Phosgene oxime - Misplaced Pages

Phosgene oxime
Names

Carbon, C Hydrogen, H Oxygen, O Nitrogen, N Chlorine, Cl
Preferred IUPAC name 1,1-Dichloro-N-hydroxymethanimine
Other names CX Dichloroformaldehyde oxime Dichloroformaldoxime Dichloroformoxime Hydroxycarbonimidic dichloride
Identifiers
CAS Number	1794-86-1
3D model (JSmol)	Interactive image
ChemSpider	59024
PubChem CID	65582
UNII	G45S3149SQ
CompTox Dashboard (EPA)	DTXSID9075292
InChI InChI=1S/CHCl2NO/c2-1(3)4-5/h5HKey: JIRJHEXNDQBKRZ-UHFFFAOYSA-N InChI=1/CHCl2NO/c2-1(3)4-5/h5HKey: JIRJHEXNDQBKRZ-UHFFFAOYAP
SMILES Cl/C(Cl)=N\O
Properties
Chemical formula	Cl₂CNOH
Molar mass	113.93 g·mol
Appearance	colorless or white solid
Odor	Strong, disagreeable and irritating
Melting point	35 to 40 °C (95 to 104 °F; 308 to 313 K)
Boiling point	128 °C (262 °F; 401 K)
Solubility in water	70%
Hazards
Occupational safety and health (OHS/OSH):
Main hazards	Highly toxic
Related compounds
Related compounds	Formaldoxime Phosgene Oxime
Except where otherwise noted, data are given for materials in their standard state (at 25 °C , 100 kPa). N verify (what is ?) Infobox references

Chemical compound

Phosgene oxime, or CX, is an organic compound with the formula Cl₂C=N−O H. It is a potent chemical weapon, specifically a nettle agent. The compound itself is a colorless solid, but impure samples are often yellowish liquids. It has a strong, disagreeable and irritating odor. It is used as a reagent in organic chemistry.

Preparation and reactions

Phosgene oxime can be prepared by reduction of chloropicrin using a combination of tin metal and hydrochloric acid as the source of the active hydrogen reducing agent:

Cl₃CNO₂ + 4 [H] → Cl₂C=N−OH + HCl + H₂O

The observation of a transient violet color in the reaction suggests intermediate formation of trichloronitrosomethane (Cl₃CNO). Early preparations, using stannous chloride as the reductant, also started with chloropicrin.

The compound is electrophilic and thus sensitive to nucleophiles, including bases, which destroy it:

Cl₂CNOH + 2 NaOH → CO₂ + NH₂OH + 2 NaCl + H₂O

Phosgene oxime has been used to prepare heterocycles that contain N-O bonds, such as isoxazoles.

Dehydrohalogenation upon contact with mercuric oxide generates chlorine fulminate, a reactive nitrile oxide:

Cl₂CNOH → Cl−C≡N−O + HCl

Toxicity

Phosgene oxime is classified as a vesicant even though it does not produce blisters. It is toxic by inhalation, ingestion, or skin contact. The effects of the poisoning occur almost immediately. No antidote for phosgene oxime poisoning is known. Generally, any treatment is supportive. Typical physical symptoms of CX exposure are as follows:

Skin: Blanching surrounded by an erythematous ring can be observed within 30 seconds of exposure. A wheal develops on exposed skin within 30 minutes. The original blanched area acquires a brown pigmentation by 24 hours. An eschar forms in the pigmented area by 1 week and sloughs after approximately 3 weeks. Initially, the effects of CX can easily be misidentified as mustard gas exposure. However, the onset of skin irritation resulting from CX exposure is a great deal faster than mustard gas, which typically takes several hours or more to cause skin irritation.
Eyes: Eye examination typically demonstrates conjunctivitis, lacrimation, lid edema, and blepharospasm after even minute exposures. More severe exposures can result in keratitis, iritis, corneal perforation, and blindness.
Respiratory: Irritation of the mucous membranes may be observed on examination of the oropharynx and nose. Evidence of pulmonary edema, including rales and wheezes, may be noted on auscultation. Pulmonary thromboses are prominent features of severe CX exposure.
Gastrointestinal: Some animal data suggest that CX may cause hemorrhagic inflammatory changes in the GI tract.

References

^ ATSDR Medical Management Guidelines for Phosgene Oxime
Wang, Xinyan; Chen, Wenwen (2017). "Dichloroformaldehyde Oxime". Encyclopedia of Reagents for Organic Synthesis. pp. 1–2. doi:10.1002/047084289X.rn02011. ISBN 9780470842898.
Prandtl, W.; Dollfus, W. (1932). "Über das Trichlor-nitroso-methan, das Dichlor-formoxim (Phosgen-oxim) und einige ihrer Derivate, 2. Mitteilung: Über zwei neue Derivate der Kohlensäure". Berichte der Deutschen Chemischen Gesellschaft. 65B (5): 754–9. doi:10.1002/cber.19320650515.
Chen, Wenwen; Zhang, Jianlan; Wang, Bo; Zhao, Zhouxing; Wang, Xinyan; Hu, Yuefei (2015). "Tandem Synthesis of 3-Chloro-4-iodoisoxazoles from 1-Copper(I) Alkynes, Dichloroformaldoxime, and Molecular Iodine". The Journal of Organic Chemistry. 80 (4): 2413–2417. doi:10.1021/jo502634h. PMID 25594794.
Pasinszki, Tibor; Westwood, Nicholas P. C. (1998). "Unstable Chloronitrile Oxide, ClCNO, and Its Stable Ring Dimer: Generation, Spectroscopy, and Structure". The Journal of Physical Chemistry A. 102 (25): 4939–4947. Bibcode:1998JPCA..102.4939P. doi:10.1021/JP981262E.
McManus, J; Huebner, K (2005). "Vesicants". Critical Care Clinics. 21 (4): 707–718. doi:10.1016/j.ccc.2005.06.005. PMID 16168310.

External links

Blood agents

Blister agents

Arsenicals	Ethyldichloroarsine (ED) Methyldichloroarsine (MD) Phenyldichloroarsine (PD) Lewisite (L) Lewisite 2 (L2) Lewisite 3 (L3)
Sulfur mustards	Levinstein mustard (EA-229) T Q CEES
Nitrogen mustards	HN1 HN2 HN3 TL-301
Nettle agents	Phosgene oxime (CX)
Other	KB-16 Dibutylchloromethyltin chloride Selenium oxychloride

Nerve agents

G-agents	Tabun (GA) Sarin (GB) Chlorosarin (ClGB) Thiosarin (SGB) Soman (GD) Chlorosoman (ClGD) Ethylsarin (GE) GH Cyclosarin (GF) GP Fluorotabun EA-1356 EA-4352 Crotylsarin
V-agents	EA-2192 EA-3148 VE VG VM VP VR VS VX EA-1763 Chinese VX V-sub x (GD-7)
GV agents	GV (EA-5365)
Novichok agents	A-208 A-232 A-234 A-242 A-262 C01-A035 C01-A039 C01-A042
Carbamates	Dimethylcarbamoyl fluoride EA-3887 EA-3887A EA-3966 EA-3990 EA-4056 T-1123 T-1152 T-1194 Octamethylene-bis(5-dimethylcarbamoxyisoquinolinium bromide) TL-599 TL-1238 TL-1299 TL-1317 Miotine (AR-28/T-1843) 3152 CT 4-686-293-01 (Agent 1-10)
Other	Diisopropyl fluorophosphate Dicyclohexyl phosphorofluoridate EA-2012 EA-2054 EA-2098 EA-2613 2-Ethoxycarbonyl-1-methylvinyl cyclohexyl methylphosphonate Neopentylene fluorophosphate Selenophos Phospholine R-16661 Ro 3-0422 Methanesulfonyl fluoride Dimefox (TL-792) MSPI
Precursors	Acetonitrile AT ATO AlP A.P.C. complex Chlorosarin Chlorosoman Cyclohexanol 1,8-Dibromooctane N,N-Diisopropylaminoethanol (KB) EA-1250 DIHP ZS DEHP EA-1224 Dimethylamidophosphoric dichloride Dimethylamidophosphoric dicyanide DMHP Ethylphosphonoselenoic dichloride Formaldoxime Nital 4-Hydroxycoumarin Isopropyl alcohol (TB) Methyldichlorophosphine (SW) Methylphosphonyl difluoride (difluoro) (DF) Methylphosphonyl dichloride (dichloro) Nitromethane OPA mixture Phosphoryl chloride Phosphorus pentachloride Phosphorus trichloride (TH) Pinacolone Pinacolyl alcohol Phenacyl chloride QL 2,4,5-Trichlorophenol 3,3,5-Trimethylcyclohexanol Triethyl phosphite Trimethyl phosphite TC TG

Neurotoxins

Anatoxin-a
Saxitoxin (TZ)
Bungarotoxin
Botulinum toxin (BTX)
Tetanospasmin (TeNT)
Ryanodine
Ciguatoxin (CTX)
Guanitoxin (GTX)
Chlorophenylsilatrane
Palytoxin (PTX)
Maitotoxin (MTX)
Tetrodotoxin
Aconitine
Brevetoxin (PbTX)
Strychnine
Antillatoxin (ATX)
Tetraethyllead
Dimethylmercury
HN1 hydrochloride
HN2 hydrochloride
HN3 hydrochloride
A-8564
Picrotoxin
Sulfuryl fluoride
Tremorine
Oxotremorine
Batrachotoxin
Tetramethylenedisulfotetramine (TETS)
Bicyclic phosphates
- IPTBO
- TBPO
- TBPS
Cloflubicyne
Trimethylolpropane phosphite
Domoic acid

Pulmonary/
choking agents

Vomiting agents

Incapacitating
agents

Lachrymatory
agents

Malodorant agents

Cornea-clouding agents

Biological toxins

Other

Methyl fluoroacetate
Napalm (variants and mixtures)
Fluoroethyl fluoroacetate
Depleted uranium
- post-combustion uranium oxides
Plutonium and its compounds
Polonium
White phosphorus

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