Nerve Chemical-Warfare Agents

Nerve agents inhibit the enzyme acetylcholinesterase (AChE), which hydrolyzes the neurotransmitter acetylcholine (ACh) once ACh has finished activating receptors in neurons, muscles, and glands. Inhibition of AChE leads to an excess of ACh at all of its receptors (cholinergic crisis), first causing increased activity of the affected tissue, followed eventually in the CNS and in skeletal muscle by fatigue and failure of the tissue. Nerve agents inhibit both muscarinic and nicotinic ACh receptors. Muscarinic ACh receptors are present in the central nervous system (CNS), autonomic ganglia, smooth-muscle fibers, and exocrine glands; nicotinic ACh receptors are present in skeletal muscle.

The binding of nerve agent to AChE is essentially irreversible without treatment; treatment with an oxime can regenerate the enzyme as long as the bond has not been further stabilized (a process termed aging) over time. Most nerve agents, like organophosphate insecticides, take hours to age fully, but GD (soman) can age essentially completely within 10 minutes of binding.

The clinical manifestations depend on the state of the agent, route of exposure, and dose.

Vapor exposure to the face causes local effects such as miosis, rhinorrhea, and bronchoconstriction within seconds, progressing to the full range of systemic manifestations of cholinergic excess.

However, inhaled vapor causes collapse within seconds.

Liquid exposure to the skin first causes local effects (local twitching, fasciculations, sweating). Systemic effects occur after a latent period that can be as long as 18 hours after exposure to a very small droplet of a G- or V-series nerve agent; even fatal doses usually take up to 20 to 30 minutes to cause symptoms and signs, which may include sudden collapse and convulsions without warning. Skin exposure to a liquid A-series agent has a latent period ranging from hours to a day or two.

Patients exhibit parts or all of the cholinergic toxidrome, or cholinergic crisis (see tables Common Toxic Syndrome and Symptoms and Treatment of Specific Poisons). Overstimulation and eventual fatigue of the CNS lead to agitation, confusion, unconsciousness, and seizures, progressing to failure of the respiratory center in the medulla. Overstimulation and eventual fatigue of skeletal muscles cause twitching and fasciculations that progress to weakness and paralysis. Overstimulation of cholinergically activated smooth muscle leads to miosis, bronchospasm, and hyperperistalsis (with nausea, vomiting, and cramping), and overstimulation of exocrine glands causes excessive tearing, nasal secretions, salivation, bronchial secretions, digestive secretions, and sweating. Death is usually due to central apnea, but direct paralysis of the diaphragm, bronchospasm, and bronchorrhea can also contribute.

Long-term neurologic and neurobehavioral effects also may occur and include a syndrome that has been called chronic organophosphate-induced neuropsychiatric disorder and organophosphorus-ester–induced chronic neuropathy.

• Clinical evaluation

Diagnosis is made clinically, although laboratory analysis of erythrocyte cholinesterase or plasma cholinesterase levels as well as more specialized laboratory tests can confirm nerve-agent exposure.

• Oxime reactivators (eg, 2-PAM, MMB-4)

• Benzodiazepines

• Respiratory support as needed

Attention to Airway, Breathing, Circulation, Immediate Decontamination, and DSymptoms and Treatment of Specific Poisons). Airway, breathing, and circulation are addressed in standard fashion, as discussed in Cardiopulmonary Resuscitation (CPR) in Adults.

> 25% from baseline during the latent period; such patients should be treated for cholinergic crisis.

The views expressed in this article are those of the author and do not reflect the official policy of the Department of Army, Department of Defense, or the US Government.