ChemicalBook > Articles Catagory List >Organic-Chemistry >sodium-chloroacetate-uses-toxicity-data

Sodium chloroacetate:USES；TOXICITY DATA

Aug 12，2021

Sodium chloroacetate is a white to off-white crystalline powder with pungent smell,the melting Point is: 170 °C (338 °F). Decomposes slowly at 150 °C by localized heating.Sodium chloroacetate is stable at normal temperatures and pressures. Incompatible with oxidizing agents, reducing agents.

Article illustration

USES

Sodium chloroacetate is used as a contact herbicide and a component in other herbicides, an intermediate in the production of carboxymethyl-cellulose, and other synthetic organic chemicals.(2,3)

ANIMAL TOXICITY DATA

Acute Toxicity

1. Lethality Data Species Route LD50 mg/kg Rat Oral 76-580(2,3,9) Rat Dermal >2000 mg/kg(2,3) Mouse Oral 165-339(2,3,9) Golden Hamster Oral 245(2,3) Guinea Pig Oral 80-115(2,3,9) Rabbit Oral 156(2,3,9) In one study systemic effects to Sprague-Dawley rats (M/F, numbers per group not indicated) given single doses of sodium chloroacetate at 94, 282, or 470 mg/kg bw demonstrated increased sodium concentration in urine, increased potassium concentration in plasma, and reduced glutathione level in the liver at the highest dose; 2/3 of males died within 24 hours of treatment in the middle and high dose groups.

2. Eye Irritation A 25% aqueous solution of sodium chloroacetate was mildly irritating to eyes in rabbits. (2)

3. Skin Absorption Sodium chloroacetate has not been shown to be absorbed in toxicologically significant quantities through the skin.(2,3,10)

4. Skin Irritation Sodium chloroacetate was shown to be a non- to moderate skin irritant but not corrosive to the skin. (3,4,15)

5. Skin Sensitization Not indicated to be a sensitizer. (2,3) 6. Acute Inhalation Toxicity No cases of “acute intoxication from MCA (sodium salt)” have been located in the literature. (10)

Subchronic Toxicity

Sprague-Dawley rats were given repeated oral doses (by gavage) for 90 days at 0, 15, 30, 60, or 120 mg/kg/day (10 animals/dose). In the highest dose group, 80 % of males and 30% of females died. In both sexes of the 60 mg/kg/day group there were significant increases in liver and kidney weights. In all dose groups there were changes to hematological parameters, and numerous clinical chemistry parameters (increases in urea nitrogen, creatinine, calcium and phosphate, increases in ALT and AST in serum). In males of the 60 mg/kg/day dose group there was a significant increase in chronic nephropathy and spleen pigmentation as well as a dose-dependent increase in vacuolated hepatocytes. The LOAEL is concluded to be 15 mg/kg/day.(2,3,11)

Chronic Toxicity/Carcinogenicity

There was no evidence of carcinogenic activity in F344N rats or B6C3F mice at 15 or 30 mg/kg, or 50 or 100 mg/kg respectively in an NTP study using the parent compound monochloroacetic acid (MCA (CAS 79-11-8). Neither structurally similar MCA or sodium chloroacetate are considered likely potential human carcinogens. (10,12,13)

Reproductive/Developmental Toxicity

Rats (strain not indicated) were dosed by gavage with 17-140 mg/kg bw (0, 17, 35, 70, or 140 mg/kg sodium chloroacetate) on gestation days 6-15. The maternal NOEL was 17 mg/kg/day and the maternal NOAEL was 70 mg/kg/day (mean adjusted percentage bodyweight gain). Cardiovascular malformations, and other soft tissue malformations were seen at the high-dose group with no effects seen at other dose levels. (2)

Genotoxicity/Mutagenicity

Ames (TA 1535, 1537, 1538, 98, 100) bacterial test: was negative (+/- S9); HPRT/V79 CHL test was negative (+/-S9); Mice (Swiss strain) micronucleus test was negative.(2,5,10,14)

Metabolism/Pharmacokinetics

After absorption, monochloroacetic acid (parent compound CAS 79-11-8) is converted to thiodiacetic acid and glycolic acid and is accumulated in the liver and kidneys of rats.(10,15) Metabolism of sodium monochloroacetate is expected to have a similar pharmacokinetic profile.

HUMAN USE AND EXPERIENCE

There are a number of case studies of the parent compound, monochloroacetic acid (MCA), involving corrosion of skin and eyes and fatalities related to skin absorption of toxicologically significant amounts of MCA and a health-based target concentration of 0.1 mg/L was calculated for MCA in drinking water(10) although Health Canada and Environment Canada have categorized MCA as not entering the environment at levels that may be hazardous to human health. (16) There are, however, no similar data or epidemiological reports for sodium chloroacetate.(2–4)

REFERENCES

(1) International Programme on Chemical Safety (IPCS). ICSC 1449 - Sodium Chloroacetate http://www.inchem.org/documents/icsc/icsc/eics1449.htm (accessed Jan 20, 2016).

(2) OECD. OCED SIDS Program: Sodium Chloroacetate; Organization for Economic Cooperation and Development (OECD), UNEP Publications. Available at: http://www.inchem.org/documents/sids/sids/3926623.pdf, 1994.

(3) IUCLID. Sodium Chloroacetate; 1995.

(4) Franklin Research Center. Monohaloacetic Acids. Contract No. 210-79-0091; Franklin Research Center: Silver Spring, MD, 1980.

(5) German Chemical Society. Monochloracetic Acid CAS-No. 79-11-8, Sodium Monochloroacetate CAS-No. 3926-62-3. BUA Report 127; GDch-Advisory Committee on Existing Chemicals of Environmental Relevance: Germany, 1993.

(6) CHEMINFO. Sodium chloroacetate http://ccinfoweb2.ccohs.ca/cheminfo/records/5049E.html (accessed Jan 20, 2016).

(7) Regulatory Affairs Government of Canada; Transport Canada; Transport Dangerous Goods. Guide 151 http://wwwapps.tc.gc.ca/saf-sec-sur/3/erg gmu/erg/guidepage.aspx/guide151/id1817/mnid1973 (accessed Jan 20, 2016).

(8) U.S. Department of Transportation. 49 CFR 172.101 - Purpose and use of hazardous materials table. https://www.law.cornell.edu/cfr/text/49/172.101 (accessed Jan 20, 2016).

(9) RTECS. RTECS Number AG1400000- Acetic acid, chloro- , sodium salt http://ccinfoweb2.ccohs.ca/rtecs/records/AG1400000.html (accessed Jan 20, 2016).

(10) Health Canada Government of Canada. Guidelines for Canadian Drinking Water Quality http://www.hc-sc.gc.ca/ewhsemt/pubs/water-eau/sum_guide-res_recom/index-eng.php (accessed Jan 20, 2016).

(11) Daniel, F. B.; Robinson, M.; Stober, J. A.; Page, N. P.; Olson, G. R. Ninety-Day Toxicity Study of Sodium Monochloracetate in Sprague-Dawley Rats. Toxicology 1991, 67, 171–185.

(12) ECHA. Registration Dossier- Sodium Chloroacetate; European Chemical Agency (ECHA). Available at: http://echa.europa.eu/registration-dossier/-/registereddossier/14347, 2015.

(13) National Toxicology Program. Chemical Properties of CAS Registry Number: 79-11-8 http://tools.niehs.nih.gov/cebs3/ntpviews/index.cfm?action=test article.properties&cas_number=79-11-8 (accessed Jan 20, 2016).

(14) Federal Institute for Consumer Health Protection and Veterinary Medicine. ZEBET Registry of Cytotoxicity Data; German Centre for the Documentation and Validation of Alternative Methods., 2005; pp. 101–112.

(15) Dartsch, P. C.; Wolburg, H.; Makdessi, S. A.; Schiek, D.; Sweidan, H.; Kimmel, R.; Schmahl, F. W. Sodium Monochloroacetate Causes Cytotoxic Effects, an Increased Lactate and Pyruvate Level and Induces Ultra Structural and Cytoskeletal Alterations in Cultured Kidney and Liver Epithelial Cells. Hum. Exp. Toxicol. 2000, 19, 138–148.

(16) Environment Canada Government of Canada. Substances on the DSL http://www.ec.gc.ca/lcpecepa/eng/subs_list/DSL/DSLsearch.cfm (accessed Jan 20, 2016).

);