Lepirudin prevents lethal effects of Shiga toxin in a canine model
Microvascular thrombosis is a major cause of organ damage in Shiga toxin-mediated hemolytic uremic syndrome (Stx-HUS). In vitro and clinical studies implicate thrombin-mediated mechanisms in the pathogenesis of Stx microvascular thrombosis. In a greyhound model, administration of 0.03 microg/kg to 0...
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| Published in | Thrombosis and haemostasis Vol. 92; no. 2; p. 387 |
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| Main Authors | , , |
| Format | Journal Article |
| Language | English |
| Published |
Germany
01.08.2004
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| Abstract | Microvascular thrombosis is a major cause of organ damage in Shiga toxin-mediated hemolytic uremic syndrome (Stx-HUS). In vitro and clinical studies implicate thrombin-mediated mechanisms in the pathogenesis of Stx microvascular thrombosis. In a greyhound model, administration of 0.03 microg/kg to 0.05 microg/kg Stx1 or Stx2 causes severe bloody diarrhea and HUS with microvascular thrombosis requiring humane euthanasia within 65 hours. Using a greyhound model of Stx-HUS we analyzed early hemostatic changes, and tested the hypothesis that thrombin blockade with lepirudin would prevent lethal Stx effects. Two Stx1-exposed greyhounds were analyzed for hemostatic changes prior to onset of clinical manifestations. Serial hemostasis studies after Stx1 challenge revealed trends of increased aPTT, fibrinogen levels, and prothrombin fragment 1+2, and appearance of abnormally large von Willebrand factor multimers. Three greyhounds were anticoagulated with lepirudin to maintain activated partial thromboplastin times (aPTT) >2.5-fold normal, followed by administration of Stx2 and observation of clinical responses. Among the 3 lepirudin-treated, Stx2-challenged greyhounds, one developed severe illness requiring euthanasia. Remarkably, 2 of the 3 greyhounds developed only hypersalivation and restlessness that resolved (P <.03 compared to 14 historical controls). These two greyhounds were clinically, hematologically and biochemically normal 74 hours after Stx administration, well beyond the time of euthanasia of any previous greyhound. This study suggests that greyhounds exposed to Stx develop procoagulant changes similar to humans, and that thrombin may be a critical factor in the pathogenesis and treatment of Stx-HUS. |
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| AbstractList | Microvascular thrombosis is a major cause of organ damage in Shiga toxin-mediated hemolytic uremic syndrome (Stx-HUS). In vitro and clinical studies implicate thrombin-mediated mechanisms in the pathogenesis of Stx microvascular thrombosis. In a greyhound model, administration of 0.03 microg/kg to 0.05 microg/kg Stx1 or Stx2 causes severe bloody diarrhea and HUS with microvascular thrombosis requiring humane euthanasia within 65 hours. Using a greyhound model of Stx-HUS we analyzed early hemostatic changes, and tested the hypothesis that thrombin blockade with lepirudin would prevent lethal Stx effects. Two Stx1-exposed greyhounds were analyzed for hemostatic changes prior to onset of clinical manifestations. Serial hemostasis studies after Stx1 challenge revealed trends of increased aPTT, fibrinogen levels, and prothrombin fragment 1+2, and appearance of abnormally large von Willebrand factor multimers. Three greyhounds were anticoagulated with lepirudin to maintain activated partial thromboplastin times (aPTT) >2.5-fold normal, followed by administration of Stx2 and observation of clinical responses. Among the 3 lepirudin-treated, Stx2-challenged greyhounds, one developed severe illness requiring euthanasia. Remarkably, 2 of the 3 greyhounds developed only hypersalivation and restlessness that resolved (P <.03 compared to 14 historical controls). These two greyhounds were clinically, hematologically and biochemically normal 74 hours after Stx administration, well beyond the time of euthanasia of any previous greyhound. This study suggests that greyhounds exposed to Stx develop procoagulant changes similar to humans, and that thrombin may be a critical factor in the pathogenesis and treatment of Stx-HUS. |
| Author | Friedman, Kenneth D Raife, Thomas Fenwick, Brad |
| Author_xml | – sequence: 1 givenname: Thomas surname: Raife fullname: Raife, Thomas email: thomas-raife@uiowa.edu organization: Department of Pathology, University of Iowa, Iowa City, Iowa 52242, USA. thomas-raife@uiowa.edu – sequence: 2 givenname: Kenneth D surname: Friedman fullname: Friedman, Kenneth D – sequence: 3 givenname: Brad surname: Fenwick fullname: Fenwick, Brad |
| BackLink | https://www.ncbi.nlm.nih.gov/pubmed/15269836$$D View this record in MEDLINE/PubMed |
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| CitedBy_id | crossref_primary_10_1002_jca_21302 crossref_primary_10_1242_dmm_035063 crossref_primary_10_1111_j_1538_7836_2005_01425_x crossref_primary_10_1097_MOG_0b013e3282f2dfb8 crossref_primary_10_1182_blood_2005_05_2111 crossref_primary_10_1182_blood_2008_07_168377 crossref_primary_10_1128_microbiolspec_EHEC_0022_2013 crossref_primary_10_1160_TH05_04_0265 crossref_primary_10_1128_IAI_00476_17 crossref_primary_10_1016_j_ijmm_2005_07_010 crossref_primary_10_1586_14787210_5_4_653 crossref_primary_10_1186_1756_0500_4_36 crossref_primary_10_1016_j_micinf_2008_03_004 |
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| SubjectTerms | Animals Anticoagulants - toxicity Blood Platelets - metabolism Cell-Free System Coagulants - pharmacology Dogs Fibrinogen - biosynthesis Fibrinogen - metabolism Hemolytic-Uremic Syndrome - drug therapy Hirudins - analogs & derivatives Hirudins - metabolism Hirudins - pharmacology Kidney Glomerulus - pathology Microscopy, Electron, Transmission Partial Thromboplastin Time Prothrombin - genetics Prothrombin Time Recombinant Proteins - metabolism Recombinant Proteins - pharmacology Shiga Toxin 1 - toxicity Shiga Toxin 2 - toxicity Thrombin - metabolism Time Factors von Willebrand Factor - genetics von Willebrand Factor - metabolism |
| Title | Lepirudin prevents lethal effects of Shiga toxin in a canine model |
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