatic metabolites, I I-dehydroTx8 2 an d 2,3-dino r-TxB2, which are index metabolites of TxA 2 acti vatio n in th e systemic circulatio n (5, 6), and by measuri ng urin ary Tx B 2 , which predominantly reflects renal TxA 2 form ation (7). In addition , c...

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Increased thromboxane biosynthesis in childhood hemolytic uremic syndrome

Cited by 29 publications

References 43 publications

Shiga Toxin 2 and Lipopolysaccharide Induce Human Microvascular Endothelial Cells To Release Chemokines and Factors That Stimulate Platelet Function

Shiga Toxin 2 and Lipopolysaccharide Induce Human Microvascular Endothelial Cells To Release Chemokines and Factors That Stimulate Platelet Function

Pathogenesis of Shiga Toxin-Associated Hemolytic Uremic Syndrome

Increased Biosynthesis of Vasoactive Prostanoids in Schönlein-Henoch Purpura

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