Literature DB >> 27244102

The emerging threat of superwarfarins: history, detection, mechanisms, and countermeasures.

Douglas L Feinstein1,2, Belinda S Akpa3, Manuela A Ayee4, Anne I Boullerne1,2, David Braun1, Sergey V Brodsky5, David Gidalevitz6, Zane Hauck7, Sergey Kalinin1, Kathy Kowal1, Ivan Kuzmenko8, Kinga Lis1, Natalia Marangoni1, Michael W Martynowycz6,8, Israel Rubinstein1,4, Richard van Breemen1, Kyle Ware5, Guy Weinberg1,2.   

Abstract

Superwarfarins were developed following the emergence of warfarin resistance in rodents. Compared to warfarin, superwarfarins have much longer half-lives and stronger affinity to vitamin K epoxide reductase and therefore can cause death in warfarin-resistant rodents. By the mid-1970s, the superwarfarins brodifacoum and difenacoum were the most widely used rodenticides throughout the world. Unfortunately, increased use was accompanied by a rise in accidental poisonings, reaching >16,000 per year in the United States. Risk of exposure has become a concern since large quantities, up to hundreds of kilograms of rodent bait, are applied by aerial dispersion over regions with rodent infestations. Reports of intentional use of superwarfarins in civilian and military scenarios raise the specter of larger incidents or mass casualties. Unlike warfarin overdose, for which 1-2 days of treatment with vitamin K is effective, treatment of superwarfarin poisoning with vitamin K is limited by extremely high cost and can require daily treatment for a year or longer. Furthermore, superwarfarins have actions that are independent of their anticoagulant effects, including both vitamin K-dependent and -independent effects, which are not mitigated by vitamin K therapy. In this review, we summarize superwarfarin development, biology and pathophysiology, their threat as weapons, and possible therapeutic approaches.
© 2016 New York Academy of Sciences.

Entities:  

Keywords:  HPLC; brodifacoum; intralipid; lipid membrane; nephrotoxicity; neuropathology; superwarfarins

Mesh:

Substances:

Year:  2016        PMID: 27244102      PMCID: PMC4940222          DOI: 10.1111/nyas.13085

Source DB:  PubMed          Journal:  Ann N Y Acad Sci        ISSN: 0077-8923            Impact factor:   5.691


  74 in total

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2.  Prolonged coagulopathy after brodifacoum exposure.

Authors:  Elizabeth L Underwood; JoLeigh Sutton; Ira Keith Ellis; Brian Qualls; Jon Zamber; Brian N Walker
Journal:  Am J Health Syst Pharm       Date:  2014-04-15       Impact factor: 2.637

3.  Control of Norway rats with residual rodenticide warfarin.

Authors:  W J HAYES
Journal:  Public Health Rep       Date:  1950-11-24       Impact factor: 2.792

4.  Expression of the receptor protein-tyrosine kinases Tyro-3, Axl, and mer in the developing rat central nervous system.

Authors:  A L Prieto; J L Weber; C Lai
Journal:  J Comp Neurol       Date:  2000-09-18       Impact factor: 3.215

5.  The vitamin K content of intravenous lipid emulsions.

Authors:  C Lennon; K W Davidson; J A Sadowski; J B Mason
Journal:  JPEN J Parenter Enteral Nutr       Date:  1993 Mar-Apr       Impact factor: 4.016

6.  Effects of sodium warfarin on capillary ultrastructure.

Authors:  R A Kahn; S A Johnson; A F DeGraff
Journal:  Am J Pathol       Date:  1971-10       Impact factor: 4.307

7.  Dispositional and pharmacodynamic characteristics of brodifacoum in warfarin-sensitive rats.

Authors:  K A Bachmann; T J Sullivan
Journal:  Pharmacology       Date:  1983       Impact factor: 2.547

Review 8.  Long-Acting Anticoagulant Rodenticide (Superwarfarin) Poisoning: A Review of Its Historical Development, Epidemiology, and Clinical Management.

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10.  Membrane Cholesterol Modulates Superwarfarin Toxicity.

Authors:  M Natalia Marangoni; Michael W Martynowycz; Ivan Kuzmenko; David Braun; Paul E Polak; Guy Weinberg; Israel Rubinstein; David Gidalevitz; Douglas L Feinstein
Journal:  Biophys J       Date:  2016-04-26       Impact factor: 4.033

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  18 in total

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10.  Chiral liquid chromatography-tandem mass spectrometry analysis of superwarfarin rodenticide stereoisomers - Bromadiolone, difenacoum and brodifacoum - In human plasma.

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