2,3,7,8-Tetrachlorodibenzodioxin

This is a good article. Click here for more information.
From Wikipedia, the free encyclopedia

2,3,7,8-Tetrachlorodibenzodioxin
Names
Preferred IUPAC name
2,3,7,8-Tetrachlorooxanthrene
Other names
2,3,7,8-Tetrachlorodibenzo[b,e][1,4]dioxine
Tetradioxin
Tetrachlorodibenzodioxin
Tetrachlorodibenzo-p-dioxin
Identifiers
3D model (JSmol)
Abbreviations TCDD; TCDBD
ChEBI
ChEMBL
ChemSpider
ECHA InfoCard 100.015.566 Edit this at Wikidata
KEGG
UNII
  • InChI=1S/C12H4Cl4O2/c13-5-1-9-10(2-6(5)14)18-12-4-8(16)7(15)3-11(12)17-9/h1-4H checkY
    Key: HGUFODBRKLSHSI-UHFFFAOYSA-N checkY
  • InChI=1/C12H4Cl4O2/c13-5-1-9-10(2-6(5)14)18-12-4-8(16)7(15)3-11(12)17-9/h1-4H
    Key: HGUFODBRKLSHSI-UHFFFAOYAA
  • ClC1=C(Cl)C=C2OC(C=C(C(Cl)=C3)Cl)=C3OC2=C1
Properties
C12H4Cl4O2
Molar mass 321.96 g·mol−1
Appearance Colorless to white crystalline solid[1]
Density 1.8 g/cm3
Melting point 305 °C (581 °F; 578 K)
0.2 μg/L[2]
log P 6.8
Vapor pressure 1.5 × 10−9 mmHg
Hazards
Occupational safety and health (OHS/OSH):
Main hazards
Developmental toxicant, Carcinogenic[1]
GHS labelling:
GHS02: Flammable GHS06: Toxic GHS08: Health hazard GHS09: Environmental hazard
Danger
H225, H304, H315, H336, H361, H373, H401, H410
P201, P202, P210, P233, P240, P241, P242, P243, P260, P264, P271, P273, P280, P301+P310, P303+P361+P353, P304+P340+P312, P308+P313, P331, P332+P313, P362+P364, P370+P378, P391, P403+P233, P403+P235, P405, P501
NFPA 704 (fire diamond)
NFPA 704 four-colored diamondHealth 4: Very short exposure could cause death or major residual injury. E.g. VX gasFlammability 1: Must be pre-heated before ignition can occur. Flash point over 93 °C (200 °F). E.g. canola oilInstability 0: Normally stable, even under fire exposure conditions, and is not reactive with water. E.g. liquid nitrogenSpecial hazards (white): no code
4
1
0
Flash point 164.2 °C (327.6 °F; 437.3 K)
NIOSH (US health exposure limits):
PEL (Permissible)
none[1]
REL (Recommended)
Ca[1]
IDLH (Immediate danger)
N.D.[1]
Safety data sheet (SDS) MSDS
Except where otherwise noted, data are given for materials in their standard state (at 25 °C [77 °F], 100 kPa).
☒N verify (what is checkY☒N ?)

2,3,7,8-Tetrachlorodibenzo-p-dioxin (TCDD) is a polychlorinated dibenzo-p-dioxin (sometimes shortened, though inaccurately, to simply 'dioxin')[3] with the chemical formula C12H4Cl4O2. Pure TCDD is a colorless solid with no distinguishable odor at room temperature. It is usually formed as an unwanted product in burning processes of organic materials or as a side product in organic synthesis.

TCDD is the most potent compound (congener) of its series (polychlorinated dibenzodioxins, known as PCDDs or simply dioxins) and became known as a contaminant in Agent Orange, a herbicide used in the Vietnam War.[4] TCDD was released into the environment in the Seveso disaster.[5] It is a persistent organic pollutant.

Biological Activity in Human and Animals[edit]

TCDD and dioxin-like compounds act via a specific receptor present in all cells: the aryl hydrocarbon (AH) receptor.[6][7][8] This receptor is a transcription factor which is involved in the expression of genes; it has been shown that high doses of TCDD either increase or decrease the expression of several hundred genes in rats.[9] Genes of enzymes activating the breakdown of foreign and often toxic compounds are classic examples of such genes (enzyme induction). TCDD increases the enzymes breaking down, e.g., carcinogenic polycyclic hydrocarbons such as benzo(a)pyrene.[10]

These polycyclic hydrocarbons also activate the AH receptor, but less than TCDD and only temporarily.[10] Even many natural compounds present in vegetables cause some activation of the AH receptor.[11][12] This phenomenon can be viewed as adaptive and beneficial, because it protects the organism from toxic and carcinogenic substances. Excessive and persistent stimulation of AH receptor, however, leads to a multitude of adverse effects.[10]

The physiological function of the AH receptor has been the subject of continuous research.[13] One obvious function is to increase the activity of enzymes breaking down foreign chemicals or normal chemicals of the body as needed. There seem to be many other functions, however, related to the development of various organs and the immune systems or other regulatory functions.[13] The AH receptor is phylogenetically highly conserved, with a history of at least 600 million years, and is found in all vertebrates. Its ancient analogs are important regulatory proteins even in more primitive species.[8] In fact, knock-out animals with no AH receptor are prone to illness and developmental problems.[8] Taken together, this implies the necessity of a basal degree of AH receptor activation to achieve normal physiological function.

Toxicity in humans[edit]

In 2000, the Expert Group of the World Health Organization considered developmental toxicity as the most pertinent risk of dioxins to human beings.[14] Because people are usually exposed simultaneously to several dioxin-like chemicals, a more detailed account is given at dioxins and dioxin-like compounds.

Developmental effects[edit]

In Vietnam and the United States, teratogenic or birth defects were observed in children of people who were exposed to Agent Orange or 2,4,5-T that contained TCDD as an impurity out of the production process. However there has been some uncertainty on the causal link between Agent Orange/dioxin exposure. In 2006 a meta-analysis indicated large amount of heterogeneity between studies and emphasized a lack of consensus on the issue.[15] Still-births, cleft palate, and neural tube defects, with spina bifida were the most statistically significant defects. Later some tooth defects and borderline neurodevelopmental effects have been reported.[3] After the Seveso accident tooth development defects, changed sex ratio and decreased sperm quality have been noted.[3] Various developmental effects have been clearly shown after high mixed exposures to dioxins and dioxin-like compounds, the most dramatic in Yusho and Yu-chen catastrophes, in Japan and Taiwan, respectively.[3]

Cancer[edit]

It is largely agreed that TCDD is not directly mutagenic or genotoxic.[16] Its main action is cancer promotion; it promotes the carcinogenicity initiated by other compounds. Very high doses may, in addition, cause cancer indirectly; one of the proposed mechanisms is oxidative stress and the subsequent oxygen damage to DNA.[17] There are other explanations such as endocrine disruption or altered signal transduction.[16][18] The endocrine disrupting activities seem to be dependent on life stage, being anti-estrogenic when estrogen is present (or in high concentration) in the body, and estrogenic in the absence of estrogen.[19]

TCDD was classified by the International Agency for Research on Cancer as a carcinogen for humans (group 1).[20][21] In the occupational cohort studies available for the classification, the risk was weak and borderline detectable, even at very high exposures.[22][23][3] Therefore, the classification was, in essence, based on animal experiments and mechanistic considerations.[20] This was criticized as a deviation from IARC's 1997 classification rules.[24] The main problem with IARC classification is that it only assesses qualitative hazard, i.e. carcinogenicity at any dose, and not the quantitative risk at different doses.[3] According to a 2006 Molecular Nutrition & Food Research article, there were debates on whether TCDD was carcinogenic only at high doses which also cause toxic damage of tissues.[16][17][25] A 2011 review concluded that, after 1997, further studies did not support an association between TCDD exposure and cancer risk.[26] One of the problems is that in all occupational studies the subjects have been exposed to a large number of chemicals, not only TCDD. By 2011, it was reported that studies that include the update of Vietnam veteran studies from Operation Ranch Hand, had concluded that after 30 years the results did not provide evidence of disease.[27] On the other hand, the latest studies on Seveso population support TCDD carcinogenicity at high doses.[19][28]

In 2004, an article in the International Journal of Cancer provided some direct epidemiological evidence that TCDD or other dioxins are not causing soft-tissue sarcoma at low doses, although this cancer has been considered typical for dioxins. There was in fact a trend of cancer to decrease.[29] This is called a J-shape dose-response, low doses decrease the risk, and only higher doses increase the risk, according to a 2005 article in the journal Dose-Response.[30]

Safety recommendations[edit]

The Joint FAO/WHO Expert Committee on Food Additives (JECFA) derived in 2001 a provisional tolerable monthly intake (PTMI) of 70 pg TEQ/kg body weight.[31] The United States Environmental Protection Agency (EPA) established an oral reference dose (RfD) of 0.7 pg/kg b.w. per day for TCDD[32] (see discussion on the differences in[3]). According to the Aspen Institute, in 2011, "The general environmental limit in most countries is 1,000 ppt TEq in soils and 100 ppt in sediment. Most industrialized countries have dioxin concentrations in soils of less than 12 ppt. The U.S. Agency for Toxic Substance and Disease Registry has determined that levels higher than 1,000 ppt TEq in soil require intervention, including research, surveillance, health studies, community and physician education, and exposure investigation. The EPA is considering reducing these limits to 72 ppt TEq. This change would significantly increase the potential volume of contaminated soil requiring treatment."[33][34]

Animal toxicology[edit]

By far most information on toxicity of dioxin-like chemicals is based on animal studies utilizing TCDD.[4][8][35][36] Almost all organs are affected by high doses of TCDD. In short-term toxicity studies in animals, the typical effects are anorexia and wasting, and even after a huge dose animals die only 1 to 6 weeks after the TCDD administration.[36] Seemingly similar species have varying sensitivities to acute effects: lethal dose for a guinea pig is about 1 μg/kg, but to a hamster it is more than 1,000 μg/kg. A similar difference can be seen even between two different rat strains.[36] Various hyperplastic (overgrowth) or atrophic (wasting away) responses are seen in different organs, thymus atrophy is very typical in several animal species. TCDD also affects the balance of several hormones. In some species, but not in all, severe liver toxicity is seen.[8][36] Taking into account the low doses of dioxins in the present human population, only two types of toxic effects have been considered to cause a relevant risk to humans: developmental effects and cancer.[3][8]

Developmental effects[edit]

Developmental effects occur at very low doses in animals. They include frank teratogenicity such as cleft palate and hydronephrosis.[37] Development of some organs may be even more sensitive: very low doses perturb the development of sexual organs in rodents,[37][38][39] and the development of teeth in rats.[40] The latter is important in that tooth deformities were also seen after the Seveso accident[41] and possibly after a long breast-feeding of babies in the 1970s and 1980s when the dioxin concentrations in Europe were about ten times higher than at present.[42]

Cancer[edit]

Cancers can be induced in animals at many sites. At sufficiently high doses TCDD has caused cancer in all animals tested. The most sensitive is liver cancer in female rats, and this has long been a basis for risk assessment.[43] Dose-response of TCDD in causing cancer does not seem to be linear,[25] and there is a threshold below which it seems to cause no cancer. TCDD is not mutagenic or genotoxic, in other words, it is not able to initiate cancer, and the cancer risk is based on promotion[16] of cancer initiated by other compounds or on indirect effects such as disturbing defense mechanisms of the body e.g. by preventing apoptosis or programmed death of altered cells.[23][7] Carcinogenicity is associated with tissue damage, and it is often viewed now as secondary to tissue damage.[16]

TCDD may in some conditions potentiate the carcinogenic effects of other compounds. An example is benzo(a)pyrene that is metabolized in two steps, oxidation and conjugation. Oxidation produces epoxide carcinogens that are rapidly detoxified by conjugation, but some molecules may escape to the nucleus of the cell and bind to DNA causing a mutation, resulting in cancer initiation. When TCDD increases the activity of oxidative enzymes more than conjugation enzymes, the epoxide intermediates may increase, increasing the possibility of cancer initiation. Thus a beneficial activation of detoxifying enzymes may lead to deleterious side effects.[44]

Sources[edit]

TCDD has never been produced commercially except as a pure chemical for scientific research. It is, however, formed as a synthesis side product when producing certain chlorophenols or chlorophenoxy acid herbicides.[45] It may also be formed along with other polychlorinated dibenzodioxins and dibenzofuranes in any burning of hydrocarbons where chlorine is present, especially if certain metal catalysts such as copper are also present.[46] Usually a mixture of dioxin-like compounds is produced,[3] therefore a more thorough treatise is under dioxins and dioxin-like compounds.

The greatest production occurs from waste incineration, metal production, and fossil-fuel and wood combustion.[47] Dioxin production can usually be reduced by increasing the combustion temperature. Total U.S. emissions of PCCD/Fs were reduced from ca. 14 kg TEq in 1987 to 1.4 kg TEq in 2000.[48]

Cases of exposure[edit]

A photograph of Viktor Yushchenko after he was poisoned by TCDD. TCDD often causes disfiguring facial swelling

There have been numerous incidents where people have been exposed to high doses of TCDD.

  • In 1976, thousands of inhabitants of Seveso, Italy were exposed to TCDD after an accidental release of several kilograms of TCDD from a pressure tank. Many animals died, and high concentrations of TCDD, up to 56,000 pg/g of fat, were noted especially in children playing outside and eating local food. The acute effects were limited to about 200 cases of chloracne.[49] Long-term effects seem to include a slight excess of multiple myeloma and myeloid leukaemia,[19] as well as some developmental effects such as disturbed development of teeth[41] and excess of girls born to fathers who were exposed as children.[50] Several other long-term effects have been suspected, but the evidence is not very strong.[5]
  • In Times Beach, Missouri, several hundred people were poisoned by extremely high concentrations of TCDD by Russell Martin Bliss, who sprayed TCDD-contaminated waste oil on dusty roads to avoid large dust clouds. Bliss himself obtained the waste oil from NEPACCO, a company that produced Agent Orange. No one was ever charged in relation to the incident, and the city of Times Beach was abandoned and disincorporated following an investigation by the CDC and EPA. This is marked as the single largest contamination of a civilian area by TCDD in United States history.
  • In Vienna, two women were poisoned at their workplace in 1997, and the measured concentrations in one of them were the highest ever measured in a human being, 144,000 pg/g of fat. This is about 100,000 times the concentrations in most people today and about 10,000 times the sum of all dioxin-like compounds in young people today. They survived but suffered from difficult chloracne for several years. The poisoning likely happened in October 1997 but was not discovered until April 1998. At the institute where the women worked as secretaries, high concentrations of TCDD were found in one of the labs, suggesting that the compound had been produced there. The police investigation failed to find clear evidence of crime, and no one was ever prosecuted. Aside from malaise and amenorrhea there were few other symptoms or abnormal laboratory findings.[51]
  • In 2004, presidential candidate Viktor Yushchenko of Ukraine was poisoned with a large dose of TCDD. His blood TCDD concentration was measured 108,000 pg/g of fat,[52] which is the second highest ever measured. This concentration implies a dose exceeding 2 mg, or 25 μg/kg of body weight. He suffered from chloracne for many years, but after initial malaise, other symptoms or abnormal laboratory findings were few.[52]
  • An area of polluted land in Italy, known as the Triangle of Death, is contaminated with TCDD from years of illegal waste disposal by organized crime.[53][54][55]

See also[edit]

References[edit]

  1. ^ a b c d e NIOSH Pocket Guide to Chemical Hazards. "#0594". National Institute for Occupational Safety and Health (NIOSH).
  2. ^ Shiu WY; et al. (1988). "Physical-chemical properties of chlorinated dibenzo-p-dioxins". Environ Sci Technol. 22 (6): 651–658. Bibcode:1988EnST...22..651S. doi:10.1021/es00171a006. S2CID 53459209.
  3. ^ a b c d e f g h i Tuomisto, Jouko (2019) Dioxins and dioxin-like compounds: toxicity in humans and animals, sources, and behaviour in the environment. WikiJournal of Medicine 6(1): 8 | https://doi.org/10.15347/wjm/2019.008
  4. ^ a b Schecter A, Birnbaum L, Ryan JJ, Constable JD (2006). "Dioxins: an overview". Environ. Res. 101 (3): 419–28. Bibcode:2006ER....101..419S. doi:10.1016/j.envres.2005.12.003. PMID 16445906.
  5. ^ a b M.H. Sweeney; P. Mocarelli (2000). "Human health effects after exposure to 2,3,7,8- TCDD". Food Addit. Contam. 17 (4): 303–316. doi:10.1080/026520300283379. PMID 10912244. S2CID 11814994.
  6. ^ L. Poellinger (2000). "Mechanistic aspects—the dioxin (aryl hydrocarbon) receptor". Food Additives and Contaminants. 17 (4): 261–6. doi:10.1080/026520300283333. PMID 10912240. S2CID 22295283.
  7. ^ a b Mandal PK (May 2005). "Dioxin: a review of its environmental effects and its aryl hydrocarbon receptor biology". J. Comp. Physiol. B. 175 (4): 221–30. doi:10.1007/s00360-005-0483-3. PMID 15900503. S2CID 20508397.
  8. ^ a b c d e f J. Lindén; S. Lensu; J. Tuomisto; R. Pohjanvirta. (2010). "Dioxins, the aryl hydrocarbon receptor and the central regulation of energy balance. A review". Frontiers in Neuroendocrinology. 31 (4): 452–478. doi:10.1016/j.yfrne.2010.07.002. PMID 20624415. S2CID 34036181.
  9. ^ Tijet N, Boutros PC, Moffat ID, et al. (2006). "Hydrocarbon receptor regulates distinct dioxin-dependent and dioxin-independent gene batteries". Molecular Pharmacology. 69 (1): 140–153. doi:10.1124/mol.105.018705. PMID 16214954. S2CID 1913812.
  10. ^ a b c Okey AB (July 2007). "An aryl hydrocarbon receptor odyssey to the shores of toxicology: the Deichmann Lecture, International Congress of Toxicology-XI". Toxicol. Sci. 98 (1): 5–38. doi:10.1093/toxsci/kfm096. PMID 17569696.
  11. ^ Mandlekar S, Hong JL, Kong AN (August 2006). "Modulation of metabolic enzymes by dietary phytochemicals: a review of mechanisms underlying beneficial versus unfavorable effects". Curr. Drug Metab. 7 (6): 661–75. doi:10.2174/138920006778017795. PMID 16918318.
  12. ^ DeGroot, Danica; He, Guochun; Fraccalvieri, Domenico; Bonati, Laura; Pandini, Allesandro; Denison, Michael S. (2011). "AHR Ligands: Promiscuity in Binding and Diversity in Response". The AH Receptor in Biology and Toxicology. John Wiley & Sons, Ltd. pp. 63–79. doi:10.1002/9781118140574.ch4. ISBN 9781118140574.
  13. ^ a b Rothhammer, V; Quintana, FJ (March 2019). "The aryl hydrocarbon receptor: an environmental sensor integrating immune responses in health and disease". Nature Reviews. Immunology. 19 (3): 184–197. doi:10.1038/s41577-019-0125-8. PMID 30718831. S2CID 59603271.
  14. ^ "Consultation on assessment of the health risk of dioxins: re-evaluation of the tolerable daily intake (TDI): Executive summary". Food Additives & Contaminants. 17 (4): 223–240. 2000. doi:10.1080/713810655. PMID 10912238. S2CID 216644694.
  15. ^ Ngo, Anh D; Taylor, Richard; Roberts, Christine L; Nguyen, Tuan V (2006). "Association between Agent Orange and birth defects: Systematic review and meta-analysis". International Journal of Epidemiology. 35 (5): 1220–1230. doi:10.1093/ije/dyl038. PMID 16543362.
  16. ^ a b c d e Y.P. Dragan; D. Schrenk (2000). "Animal studies addressing the carcinogenicity of TCDD (or related compounds) with an emphasis on tumour promotion". Food Additives and Contaminants. 17 (4): 289–302. doi:10.1080/026520300283360. PMID 10912243. S2CID 24500449.
  17. ^ a b M. Viluksela; et al. (2000). "Liver tumor-promoting activity of 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD) in TCDD-sensitive and TCDD resistant rat strains". Cancer Res. 60 (24): 6911–620. PMID 11156390.
  18. ^ Knerr S, Schrenk D (October 2006). "Carcinogenicity of 2,3,7,8-tetrachlorodibenzo-p-dioxin in experimental models". Mol Nutr Food Res. 50 (10): 897–907. doi:10.1002/mnfr.200600006. PMID 16977593.
  19. ^ a b c Angela Cecilia Pesatori; Dario Consonni; Maurizia Rubagotti; Paolo Grillo; Pier Alberto Bertazzi (2009). "Cancer incidence in the population exposed to dioxin after the "Seveso accident": twenty years of follow-up". Environmental Health. 8 (1): 39. Bibcode:2009EnvHe...8...39P. doi:10.1186/1476-069X-8-39. PMC 2754980. PMID 19754930.
  20. ^ a b International Agency for Research on Cancer (1997). Polychlorinated dibenzo-para-dioxins and polychlorinated dibenzofurans. Monographs on the Evaluation of Carcinogenic Risks to Humans. Vol. 69. Lyon: IARC. ISBN 978-92-832-1269-0.
  21. ^ IARC Working Group on the Evaluation of Carcinogenic Risk to Humans (2012). 2,3,7,8-tetrachlorodibenzopara-dioxin, 2,3,4,7,8-pentachlorodibenzofuran, and 3,3',4,4',5-pentachlorobiphenyl. Vol. 100F. International Agency for Research on Cancer. pp. 339–378.
  22. ^ Kogevinas M, Becher H, Benn T, Bertazzi PA, Boffetta P, Bueno-de-Mesquita HB, Coggon D, Colin D, Flesch-Janys D, Fingerhut M, Green L, Kauppinen T, Littorin M, Lynge E, Mathews JD, Neuberger M, Pearce N, Saracci R (1997). "Cancer mortality in workers exposed to phenoxy herbicides, chlorophenols, and dioxins". Am J Epidemiol. 145 (12): 1061–1075. doi:10.1093/oxfordjournals.aje.a009069. PMID 9199536.
  23. ^ a b Schwarz M, Appel KE (October 2005). "Carcinogenic risks of dioxin: mechanistic considerations". Regul. Toxicol. Pharmacol. 43 (1): 19–34. doi:10.1016/j.yrtph.2005.05.008. PMID 16054739.
  24. ^ Cole P, Trichopoulos D, Pastides H, Starr T, Mandel JS (December 2003). "Dioxin and cancer: a critical review". Regul. Toxicol. Pharmacol. 38 (3): 378–388. doi:10.1016/j.yrtph.2003.08.002. PMID 14623487.
  25. ^ a b Walker NJ, Wyde ME, Fischer LJ, Nyska A, Bucher JR (October 2006). "Comparison of chronic toxicity and carcinogenicity of 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD) in 2-year bioassays in female Sprague-Dawley rats". Mol Nutr Food Res. 50 (10): 934–944. doi:10.1002/mnfr.200600031. PMC 1934421. PMID 16977594.
  26. ^ Boffetta P, Mundt KA, Adami HO, Cole P, Mandel JS (August 2011). "TCDD and cancer: a critical review of epidemiologic studies". Crit. Rev. Toxicol. 41 (7): 622–636. doi:10.3109/10408444.2011.560141. PMC 3154583. PMID 21718216.
  27. ^ Buffler PA, Ginevan ME, Mandel JS, Watkins DK (September 2011). "The Air Force health study: an epidemiologic retrospective". Ann Epidemiol. 21 (9): 673–687. doi:10.1016/j.annepidem.2011.02.001. PMID 21441038.
  28. ^ Warner, M; Mocarelli, P; Samuels, S; Needham, L; Brambilla, P; Eskenazi, B (December 2011). "Dioxin exposure and cancer risk in the Seveso Women's Health Study". Environmental Health Perspectives. 119 (12): 1700–1705. doi:10.1289/ehp.1103720. PMC 3261987. PMID 21810551.
  29. ^ J.T. Tuomisto; J. Pekkanen; H. Kiviranta; E. Tukiainen; T. Vartiainen; J. Tuomisto (2004). "Soft-tissue sarcoma and dioxin: a case-control study". Int. J. Cancer. 108 (6): 893–900. doi:10.1002/ijc.11635. PMID 14712494.
  30. ^ Tuomisto, J.; et al. (2005). "Dioxin cancer risk –example of hormesis?". Dose-Response. 3 (3): 332–341. doi:10.2203/dose-response.003.03.004. PMC 2475943. PMID 18648613.
  31. ^ Malisch R, Kotz A (2014). "Dioxins and PCBs in feed and food – review from European perspective". The Science of the Total Environment. 491: 2–10. Bibcode:2014ScTEn.491....2M. doi:10.1016/j.scitotenv.2014.03.022. PMID 24804623.
  32. ^ Rice, Glenn. "EPA's Reanalysis of Key Issues Related to Dioxin Toxicity and Response to NAS Comments (External Review Draft)". cfpub.epa.gov. US EPA National Center for Environmental Assessment,Cincinnati Oh. Retrieved 16 December 2019.
  33. ^ "Health Effects". The Aspen Institute. August 2011. Retrieved 23 September 2019.
  34. ^ "Toxic Substances Portal" (PDF).
  35. ^ A. Poland; J.C. Knutson (1982). "2,3,7,8-Tetrachlorodibenzo-p-dioxin and related halogenated aromatic hydrocarbons: examination of the mechanism of toxicity". Annu. Rev. Pharmacol. Toxicol. 22 (1): 517–554. doi:10.1146/annurev.pa.22.040182.002505. PMID 6282188.
  36. ^ a b c d R. Pohjanvirta; J. Tuomisto (1994). "Short-term toxicity of 2,3,7,8-tetrachlorodibenzop-dioxin in laboratory animals: effects, mechanisms, and animal models". Pharmacol. Rev. 46 (4): 483–549. PMID 7899475.
  37. ^ a b L.S. Birnbaum; J. Tuomisto (2000). "Non-carcinogenic effects of TCDD in animals". Food Addit. Contam. 17 (4): 275–288. doi:10.1080/026520300283351. PMID 10912242. S2CID 45117354.
  38. ^ T.A. Mably; D.L. Bjerke; R.W. Moore; A. Gendron-Fitzpatrick; R.E. Peterson (1992). "In utero and lactational exposure of male rats to 2,3,7,8-tetrachlorodibenzo-pdioxin. 3. Effects on spermatogenesis and reproductive capability". Toxicol. Appl. Pharmacol. 114 (1): 118–126. doi:10.1016/0041-008X(92)90103-Y. PMID 1585364.
  39. ^ L.E. Gray; J.S. Ostby; W.R. Kelce (1997). "A dose-response analysis of the reproductive effects of a single gestational dose of 2,3,7,8-tetrachlorodibenzo-p-dioxin in male Long Evans Hooded rat offspring". Toxicol. Appl. Pharmacol. 146 (1): 11–20. doi:10.1006/taap.1997.8223. PMID 9299592.
  40. ^ H. Kattainen; et al. (2001). "In utero/lactational 2,3,7,8- tetrachlorodibenzo-p-dioxin exposure impairs molar tooth development in rats". Toxicol. Appl. Pharmacol. 174 (3): 216–224. doi:10.1006/taap.2001.9216. PMID 11485382.
  41. ^ a b S. Alaluusua; et al. (2004). "Developmental dental aberrations after the dioxin accident in Seveso". Environ. Health Perspect. 112 (13): 1313–1318. doi:10.1289/ehp.6920. PMC 1247522. PMID 15345345.
  42. ^ S. Alaluusua; P.L. Lukinmaa; J. Torppa; J. Tuomisto; T. Vartiainen (1999). "Developing teeth as biomarker of dioxin exposure". Lancet. 353 (9148): 206. doi:10.1016/S0140-6736(05)77214-7. PMID 9923879. S2CID 31562457.
  43. ^ R.J. Kociba; et al. (1978). "Results of a two-year chronic toxicity and oncogenicity study of 2,3,7,8- tetrachlorodibenzo-p-dioxin in rats". Toxicol. Appl. Pharmacol. 46 (2): 279–303. doi:10.1016/0041-008X(78)90075-3. PMID 734660.
  44. ^ Pitot III, H. C.; Dragan, Y. P. (2001). "Chemical carcinogenesis". In Klaassen, C. D. (ed.). Casarett & Doull's Toxicology: the basic science of poisons (6th ed.). New York: McGraw-Hill. pp. 201–267. ISBN 978-0-07-134721-1.
  45. ^ Saracci, R.; Kogevinas, M.; Winkelmann, R.; Bertazzi, P. A.; Bueno De Mesquita, B. H.; Coggon, D.; Green, L. M.; Kauppinen, T.; l'Abbé, K. A.; Littorin, M.; Lynge, E.; Mathews, J. D.; Neuberger, M.; Osman, J.; Pearce, N. (1991). "Cancer mortality in workers exposed to chlorophenoxy herbicides and chlorophenols". The Lancet. 338 (8774): 1027–1032. doi:10.1016/0140-6736(91)91898-5. PMID 1681353. S2CID 23115128.
  46. ^ Harnly, M.; Stephens, R.; McLaughlin, C.; Marcotte, J.; Petreas, M.; Goldman, L. (1995). "Polychlorinated Dibenzo-p-dioxin and Dibenzofuran Contamination at Metal Recovery Facilities, Open Burn Sites, and a Railroad Car Incineration Facility". Environmental Science & Technology. 29 (3): 677–684. Bibcode:1995EnST...29..677H. doi:10.1021/es00003a015. PMID 22200276.
  47. ^ DHHS: Report on Carcinogens, Twelfth Edition (2011) Archived 17 February 2013 at the Wayback Machine (accessed 2013-08-01)
  48. ^ Jouko Tuomisto &al.: Synopsis on Dioxins and PCBs Archived 27 September 2011 at the Wayback Machine (accessed 2013-08-01), p.40; using data from EPA's National Center for Environmental Assessment
  49. ^ P. Mocarelli; et al. (1991). "Serum concentrations of 2,3,7,8- tetrachlorodibenzo-p-dioxin and test results from selected residents of Seveso, Italy". J. Toxicol. Environ. Health. 32 (4): 357–366. doi:10.1080/15287399109531490. PMID 1826746.
  50. ^ P. Mocarelli; et al. (2000). "Paternal concentrations of dioxin and sex ratio of offspring" (PDF). Lancet. 355 (9218): 1858–1863. doi:10.1016/S0140-6736(00)02290-X. hdl:10281/16136. PMID 10866441. S2CID 6353869.
  51. ^ A. Geusau; K. Abraham; K. Geissler; M.O. Sator; G. Stingl; E. Tschachler (2001). "Severe 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD) intoxication: clinical and laboratory effects". Environ. Health Perspect. 109 (8): 865–869. doi:10.1289/ehp.01109865. PMC 1240417. PMID 11564625.
  52. ^ a b Sorg, O.; Zennegg, M.; Schmid, P.; Fedosyuk, R.; Valikhnovskyi, R.; Gaide, O.; Kniazevych, V.; Saurat, J.-H. (2009). "2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD) poisoning in Victor Yushchenko: identification and measurement of TCDD metabolites". The Lancet. 374 (9696): 1179–1185. doi:10.1016/S0140-6736(09)60912-0. PMID 19660807. S2CID 24761553.
  53. ^ Senior, K; Mazza, A (September 2004). "Italian "Triangle of death" linked to waste crisis". Lancet Oncol. 5 (9): 525–527. doi:10.1016/s1470-2045(04)01561-x. PMID 15384216.
  54. ^ "Il triangolo della morte". rassegna.it. March 2007. Archived from the original on 15 February 2009. Retrieved 25 September 2014.
  55. ^ "Discariche piene di rifiuti tossici quello è il triangolo della morte". la Repubblica. 31 August 2004.

External links[edit]