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AUTHOR AND EDITOR INFORMATION

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Author: Geoffrey M Fitzgerald, MD, Consulting Staff, Concord Emergency Medical Associates

Coauthor(s): Timothy Vollmer, MD, Consulting Staff, Department of Emergency Medicine, Geisinger Medical Center

Editors: Fred Henretig, MD, Medical Director, Delaware Valley Regional Poison Control Center, Departments of Emergency Medicine and Pediatrics, Director, Section of Clinical Toxicology, Professor, University of Pennsylvania School of Medicine, Children's Hospital; Francisco Talavera, PharmD, PhD, Senior Pharmacy Editor, eMedicine; Rick Kulkarni, MD, Medical Director, Assistant Professor of Surgery, Section of Emergency Medicine, Yale-New Haven Hospital; John D Halamka, MD, MS, Associate Professor of Medicine, Harvard Medical School, Beth Israel Deaconess Medical Center; Chief Information Officer, CareGroup Healthcare System and Harvard Medical School; Attending Physician, Division of Emergency Medicine, Beth Israel Deaconess Medical Center; Robert G Darling, MD, FACEP, Clinical Assistant Professor of Military and Emergency Medicine, Uniformed Services University of the Health Sciences, F Edward Hebert School of Medicine; Director, Center for Disaster and Humanitarian Assistance Medicine

Author and Editor Disclosure

Synonyms and related keywords: chemical warfare, vesicant, blistering agents, lewisite, L, ethyldichloroarsine, ED, methyldichloroarsine, MD, phenyldichloroarsine, PD, arsenic poisoning, arsenic ingestion

INTRODUCTION

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Background

Vesicants are a class of chemical weapons named for their ability to cause vesicular skin lesions. The 4 organic arsenicals are lewisite (L), methyldichloroarsine (MD), phenyldichloroarsine (PD), and ethyldichloroarsine (ED). These agents, together with the mustard agents and phosgene oxime, make up the vesicant class. Although not as well known as the mustards, the organic arsenicals are a group of potent vesicants that medical planners should not overlook.

Interest in organic arsenicals dates back to the mid-19th century. While investigating possible new fumigants, European chemists discovered that chloroarsines (ie, arsenic-chloride compound in which 1 of the chlorine atoms is replaced by an organic radical) tended to be destructive both to insects and to human tissue. With the start of World War I, both sides employed chemists to create chemical warfare (CW) agents. The trench warfare stalemate created a tactical need for a chemical weapon that was both short acting (eg, nonpersistent, volatile) and lethal. To fill this need, German chemists delivered the first weaponized organic arsenical, MD. Two additional organic arsenicals, PD and ED, soon augmented MD. While MD, PD, and ED were being deployed on the battlefields of Europe in 1917 and 1918, a team of American researchers, lead by Captain Lewis of the US Army Medical Corps, was working on the fourth and final organic arsenical. Lewisite, as it was named, never was deployed in World WarI.

Although mustard vesicants have been used in numerous regional wars since 1918, organic arsenical weapons have had limited use. L may have been used by Italy against Ethiopia in 1935 and again by Japan in China from 1937-1944.

Today, arsenicals still are considered a threat, not so much from large nation states but from smaller, less developed nations and/or by terrorist organizations. The relative ease of production coupled with their effectiveness against an unprotected population make organic arsenicals a continued threat in the 21st century.

Pathophysiology

The exact mechanism of biological activity and toxicity of the organic arsenicals is unknown. DNA alkylation and/or inhibition of glutathione-scavenging pathways are 2 postulated mechanisms of action. What is certain is that a blistering reaction occurs on any tissue that an arsenical contacts, whether it is skin, eye, or pulmonary tissue. The onset of symptoms after arsenical exposure occurs in seconds as compared to 4-8 hours for mustard exposure. Either a liquid or vapor (ie, gaseous form of a substance at temperatures below boiling point) can cause toxicity. The organic arsenicals tend to have high volatility at room temperature and thus pose a significant vapor threat to exposed personnel.

Animal data and limited human trials demonstrated that organic arsenicals readily penetrate the skin. Within seconds of contact, the chemical fixes itself to the epidermis and dermis. Pain is immediate. Since the agent penetrates deeper, destruction of subcutaneous tissue results. Protease digestion of anchoring filament at the epidermal-dermal junction occurs. The separation of dermis from epidermis together with capillary leakage causes fluid-filled vesicles.

Vapor contact with the conjunctiva may be the victims' first symptom. Severe conjunctival irritation and blepharospasm result upon eye contact. More severe exposure can cause loosening of corneal epithelial cells and swelling and edema of the cornea.

The respiratory tract's mucosa and submucosa are susceptible to vapor exposure. Mucosal damage starts in the nose and descends down the respiratory mucosa in a dose-dependent fashion. Immediate pain, lacrimation, and irritation accompany the damage. Damaged respiratory mucosa slough off, filling the airways with debris. Damage to the lung parenchyma causes the secretion of blood and mucous that, with the pseudomembranes, can cause asphyxiation. In animal studies, large doses of L caused this "dry land drowning" within 10 minutes.

The gastrointestinal tract also is susceptible. PD vapor in particular produces a phenyl radical that causes vomiting. Vomiting usually develops within 1-2 minutes after exposure to PD.

The immediate onset of symptoms following exposure makes severe or systemic toxicity to organic arsenical unlikely. However, if a victim does not have protective gear or cannot move out of a contaminated area, prolonged contact may lead to multiorgan involvement. Blood-borne arsenicals can trigger increased permeability of capillaries throughout the body. Leakage of proteins and plasma then can cause third space fluid shifts, hypovolemia, and shock. Intravascular hemolysis of erythrocytes with subsequent hemolytic anemia may result.

Frequency

United States

Organic arsenical weapons never have been used within the US. Other sources of arsenic poisoning are common, and arsenic ingestion is the most common cause of acute metal poisoning in the US. Inorganic arsenic is found in insecticides, rodenticides, and herbicides and is used in mining and smelting industries.

International

Any nation or terrorist group that has access to a basic pesticide production facility can produce these agents with relative ease. The former Soviet Union is known to have combined sulfur mustard (H) and L into a binary weapon known as HL.

Mortality/Morbidity

Although vesicants have a relatively low mortality rate when compared to other CW agents, survivors usually require prolonged care and rehabilitation. These requirements placed a tremendous burden on the medical infrastructure during World War I.


CLINICAL

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History

Victims of an L attack may remember observing puddles of a brown liquid or of smelling an odor similar to geranium. MD and ED reportedly smell like rotting fruit. Almost instantaneous pain and irritation of the skin, eyes, and nasal pharynx follow exposure. The patient usually relates a history of trying to remove himself or herself from the noxious stimuli.

  • The skin burns and itches. A history of erythema followed by the appearance of vesicles may be obtained.
  • Eye pain is severe and is accompanied by blepharospasm and/or photophobia.
  • Extreme irritation of the nasal mucosa and upper airway induces coughing and sneezing. Coughing may become productive, and shortness of breath may appear as the irritation of the airway mucosa progresses.
  • PD often precipitates severe vomiting within 1-2 minutes after exposure.

Physical

Physical signs of organic arsenical exposure are similar to those of mustard agents. The major difference is the time of onset of signs. Organic arsenicals cause immediate signs, whereas signs of mustard exposure appear after a latent period of several hours.

  • An erythematous rash appears within 15-30 minutes. This is followed by the development of fluid-filled vesicles.
    • Vesicles initially are filled with clear fluid and may coalesce to form large bullae.
    • In more severe exposures, the vesicular fluid may take on a yellow and then red color, and a central area of necrosis may form.
    • An L skin lesion has more actual tissue destruction (but less surrounding erythema) than a mustard lesion. Compared to distilled mustard, L is gram-for-gram more toxic. The LD50 (lethal dose for 50% of the population) of L is 2.8 g on the skin.
  • Conjunctival injection and edema of the lids, cornea, and conjunctiva occur with either a vapor or liquid exposure.
    • Corneal vascularization with secondary edema results and may last for weeks.
    • One drop of liquid L on the cornea can cause severe corneal damage up to and including perforation.
  • Vapor damage to the upper respiratory mucosa causes epistaxis, massive rhinorrhea, and lacrimation.
    • Laryngitis and dysphonia changes result from exposure and can lead to laryngospasm.
    • With larger vapor exposure, destruction of the bronchiolar mucosa and submucosa causes pseudomembrane formation and obstruction.
  • Systemic signs of organic toxicity may include evidence of hypovolemia and shock.

Causes

Organic arsenical exposure can be caused by military CW attack or potentially from terrorist incident.


DIFFERENTIALS

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CBRNE - Irritants: Cs, Cn, Cnc, Ca, Cr, Cnb, PS
CBRNE - Lung-Damaging Agents, Phosgene
CBRNE - Vesicants, Mustard: Hd, Hn1-3, H

Other Problems to be Considered

Exposure to plants (eg, poison ivy) or adverse drug reactions can cause the same skin changes as those found in organic arsenical exposure. Mustard gas causes the same signs and symptoms; however, a latent period of several hours occurs between exposure and symptoms. The eye and respiratory irritation produced by organic arsenical vapor is similar to that of the choking agents (eg, phosgene) or riot control agents (eg, CS).

Maintain a high index of suspicion to make the diagnosis of organic arsenical exposure. Diagnosis in solitary cases is difficult.


WORKUP

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Lab Studies

  • The US military and the North Atlantic Treaty Organization (NATO) have developed several field tests to detect various CW agents. The field tests that reliably detect L and the other organic arsenicals include the M256A1, individual chemical agent detector (ICAD), miniature chemical agent monitor (MINICAMS), M18A2, M21, M90, M93A1 Fox, chemical agent monitor (CAM), and depot area air monitoring system (DAAMS). Less sophisticated means of detection are M8 detection paper (turns red with L) and M9 paper (turns color when exposed to arsenicals).
  • With exception of urinary arsenic excretion, no specific tests exist for organic arsenical exposure. Leukocytosis and other nonspecific markers of tissue destruction may appear.
  • Culture damaged skin routinely to stave off opportunistic skin infections.
  • Also perform sputum Gram stain and culture if the respiratory system is affected.

Imaging Studies

  • Pneumonia commonly follows pulmonary damage in 3-5 days. Obtain a chest x-ray as indicated.

Procedures

  • Massive tissue damage to the respiratory mucosa can cause acute airway compromise from laryngospasm and/or necrotic debris. Emergent endotracheal intubation may be required. Obtain a bronchoscopy consultation if pseudomembrane formation is suggested.


TREATMENT

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Prehospital Care

  • The top 2 priorities are protecting the caregiver and removing the offending agent from the casualty as quickly as possible. Then assess airway, breathing, and circulation (ABCs) as usual.
    • All medical personnel who may come into contact with vesicant vapor or liquid should wear protective gear.
    • The activated charcoal in the chemical protective mask adequately adsorbs these agents.
    • Protective boots, gloves, pants, and jacket (eg, mission-oriented protective posture [MOPP] gear) protect the skin; however, organic arsenicals attack rubber and can cause it to break down with prolonged exposure. This is especially true of L.
  • Vesicant agents irreversibly bind to the skin within minutes. Remove the agent as quickly as possible.
    • Remove liquids via any means available. The military has specially developed charcoal-based kits (eg, M258A1 kit, M291 kit). If specialized kits are not available, rags, leaves, sticks, or just about any other material can be used to blot off liquid agent.
    • Flushing the eyes or skin is another solution. Dilute hypochlorite (0.5% solution) can be used on the skin. Live steam or alkaline solutions (eg, sodium hydroxide) can be used to decontaminate closed spaces.

Emergency Department Care

  • As with any chemical disaster, the emergency department's disaster plan should have a system in place to efficiently triage contaminated patients.
    • After assessing for life-threatening conditions, additionally decontaminate patients in the triage area as indicated.
    • Once in the emergency department, reassess ABCs as usual.
    • Assessment of volume status is a must. Patients who have been in hot protective gear are predisposed to volume depletion and hyperthermia. Correction of fluid and/or electrolyte abnormalities is essential in these patients.
    • Once a victim has been undressed and fully decontaminated, no danger to the caretakers remains.
  • Blisters smaller than 2 cm and erythematous areas can be covered with topical antibiotics, calamine lotion, or other soothing creams.
  • Denude fluid-filled vesicles larger than 2 cm and irrigate them with sterile saline. Apply topical antibiotics such as silver sulfadiazine. Intense pain and itching may require systemic analgesics and antipruritics.
  • Upper respiratory symptoms can be alleviated with humidified oxygen and cough suppressants. Reserve antibiotics for patients with pulmonary damage who develop fever. Specific antimicrobial therapy then is based on Gram stain and cultures.
  • Eyes may be irrigated with normal saline, followed by application of topical antibiotics. Petroleum jelly can be applied to the edges of the lids to prevent them from sticking together.

Consultations

  • Consultation can be made to various departments (eg, dermatology, ophthalmology) as needed.
  • A 24-hour hotline regarding CW agents is available at 800-424-8802.
  • Help also can be obtained by calling the US Army Medical Research Institute of Chemical Defense at 410-436-3628.


MEDICATION

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In addition to the medications mentioned in the preceding section, the organic arsenicals have an antidote in the form of British antilewisite agent (BAL, dimercaprol). BAL is a chelating agent that was developed at the end of World War I specifically to treat L casualties.

Drug Category: Chelating agents

As a chelating agent, BAL binds to the arsenic moiety, thereby preventing or reversing its binding to tissue enzymes. The BAL-arsenic moiety then is excreted renally. Dimercaprol currently is used as a chelating agent for heavy metals such as arsenic, gold, and mercury.

Drug NameDimercaprol (BAL in oil)
DescriptionPackaged in 3-mL ampules with 100 mg/mL. Formerly supplied as an ophthalmic and dermatologic ointment during World War II; these preparations are no longer available.
Adult Dose4-5 mg/kg (approximately 1 mL/50 lb) IM, not to exceed 4 mL; repeat q4h for a total of 4 doses; in severe exposure, additional doses can be administered as 2 mg/kg qd for 3-4 d
Pediatric DoseAdminister as in adults
ContraindicationsIn pregnant women, only use in life-threatening toxicities
InteractionsNone reported
PregnancyC - Safety for use during pregnancy has not been established.
PrecautionsHigh incidence of adverse effects; 4 mg/kg dose is estimated to have a 14% chance of adverse reaction; reactions can include nausea, vomiting, burning sensation of mouth and eyes, lacrimation, rhinorrhea, salivation, burning of the extremities, dental pain, chest pain, anxiety, agitation, hypertension, and tachycardia; adverse effects usually peak 10-30 min after administration and usually subside within 1 h; treatment for BAL overdose is supportive

Drug Category: Analgesics

Pain is common and can be severe.

Drug NameMorphine sulphate (Duramorph, Astramorph, MS Contin)
DescriptionMechanism of action is via the opiate receptors.
Adult DoseStarting dose: 0.1 mg/kg IV/IM/SC
Maintenance dose: 5-20 mg/70 kg IV/IM/SC q4h
Pediatric DoseAdminister as in adults using weight-based dosing
ContraindicationsDocumented hypersensitivity; respiratory depression
InteractionsPhenothiazines may antagonize analgesic effects of opiate agonists; TCAs, MAOIs, and other CNS depressants may potentiate adverse effects of morphine
PregnancyC - Safety for use during pregnancy has not been established.
PrecautionsCaution in hypotension, respiratory depression, nausea, emesis, constipation, urinary retention, atrial flutter, and other supraventricular tachycardias; has vagolytic action and may increase ventricular response rate

Drug Category: Antipruritic agents

Cutaneous exposure can produce severe pruritus.

Drug NameDiphenhydramine (Benylin, Benadryl)
DescriptionFor symptomatic relief of symptoms caused by release of histamine in allergic reactions.
Adult Dose25-50 mg PO qid 10-50 mg IV, not to exceed 400 mg/d
Pediatric Dose5 mg/kg/d PO/IV divided qid
ContraindicationsDocumented hypersensitivity; neonates
InteractionsPotentiates effect of CNS depressants; due to alcohol content, do not give syrup dosage form to patient taking medications that can cause disulfiramlike reactions
PregnancyB - Usually safe but benefits must outweigh the risks.
PrecautionsMay exacerbate angle-closure glaucoma, hyperthyroidism, peptic ulcer, or urinary tract obstruction; xerostomia may occur

Drug Category: Antibiotics

Cutaneous damage caused by vesicants can leave the victim susceptible to bacterial infection.

Drug NameSilver sulfadiazine 1% (Silvadene)
DescriptionUseful in prevention of infections. Has bactericidal activity against many gram-positive and gram-negative bacteria, including yeast.
Adult DoseApply 1/16-inch thin film of ointment to cleansed and débrided burn wound bid; reapply if removed accidentally
Pediatric DoseAdminister as in adults
ContraindicationsDocumented hypersensitivity; neonates <2 mo and late pregnancy
InteractionsEffect of proteolytic enzymes is reduced when used concomitantly with this product; leukopenia increased with concomitant cimetidine
PregnancyB - Usually safe but benefits must outweigh the risks.
PrecautionsG-6-PD deficiency and impaired renal or hepatic function; not recommended in nursing mothers


FOLLOW-UP

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Further Inpatient Care

  • Victims of severe toxicity may require prolonged care for dermatologic, ophthalmic, and pulmonary sequelae.

Further Outpatient Care

  • Patients with only minor skin and eye lesions can be discharged with outpatient follow-up care.

Complications

  • Permanent discoloration can occur at blister sites, especially with PD.
  • Patients with mild conjunctival irritation can be expected to fully recover in 1-2 weeks. Patients with moderate conjunctival irritation with mild corneal damage can expect recovery in 4-6 weeks, but severe corneal damage may be irreversible, especially in PD exposure.
  • Victims who suffered mild-to-moderate pulmonary exposure can expect full recovery in 1-4 weeks. Severe vapor exposure can lead to permanent damage to the respiratory mucosa. This can lead to an increased risk of future infection and/or neoplasia. Secondary bacterial pneumonia is most common 3-6 days postexposure.
  • Victims with severe exposure to an organic arsenical can experience long-term complications in a number of organ systems, including neurologic, endocrine, and thermoregulatory disorders. The exact mechanism of these effects is unknown.

Prognosis

  • Prognosis is good in all but the most severe cases.

Patient Education


MISCELLANEOUS

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Medical/Legal Pitfalls

  • The use of BAL as an antidote for organic arsenical toxicity is sound medicolegal practice.


MULTIMEDIA

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Media file 1:  Chemical Terrorism Agents and Syndromes. Signs and symptoms. Chart courtesy of North Carolina Statewide Program for Infection Control and Epidemiology (SPICE), copyright University of North Carolina at Chapel Hill, www.unc.edu/depts/spice/chemical.html.
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Media type:  Image


REFERENCES

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  • Comptom JA. The arsenicals. In: Military Chemical and Biological Agents: Chemical and Toxicological Properties. 1987:17-43.
  • Devereaux A, Amundson DE, Parrish JS. Vesicants and nerve agents in chemical warfare. Decontamination and treatment strategies for a changed world. Postgrad Med. Oct 2002;112(4):90-6; quiz 4. [Medline].
  • Ford MD. Arsenic. In: Goldfrank's Toxicology Emergencies. 6th ed. 1998:1261-1270.
  • Ford MD. Metal and metalloids. In: Emergency Medicine: A Comprehensive Study Guide. 5th ed. 2000:1185-1191.
  • Karalliedde L, Wheeler H, Maclehose R, Murray V. Possible immediate and long-term health effects following exposure to chemical warfare agents. Public Health. Jul 2000;114(4):238-48. [Medline].
  • NATO. Blistering agents. In: Emergency War Surgery NATO Handbook. 2nd US revision. 1988:88-90.
  • Sidell FR, Urbanetti JS, Smith WJ. Vesicants. In: Medical Aspects of Chemical and Biological Warfare. 1997:197-228.

CBRNE - Vesicants, Organic Arsenicals: L, ED, MD, PD, HL excerpt

Article Last Updated: Jun 19, 2006