Journal ArticleDOI
Enzyme reactivator treatment in organophosphate exposure: clinical relevance of thiocholinesteratic activity of pralidoxime.
Georg Petroianu,Georg Petroianu,Anke Missler,Katia Zuleger,Caroline Thyes,Vanessa Ewald,Wolfgang H. Maleck +6 more
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TLDR
The extent of pralidoxime‐induced cholinesteratic pseudo‐activity ex vivo (human blood) and in vivo (minipig) is quantified in order to be able to correct values obtained by photometric methods.Abstract:
Organophosphate compounds are responsible for a large number of accidental and/or suicidal exposures and have been used also for warfare and terrorism. The mechanism of toxicity is by inhibition of cholinesterase. Oximes are the only enzyme reactivators clinically available but clinical experience with oximes is disappointing. There is a gap between laboratory data and clinical impression concerning the efficacy of oxime compounds. Oximes are responsible for thiocholinesteratic activity, a spurious signal caused by interaction between pralidoxime and the thiocholine substrate used for photometric enzyme activity determinations. In a prospective, controlled, non-randomized study performed in anaesthetized miniature pigs, we quantified the extent of pralidoxime-induced cholinesteratic pseudo-activity ex vivo (human blood) and in vivo (minipig) in order to be able to correct values obtained by photometric methods. Plasma cholinesteratic activity using two substrates (acetylthiocholine and butyrylthiocholine) was determined in vitro and in vivo in the presence of pralidoxime. Pralidoxime reacts with the substrate (acetyl- and butyrylthiocholine) used for enzyme activity determinations, producing a spurious signal implying cholinesterase activity (even in the absence of plasma and thus of any enzyme). Cholinesterase activities determined photometrically after pralidoxime therapy can be erroneously high. Although in theory this could mislead clinicians into assuming an efficacious therapy, this is unlikely to occur in vivo under normal pralidoxime dosing conditions. To avoid any ambiguity it is recommended that blood be drawn for enzyme activity determinations prior to reactivator use and no less than 1 h after its administration.read more
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Design, evaluation and structure-activity relationship studies of the AChE reactivators against organophosphorus pesticides.
TL;DR: This review is the summarized design, evaluation, and structure–activity relationship studies of recently produced AChE reactivators against OPP, and several novel compounds show very promising abilities as comparable to commercial oximes.
Journal ArticleDOI
Limitation of the Ellman method: cholinesterase activity measurement in the presence of oximes.
TL;DR: In this article, the authors measured the oximolysis between oximes (K027 and HI-6) and ATCh in the presence of DTNB at different pH values, taking into account the final concentration of a product that is thiocholine.
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Increased morbidity and mortality in acute human organophosphate-poisoned patients treated by oximes: a meta-analysis of clinical trials.
TL;DR: It can be concluded that oximes are not effective in the management of organophosphate-poisoned patients and, surprisingly, they can be dangerous and worsen the patient's clinical situation.
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Five oximes (K-27, K-33, K-48, BI-6 and methoxime) in comparison with pralidoxime: in vitro reactivation of red blood cell acetylcholinesterase inhibitied by paraoxon
TL;DR: There is a clear demand for ‘broad spectrum’ cholinesterase reactivators with a higher efficacy than PRX, and clinical experience with PRX is disappointing and routine use has been questioned.
Journal ArticleDOI
Reversible cholinesterase inhibitors as pretreatment for exposure to organophosphates. A review.
TL;DR: Experimental oxime K‐27 was the most efficacious compound, affording best protection, when administered before terbufos sulfone, azinphos‐methyl and dicrotophos, second best before ethyl‐ and methyl‐paraoxon exposure and third best before diisopropylfluorophosphate administration.
References
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Journal ArticleDOI
A new and rapid colorimetric determination of acetylcholinesterase activity.
TL;DR: A photometric method for determining acetylcholinesterase activity of tissue extracts, homogenates, cell suspensions, etc., has been described and Kinetic constants determined by this system for erythrocyte eholinesterases are presented.
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Poisoning due to organophosphate insecticides. acute and chronic manifestations
TL;DR: Two patients with Diazinon ® poisoning and the second with parathion poisoning illustrate the acute manifestations, the criteria for diagnosis, and treatment with pralidoxime and atropine in organophosphate poisoning.
Journal ArticleDOI
Evaluation of antidotes for poisoning by organophosphorus pesticides
Martin K Johnson,Dag Jacobsen,Tim Meredith,Peter Eyer,Andrew J.W. Heath,David A Ligtenstein,Tim C Marrs,Ladislaus Szinicz,J Allister Vale,John A. Haines +9 more
Journal Article
Cholinesterase inhibition by organophosphorus compounds and its clinical effects.
TL;DR: Poisoning by organophosphorus compounds in man differs from animal experiments in several ways: in man, exposure may occur by several different routes, the manifestations are detected more easily, and therapy is given throughout the course of illness.
Journal ArticleDOI
Pharmacological effects of oximes: how relevant are they?
TL;DR: A new concept for further treatment is suggested: maintenance of neuronal transmission in spite of continued AChE-inhibition by pharmacological manipulation of the cholinergic receptor.