VX (nerve agent)

VX (nerve agent)

Chembox new
ImageFile = VX-S-enantiomer-2D-skeletal.png ImageName = Skeletal formula of the S enantiomer of VX
ImageFile1 = VX-S-enantiomer-3D-balls.png ImageName1 = Ball-and-stick model of the S enantiomer of VX
IUPACName = Ethyl { [2- [di(propan-2-yl)amino] ethylsulfanyl} methylphosphinate; S- [2-(diisopropylamino)ethyl] -O-ethyl methylphosphonothioate (non-IUPAC synonym)
Section1 = Chembox Identifiers
CASNo = 50782-69-9

Section2 = Chembox Properties
Formula = C11H26NO2PS
BoilingPtC = 298
MeltingPtC = -50
VaporPressure = 0.0007 mm Hg (0.0933256 Pa) at 25 °C
Density = 1.00083 g/mL

Section7 = Chembox Hazards
NFPA-H = 4 | NFPA-F = 1 | NFPA-R = 1
FlashPt = 159 °C [ cite web|url=http://www.ilpi.com/msds/vx.html |title=MSDS: Nerve Agent (VX) |accessdate=2007-10-25 |date=22 December 2000 |publisher=Edgewood Chemical Biological Center (ECBC), Department of the Army ]

VX (S- [2-(diisopropylamino)ethyl] -O-ethyl methylphosphonothioate) is an extremely toxic substance whose sole application is as a nerve agent. As a chemical weapon, it is classified as a weapon of mass destruction by the United Nations in UN Resolution 687. Production and stockpiling of VX was outlawed by the Chemical Weapons Convention of 1993.

The VX nerve agent is the most well-known of the V-series of nerve agents and is considered an area denial weapon due to its physical properties.


Dr. Ranajit Ghosh, a chemist at the Plant Protection Laboratories of Imperial Chemical Industries was investigating a class of organophosphate compounds (organophosphate esters of substituted aminoethanethiols). Like the earlier investigator of organophosphates, Dr. Schrader, Dr. Ghosh found that they were quite effective pesticides. In 1954, ICI put one of them on the market under the trade name Amiton. It was subsequently withdrawn, as it was too toxic for safe use. The toxicity did not go unnoticed, and samples of it had been sent to the British Armed Forces research facility at Porton Down for evaluation. After the evaluation was complete, several members of this class of compounds would become a new group of nerve agents, the V agents. The best known of these is probably VX, with the Russian V-Agent coming a close second (Amiton is largely forgotten as VG). This class of compounds is also sometimes known as Tammelin's esters, after Lars-Erik Tammelin of the Swedish Institute of Defense Research. Dr. Tammelin was also conducting research on this class of compounds in 1952, but for obvious reasons he did not publicize his work widely.

Chemical characteristics

With its high viscosity and low volatility, VX has the texture and feel of high-grade motor oil. This makes it especially dangerous, as it has a high persistence in the environment. It is odorless and tasteless, and can be distributed as a liquid or, through evaporation, into small amounts of vapor. It works as a nerve agent by blocking the function of the enzyme acetylcholinesterase. Normally, an electric nerve pulse would cause the release of acetylcholine over a synapse that would stimulate muscle contraction. The acetylcholine is then broken down to non-reactive substances (acetic acid and choline) by the acetylcholinesterase enzyme. If more muscle tension is needed the nerve must release more acetylcholine. VX blocks the action of acetylcholinesterase, thus resulting in sustained contractions of all the muscles in the body. Sustained contraction of the diaphragm muscle causes death by asphyxiation.


VX is produced via the "Transester Process". This entails a series of steps whereby phosphorus trichloride is methylated to produce methyl phosphonous dichloride. The resulting material is reacted with ethanol to form a diester. This is then transesterified with 'N,N'-diisopropylaminoethanol to produce the mixed phosphonite. Finally, this immediate precursor is reacted with sulfur to form VX.

VX can also be delivered in binary chemical weapons which mix in-flight to form the agent prior to release. Binary VX is referred to as VX2, and is created by mixing O-(2-diisopropylaminoethyl) O'-ethyl methylphosphonite (Agent QL) with elemental sulfur (Agent NE) as is done in the BIGEye aerial chemical bomb. It may also be produced by mixing with sulfur compounds, as with the liquid dimethyl polysulfide mixture (Agent NM) in the cancelled XM-768 8-inch binary projectile program.


Like other organophosphorus nerve agents, VX may be destroyed by reaction with strong nucleophiles such as pralidoxime. The reaction of VX with concentrated aqueous sodium hydroxide results in competing cleavage of the P-O and P-S esters, with P-S cleavage dominating. This is somewhat problematic, since the product of P-O bond cleavage (named EA 2192) remains toxic. In contrast, reaction with the anion of hydrogen peroxide (hydroperoxidolysis) leads to exclusive cleavage of the P-S bond. [cite news |first=Yu-Chu |last=Yang |title=Chemical Detoxification of Nerve Agent VX |publisher=Acc. Chem. Res. |date=1999 |page=109-115. ]

Biological effects

VX is the most toxic nerve agent ever synthesized for which activity has been independently confirmed,cite web |url= http://www.cfr.org/publication/9556/ |title= VX |publisher= Council on Foreign Relations |date= 2006-01 |accessdate= 2007-03-27 ] although unsubstantiated claims that some of the Novichok agents developed by the former Soviet Union are up to eight times more potent than VX have yet to be proved or disproved. The median lethal dose (LD50) for humans is estimated to be about 10 milligrams through skin contact and the LCt50 for inhalation is estimated to be 30-50 mg•min/m³. [ [http://www.fas.org/cw/cwagents.htm Federation of American Scientists :: Types of Chemical Weapons ] ]

Early symptoms of percutaneous exposure (skin contact) may be local muscular twitching or sweating at the area of exposure followed by nausea or vomiting. Some of the early symptoms of a VX vapor exposure to nerve agent may be rhinorrhea (runny nose) and/or tightness in the chest with shortness of breath (bronchial constriction). Miosis (pinpointing of the pupils) may be an early sign of agent exposure but is not usually used as the only indicator of exposure. cite web|url=http://www.army.mil/usapa/epubs/pdf/p385_61.pdf |title=US Army Toxic Chemical Agent Safety Standards |accessdate=2007-12-15 |work=DA PAM 385-61. Section 7-8 Self/Buddy Aid Procedures |publisher=US Army ]


Primary consideration should be given to removal of the liquid agent from the skin before removal of the individual to an uncontaminated area or atmosphere. After removal from the contaminated area, the casualty will be decontaminated by washing the contaminated areas with household bleach and flushing with clean water. After decontamination, the contaminated clothing is removed and skin contamination washed away. If possible, decontamination is completed before the casualty is taken for further medical treatment.

An individual who has received a known nerve-agent exposure or who exhibits definite signs or symptoms of nerve-agent exposure should immediately have the nerve agent antidote drugs atropine, pralidoxime (2-PAM), and diazepam injected. In several nations the nerve agent antidotes are issued for military personnel in the form of an autoinjector such as the United States military Mark I NAAK.

Atropine works by binding and blocking a subset of acetylcholine receptors (known as muscarinic acetylcholine receptor, mAchR), so that the build up of acetylcholine produced by loss of the acetylcholinesterase function can no longer affect their target. The injection of pralidoxime regenerates bound acetylcholinesterase.


The following is the specific history of VX, which is closely linked to the history of similar nerve agents also discovered in Germany during or soon after World War II. That broader history is detailed in .

The chemists Ranajit Ghosh and J.F. Newman discovered the V-series nerve agents at ICI in 1952, patenting diethyl S-2-diethylaminoethyl phosphor-othiolate (VG) in November, 1952. Further commercial research on similar compounds ceased in 1955 when its lethality to humans was discovered. Information on the substance was passed to Porton Down in 1954 and research there led to VX within a year. This was traded to the United States as the British passed over VX in favour of continuing with sarin as the UK chemical weapon of choice, the reasoning behind the decision is unclear, although the recent completion of a sarin production facility at Nancekuke may have played a part.

The US then went into production of large amounts of VX in 1961 at Newport Chemical Depot.

Iraq under Saddam Hussein admitted to UNSCOM that it had researched VX, but had failed to weaponize the agent due to production failure. After U.S. and allied forces had invaded Iraq, no proof of weaponized VX was found. [http://www.globalsecurity.org/wmd/library/report/2004/isg-final-report/isg-final-report_vol1_rsi-06.htm] Subsequent investigation after the 2003 Invasion of Iraq indicates that Iraq had indeed weaponized VX in 1988, and had dropped three VX-filled bombs on Iran. [http://www.globalsecurity.org/wmd/library/report/2004/isg-final-report/isg-final-report_vol3_cw-05.htm]

In December 1994 and January 1995, Masami Tsuchiya of AUM Shinrikyo synthesized 100 to 200 g of VX which was used to attack three persons. Two persons were injured and one 28-year-old man died, who is believed to be the only victim of VX ever documented in the world. [Pamela Zurer, "Japanese cult used VX to slay member" Chemical and Engineering News 1998, Vol 76 (no. 35).] The VX victim, whom Shoko Asahara had suspected as a spy, was attacked at 7:00 am on December 12, 1994 on the street in Osaka by Tomomitsu Niimi and another AUM member, who sprinkled the nerve agent on his neck. He chased them for about 100 yards before collapsing, dying 10 days later without ever coming out of a deep coma. Doctors in the hospital suspected at the time he had been poisoned with an organophosphate pesticide. But the cause of death was pinned down only after cult members arrested for the subway attack confessed to the killing. Ethyl methylphosphonate, methylphosphonic acid and diisopropyl-2-(methylthio)ethylamine were later found from the body of the victim. Unlike the cases for sarin (Matsumoto incident and Sarin gas attack on the Tokyo subway), VX was not used for mass murder.

The only countries known to possess VX are the United States and Russia.cite web |url=http://www.cfr.org/publication/9556/ |title = VX - Council on Foreign Relations |accessdate = 2007-06-12 |publisher= Council on Foreign Relations ] However, under Saddam Hussein's regime, Iraq was suspected of buying VX;cite web |url=http://www.cfr.org/publication/9556/ |title = VX - Council on Foreign Relations |accessdate = 2007-06-12 |publisher= Council on Foreign Relations ] a Sudanese pharmaceutical facility was bombed by the U.S. in 1998 following allegations that it in some way used VX and that the origin of the agent was associated with both Iraq and Al Qaeda. [cite book
publisher=Open Media|date=Oct. 2001
] The chemical in question was later identified as ethyl methyorthophosphric thionate (EMPTA), used to treat seeds and turf grasses. [cite book
title=History of Chemical Warfare
publisher=Palmgrave MacMillan|date=2005

VX stockpile elimination

In the late 1960s, the US cancelled its chemical weapons programs and began the destruction of its stockpiles of agents by a variety of methods. Early disposal included the US Army's CHASE (Cut Holes And Sink 'Em) program, in which old ships were filled with chemical weapons stockpiles and then scuttled. CHASE 8Fact|date=September 2008 was conducted on June 15, 1967, in which the S.S. "Cpl. Eric G. Gibson" was filled with 7,380 VX rockets and scuttled in 7,200 feet of water, off the coast of Atlantic City, New Jersey. Later incineration was used at Johnston Atoll in the North Pacific starting in 1990 (with the stockpile there eliminated in 2000). Newport Chemical Depot began stockpile elimination using chemical neutralization in 2005. VX is hydrolyzed to much less toxic byproducts by using concentrated caustic solution, and the resulting waste is then shipped off-site for further processing. Technical and political issues regarding this secondary byproduct resulted in some delays but most of Newport's stockpile was eliminated in 2007.

Worldwide, VX disposal continues, since 1997 under the mandate of the Chemical Weapons Convention. The US is destroying chemical weapons stockpiles containing VX in several locations and providing support for Russian destruction activities. A new destruction plant, being built for an amount of 140 million € and paid for by Germany, is to open at Potshep, region Brjansk, in 2009.


External links

* [http://www.chem.ox.ac.uk/mom/vx/VX.htm Oxford website on Nerve Agents]
* [http://cfrterrorism.org/weapons/vx.html Questions and Answers for VX]
* [http://www.bt.cdc.gov/agent/vx/basics/facts.asp CDC Facts About VX]
* [http://www.cma.army.mil/home.aspx U.S. Army's Chemical Materials Agency (CMA)]
* [http://www.cbwinfo.com/Chemical/Nerve/VX.shtml CBW Info]
* [http://www.iom.edu/Object.File/Master/43/464/VX%20NERVE%20AGENT.pdf National Academies: Health effects of VX]
* [http://www.army.mil/usapa/epubs/pdf/p385_61.pdf DA PAM 385-61 US Army Toxic Chemical Agent Safety Standards]
* [http://www.nytimes.com/2008/02/25/us/25land.html Decommissioning Surplus VX - Article from NYTimes.com]

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