5th Draft (January 2010) Table of Contents 1 Introduction 6



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1.4Human Health Risk

1.4.1Methylmercury


  1. In the aquatic environment, elemental mercury is bioconverted into methylmercury which is the environmental neurotoxicant with well-defined neuropathological and developmental effects (Ozonoff 2006). Methylmercury bioaccumulates, is biomagnified in the food web and enters the human body mainly through the consumption of fish and seafood, particularly large predatory marine species such as tuna, swordfish, shark, whale, etc (Sanborn 2006). Most humans, particularly high-fish-consuming populations, are exposed to methylmercury through fish and seafood consumption (Sakamoto 2005).

  2. Ingested methylmercury in the human body is readily and completely absorbed by the gastrointestinal tract, almost completely absorbed into the bloodstream and distributed to all tissues within about 4 days (WHO 1990). Methylmercury is accumulated in the liver and kidney. In addition, methylmercury transported into tissues combines with cysteine which is an amino acid found in most proteins and appears to be mediated by the formation of a methylmercury-cysteine conjugate, which is transported into cells via a neutral amino acid carrier protein (Kanai 2003). A methylmercury-cysteine conjugate can pass through not only the blood-brain barrier but also the placenta via an amino acid transporter (Kerper 1992). Methylmercury can cross to the brain where methylmercury is oxidized and accumulated and eventually causes the chronic exposure to human health (Mottet 1985; Sakamoto 2004).

1.4.2Elemental Mercury


  1. Most cases of the adverse effects to human health caused by elemental mercury are due to inhalation of mercury vapour via the lungs (Oikawa 1983). Elemental mercury exposure in the general population is primarily the result of the use of dental amalgam (50% Hg0 by weight) as a dental restorative material (Richardson 2003; Richardson and Allan 1996; Gay 1979). Exposure also result from the spillage of mercury-containing products, such as breakage of fluorescent lamps and thermometers, or caused by the environmentally unsound uses and disposal of elemental mercury, such as the disposal of dental clinic wastes to sewers and landfills (Boom 2003), mercury vapour released from ASM (Hylander 2005) as well as spills resulting from the industrial use of mercury manometers. Elemental mercury released by these causes becomes mercury vapour at normal room temperature (Bull 2006). Dental waste in sewage sludge applied as a soil amendment to agricultural land is also released into the atmosphere as the vapour (Boom 2003).

  2. Approximately 80% of mercury vapour crosses the alveolar membrane and is rapidly absorbed into the blood (WHO 1990). Absorbed elemental mercury is rapidly distributed to all tissues, although it accumulates to the greatest extent in the kidney (WHO 1990; 1991). Due to the high lipophilicity, elemental mercury vapour passes the blood-brain barrier and the placenta (WHO 1991).

  3. When mercury is accidentally swallowed, the gastrointestinal absorption of elemental mercury is very low (less than 0.01%) (Japan Public Health Association 2001). Most of it is excreted in the faeces (Canadian Centre for Occupational Health and Safety 1998).

  4. An acute exposure (>0.1 mgmercury/m3) to mercury vapour causes respiratory effects such as cough, dyspnoea and chest tightness as well as bronchitis and bronchiolitis with interstitial pneumonitis, airway obstruction, and decreased pulmonary function. In addition, pulmonary oedema, respiratory distress and fibrosis would occur (WHO 1991; 2003).

  5. The WHO air quality guideline for mercury is 1 µgHg/m3 (annual average) (WHO 2003). The recommended health-based exposure limit for metallic mercury is 25 gHg/m3 for long-term exposure as TWA which means the time weighted average concentration for a normal 8 hour-day and 40 hour-workweek, to which nearly all workers can be repeatedly exposed without adverse effect (WHO 1991).

  6. However, recent studies suggest that mercury may have no threshold below which some adverse effects do not occur (WHO 2005).

1.4.3Inorganic Mercury Compounds


  1. Exposure to inorganic mercury compounds may occur due to accidental ingestion of mercury (II) chloride or ingestion with the intent of suicide (Japan Public Health Association 2001). In human, about 5-10% of inorganic mercury in food is absorbed after ingestion (WHO 1972). Inorganic mercury is distributed to all tissues following absorption, but due to the poor lipid solubility only a small fraction crosses the blood-brain barrier and the placenta (Asano 2000). As is the case for elemental mercury, the largest systemic deposition of inorganic mercury occurs in the kidney (Asano 2000). The main pathway of excretion of inorganic mercury is via the urine and faeces, with a half-life of about 70 days (WHO 1990; 1991).

  2. With ingestion of inorganic mercury at high concentration, the corrosive effects first damage the digestive tract, cause vomiting and stomach pain, and, in severe cases, may result in shock (Japan Public Health Association 2001). Finally, renal tubule degeneration, kidney dysfunction and nephritic syndrome may be seen (Japan Public Health Association 2001). Mercurochrome, which was previously used as an antiseptic, also contains mercury and may cause poisoning when spread in large quantities, as with abdominal wall hernia treatment (Japan Public Health Association 2001).

  3. The occupational exposure limit of inorganic compounds is 25 gHg/m3 as TWA exposure limit (for 8 hours per day, 5 days per week) (ILO 2004). Five agencies have established reference exposure levels (RELs) for Hg0 in the general non-occupational population:

  • WHO prescribes an air quality guideline of 1 μg Hg0/m3 of air (annual average concentration) (WHO Regional Office for Europe 2000);

  • US EPA prescribes a chronic reference air concentration of 0.3 μg/m3 (US EPA 2008);

  • US Agency for Toxic Substances and Disease Registry prescribes a minimal risk level (MRL) for chronic inhalation exposure of 0.2 μg/m3 (Agency for Toxic Substances & Disease Registry 2006);

  • California Environmental Protection Agency prescribes an inhalation reference exposure level of 0.09 μg/m3(CalEPA 2005); and

  • Health Canada proposed a chronic tolerable air concentration of 0.06 μg/m3 (Environment Canada 2008).

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