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Title: The biodistribution and pharmacokinetics of the oxime acetylcholinesterase reactivator RS194B in guinea pigs

Journal Article · · Chemico-Biological Interactions
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  1. Lawrence Livermore National Lab. (LLNL), Livermore, CA (United States)
  2. Lawrence Livermore National Lab. (LLNL), Livermore, CA (United States); Veterans Affairs, Palo Alto, CA (United States)
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Organophosphorus-based (OP) nerve agents represent some of the most toxic substances known to mankind. The current standard of care for exposure has changed very little in the past decades, and relies on a combination of atropine to block receptor activity and oxime-type acetylcholinesterase (AChE) reactivators to reverse the OP binding to AChE. Although these oximes can block the effects of nerve agents, their overall efficacy is reduced by their limited capacity to cross the blood-brain barrier (BBB). RS194B, a new oxime developed by Radic et al. (J. Biol. Chem., 2012) has shown promise for enhanced ability to cross the BBB. To fully assess the potential of this compound as an effective treatment for nerve agent poisoning, a comprehensive evaluation of its pharmacokinetic (PK) and biodistribution profiles was performed using both intravenous and intramuscular exposure routes. The ultra-sensitive technique of accelerator mass spectrometry was used to quantify the compound’s PK profile, tissue distribution, and brain/plasma ratio at four dose concentrations in guinea pigs. PK analysis revealed a rapid distribution of the oxime with a plasma t1/2 of ~1 hr. Kidney and liver had the highest concentrations per gram of tissue followed by lung, spleen, heart and brain for all dose concentrations tested. The Cmax in the brain ranged between 0.03-0.18% of the administered dose, and the brain-to-plasma ratio ranged from 0.04 at the 10 mg/kg dose to 0.18 at the 200 mg/kg dose demonstrating dose dependent differences in brain and plasma concentrations. In vitro studies show that both passive diffusion and active transport contribute little to RS194B traversal of the BBB. These results indicate that biodistribution is widespread, but very low quantities accumulate in the guinea pig brain, indicating this compound may not be suitable as a centrally active reactivator.

Research Organization:
Lawrence Livermore National Lab. (LLNL), Livermore, CA (United States)
Sponsoring Organization:
USDOE National Nuclear Security Administration (NNSA)
Grant/Contract Number:
AC52-07NA27344
OSTI ID:
1458634
Alternate ID(s):
OSTI ID: 1549214
Report Number(s):
LLNL-JRNL-738714; 891966
Journal Information:
Chemico-Biological Interactions, Vol. 277, Issue C; ISSN 0009-2797
Publisher:
ElsevierCopyright Statement
Country of Publication:
United States
Language:
English
Citation Metrics:
Cited by: 13 works
Citation information provided by
Web of Science

References (32)

Species Difference of Esterase Expression and Hydrolase Activity in Plasma journal October 2012
Evaluation of Microdosing to Assess Pharmacokinetic Linearity in rats Using Liquid Chromatography-Tandem mass Spectrometry journal December 2005
Predicting a Drug’s Membrane Permeability: A Computational Model Validated With in Vitro Permeability Assay Data journal May 2017
Comparison of human and guinea pig acetylcholinesterase sequences and rates of oxime-assisted reactivation journal September 2010
The permeation of several materials into the fluids of the rabbit's brain journal October 1971
Permeability Studies on In Vitro Blood–Brain Barrier Models: Physiology, Pathology, and Pharmacology journal February 2005
Pro-2-PAM therapy for central and peripheral cholinesterases journal September 2010
High throughput artificial membrane permeability assay for blood–brain barrier journal March 2003
Syrian gas attack reinforces need for better anti-sarin drugs journal October 2013
In Vitro P-glycoprotein Assays to Predict the in Vivo Interactions of P-glycoprotein with Drugs in the Central Nervous System journal October 2007
Novel oximes as blood–brain barrier penetrating cholinesterase reactivators journal September 2010
Human microdosing for the prediction of patient response journal March 2010
Elimination of Glyceryl Trinitrate: Effects of sex, age, Species and Route of Administration journal September 1982
Kinetic profile in blood and brain of the cholinesterase reactivating oxime HI-6 after intravenous administration to the rat journal November 1983
Human in Vivo Pharmacokinetics of [ 14 C]Dibenzo[ def,p ]chrysene by Accelerator Mass Spectrometry Following Oral Microdosing journal December 2014
Determining the Pharmacokinetics and Long-Term Biodistribution of SiO 2 Nanoparticles In Vivo Using Accelerator Mass Spectrometry journal October 2012
Use of Microdosing and Accelerator Mass Spectrometry To Evaluate the Pharmacokinetic Linearity of a Novel Tricyclic GyrB/ParE Inhibitor in Rats journal August 2014
A High-Throughput Method for the Conversion of CO 2 Obtained from Biochemical Samples to Graphite in Septa-Sealed Vials for Quantification of 14 C via Accelerator Mass Spectrometry journal May 2003
Preclinical Studies of Noncharged Oxime Reactivators for Organophosphate Exposure: NONCHARGED OXIME REACTIVATORS journal August 2013
Report on 640 Victims of the Tokyo Subway Sarin Attack journal August 1996
Acute and chronic effects of sarin exposure from the Tokyo subway incident journal May 2005
The Tokyo subway sarin attack—lessons learned journal September 2005
Clinical evaluation of pesticide exposure and poisonings journal April 1997
Paraoxon has only a minimal effect on pralidoxime brain concentration in rats journal January 2007
Refinement of Structural Leads for Centrally Acting Oxime Reactivators of Phosphylated Cholinesterases journal February 2012
Mechanism of interaction of novel uncharged, centrally active reactivators with OP-hAChE conjugates journal March 2013
Kinetics of movement of iodide, sucrose, inulin and radio-iodinated serum albumin in the central nervous system and cerebrospinal fluid of the rat journal December 1963
Brain distribution spaces of mannitol-3H, inulin-14C, and dextran-14C in the rat journal July 1971
New Structural Scaffolds for Centrally Acting Oxime Reactivators of Phosphylated Cholinesterases journal April 2011
The role of excitotoxicity in organophosphorous nerve agents central poisoning journal June 1997
Accelerator Mass Spectrometry journal June 1995
A Combined Accelerator Mass Spectrometry-Positron Emission Tomography Human Microdose Study with 14C- and 11C-Labelled Verapamil journal January 2011

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Oxime K203: a drug candidate for the treatment of tabun intoxication journal December 2018

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