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Vinyl chloride is flammable, emitting corrosive [[hydrogen chloride]] and toxic [[phosgene]] in the process.
Vinyl chloride is flammable, emitting corrosive [[hydrogen chloride]] and toxic [[phosgene]] in the process.


The [[hepatotoxicity]] of vinyl chloride has long been established since the 1930s when the PVC industry was just in its infant stages. In the very first study about the dangers of vinyl chloride, published by Patty in 1930, it was disclosed that exposure of test animals to just a single short-term high dose of vinyl chloride caused liver damage.<ref>Patty, F.A. et al. "Acute Response of Guinea Pigs to Vapors of Some Commercial Organic Compounds." Public Health Reports. Volume 45, Number 24. August 22, 1930</ref> In 1949, a Russian publication discussed the finding that vinyl chloride caused liver injury among workers.<ref>Tribukh, S L et al. "Working Conditions and Measures for Their Improvement in Production and Use of Vinylchloride Plastics" (1949)</ref> In 1954, B.F. Goodrich Chemical stated that vinyl chloride caused liver injury upon short-term exposures. Almost nothing was known about its long-term effects. They also recommended that long-term animal toxicology studies.{{Clarify|date=October 2015}} The study noted that if a chemical did justify the cost of testing, and its ill-effects on workers and the public were known, the chemical should not be made.<ref>Wilson, Rex H et al. "Toxicology of Plastics and Rubber- Plastomers and Monomers." Reprinted from Industrial Medicine and Surgery. 23:11, 479–786. November 1954.</ref> In 1963, research paid for in part by Allied Chemical, found liver damage in test animals from exposures below 500 parts per million (ppm).<ref>Lester, D. et al. "Effects of Single and Repeated Exposures of Humans and Rats to Vinyl Chloride" Laboratory of applied biodynamics, Yale University and Department of Pathology. School of Medicine, Yale University, New Haven, Connecticut.</ref> Also in 1963, a Romanian researcher published findings of liver disease in vinyl chloride workers.<ref>Suciu, I et al. "Clinical Manifestations in Vinyl Chloride Poisoning" Clinic of Professional Diseases. Cluj, Romania.</ref> In 1968, Mutchler and Kramer, two Dow researchers, reported their finding that exposures as low as 300 ppm caused liver damage in vinyl chloride workers thus confirming earlier animal data in humans.<ref>Kramer, G.C., M.D. "The Correlation of Clinical and Environmental Measurements for Workers Exposed to Vinyl Chloride." The Dow Chemical Company. Midland Michigan.</ref> In a 1969 presentation given in Japan, P. L. Viola, a European researcher working for the European vinyl chloride industry, indicated, "every monomer used in V.C. manufacture is hazardous....various changes were found in bone and liver. Particularly, much more attention should be drawn to liver changes. The findings in rats at the concentration of 4 to 10 ppm are shown in pictures." In light of the finding of liver damage in rats from just 4–10 ppm of vinyl chloride exposure, Viola added that he "should like some precautions to be taken in the manufacturing plants polymerizing vinyl chloride, such as a reduction of the threshold limit value of monomer …" <ref>Viola, P.L. "Pathology of Vinyl Chloride" International Congress on Occupational Health. Japan. 1969.</ref> In 1970, Viola, reported that test animals exposed to 30,000 ppm of vinyl chloride developed cancerous tumors. Viola began his research looking for the cause of liver and bone injuries found in vinyl chloride workers. Viola's findings in 1970 were a "red flag" to [[Goodrich Corporation|B.F. Goodrich]] and the industry.<ref>Viola, P L. "Carcinogenic Effect of Vinyl Chloride" Presented at the Tenth International Cancer Congress. Houston, Texas. May 22–29, 1970.</ref> In 1972, Maltoni, another Italian researcher for the European vinyl chloride industry, found liver tumors (including angiosarcoma) from vinyl chloride exposures as low as 250 ppm for four hours a day.<ref>Maltoni, C. "Cancer Detection and Prevention" (1972) Presented at the Second International Symposium on Cancer Detection and Prevention. Bologna, April 9–12, 1973.</ref>
The [[hepatotoxicity]] of vinyl chloride has long been established since the 1930s when the PVC industry was just in its infant stages. In the very first study about the dangers of vinyl chloride, published by Patty in 1930, it was disclosed that exposure of test animals to just a single short-term high dose of vinyl chloride caused liver damage.<ref>Patty, F.A. et al. "Acute Response of Guinea Pigs to Vapors of Some Commercial Organic Compounds." Public Health Reports. Volume 45, Number 24. August 22, 1930</ref> In 1949, a Russian publication discussed the finding that vinyl chloride caused liver injury among workers.<ref>Tribukh, S L et al. "Working Conditions and Measures for Their Improvement in Production and Use of Vinylchloride Plastics" (1949)</ref> In 1954, B.F. Goodrich Chemical stated that vinyl chloride caused liver injury upon short-term exposures. Almost nothing was known about its long-term effects. They also recommended long-term animal toxicology studies. The study noted that if a chemical did justify the cost of testing, and its ill-effects on workers and the public were known, the chemical should not be made.<ref>Wilson, Rex H et al. "Toxicology of Plastics and Rubber- Plastomers and Monomers." Reprinted from Industrial Medicine and Surgery. 23:11, 479–786. November 1954.</ref> In 1963, research paid for in part by Allied Chemical found liver damage in test animals from exposures below 500 parts per million (ppm).<ref>Lester, D. et al. "Effects of Single and Repeated Exposures of Humans and Rats to Vinyl Chloride" Laboratory of applied biodynamics, Yale University and Department of Pathology. School of Medicine, Yale University, New Haven, Connecticut.</ref> Also in 1963, a Romanian researcher published findings of liver disease in vinyl chloride workers.<ref>Suciu, I et al. "Clinical Manifestations in Vinyl Chloride Poisoning" Clinic of Professional Diseases. Cluj, Romania.</ref> In 1968, Mutchler and Kramer, two Dow researchers, reported their finding that exposures as low as 300 ppm caused liver damage in vinyl chloride workers thus confirming earlier animal data in humans.<ref>Kramer, G.C., M.D. "The Correlation of Clinical and Environmental Measurements for Workers Exposed to Vinyl Chloride." The Dow Chemical Company. Midland Michigan.</ref> In a 1969 presentation given in Japan, P. L. Viola, a European researcher working for the European vinyl chloride industry, indicated, "every monomer used in V.C. manufacture is hazardous....various changes were found in bone and liver. Particularly, much more attention should be drawn to liver changes. The findings in rats at the concentration of 4 to 10 ppm are shown in pictures." In light of the finding of liver damage in rats from just 4–10 ppm of vinyl chloride exposure, Viola added that he "should like some precautions to be taken in the manufacturing plants polymerizing vinyl chloride, such as a reduction of the threshold limit value of monomer …" <ref>Viola, P.L. "Pathology of Vinyl Chloride" International Congress on Occupational Health. Japan. 1969.</ref> In 1970, Viola, reported that test animals exposed to 30,000 ppm of vinyl chloride developed cancerous tumors. Viola began his research looking for the cause of liver and bone injuries found in vinyl chloride workers. Viola's findings in 1970 were a "red flag" to [[Goodrich Corporation|B.F. Goodrich]] and the industry.<ref>Viola, P L. "Carcinogenic Effect of Vinyl Chloride" Presented at the Tenth International Cancer Congress. Houston, Texas. May 22–29, 1970.</ref> In 1972, Maltoni, another Italian researcher for the European vinyl chloride industry, found liver tumors (including angiosarcoma) from vinyl chloride exposures as low as 250 ppm for four hours a day.<ref>Maltoni, C. "Cancer Detection and Prevention" (1972) Presented at the Second International Symposium on Cancer Detection and Prevention. Bologna, April 9–12, 1973.</ref>


In the late 1960s, the cancers that all of these studies warned of finally manifested themselves in workers. John Creech from [[Goodrich Corporation|B.F. Goodrich]] discovered [[angiosarcoma]] (a very rare cancer) in the liver of a worker at the B.F. Goodrich plant in Louisville, Kentucky. Then, finally, on January 23, 1974, [[Goodrich Corporation|B.F. Goodrich]] informed the government and issued a press release stating that it was "investigating whether the cancer deaths of three employees in the polyvinyl chloride operations at its Louisville, Ky. plant were related to occupational causes."
In the late 1960s, the cancers that all of these studies warned of finally manifested themselves in workers. John Creech from [[Goodrich Corporation|B.F. Goodrich]] discovered [[angiosarcoma]] (a very rare cancer) in the liver of a worker at the B.F. Goodrich plant in Louisville, Kentucky. Then, finally, on January 23, 1974, [[Goodrich Corporation|B.F. Goodrich]] informed the government and issued a press release stating that it was "investigating whether the cancer deaths of three employees in the polyvinyl chloride operations at its Louisville, Ky. plant were related to occupational causes."


In 1997 the U.S. [[Centers for Disease Control and Prevention]] (CDC) concluded that the development and acceptance by the PVC industry of a closed loop polymerization process in the late 1970s "almost completely eliminated worker exposures" and that "new cases of hepatic angiosarcoma in vinyl chloride polymerization workers have been virtually eliminated."<ref>Epidemiologic Notes and Reports Angiosarcoma of the Liver Among Polyvinyl Chloride Workers – Kentucky, Centers for Disease Control and Prevention Web site. 1997. Available at: http://www.cdc.gov/mmwr/preview/mmwrhtml/00046136.htm</ref>
In 1997 the U.S. [[Centers for Disease Control and Prevention]] (CDC) concluded that the development and acceptance by the PVC industry of a closed loop polymerization process in the late 1970s "almost completely eliminated worker exposures" and that "new cases of hepatic angiosarcoma in vinyl chloride polymerization workers have been virtually eliminated."<ref>[http://www.cdc.gov/mmwr/preview/mmwrhtml/00046136.htm Epidemiologic Notes and Reports Angiosarcoma of the Liver Among Polyvinyl Chloride Workers – Kentucky]. Centers for Disease Control and Prevention. 1997.</ref>


According to the [[United States Environmental Protection Agency]] (EPA), "vinyl chloride emissions from polyvinyl chloride (PVC), ethylene dichloride (EDC), and vinyl chloride monomer (VCM) plants cause or contribute to air pollution that may reasonably be anticipated to result in an increase in mortality or an increase in serious irreversible, or incapacitating reversible illness. Vinyl chloride is a known human carcinogen that causes a rare cancer of the liver."<ref>National Emission Standards for Hazardous Air Pollutants (NESHAP) for Vinyl Chloride Subpart F, OMB Control Number 2060-0071, EPA ICR Number 0186.09 ([http://www.epa.gov/fedrgstr/EPA-AIR/2001/September/Day-25/a23920.htm Federal Register: September 25, 2001 (Volume 66, Number 186)])</ref> EPA's 2001 updated Toxicological Profile and Summary Health Assessment for VCM in its Integrated Risk Information System (IRIS) database lowers EPA's previous risk factor estimate by a factor of 20 and concludes that "because of the consistent evidence for liver cancer in all the studies...and the weaker association for other sites, it is concluded that the liver is the most sensitive site, and protection against liver cancer will protect against possible cancer induction in other tissues."<ref>EPA Toxicologica Review of Vinyl Chloride i Support of Information on the IRIS. May 2000</ref>
According to the [[United States Environmental Protection Agency]] (EPA), "vinyl chloride emissions from polyvinyl chloride (PVC), ethylene dichloride (EDC), and vinyl chloride monomer (VCM) plants cause or contribute to air pollution that may reasonably be anticipated to result in an increase in mortality or an increase in serious irreversible, or incapacitating reversible illness. Vinyl chloride is a known human carcinogen that causes a rare cancer of the liver."<ref>National Emission Standards for Hazardous Air Pollutants (NESHAP) for Vinyl Chloride Subpart F, OMB Control Number 2060-0071, EPA ICR Number 0186.09 ([http://www.epa.gov/fedrgstr/EPA-AIR/2001/September/Day-25/a23920.htm Federal Register: September 25, 2001 (Volume 66, Number 186)])</ref> EPA's 2001 updated Toxicological Profile and Summary Health Assessment for VCM in its Integrated Risk Information System (IRIS) database lowers EPA's previous risk factor estimate by a factor of 20 and concludes that "because of the consistent evidence for liver cancer in all the studies...and the weaker association for other sites, it is concluded that the liver is the most sensitive site, and protection against liver cancer will protect against possible cancer induction in other tissues."<ref>EPA Toxicological Review of Vinyl Chloride in Support of Information on the IRIS. May 2000</ref>


A 1998 front-page series in the ''[[Houston Chronicle]]'' claimed the vinyl industry has manipulated vinyl chloride studies to avoid liability for worker exposure and to hide extensive and severe chemical spills into local communities.<ref>Jim Morris, "In Strictest Confidence. The chemical industry's secrets," Houston Chronicle. Part One: "Toxic Secrecy," June 28, 1998, pgs. 1A, 24A–27A; Part Two: "High-Level Crime," June 29, 1998, pgs. 1,A, 8A, 9A; and Part Three: "Bane on the Bayou," July 26, 1998, pgs. 1A, 16A.</ref> Retesting of community residents in 2001 by the U.S. [[Agency for Toxic Substances and Disease Registry]] (ATSDR) found [[dioxins and dioxin-like compounds|dioxin]] levels similar to those in a comparison community in Louisiana and to the U.S. population.<ref>"ATSDR Study Finds Dioxin Levels in Calcasieu Parish Residents Similar to National Levels," available at: http://www.atsdr.cdc.gov/NEWS/calcasieula031506.html; "ATSDR Study Finds Dioxin Levels Among Lafayette Parish Residents Similar to National Levels," available at: http://www.atsdr.cdc.gov/NEWS/lafayettela031606.html; ATSDR Report: Serum Dioxin Levels In Residents Of Calcasieu Parish, Louisiana, October 2005, Publication Number PB2006-100561, available from the National Technical Information Services, Springfield, Virginia, phone: 1-800-553-6847/1-703-605-6244</ref> Cancer rates in the community were similar to Louisiana and US averages.<ref>"Calcasieu Cancer Rates Similar to State/National Averages." News Release, State of Louisiana Dept. of Health and Hospitals. January 17, 2002</ref> Vinyl Chloride finds its major application in the production of PVC. Being volatile the source of exposure is majorly via inhalation as against food or water with occupational hazards being highest. Prior to 1974 workers were commonly exposed to 1000 ppm Vinyl Chloride causing “Vinyl Chloride Illness”-with Acrosteolysis, Raynaud’s Phenomenon .The 2008, Version 1, Henrietta Harrison CHAP DHQ, HPA Report classifies symptoms of Vinyl Chloride Hazards based on ppm levels with 4000 ppm having a threshold effect. 1999 IPCS report on Vinyl Chloride states the intensity of symptoms vary from acute (1000-8000 ppm) including dizziness, nausea, visual disturbances, headache, ataxia to chronic (above 12000 ppm) including narcotic effect, cardiac arrhythmias, fatal respiratory failure. In 2004, the DEFRA, Bristol Report suggested the occurrence of RADS (Reactive Airway Dysfunction Syndrome) due to acute exposure to Vinyl Chloride. The 1997,1999 IPCS, WHO, Geneva Report highlighted the Acute Dermal and Occular effects of Vinyl Chloride Exposure. Dermal exposure hazards are thickening of skin, oedema, decreased elasticity, local frost bites, blistering and irritation. The complete loss of skin elasticity expresses itself in Raynaud’s Disease as stated in ASTDR, Atlanta (2006) Report for Toxicological effect of Vinyl Chloride. Chronic Exposure leads to much popular respiratory failure (emphysema, pulmonary fibrosis) and the focused Hepatotoxicity (Hepatomegaly, Hepatic fibrosis) .Continuous exposure can cause CNS depression including euphoria and disorientation. The IPCS 1999 and 2006 ASTDR Reports identify Vinyl Chloride as a mutagen having clastogenic effects affecting lymphocyte chromosomal structure. According to ICAR, Vinyl Chloride is Group 1 human carcinogen posing elevated risks of rare Anginosarcoma, brain &lung tumors and malignant haematopoeitic, lymphatic tumors. Decreased male libido, spontaneous abortion and birth defects are major reproductive defects. Considering above,the OSHA regulates the Vinyl Chloride levels for workers not greater than 1 ppm for 8 hours or 5 ppm for 15 minutes. The EPA in collaboration with FDA has given out permissible Vinyl Chloride in drinking water as 0.002 ppm.Food(ingestion) is a trivial source of exposure.
A 1998 front-page series in the ''[[Houston Chronicle]]'' claimed the vinyl industry has manipulated vinyl chloride studies to avoid liability for worker exposure and to hide extensive and severe chemical spills into local communities.<ref>Jim Morris, "In Strictest Confidence. The chemical industry's secrets," ''Houston Chronicle''. Part One: "Toxic Secrecy," June 28, 1998, pgs. 1A, 24A–27A; Part Two: "High-Level Crime," June 29, 1998, pgs. 1,A, 8A, 9A; and Part Three: "Bane on the Bayou," July 26, 1998, pgs. 1A, 16A.</ref> Retesting of community residents in 2001 by the U.S. [[Agency for Toxic Substances and Disease Registry]] (ATSDR) found [[dioxins and dioxin-like compounds|dioxin]] levels similar to those in a comparison community in Louisiana and to the U.S. population.<ref>[http://www.atsdr.cdc.gov/NEWS/calcasieula031506.html ATSDR Study Finds Dioxin Levels in Calcasieu Parish Residents Similar to National Levels], [http://www.atsdr.cdc.gov/NEWS/lafayettela031606.html ATSDR Study Finds Dioxin Levels Among Lafayette Parish Residents Similar to National Levels]; ATSDR Report ''Serum Dioxin Levels In Residents Of Calcasieu Parish, Louisiana, October 2005'', Publication Number PB2006-100561, available from the National Technical Information Services, Springfield, Virginia</ref> Cancer rates in the community were similar to Louisiana and US averages.<ref>"Calcasieu Cancer Rates Similar to State/National Averages." News Release, State of Louisiana Dept. of Health and Hospitals. January 17, 2002</ref>

<ref>"International Agency for the Research on Cancer (IARC) (1979). Vinyl chloride,
Vinyl chloride finds its major application in the production of PVC. It is volatile, so the primary exposure is via inhalation as against food or water with occupational hazards being highest. Prior to 1974, workers were commonly exposed to 1,000 ppm vinyl chloride, causing "vinyl chloride illness" such as acrosteolysis and [[Raynaud's Phenomenon]]. The symptoms of vinyl chloride exposure are classified by ppm levels in ambient air with 4,000 ppm having a threshold effect.<ref>Harrison, Henrietta (2008). HPA Report Version 1. CHAP DHQ</ref> The intensity of symptoms varies from acute (1,000-8,000 ppm), including dizziness, nausea, visual disturbances, headache, and [[ataxia]], to chronic (above 12,000 ppm), including narcotic effect, cardiac arrhythmias, and fatal respiratory failure.<ref name=IPCS1999> International Programme on Chemical Safety (IPCS) (1999). [http://www.who.int/ipcs/publications/ehc/ehc_215/en/ Vinyl chloride]. Environmental Health Criteria 215. WHO. Geneva.</ref> RADS (Reactive Airway Dysfunction Syndrome) may be caused by acute exposure to vinyl chloride.<ref>UK Department for Environment, Food, and Rural Affairs (DEFRA) and Environment Agency (EA) (2004). "Contaminants in soil: Collation of toxicological data and intake values for humans. Vinyl chloride."</ref>
polyvinyl chloride and vinyl chloride-vinyl acetate copolymers. Vol 19. IARC. Lyon.

[2] International Agency for the Research on Cancer (IARC) (1987). Vinyl chloride.
Vinyl chloride can have acute dermal and ocular effects. Dermal exposure effects are thickening of skin, edema, decreased elasticity, local frostbites, blistering, and irritation.<ref name=IPCS1999/> The complete loss of skin elasticity expresses itself in Raynaud’s Phenomenon.<ref name=ATSRD>Agency for Toxic Substances and Disease Registry (ATSDR) (2006). "Toxicological Profile for vinyl chloride". US Department of Health and Human Services. Atlanta, US.</ref>
Supplement 7. IARC. Lyon.

[3] International Programme on Chemical Safety (IPCS) (1999). [http://www.who.int/ipcs/publications/ehc/ehc_215/en/ Vinyl chloride]. Environmental Health Criteria 215. WHO. Geneva.
Chronic exposure leads to common forms of respiratory failure ([[emphysema]], [[pulmonary fibrosis]]) and focused hepatotoxicity ([[hepatomegaly]], [[hepatic fibrosis]]). Continuous exposure can cause CNS depression including euphoria and disorientation.
[4] International Programme on Chemical Safety (IPCS) (1997). Vinyl chloride. Poisons

Information Monograph. PIM 558. WHO. Geneva.
Vinyl chloride is a mutagen having clastogenic effects which affect lymphocyte chromosomal structure.<ref name=IPCS1999/><ref name=ATSRD/>
[5] National Poisons Information Service (NPIS) (2004). Vinyl chloride. TOXBASE®.

[6] Department for Environment Food and Rural Affairs (DEFRA) and Environment
Vinyl chloride is a Group 1 human carcinogen posing elevated risks of rare angiosarcoma, brain and lung tumors, and malignant [Haematopoiesis|haematopoeitic]] lymphatic tumors.<ref>International Agency for Research on Cancer (IARC). "Vinyl chloride, polyvinyl chloride, and vinyl chloride-vinyl acetate copolymers." Vol 19, 1979. IARC. "Vinyl chloride." Supplement 7, 1987. Lyon.</ref>
Agency (EA) (2004). Contaminants in soil: Collation of toxicological data and intake

values for humans. Vinyl chloride. Environment Agency. Bristol.
Decreased male libido, spontaneous abortion, and birth defects are known major reproductive defects associated with vinyl chloride.
[7] Agency for Toxic Substances and Disease Registry (ATSDR) (2006). Toxicological

Profile for vinyl chloride. US department of Health and Human Services. Atlanta, US.
The US OSHA limits vinyl chloride exposure of workers to no more than 1 ppm for eight hours or 5 ppm for 15 minutes. The US EPA and FDA limit vinyl chloride in drinking water to 0.002 ppm. Food (ingestion) is a trivial source of exposure.
[8] World Health Organisation (WHO) (2000). Air quality guidelines for Europe. WHO

Regional Publications, European Series, No. 91. 2nd edition. WHO Regional Office
===Additional references===
for Europe. Copenhagen.
* International Programme on Chemical Safety (IPCS) (1997). '"Vinyl chloride. Poisons Information Monograph.'' PIM 558. WHO. Geneva.
[9] Hathaway G.J. and Proctor N.H. (2004). Chemical Hazards of the Workplace. 5th
* National Poisons Information Service (NPIS) (2004). "Vinyl chloride." TOXBASE®.
edition. Inc. John Wiley & Sons, New Jersey.
* World Health Organisation (WHO) (2000). "Air quality guidelines for Europe." WHO Regional Publications, European Series, No. 91. 2nd edition. WHO Regional Office for Europe. Copenhagen.
[10] Risk Assessment Information System (RAIS) (1993). Toxicity summary for vinyl
* Hathaway G.J. and Proctor N.H. (2004). ''Chemical Hazards of the Workplace''. 5th edition. John Wiley & Sons, New Jersey.
chloride. Chemical Hazard Evaluation and Communication Group, Biomedical and
Environmental Information Analysis Section, Health and Safety Research Division.
* Risk Assessment Information System (RAIS) (1993). "Toxicity summary for vinyl chloride. "Chemical Hazard Evaluation and Communication Group, Biomedical and Environmental Information Analysis Section, Health and Safety Research Division.
[11] Agency for Toxic Substances and Disease Registry (ATSDR) (2007). Vinyl chloride.
US Department of Health and Human Services. Atlanta, US.
"</ref>


==Microbial Remediation==
==Microbial Remediation==

Revision as of 07:44, 21 June 2016

Vinyl chloride
Structural formula of vinyl chloride
Structural formula of vinyl chloride
Space-filling model
Space-filling model
Names
IUPAC name
Chloroethene
Other names
Vinyl chloride monomer
VCM
Chloroethylene
Refrigerant-1140
Identifiers
3D model (JSmol)
ChEBI
ChemSpider
ECHA InfoCard 100.000.756 Edit this at Wikidata
KEGG
  • InChI=1S/C2H3Cl/c1-2-3/h2H,1H2 checkY
    Key: BZHJMEDXRYGGRV-UHFFFAOYSA-N checkY
  • InChI=1/C2H3Cl/c1-2-3/h2H,1H2
    Key: BZHJMEDXRYGGRV-UHFFFAOYAW
  • ClC=C
Properties
Appearance Colorless gas
Odor pleasant[1]
Density 0.911 g/ml
Melting point −153.8 °C (−244.8 °F; 119.3 K)
Boiling point −13.4 °C (7.9 °F; 259.8 K)
2.7 g/L (0.0432 mol/L)
Vapor pressure 2580 mm. of mercury 20 °C (68 °F)
Thermochemistry
0.8592 J/K/g (gas)
0.9504 J/K/g (solid)
−94.12 kJ/mol (solid)
Hazards
NFPA 704 (fire diamond)
NFPA 704 four-colored diamondHealth 3: Short exposure could cause serious temporary or residual injury. E.g. chlorine gasFlammability 4: Will rapidly or completely vaporize at normal atmospheric pressure and temperature, or is readily dispersed in air and will burn readily. Flash point below 23 °C (73 °F). E.g. propaneInstability 2: Undergoes violent chemical change at elevated temperatures and pressures, reacts violently with water, or may form explosive mixtures with water. E.g. white phosphorusSpecial hazards (white): no code
3
4
2
Flash point −61 °C (−78 °F; 212 K)
Explosive limits 3.6%-33%[1]
NIOSH (US health exposure limits):
PEL (Permissible)
TWA 1 ppm C 5 ppm [15-minute][1]
REL (Recommended)
Ca[1]
IDLH (Immediate danger)
Ca [N.D.][1]
Except where otherwise noted, data are given for materials in their standard state (at 25 °C [77 °F], 100 kPa).
checkY verify (what is checkY☒N ?)

Vinyl chloride is an organochloride with the formula H2C=CHCl that is also called vinyl chloride monomer (VCM) or chloroethene. This colorless compound is an important industrial chemical chiefly used to produce the polymer polyvinyl chloride (PVC).[2] About 13 billion kilograms are produced annually. VCM is among the top twenty largest petrochemicals (petroleum-derived chemicals) in world production. The United States currently remains the largest VCM manufacturing region because of its low-production-cost position in chlorine and ethylene raw materials. China is also a large manufacturer and one of the largest consumers of VCM.[3] Vinyl chloride is a gas with a sweet odor. It is highly toxic, flammable, and carcinogenic. It can be formed in the environment when soil organisms break down "chlorinated" solvents. Vinyl chloride that is released by industries or formed by the breakdown of other chlorinated chemicals can enter the air and drinking water supplies. Vinyl chloride is a common contaminant found near landfills.[4] In the past VCM has been used as a refrigerant.[5]

Production

Vinyl chloride was first produced in 1835 by Justus von Liebig and his student Henri Victor Regnault. They obtained it by treating 1,2-dichloroethane with a solution of potassium hydroxide in ethanol.

In 1912, Fritz Klatte, a German chemist working for Griesheim-Elektron, patented a means to produce vinyl chloride from acetylene and hydrogen chloride using mercuric chloride as a catalyst. While this method was widely used during the 1930s and 1940s in the West, it has since been superseded by more economical processes based on ethylene in the United States and Europe. It remains the main production method in China.

Vinyl chloride is produced on a substantial scale—approximately 31.1 million tons (7.5 Bel tons) were produced in 2000.[6] Two methods are employed, the hydrochlorination of acetylene and the dehydrochlorination of ethylene dichloride (1,2-dichloroethane). Numerous attempts have been made to convert ethane directly to vinyl chloride.[2]

Vinyl chloride can also be obtained as byproducts in the synthesis of chlorofluorocarbons when saturated chlorofluorocarbons are catalytically dechlorinated by ethylene. Ethane sulfochlorination has been proposed as a route to produce vinyl chloride using sulfur instead of oxygen.[2]

Production from ethylene

About 85% of vinyl chloride is produced by an integrated set of reactions starting with chlorine, ethylene, and air. Two processes are used to generate 1,2-dichloroethane (EDC), commonly known by its old name of ethylene dichloride (EDC). The expected consumption for raw materials and utilities per 1000 kg VCM product are:[7]

Raw material Amount required
Ethylene 459 kg
Chlorine 575 kg
Oxygen 139 kg
Steam 250 kg
Fuel gas 2.7 GJ

Direct chlorination

EDC (Ethylene dichloride) is prepared by reacting ethylene and chlorine.[8] In the presence of iron(III) chloride as a catalyst, these compounds react exothermically:

CH2=CH2 + Cl2 → ClCH2CH2Cl

This process results in high purity EDC and high yields. Dissolved catalyst and moisture must be removed before EDC enters the vinyl chloride production process.

Oxychlorination

Vinyl chloride plants use recycled HCl to produce more EDC via oxychlorination, which entails the reaction of ethylene, oxygen, and hydrogen chloride over a copper(II) chloride catalyst to produce EDC:

CH2=CH2 + 2 HCl + 12 O2 → ClCH2CH2Cl + H2O.

The reaction is highly exothermic.

Due to the relatively low cost of ethylene, compared to acetylene, most vinyl chloride has been produced via this technique since the late 1950s. This is despite the lower yields, lower product purity and higher costs for waste treatment. By-products of the oxychlorination reaction, may be recovered, as feedstocks for chlorinated solvents production. One useful byproduct of the oxychlorination is ethyl chloride, a topical anesthetic.

Thermal cracking

When heated to 500 °C at 15–30 atm (1.5 to 3 MPa) pressure, EDC vapor decomposes to produce vinyl chloride and anhydrous HCl.

ClCH2CH2Cl → CH2=CHCl + HCl

The thermal cracking reaction is highly endothermic, and is generally carried out in a fired heater. Even though residence time and temperature are carefully controlled, it produces significant quantities of chlorinated hydrocarbon side products. In practice, EDC conversion is relatively low (50 to 60 percent). The furnace effluent is immediately quenched with cold EDC to stop undesirable side reactions. The resulting vapor-liquid mixture then goes to a purification system. Some processes use an absorber-stripper system to separate HCl from the chlorinated hydrocarbons, while other processes use a refrigerated continuous distillation system.

Waste treatment

For environmental reasons, the acidic aqueous wastestream is treated to remove organic compounds and neutralized before it can be sent to the plant's "outfall". An outfall is a monitored wastewater stream that must conform to the plant's standards. Some very hazardous wastes are generated in the recovery of the product vinyl chloride. These wastes require specialized procedures. These wastes are burned onsite in hazardous waste burners that again are subject to strict standards.

Production from acetylene

Acetylene reacts with anhydrous hydrogen chloride gas over a mercuric chloride catalyst to give vinyl chloride:

C2H2 + HCl → CH2=CHCl

The reaction is exothermic and highly selective. Product purity and yields are generally very high.

This industrial route to vinyl chloride was common before ethylene became widely distributed. When vinyl chloride producers shifted to using the thermal cracking of EDC described above, some used byproduct HCl in conjunction with a colocated acetylene-based unit. The hazards of storing and shipping acetylene meant that the vinyl chloride facility needed to be located very close to the acetylene generating facility. China still uses this method to produce vinyl chloride due to the large reserves of coal from which acetylene is produced.[3]

Production from ethane

Ethane is readily available, particularly on the U.S. gulf coast. Ethylene is made from ethane by cracking ethane and then ethylene is used for production of vinyl chloride. Hence, to save the processing cost for manufacturing ethylene, numerous attempts have been made to convert ethane directly to vinyl chloride. The direct feed of ethane to vinyl chloride plants could, thus, considerably decrease the raw material costs and make the plants less dependent on cracker capacity. The conversion of ethane to vinyl chloride can be performed by various routes:[9]

High-temperature chlorination:

C2H6 + 2 Cl2 → C2H3Cl + 3 HCl

High-temperature oxychlorination:

C2H6 + HCl + O2 → C2H3Cl + 2 H2O

High-temperature oxidative chlorination:

2 C2H6 + 32 O2 + Cl2 → 2 C2H3Cl + 3 H2O

A major drawback to the use of ethane are the forcing conditions required for its use, which can be attributed to its lack of molecular functionality. In contrast to ethylene, which easily undergoes chlorine addition, ethane must first be functionalized by substitution reactions, which gives rise to a variety of consecutive and side-chain reactions. The reaction must, therefore, be kinetically controlled in order to obtain a maximal vinyl chloride yield. Vinyl chloride yields average 20–50% per pass. Ethylene, ethyl chloride, and 1,2-dichloroethane are obtained as major byproducts With special catalysts and at optimized conditions, however, ethane conversions of greater 96% have been reported from oxychlorination reactions. Ethylene, ethyl chloride, and 1,2-dichloroethane are obtained as major byproducts. The ethylene formed can either be recycled or oxychlorinated and cracked in a conventional manner. Many such ethane based processes have been and are being developed.

Storage and Transportation

Vinyl chloride is stored as a liquid. The presently accepted upper limit of safety as a health hazard is 500 ppm. Often, the storage containers for the product vinyl chloride are high capacity spheres. The spheres have an inside sphere and an outside sphere. Several inches of empty space separate the inside sphere from the outside sphere. This void area between the spheres is purged with an inert gas such as nitrogen. As the nitrogen purge gas exits the void space it passes through an analyzer that is designed to detect if any vinyl sechloride is leaking from the internal sphere. If vinyl chloride starts to leak from the internal sphere or if a fire is detected on the outside of the sphere then the contents of the sphere are automatically dumped into an emergency underground storage container. Containers used for handling vinyl chloride at atmospheric temperature are always under pressure. Inhibited vinyl chloride may be stored at normal atmospheric conditions in suitable pressure vessel. Uninhibited vinyl chloride may be stored either under refrigeration or at normal atmospheric temperature in the absence of air or sunlight but only for a duration of a few days. If for longer periods, regular checks should be made for the presence of polymers.[10] Transporting VCM presents the same risks as transporting other flammable gases such as propane, butane (LPG) or natural gas (for which the same safety regulations apply).The equipment used for VCM transport is specially designed to be impact and corrosion resistant.[11]

Companies associated with Vinyl Chloride production

Ethylene can be converted to vinyl chloride by direct chlorination and subsequent thermal cracking. The first large scale production units for this route were constructed by Dow Chemical Co., Monsanto Chemical Co. and the Shell Oil Co. The complete changeover to the exclusive use of ethylene as a feedstock became possible when the large-scale oxychlorination of ethylene to 1,2-dichloroethane had been proven to be technically feasible by Dow Chemical in the period 1955 – 1958. Since then, most plants now are using integrated, balanced DC– EDC – Oxy – EDC –VCM processes and more than 90% of the vinyl chloride presently produced in the Western World is derived from ethylene.[9]

Uses

Vinyl chloride is a chemical intermediate, not a final product. Due to the hazardous nature of vinyl chloride to human health there are no end products that use vinyl chloride in its monomer form. Polyvinyl chloride is very stable, storable, and nowhere near as acutely hazardous as the monomer.

Vinyl chloride liquid is fed to polymerization reactors where it is converted from a monomer to a polymer PVC. The final product of the polymerization process is PVC in either a flake or pellet form. From its flake or pellet form PVC is sold to companies that heat and mold the PVC into end products such as PVC pipe and bottles. Tens of billions of pounds of PVC are sold on the global market each year.

Until 1974, vinyl chloride was used in aerosol spray propellant.[12] Vinyl chloride was briefly used as an inhalational anaesthetic, in a similar vein to ethyl chloride, though its toxicity forced this practice to be abandoned.

Smaller amounts of vinyl chloride are used in furniture and automobile upholstery, wall coverings, housewares, and automotive parts. Vinyl chloride has also been used in the past as a refrigerant.[13]

Fire and explosion hazard

In the U.S., OSHA lists vinyl chloride as a Class IA Flammable Liquid, with an National Fire Protection Association Flammability Rating of 4. Because of its low boiling point, liquid VCM will undergo flash evaporation (i.e., autorefrigerate) upon its release to atmospheric pressure. The portion vaporized will form a dense cloud (more than twice as heavy as the surrounding air). The risk of subsequent explosion or fire is significant. According to OSHA, the flash point of vinyl chloride is −78 °C (−108.4 °F).[14] Its flammable limits in air are: lower 3.6 volume% and upper 33.0 volume%. The explosive limits are: lower 4.0%, upper 22.05 by volume in air. Fire may release toxic hydrogen chloride (HCl) and carbon monoxide (CO).[15] VCM can polymerise rapidly due to heating and under the influence of air, light and contact with a catalyst, strong oxidisers and metals such as copper and aluminium, with fire or explosion hazard. As a gas mixed with air, VCM is a fire and explosion hazard. On standing VCM can form peroxides, which may then explode. VCM will react with iron and steel in the presence of moisture.[5][16] Vinyl chloride is a gas at normal atmospheric temperature and pressure.

Health effects

Vinyl chloride is flammable, emitting corrosive hydrogen chloride and toxic phosgene in the process.

The hepatotoxicity of vinyl chloride has long been established since the 1930s when the PVC industry was just in its infant stages. In the very first study about the dangers of vinyl chloride, published by Patty in 1930, it was disclosed that exposure of test animals to just a single short-term high dose of vinyl chloride caused liver damage.[17] In 1949, a Russian publication discussed the finding that vinyl chloride caused liver injury among workers.[18] In 1954, B.F. Goodrich Chemical stated that vinyl chloride caused liver injury upon short-term exposures. Almost nothing was known about its long-term effects. They also recommended long-term animal toxicology studies. The study noted that if a chemical did justify the cost of testing, and its ill-effects on workers and the public were known, the chemical should not be made.[19] In 1963, research paid for in part by Allied Chemical found liver damage in test animals from exposures below 500 parts per million (ppm).[20] Also in 1963, a Romanian researcher published findings of liver disease in vinyl chloride workers.[21] In 1968, Mutchler and Kramer, two Dow researchers, reported their finding that exposures as low as 300 ppm caused liver damage in vinyl chloride workers thus confirming earlier animal data in humans.[22] In a 1969 presentation given in Japan, P. L. Viola, a European researcher working for the European vinyl chloride industry, indicated, "every monomer used in V.C. manufacture is hazardous....various changes were found in bone and liver. Particularly, much more attention should be drawn to liver changes. The findings in rats at the concentration of 4 to 10 ppm are shown in pictures." In light of the finding of liver damage in rats from just 4–10 ppm of vinyl chloride exposure, Viola added that he "should like some precautions to be taken in the manufacturing plants polymerizing vinyl chloride, such as a reduction of the threshold limit value of monomer …" [23] In 1970, Viola, reported that test animals exposed to 30,000 ppm of vinyl chloride developed cancerous tumors. Viola began his research looking for the cause of liver and bone injuries found in vinyl chloride workers. Viola's findings in 1970 were a "red flag" to B.F. Goodrich and the industry.[24] In 1972, Maltoni, another Italian researcher for the European vinyl chloride industry, found liver tumors (including angiosarcoma) from vinyl chloride exposures as low as 250 ppm for four hours a day.[25]

In the late 1960s, the cancers that all of these studies warned of finally manifested themselves in workers. John Creech from B.F. Goodrich discovered angiosarcoma (a very rare cancer) in the liver of a worker at the B.F. Goodrich plant in Louisville, Kentucky. Then, finally, on January 23, 1974, B.F. Goodrich informed the government and issued a press release stating that it was "investigating whether the cancer deaths of three employees in the polyvinyl chloride operations at its Louisville, Ky. plant were related to occupational causes."

In 1997 the U.S. Centers for Disease Control and Prevention (CDC) concluded that the development and acceptance by the PVC industry of a closed loop polymerization process in the late 1970s "almost completely eliminated worker exposures" and that "new cases of hepatic angiosarcoma in vinyl chloride polymerization workers have been virtually eliminated."[26]

According to the United States Environmental Protection Agency (EPA), "vinyl chloride emissions from polyvinyl chloride (PVC), ethylene dichloride (EDC), and vinyl chloride monomer (VCM) plants cause or contribute to air pollution that may reasonably be anticipated to result in an increase in mortality or an increase in serious irreversible, or incapacitating reversible illness. Vinyl chloride is a known human carcinogen that causes a rare cancer of the liver."[27] EPA's 2001 updated Toxicological Profile and Summary Health Assessment for VCM in its Integrated Risk Information System (IRIS) database lowers EPA's previous risk factor estimate by a factor of 20 and concludes that "because of the consistent evidence for liver cancer in all the studies...and the weaker association for other sites, it is concluded that the liver is the most sensitive site, and protection against liver cancer will protect against possible cancer induction in other tissues."[28]

A 1998 front-page series in the Houston Chronicle claimed the vinyl industry has manipulated vinyl chloride studies to avoid liability for worker exposure and to hide extensive and severe chemical spills into local communities.[29] Retesting of community residents in 2001 by the U.S. Agency for Toxic Substances and Disease Registry (ATSDR) found dioxin levels similar to those in a comparison community in Louisiana and to the U.S. population.[30] Cancer rates in the community were similar to Louisiana and US averages.[31]

Vinyl chloride finds its major application in the production of PVC. It is volatile, so the primary exposure is via inhalation as against food or water with occupational hazards being highest. Prior to 1974, workers were commonly exposed to 1,000 ppm vinyl chloride, causing "vinyl chloride illness" such as acrosteolysis and Raynaud's Phenomenon. The symptoms of vinyl chloride exposure are classified by ppm levels in ambient air with 4,000 ppm having a threshold effect.[32] The intensity of symptoms varies from acute (1,000-8,000 ppm), including dizziness, nausea, visual disturbances, headache, and ataxia, to chronic (above 12,000 ppm), including narcotic effect, cardiac arrhythmias, and fatal respiratory failure.[33] RADS (Reactive Airway Dysfunction Syndrome) may be caused by acute exposure to vinyl chloride.[34]

Vinyl chloride can have acute dermal and ocular effects. Dermal exposure effects are thickening of skin, edema, decreased elasticity, local frostbites, blistering, and irritation.[33] The complete loss of skin elasticity expresses itself in Raynaud’s Phenomenon.[35]

Chronic exposure leads to common forms of respiratory failure (emphysema, pulmonary fibrosis) and focused hepatotoxicity (hepatomegaly, hepatic fibrosis). Continuous exposure can cause CNS depression including euphoria and disorientation.

Vinyl chloride is a mutagen having clastogenic effects which affect lymphocyte chromosomal structure.[33][35]

Vinyl chloride is a Group 1 human carcinogen posing elevated risks of rare angiosarcoma, brain and lung tumors, and malignant [Haematopoiesis|haematopoeitic]] lymphatic tumors.[36]

Decreased male libido, spontaneous abortion, and birth defects are known major reproductive defects associated with vinyl chloride.

The US OSHA limits vinyl chloride exposure of workers to no more than 1 ppm for eight hours or 5 ppm for 15 minutes. The US EPA and FDA limit vinyl chloride in drinking water to 0.002 ppm. Food (ingestion) is a trivial source of exposure.

Additional references

  • International Programme on Chemical Safety (IPCS) (1997). '"Vinyl chloride. Poisons Information Monograph. PIM 558. WHO. Geneva.
  • National Poisons Information Service (NPIS) (2004). "Vinyl chloride." TOXBASE®.
  • World Health Organisation (WHO) (2000). "Air quality guidelines for Europe." WHO Regional Publications, European Series, No. 91. 2nd edition. WHO Regional Office for Europe. Copenhagen.
  • Hathaway G.J. and Proctor N.H. (2004). Chemical Hazards of the Workplace. 5th edition. John Wiley & Sons, New Jersey.
  • Risk Assessment Information System (RAIS) (1993). "Toxicity summary for vinyl chloride. "Chemical Hazard Evaluation and Communication Group, Biomedical and Environmental Information Analysis Section, Health and Safety Research Division.

Microbial Remediation

The bacteria species Nitrosomonas europaea can degrade a variety of halogenated compounds including trichloroethylene, benzene, and vinyl chloride.[37]

See also

References

  1. ^ a b c d e NIOSH Pocket Guide to Chemical Hazards. "#0658". National Institute for Occupational Safety and Health (NIOSH).
  2. ^ a b c E.-L. Dreher, T. R. Torkelson, K. K. Beutel "Chlorethanes and Chloroethylenes" in Ullmann's Encyclopedia of Industrial Chemistry 2011, Wiley-VCH, Weinheim. doi:10.1002/14356007.o06_o01
  3. ^ a b http://www.ihs.com/products/chemical/planning/ceh/vinyl-chloride-monomer.aspx
  4. ^ "http://www.dhs.wisconsin.gov/eh/chemfs/fs/vc.htm"
  5. ^ a b "http://www.npi.gov.au/resource/vinyl-chloride-monomer-vcm"
  6. ^ Klaus Weissermel, Hans-Jürgen Arpe in "Industrial organic chemistry"
  7. ^ http://www.thyssenkrupp-uhde.de/fileadmin/documents/brochures/uhde_brochures_pdf_en_8.pdf
  8. ^ Allen, D. T. "Chapter 4 - Industrial Ecology". Green Engineering. United States Environmental Protection Agency.
  9. ^ a b Ullmann's Encyclopedia of Industrial Chemistry (Wiley, 2007)(ISBN 3527316027)(O)(28029s)_ChGe_-Chlorinated hydrocarbons
  10. ^ "http://aseh.net/resources/restored/resources/teaching-units/teaching-unit-better-living-through-chemistry/historical-sources/lesson-1/MCA-Vinal%20Chloride%20Safety%20Sheet-1954.pdf"
  11. ^ "http://www.pvc.org/en/p/vinyl-chloride-monomer-vcm"
  12. ^ Markowitz, Gerald; Rosner, David (2013). Deceit and Denial: The Deadly Politics of Industrial Pollution. Berkeley, California Press: University of California Press. p. 185 – via Questia. {{cite book}}: Unknown parameter |subscription= ignored (|url-access= suggested) (help)
  13. ^ http://www.epa.gov/ttnatw01/hlthef/vinylchl.html
  14. ^ http://aseh.net/resources/restored/resources/teaching-units/teaching-unit-better-living-through-chemistry/historical-sources/lesson-1/MCA-Vinal%20Chloride%20Safety%20Sheet-1954.pdf
  15. ^ "Occupational Safety and Health Guideline for Vinyl Chloride"1988."
  16. ^ http://www.hpa.org.uk/webc/HPAwebFile/HPAweb_C/1194947326060
  17. ^ Patty, F.A. et al. "Acute Response of Guinea Pigs to Vapors of Some Commercial Organic Compounds." Public Health Reports. Volume 45, Number 24. August 22, 1930
  18. ^ Tribukh, S L et al. "Working Conditions and Measures for Their Improvement in Production and Use of Vinylchloride Plastics" (1949)
  19. ^ Wilson, Rex H et al. "Toxicology of Plastics and Rubber- Plastomers and Monomers." Reprinted from Industrial Medicine and Surgery. 23:11, 479–786. November 1954.
  20. ^ Lester, D. et al. "Effects of Single and Repeated Exposures of Humans and Rats to Vinyl Chloride" Laboratory of applied biodynamics, Yale University and Department of Pathology. School of Medicine, Yale University, New Haven, Connecticut.
  21. ^ Suciu, I et al. "Clinical Manifestations in Vinyl Chloride Poisoning" Clinic of Professional Diseases. Cluj, Romania.
  22. ^ Kramer, G.C., M.D. "The Correlation of Clinical and Environmental Measurements for Workers Exposed to Vinyl Chloride." The Dow Chemical Company. Midland Michigan.
  23. ^ Viola, P.L. "Pathology of Vinyl Chloride" International Congress on Occupational Health. Japan. 1969.
  24. ^ Viola, P L. "Carcinogenic Effect of Vinyl Chloride" Presented at the Tenth International Cancer Congress. Houston, Texas. May 22–29, 1970.
  25. ^ Maltoni, C. "Cancer Detection and Prevention" (1972) Presented at the Second International Symposium on Cancer Detection and Prevention. Bologna, April 9–12, 1973.
  26. ^ Epidemiologic Notes and Reports Angiosarcoma of the Liver Among Polyvinyl Chloride Workers – Kentucky. Centers for Disease Control and Prevention. 1997.
  27. ^ National Emission Standards for Hazardous Air Pollutants (NESHAP) for Vinyl Chloride Subpart F, OMB Control Number 2060-0071, EPA ICR Number 0186.09 (Federal Register: September 25, 2001 (Volume 66, Number 186))
  28. ^ EPA Toxicological Review of Vinyl Chloride in Support of Information on the IRIS. May 2000
  29. ^ Jim Morris, "In Strictest Confidence. The chemical industry's secrets," Houston Chronicle. Part One: "Toxic Secrecy," June 28, 1998, pgs. 1A, 24A–27A; Part Two: "High-Level Crime," June 29, 1998, pgs. 1,A, 8A, 9A; and Part Three: "Bane on the Bayou," July 26, 1998, pgs. 1A, 16A.
  30. ^ ATSDR Study Finds Dioxin Levels in Calcasieu Parish Residents Similar to National Levels, ATSDR Study Finds Dioxin Levels Among Lafayette Parish Residents Similar to National Levels; ATSDR Report Serum Dioxin Levels In Residents Of Calcasieu Parish, Louisiana, October 2005, Publication Number PB2006-100561, available from the National Technical Information Services, Springfield, Virginia
  31. ^ "Calcasieu Cancer Rates Similar to State/National Averages." News Release, State of Louisiana Dept. of Health and Hospitals. January 17, 2002
  32. ^ Harrison, Henrietta (2008). HPA Report Version 1. CHAP DHQ
  33. ^ a b c International Programme on Chemical Safety (IPCS) (1999). Vinyl chloride. Environmental Health Criteria 215. WHO. Geneva.
  34. ^ UK Department for Environment, Food, and Rural Affairs (DEFRA) and Environment Agency (EA) (2004). "Contaminants in soil: Collation of toxicological data and intake values for humans. Vinyl chloride."
  35. ^ a b Agency for Toxic Substances and Disease Registry (ATSDR) (2006). "Toxicological Profile for vinyl chloride". US Department of Health and Human Services. Atlanta, US.
  36. ^ International Agency for Research on Cancer (IARC). "Vinyl chloride, polyvinyl chloride, and vinyl chloride-vinyl acetate copolymers." Vol 19, 1979. IARC. "Vinyl chloride." Supplement 7, 1987. Lyon.
  37. ^ http://genome.jgi-psf.org/finished_microbes/niteu/niteu.home.html

Further reading