Diethyl phthalate

Diethyl phthalate (DEP) is a phthalate ester. It is a colourless liquid without significant odour but with a bitter disagreeable taste.

Diethyl phthalate^[1]

Names
Preferred IUPAC name Diethyl benzene-1,2-dicarboxylate
Other names Diethyl phthalate
Identifiers
CAS Number	84-66-2 Y
3D model (JSmol)	Interactive image
ChEBI	CHEBI:34698 Y
ChEMBL	ChEMBL388558 Y
ChemSpider	13837303 Y
ECHA InfoCard	100.001.409
KEGG	D03804 Y
PubChem CID	6781
UNII	UF064M00AF Y
CompTox Dashboard (EPA)	DTXSID50892134, DTXSID201024388 DTXSID7021780, DTXSID50892134, DTXSID201024388
InChI InChI=1S/C12H14O4/c1-3-15-11(13)9-7-5-6-8-10(9)12(14)16-4-2/h5-8H,3-4H2,1-2H3 Y Key: FLKPEMZONWLCSK-UHFFFAOYSA-N Y InChI=1/C12H14O4/c1-3-15-11(13)9-7-5-6-8-10(9)12(14)16-4-2/h5-8H,3-4H2,1-2H3 Key: FLKPEMZONWLCSK-UHFFFAOYAV
SMILES CCOC(=O)c1ccccc1C(=O)OCC
Properties
Chemical formula	C12H14O4
Molar mass	222.24 g/mol
Appearance	Colourless, oily liquid
Density	1.12 g/cm3 at 20 °C
Melting point	−4 °C (25 °F; 269 K)
Boiling point	295 °C (563 °F; 568 K)
Solubility in water	1080 mg/L at 25 °C
log P	2.42
Vapor pressure	0.002 mmHg (25 °C)[2]
Magnetic susceptibility (χ)	−127.5·10−6 cm3/mol
Hazards
NFPA 704 (fire diamond)	1 1 0
Flash point	161.1 °C (322.0 °F; 434.2 K)[2]
Explosive limits	0.7%, lower[2]
Lethal dose or concentration (LD, LC):
LD50 (median dose)	8600 mg/kg (rat)
NIOSH (US health exposure limits):
PEL (Permissible)	None[2]
REL (Recommended)	TWA 5 mg/m3[2]
IDLH (Immediate danger)	N.D.[2]
Except where otherwise noted, data are given for materials in their standard state (at 25 °C [77 °F], 100 kPa). Y verify (what is YN ?) Infobox references

Synthesis and applications

Diethyl phthalate is produced by the reaction of ethanol with phthalic anhydride, in the presence of a strong acid catalyst:

It finds some use as a specialist plasticiser in PVC, it has also been used as a blender and fixative in perfume.^[3]

Biodegradation

Biodegradation by microorganisms

Biodegradation of DEP in soil occurs by sequential hydrolysis of the two diethyl chains of the phthalate to produce monoethyl phthalate, followed by phthalic acid. This reaction occurs very slowly in an abiotic environment. Thus there exists an alternative pathway of biodegradation which includes transesterification or demethylation by microorganisms, if the soil is also contaminated with methanol, that would produce another three intermediate compounds, ethyl methyl phthalate, dimethyl phthalate and monomethyl phthalate. This biodegradation has been observed in several soil bacteria.^[4] Some bacteria with these abilities have specific enzymes involved in the degradation of phthalic acid esters such as phthalate oxygenase, phthalate dioxygenase, phthalate dehydrogenase and phthalate decarboxylase.^[5] The developed intermediates of the transesterification or demethylation, ethyl methyl phthalate and dimethyl phthalate, enhance the toxic effect and are able to disrupt the membrane of microorganisms.

Biodegradation by mammals

Recent studies show that DEP, a phthalic acid ester (PAE), is enzymatically hydrolyzed to its monoesters by pancreatic cholesterol esterase (CEase) in pigs and cows. These mammalian pancreatic CEases have been found to be nonspecific for degradation in relation to the diversity of the alkyl side chains of PAEs.^[5]

Toxicity

Little is known about the chronic toxicity of diethyl phthalate, but existing information suggests only a low toxic potential.^[6] Studies suggest that some phthalates affect male reproductive development via inhibition of androgen biosynthesis. In rats, for instance, repeated administration of DEP results in loss of germ cell populations in the testis. However, diethyl phthalate does not alter sexual differentiation in male rats.^{[7][8][9][10]} Dose response experiments in fiddler crabs have shown that seven-day exposure to diethyl phthalate at 50 mg/L significantly inhibited the activity of chitobiase in the epidermis and hepatopancreas.^[11] Chitobiase plays an important role in degradation of the old chitin exoskeleton during the pre-moult phase.^[12]

Teratogenicity

When pregnant rats were treated with diethyl phthalate, it became evident that certain doses caused skeletal malformations, whereas the untreated control group showed no resorptions. The amount of skeletal malformations was highest at highest dose.^[13] In a following study it was found that both phthalate diesters and their metabolic products were present in each of these compartments, suggesting that the toxicity in embryos and fetuses could be the result of a direct effect.^[14]

Future investigation

Some data suggest that exposure to multiple phthalates at low doses significantly increases the risk in a dose additive manner.^[15][16][17] Therefore, the risk from a mixture of phthalates or phthalates and other anti-androgens, may not be accurately assessed studying one chemical at a time. The same may be said about risks from several exposure routes together. Humans are exposed to phthalates by multiple exposure routes (predominantly dermal), while toxicological testing is done via oral exposure.^[18]