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Chromium toxicity

Chromium toxicity refers to any poisonous toxic effect in an organism or cell that results from exposure to specific forms of chromium—especially hexavalent chromium.[1] Hexavalent chromium and its compounds are toxic when inhaled or ingested. Trivalent chromium is a trace mineral that is essential to human nutrition. There is a hypothetical risk of genotoxicity in humans if large amounts of trivalent chromium were somehow able to enter living cells, but normal metabolism and cell function prevent this.[2]

Forms of chromium edit

Hexavalent chromium and trivalent chromium are chromium ions—they have different numbers of electrons and, therefore, different properties. Trivalent chromium, or chromium(III), is the form of chromium that is essential to human health.[3] Hexavalent chromium, or chromium(VI), is an unequivocally toxic form.

Hexavalent chromium edit

Hexavalent chromium, also called chromium(VI), is hemotoxic, genotoxic, and carcinogenic.[4] When hexavalent chromium enters the bloodstream, it damages blood cells by causing oxidation reactions. This oxidative damage can lead to hemolysis and, ultimately, kidney and liver failure. Patients might be treated with dialysis.[5]

The median lethal dose of hexavalent chromium is 50–150 mg/kg.[6] The World Health Organization recommends a maximum allowable concentration of 0.05 milligrams per litre of chromium(VI) in drinking water.[7] In Europe, the use of hexavalent chromium is regulated by the Restriction of Hazardous Substances Directive.

Hexavalent chromium can be found in some dyes and paints, as well as in some leather tanning products. Primer paint containing hexavalent chromium is widely used in aerospace and automobile refinishing applications. Metal workers (such as welders)—as well as people with a surgical implant made from cobalt-chromium alloy—may also be exposed to hexavalent chromium.[8] Chromium concentrations in whole blood, plasma, serum, or urine may be measured to monitor for safety in exposed workers, to confirm the diagnosis in potential poisoning victims, or to assist in the forensic investigation in a case of fatal overdosage.[9]

In the U.S. state of California, an epidemic of hexavalent chromium exposure led to a class-action lawsuit in 1993: Anderson, et al. v. Pacific Gas and Electric. The Pacific Gas and Electric Company had dumped more than 1.4 billion litres (370 million gallons) of wastewater tainted with hexavalent chromium into the Mojave Desert. This contaminated the groundwater, and caused widespread illness among the people of Hinkley, California, a small community nearby. As of May 2017, the mandated environmental remediation measures are ongoing.[10]

Chromate edit

Chromates (chromium salts) formed from hexavalent chromium are used to manufacture leather products, paints, cement, mortar, anti-corrosives, and other things.[11] They are carcinogenic and allergenic. The carcinogenity of chromate dust has been documented since the late 19th century, when workers in a chromate dye company were found to exhibit high incidence of cancer.[12][13] Chromate enters cells by means of the same transport mechanism that carries sulfate and phosphate ions into cells.

Contact with products containing chromates can lead to allergic contact dermatitis and irritant dermatitis, resulting in ulceration of the skin—a condition sometimes called chrome ulcers. Workers that have been exposed to strong chromate solutions in electroplating, tanning, and chrome-producing manufacturers may also develop chrome ulcers.[14][15][16]

Genotoxicity edit

Hexavalent chromium is genotoxic: it damages genetic information in living cells, which results in DNA mutations, and possibly the formation of cancerous tumors. As of 2021, the mechanism of the genotoxic action of chromium(VI) is understood to involve the formation of reactive oxygen species as it is reduced to Cr(III), as well as interactions between DNA and Cr(V)/(IV) intermediates in the metabolism of Cr(VI).[17] However, the carcinogenic potential of Cr intermediates and the mechanisms of Cr-induced carcinogenicity remain to be further defined.

The potential genotoxicity of chromium(III) has been explored in recent literature, and it has been observed in vitro generating hydroxyl radicals and binding to DNA; however, in vivo genotoxicity of Cr(III) is not well-established and the toxicity of Cr(III) compounds is generally considered to be at least 100 times lower than that of Cr(VI) compounds.[17] This is in part due to the fact that Cr(III) is not an anion and therefore, unlike Cr(VI) anions like chromate, cannot be transported across cell membranes by anion channels.

Trivalent chromium edit

Trivalent chromium, or chromium(III), is an essential trace mineral in the human diet.[3] In some nutritional supplements, chromium(III) occurs as chromium(III) picolinate (in which chromium is bound to picolinic acid) or chromium(III) nicotinate (in which chromium is bound to nicotinic acid). Nicotinic acid is also known as the B vitamin niacin.

Chromium(III) is poorly absorbed in humans; most dietary chromium is excreted in the urine.[18] The threshold for acute oral toxicity is 1900–3300 mg/kg.[6] In rats, nonsteroidal anti-inflammatory drugs such as aspirin and indometacin can increase chromium absorption.[19]

Ordinarily, cellular transport mechanisms in humans and some other animals limit the amount of chromium(III) that enters a cell. Hypothetically, if an excessive amount was able to enter a cell, free radical damage to DNA might result.[20]

References edit

  1. ^ "Chromium (Cr) Toxicity: What Are the Physiologic Effects of Chromium Exposure? | Environmental Medicine | ATSDR". www.atsdr.cdc.gov. 2021-02-09. Retrieved 2022-06-05.
  2. ^ Hartwig A, Arand M, Epe B, Guth S, Jahnke G, Lampen A, et al. (June 2020). "Mode of action-based risk assessment of genotoxic carcinogens". Archives of Toxicology. 94 (6): 1787–1877. doi:10.1007/s00204-020-02733-2. PMC 7303094. PMID 32542409.
  3. ^ a b Bogden JD, Klevay LM, eds. (2000). "Trace Elements and Minerals in the Elderly § Chromium". Clinical Nutrition of the Essential Trace Elements and Minerals: The Guide for Health Professionals. Springer Science+Business Media. p. 189. ISBN 978-1-61737-090-8 – via Google Books.
  4. ^ Barceloux DG (1999). "Chromium". Journal of Toxicology. Clinical Toxicology. 37 (2): 173–194. doi:10.1081/CLT-100102418. PMID 10382554.
  5. ^ Dayan AD, Paine AJ (September 2001). "Mechanisms of chromium toxicity, carcinogenicity and allergenicity: review of the literature from 1985 to 2000". Human & Experimental Toxicology. 20 (9): 439–451. doi:10.1191/096032701682693062. PMID 11776406. S2CID 31351037.
  6. ^ a b Katz SA, Salem H (1992). "The toxicology of chromium with respect to its chemical speciation: a review". Journal of Applied Toxicology. 13 (3): 217–224. doi:10.1002/jat.2550130314. PMID 8326093. S2CID 31117557.
  7. ^ "WHO Guidelines on Drinking-Water Quality" (PDF). WHO.int. World Health Organization. Section 12.30: Chromium.
  8. ^ Merritt K, Brown SA (May 1995). "Release of hexavalent chromium from corrosion of stainless steel and cobalt-chromium alloys". Journal of Biomedical Materials Research. 29 (5): 627–633. doi:10.1002/jbm.820290510. PMID 7622548.
  9. ^ Baselt R (2008). Disposition of Toxic Drugs and Chemicals in Man (8th ed.). Foster City: Biomedical Publications. pp. 305–7. ISBN 978-0962652370.
  10. ^ Izbicki JA, Groover K. "Natural and Man-Made Hexavalent Chromium, Cr(VI), in Groundwater near a Mapped Plume, Hinkley, California—Study Progress as of May 2017, and a Summative-Scale Approach to Estimate Background Cr(VI) Concentrations" (PDF). Open-file Report. United States Geological Survey. ISSN 2331-1258. Retrieved 2018-05-15.
  11. ^ Hedberg Y, Lidén C, Wallinder IO (March 2015). "Corrigendum to "Correlation between bulk- and surface chemistry of Cr-tanned leather and the release of Cr(III) and Cr(VI)" [J. Hazard. Mater. 280 (2014) 654–661]". Journal of Hazardous Materials. 285: 542. doi:10.1016/j.jhazmat.2014.12.062. ISSN 0304-3894.
  12. ^ Newman D (1890). "A case of adeno-carcinoma of the left inferior turbinated body, and perforation of the nasal septum, in the person of a worker in chrome pigments". Glasgow Medical Journal. 33: 469–470.
  13. ^ Langård S (1990). "One hundred years of chromium and cancer: a review of epidemiological evidence and selected case reports". American Journal of Industrial Medicine. 17 (2): 189–215. doi:10.1002/ajim.4700170205. PMID 2405656.
  14. ^ "Chrome Contact Allergy". DermNet NZ.
  15. ^ Basketter D, Horev L, Slodovnik D, Merimes S, Trattner A, Ingber A (February 2001). "Investigation of the threshold for allergic reactivity to chromium". Contact Dermatitis. 44 (2): 70–74. doi:10.1034/j.1600-0536.2001.440202.x. PMID 11205406. S2CID 45426346.
  16. ^ Basketter DA, Briatico-Vangosa G, Kaestner W, Lally C, Bontinck WJ (January 1993). "Nickel, cobalt and chromium in consumer products: a role in allergic contact dermatitis?". Contact Dermatitis. 28 (1): 15–25. doi:10.1111/j.1600-0536.1993.tb03318.x. PMID 8428439. S2CID 35966310.
  17. ^ a b Sawicka, E; Jurkowska, K; Piwowar, A (18 March 2021). "Chromium (III) and chromium (VI) as important players in the induction of genotoxicity - current view". Annals of Agricultural and Environmental Research. 28 (1): 1–10. doi:10.26444/aaem/118228. PMID 33775062.
  18. ^ "Chromium § Toxicity". Micronutrient Information Center. Oregon State University. 22 April 2014. Retrieved 2018-04-15.
  19. ^ "Chromium § Drug interactions". Micronutrient Information Center. Oregon State University. 22 April 2014. Retrieved 2018-04-15.
  20. ^ Eastmond DA, Macgregor JT, Slesinski RS (2008). "Trivalent chromium: assessing the genotoxic risk of an essential trace element and widely used human and animal nutritional supplement". Critical Reviews in Toxicology. 38 (3): 173–190. doi:10.1080/10408440701845401. PMID 18324515. S2CID 21033504.

External links edit

chromium, toxicity, refers, poisonous, toxic, effect, organism, cell, that, results, from, exposure, specific, forms, chromium, especially, hexavalent, chromium, hexavalent, chromium, compounds, toxic, when, inhaled, ingested, trivalent, chromium, trace, miner. Chromium toxicity refers to any poisonous toxic effect in an organism or cell that results from exposure to specific forms of chromium especially hexavalent chromium 1 Hexavalent chromium and its compounds are toxic when inhaled or ingested Trivalent chromium is a trace mineral that is essential to human nutrition There is a hypothetical risk of genotoxicity in humans if large amounts of trivalent chromium were somehow able to enter living cells but normal metabolism and cell function prevent this 2 Chromium toxicityChromiumSpecialtyToxicology Contents 1 Forms of chromium 1 1 Hexavalent chromium 1 1 1 Chromate 1 1 2 Genotoxicity 1 2 Trivalent chromium 2 References 3 External linksForms of chromium editHexavalent chromium and trivalent chromium are chromium ions they have different numbers of electrons and therefore different properties Trivalent chromium or chromium III is the form of chromium that is essential to human health 3 Hexavalent chromium or chromium VI is an unequivocally toxic form Hexavalent chromium edit Main article Hexavalent chromium Toxicity Hexavalent chromium also called chromium VI is hemotoxic genotoxic and carcinogenic 4 When hexavalent chromium enters the bloodstream it damages blood cells by causing oxidation reactions This oxidative damage can lead to hemolysis and ultimately kidney and liver failure Patients might be treated with dialysis 5 The median lethal dose of hexavalent chromium is 50 150 mg kg 6 The World Health Organization recommends a maximum allowable concentration of 0 05 milligrams per litre of chromium VI in drinking water 7 In Europe the use of hexavalent chromium is regulated by the Restriction of Hazardous Substances Directive Hexavalent chromium can be found in some dyes and paints as well as in some leather tanning products Primer paint containing hexavalent chromium is widely used in aerospace and automobile refinishing applications Metal workers such as welders as well as people with a surgical implant made from cobalt chromium alloy may also be exposed to hexavalent chromium 8 Chromium concentrations in whole blood plasma serum or urine may be measured to monitor for safety in exposed workers to confirm the diagnosis in potential poisoning victims or to assist in the forensic investigation in a case of fatal overdosage 9 In the U S state of California an epidemic of hexavalent chromium exposure led to a class action lawsuit in 1993 Anderson et al v Pacific Gas and Electric The Pacific Gas and Electric Company had dumped more than 1 4 billion litres 370 million gallons of wastewater tainted with hexavalent chromium into the Mojave Desert This contaminated the groundwater and caused widespread illness among the people of Hinkley California a small community nearby As of May 2017 the mandated environmental remediation measures are ongoing 10 Chromate edit See also Chromate and dichromate Toxicity Chromates chromium salts formed from hexavalent chromium are used to manufacture leather products paints cement mortar anti corrosives and other things 11 They are carcinogenic and allergenic The carcinogenity of chromate dust has been documented since the late 19th century when workers in a chromate dye company were found to exhibit high incidence of cancer 12 13 Chromate enters cells by means of the same transport mechanism that carries sulfate and phosphate ions into cells Contact with products containing chromates can lead to allergic contact dermatitis and irritant dermatitis resulting in ulceration of the skin a condition sometimes called chrome ulcers Workers that have been exposed to strong chromate solutions in electroplating tanning and chrome producing manufacturers may also develop chrome ulcers 14 15 16 Genotoxicity edit Hexavalent chromium is genotoxic it damages genetic information in living cells which results in DNA mutations and possibly the formation of cancerous tumors As of 2021 the mechanism of the genotoxic action of chromium VI is understood to involve the formation of reactive oxygen species as it is reduced to Cr III as well as interactions between DNA and Cr V IV intermediates in the metabolism of Cr VI 17 However the carcinogenic potential of Cr intermediates and the mechanisms of Cr induced carcinogenicity remain to be further defined The potential genotoxicity of chromium III has been explored in recent literature and it has been observed in vitro generating hydroxyl radicals and binding to DNA however in vivo genotoxicity of Cr III is not well established and the toxicity of Cr III compounds is generally considered to be at least 100 times lower than that of Cr VI compounds 17 This is in part due to the fact that Cr III is not an anion and therefore unlike Cr VI anions like chromate cannot be transported across cell membranes by anion channels Trivalent chromium edit See also Chromium deficiency Trivalent chromium or chromium III is an essential trace mineral in the human diet 3 In some nutritional supplements chromium III occurs as chromium III picolinate in which chromium is bound to picolinic acid or chromium III nicotinate in which chromium is bound to nicotinic acid Nicotinic acid is also known as the B vitamin niacin Chromium III is poorly absorbed in humans most dietary chromium is excreted in the urine 18 The threshold for acute oral toxicity is 1900 3300 mg kg 6 In rats nonsteroidal anti inflammatory drugs such as aspirin and indometacin can increase chromium absorption 19 Ordinarily cellular transport mechanisms in humans and some other animals limit the amount of chromium III that enters a cell Hypothetically if an excessive amount was able to enter a cell free radical damage to DNA might result 20 References edit Chromium Cr Toxicity What Are the Physiologic Effects of Chromium Exposure Environmental Medicine ATSDR www atsdr cdc gov 2021 02 09 Retrieved 2022 06 05 Hartwig A Arand M Epe B Guth S Jahnke G Lampen A et al June 2020 Mode of action based risk assessment of genotoxic carcinogens Archives of Toxicology 94 6 1787 1877 doi 10 1007 s00204 020 02733 2 PMC 7303094 PMID 32542409 a b Bogden JD Klevay LM eds 2000 Trace Elements and Minerals in the Elderly Chromium Clinical Nutrition of the Essential Trace Elements and Minerals The Guide for Health Professionals Springer Science Business Media p 189 ISBN 978 1 61737 090 8 via Google Books Barceloux DG 1999 Chromium Journal of Toxicology Clinical Toxicology 37 2 173 194 doi 10 1081 CLT 100102418 PMID 10382554 Dayan AD Paine AJ September 2001 Mechanisms of chromium toxicity carcinogenicity and allergenicity review of the literature from 1985 to 2000 Human amp Experimental Toxicology 20 9 439 451 doi 10 1191 096032701682693062 PMID 11776406 S2CID 31351037 a b Katz SA Salem H 1992 The toxicology of chromium with respect to its chemical speciation a review Journal of Applied Toxicology 13 3 217 224 doi 10 1002 jat 2550130314 PMID 8326093 S2CID 31117557 WHO Guidelines on Drinking Water Quality PDF WHO int World Health Organization Section 12 30 Chromium Merritt K Brown SA May 1995 Release of hexavalent chromium from corrosion of stainless steel and cobalt chromium alloys Journal of Biomedical Materials Research 29 5 627 633 doi 10 1002 jbm 820290510 PMID 7622548 Baselt R 2008 Disposition of Toxic Drugs and Chemicals in Man 8th ed Foster City Biomedical Publications pp 305 7 ISBN 978 0962652370 Izbicki JA Groover K Natural and Man Made Hexavalent Chromium Cr VI in Groundwater near a Mapped Plume Hinkley California Study Progress as of May 2017 and a Summative Scale Approach to Estimate Background Cr VI Concentrations PDF Open file Report United States Geological Survey ISSN 2331 1258 Retrieved 2018 05 15 Hedberg Y Liden C Wallinder IO March 2015 Corrigendum to Correlation between bulk and surface chemistry of Cr tanned leather and the release of Cr III and Cr VI J Hazard Mater 280 2014 654 661 Journal of Hazardous Materials 285 542 doi 10 1016 j jhazmat 2014 12 062 ISSN 0304 3894 Newman D 1890 A case of adeno carcinoma of the left inferior turbinated body and perforation of the nasal septum in the person of a worker in chrome pigments Glasgow Medical Journal 33 469 470 Langard S 1990 One hundred years of chromium and cancer a review of epidemiological evidence and selected case reports American Journal of Industrial Medicine 17 2 189 215 doi 10 1002 ajim 4700170205 PMID 2405656 Chrome Contact Allergy DermNet NZ Basketter D Horev L Slodovnik D Merimes S Trattner A Ingber A February 2001 Investigation of the threshold for allergic reactivity to chromium Contact Dermatitis 44 2 70 74 doi 10 1034 j 1600 0536 2001 440202 x PMID 11205406 S2CID 45426346 Basketter DA Briatico Vangosa G Kaestner W Lally C Bontinck WJ January 1993 Nickel cobalt and chromium in consumer products a role in allergic contact dermatitis Contact Dermatitis 28 1 15 25 doi 10 1111 j 1600 0536 1993 tb03318 x PMID 8428439 S2CID 35966310 a b Sawicka E Jurkowska K Piwowar A 18 March 2021 Chromium III and chromium VI as important players in the induction of genotoxicity current view Annals of Agricultural and Environmental Research 28 1 1 10 doi 10 26444 aaem 118228 PMID 33775062 Chromium Toxicity Micronutrient Information Center Oregon State University 22 April 2014 Retrieved 2018 04 15 Chromium Drug interactions Micronutrient Information Center Oregon State University 22 April 2014 Retrieved 2018 04 15 Eastmond DA Macgregor JT Slesinski RS 2008 Trivalent chromium assessing the genotoxic risk of an essential trace element and widely used human and animal nutritional supplement Critical Reviews in Toxicology 38 3 173 190 doi 10 1080 10408440701845401 PMID 18324515 S2CID 21033504 External links edit Retrieved from https en wikipedia org w index php title Chromium toxicity amp oldid 1199969062, wikipedia, wiki, book, books, library,

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