Blood metal analysis to biomonitor and diagnose acute vs. chronic Metal intoxication.Defining Metal Intoxication Blood is a part of the human circulatory system circulatory system, group of organs that transport blood and the substances it carries to and from all parts of the body. The circulatory system can be considered as composed of two parts: the systemic circulation, which serves the body as a whole except for the . It transports oxygen, nutrients, and toxins to and from the cells and organs. The nutrients and toxins taken in will either "feed" body cells, be stored, or be excreted through the urinary or digestive tract digestive tract n. See alimentary canal. Digestive tract The organs that perform digestion, or changing of food into a form that can be absorbed by the body. , through breathing and sweating. While circulating in the bloodstream, toxins can be measured and monitored, hence the term "Human Biomonitoring." Human monitoring of occupational exposures started in the 1890s through a variety of blood lead monitoring programs. Population-based biomonitoring is more recent and has been implemented at various levels within the United States (both federally and among states) and internationally. In the US, the recent advent of the National Health and Nutrition Examination Survey (NHANES NHANES National Health and Nutrition Examination Survey (US CDC) )resulted in population-based biomonitoring studies of lead and cadmium in clinical specimens. The combined effort, nationally and internationally, improved our understanding of how widespread, improved our understanding of how widespread some chemical exposures are in the general population. (1) New technology allows the detection of minute amounts of potentially toxic metals. Never before in the history of medicine have we had the analytical accuracy to correlate such traces of toxins with early onset of disease. Modern analytic chemistry allows physicians to take early action. Through early diagnosis, we can utilize chelation therapy Chelation Therapy Definition Chelation therapy is an intravenous treatment designed to bind heavy metals in the body in order to treat heavy metal toxicity. or metal detoxification Detoxification Definition Detoxification is one of the more widely used treatments and concepts in alternative medicine. It is based on the principle that illnesses can be caused by the accumulation of toxic substances (toxins) in the body. treatments not only for the treatment of acute metal intoxication, but also for preventive and curative measures. Diagnostic abilities improve treatment potential. Specific monitoring of low-dose intoxication allows early removal of harmful toxins from the body to prevent disease Early intervention ear·ly intervention n. Abbr. EI A process of assessment and therapy provided to children, especially those younger than age 6, to facilitate normal cognitive and emotional development and to prevent developmental disability or delay. enables us to remove the potential cause (s) of an existing disease. First Diagnose, Then Treat To treat metal intoxication, we must first define the degree of toxicity. An acute intoxication at the workplace demands a more aggressive treatment than one for a chronic case of metal intoxication. While a low-level metal exposure can be one cause of chronic diseases and disease patterns, it is important that we first identify the type of metal toxicity (lead, mercury, etc.) and the severity thereof. From that information, we can safely select a) the appropriate chelating agent chelating agent a substance which combines with a metallic ion to produce an inert chelate, e.g. ethylenediamine tetra-acetic acid, penicillamine. and b) the route of delivery and the frequency of treatment. Diagnosing Acute Metal Intoxication Medically, a patient is considered acutely exposed, or toxic, when his blood levels exceed the Biological Tolerance Value, also referred to as the BAT level. The BAT value is defined as the maximum permissible quantity of a chemical substance or its metabolites, or the maximum permissible deviation from the norm of biological parameters induced by these substances in exposed humans. The BAT value is established on the basis of currently available scientific data that indicate that these concentrations generally do not affect the health of the employee in any significant adverse way, even when they are attained regularly under workplace conditions. BAT values are established on the assumption that persons are exposed at work for at most eight hours daily and 40 hours weekly. BAT values established on this basis may also be applied without the use of correction factors to other patterns of working hours. Interestingly, BAT values are lower for the German than the US population. A cynic cyn·ic n. 1. A person who believes all people are motivated by selfishness. 2. A person whose outlook is scornfully and often habitually negative. 3. might say that either Germans are more sensitive than US citizens or that US BAT values protect employers more than employees. BAT values are conceived as ceiling values for healthy individuals. They are generally established for blood and/or urine and take into account the effects of the substances and an appropriate safety margin, being based on occupational medical and toxicological criteria for the prevention of adverse effects on health. Whole blood, serum, an urine samples are used as assay materials. Hair samples are not suitable assay materials for occupational medical testing, because hair growth is slow and thus the immediate exposure cannot be verified. Under workplace conditions, the employee's immediate intoxication is of concern, not the chronic or long-term exposure. Therefore, in occupational medicine, the diagnosis concerns itself with immediate intoxication. the diagnosis concerns itself with immediate intoxication. Occupational medical treatment is aimed at reducing the toxicity level to below the BAT level The most common "treatment" of acute workplace intoxication is the removal of the patient from the workplace. Chelation Chelation The process by which a molecule encircles and binds to a metal and removes it from tissue. Mentioned in: Heavy Metal Poisoning chelation is considered in serious conditions only, and reported cases are rare. Instead, the patient is monitored via blood or urine analysis, and as soon as levels fall below the accepted BAT range (usually within a day or two after exposure), "treatment" is considered successful. The patient is brought back to the workplace. In serious cases of intoxication, the patient is voluntarily removed from the workplace for one week or longer. In debilitating accidents, a patient is placed into early retirement, and treatment is palliative. Comparison of Reference Ranges for the Unexposed and Those Exposed at the Workplace It is apparent from the data below that, for most metals, a definite ceiling range does not exist. Different countries and regulatory agencies provide differing ranges, and these differences are usually due to the use of various analytical techniques of population models. For the general population, even for physicians, comparing reference ranges is cumbersome, because units may be given in mmol/L or [mu]g/dl, instead of the more common [mu]g/L. The Toxicity of (Some) Blood Metals Arsenic (Blood): Blood arsenic levels are not considered diagnostically useful, and the total arsenic concentration may be markedly increased after dietary consumption of seafood. Urine samples are more valid for the diagnosis of arsenic intoxication arsenic intoxication Arsenic poisoning A toxic trace metal that is a key component of herbicides, insecticides, rodenticides, wood preservatives, and used in manufacturing glass, and paints; the usual fatal dose is 100–200 mg; there are ± 1900 arsenic , but these too are influenced and often rise dramatically after a seafood meal. Hence, when taking a blood specimen for blood metal testing, the patient should be instructed not to eat seafood for at least one day prior to sample-taking and to refrain from smoking for as long as possible. Cigarette smoke does contain arsenic, beryllium beryllium (bərĭl`ēəm) [from beryl ], metallic chemical element; symbol Be; at. no. 4; at. wt. 9.01218; m.p. about 1,278°C;; b.p. 2,970°C; (estimated); sp. gr. 1.85 at 20°C;; valence +2. , nickel, cadmium, lead, and other potentially harmful metals. Hair and nail levels are useful only for diagnosing a past exposure. Lead (Blood): Lead in the human body can be measured in blood, urine, bones, teeth, or hair. By measuring an individual's blood lead level (BLL BLL Blood Lead Level BLL Bovis Lend Lease BLL Business Logic Layer BLL Buraku Liberation League (Japan) BLL Billund, Denmark - Billund (Airport Code) BLL Base Locator for Linkage ), we can detect lead poisoning lead poisoning or plumbism (plŭm`bĭz'əm), intoxication of the system by organic compounds containing lead. in adults or children. When blood lead is high, an increase in erythrocyte erythrocyte (ĭrĭth`rəsīt'): see blood. erythrocyte or red blood cell or red blood corpuscle Blood cell that carries oxygen from the lungs to the body tissues. protoporphyrin protoporphyrin /pro·to·por·phy·rin/ (-por´fi-rin) any of several porphyrin isomers, one of which is an intermediate in heme biosynthesis; it is accumulated and excreted excessively in feces in erythropoietic protoporphyria and variegate (EP) follows. (2) * The standard elevated blood lead level (BLL) for adults' set by the Centers for Disease Control (CDC See Control Data, century date change and Back Orifice. CDC - Control Data Corporation ) is 25 micrograms per deciliter deciliter /dec·i·li·ter/ (dL) (des´i-le?ter) one tenth (10minus;1) of a liter; 100 milliliters. Deciliter (dL) 100 cubic centimeters (cc). Mentioned in: Hypercholesterolemia (25 [micro]g/dl) of whole blood. This level recognizes that every adult has accumulated some lead contamination. * The level for a child is lower; currently it is 10 micrograms per deciliter (10 [micro]g/dl) of blood. (2) The CDC states that a blood lead level above 10 [micro]g/dL is a cause for concern. It also states that lead can impair development even at BLLs below 10 [micro]g/DL. (3) The German Environmental Agency's BLLs are lower than those set by US agencies. (See Table 1.)
Table 1: Blood Levels in Washington State Construction Workers
SIC Description Reports Reports Reports
Codes 25-39 40-49 50-59
[micro]g/dl [micro]g/dl [micro]g/dl
36 * Electronic & Other 197 162 51
Electric Equipment
3211 Flat Glass 369 43 2
1721 Painting and Paper Hanging 265 72 11
7539 Automotive Repair-Shops. 193 40 24
NEC
1622 Bridge, Tunnel & Elevated 118 19 9
Highway Construction
3321 Gray and Ductile iron 79 24 7
Foundries
2819 Industrial Inorganic 99 8 1
Chemicals, NEC
28 * Chemicals and Allied 70 3 1
Products
5051 Metals Service Centers & 63 8 1
Offices
3714 Motor Vehicle Parts & 48 12 1
Accessories
3229 Pressed and Blown Glass 43 7 2
and Glassware, NEC
5093 Scrap & Waste Materials 21 6 1
5531 Auto & Home Supply Stores 23 2 2
3731 Ship Building & Repairing 20 4 0
3364 Nonferrous Die Casting, 16 5 2
Exc. Aluminum
SIC Description Reports 60 Total
Codes [greater Reports
than or [mu]g/dl
equal [greater
to][mu]g/dl than or
equal to]
25
36 * Electronic & Other Electric 5 415
Equipment
3211 Flat Glass 1 415
1721 Painting and Paper Hanging 3 351
7539 Automotive Repair-Shops. NEC 9 266
1622 Bridge, Tunnel & Elevated Highway 1 147
Construction
3321 Gray and Ductile iron Foundries 7 117
2819 Industrial Inorganic Chemicals, 0 108
NEC
28 * Chemicals and Allied Products 0 74
5051 Metals Service Centers & Offices 0 72
3714 Motor Vehicle Parts & Accessories 0 61
3229 Pressed and Blown Glass and 1 53
Glassware, NEC
5093 Scrap & Waste Materials 4 32
5531 Auto & Home Supply Stores 1 28
3731 Ship Building & Repairing 0 25
3364 Nonferrous Die Casting, Exc. 0 23
Aluminum
* Figures are reported by 2-digit SIC if there were fewer than three WA
State employers in a 4-digit SIC category (WA State Employment
Security, 1999 employer units).
From Washington State Adult Blood Lead Registry Update, February 2003
Exit Ecology. Technical report 38-2003, Safety and Health Assessment
and Research for prevention (SHARP Exit Ecology), Washington State
Department of Labor and Industries Exit Ecology, Olympia, Washington.
In Australia, the acceptable level of lead in blood was lowered from 25 [micro]g/dL in 1992. In 1993, the National Health and Medical Research Council (NH&MRC See Maximum return criterion. ) set a national target for 1998 for all Australian to have a BLL less than 15 [micro]g/dL (except where they worked with lead), and strategies were put in place whereby 90% of pre-school children would have BLLs below 15 [micro]g.dL. In 1996, the National Blood Lead Survey (the Donovan Survey) found 7.7% of children aged one to four were above 10[micro]g/dL, and 1.7% were above 15 [micro]g/dL. (4) Biomonitoring Ranges for a Normal, i.e., Non-Exposed, Population; Levels Above the Given Range Indicate Need for Action: * CDC recommends that all children be screened for lead poisoning yearly. This is especially important for children between six months and six years of age. * Children with an erythrocyte protoporphyrin level (EP) of 35 micrograms per deciliter (= 360 [micro]g/l) should be tested for a blood lead level. * Children with a BLL of 20 micrograms per deciliter (= 200 [micro]g/L) or higher should be screened by their doctor for lead poisoning. * Medical treatment is necessary if the BLL is higher than 45 micrograms per decilitre (= 450 [micro]g/l). Levels of Acute Exposure as Utilized in Occupational Medicine The OSHA Safety and Health Achievement Recognition Program (SHARP) collects and maintains a registry of blood lead levels by occupation and industry. Table 1 shows elevated blood lead levels measured in Washington State construction workers. Blood results are reported in micrograms per deciliter ([mu]g/dl), and the data shows that exposure is common. Companies that do not test their workers are not represented, and sadly, many exposed workers do not have their blood tested. (2) (Note: 1mcg/dl = 10mcg/L) Treatment Options for Lead All forms of EDTA EDTA: see chelating agents. (NaEDTA, NaMgEDTA, CaEDTA) have a high lead-binding capacity. CaEDTA has been approved by the FDA to chelate chelate Any of a class of coordination or complex compounds consisting of a central atom of a metal (usually a transition element) attached to a large molecule (ligand). lead, and the proper infusion rate is 1gr/hr. If infused too quickly, EDTA is nephrotoxic nephrotoxic /neph·ro·tox·ic/ (nef´ro-tok?sik) destructive to kidney cells. Nephrotoxic Toxic, or damaging, to the kidney. . Although CaEDTA bolus injections are becoming increasingly popular, it is dangerous to administer EDTA at such a fast rate. The International Board of Clinical Metal Toxicology (IBCMT) strongly advises against it. (7) Cadmium (Blood): According to the Agency for Toxic Substances and Disease Registry The United States Agency for Toxic Substances and Disease Registry, (ATSDR) is an agency for the U.S. Department of Health and Human Services that is directed by a congressional mandate to perform specific functions concerning the effect on public health of hazardous (ATSDR ATSDR Agency for Toxic Substances & Disease Registry ), elevated blood cadmium levels confirm acute exposure, (Jarup 2002; ATSDR 1999) but do not correlate with body burden or clinical outcome. (5) According to the ATSDR, a blood test alone is not sufficient validation for treatment, possibly because blood cadmium levels are easily influenced through smoking or smoke exposure. The 95% confidence limit for blood cadmium levels in the United States for healthy nonexposed, nonsmokers is 0.4 micrograms per liter ([mu]g/L) (CDC 2005). ATSDR recognizes that occupationally exposed persons may have higher blood levels than the general population. OSHA (www.osha.gov) considers a whole blood level of 5[micro]g/l or higher hazardous. (5) Treatment Options for Cadmium All forms of EDTA (NaEDTA, NaMgEDTA, CaEDTA) bind cadmium. A recent statistical evaluation by Micro Trace Minerals Laboratory of post chelation urine tests (Figure 1) indicates that EDTA seems to be the best option available at this time. [FIGURE 1 OMITTED] Mercury (Blood): Blood levels are used as markers to determine the severity of a mercury exposure. For a standard blood mercury test, mercury is measured as total mercury (inorganic and organic). Except for methylmercury exposures, blood is considered useful if samples are taken within a few days of exposure. This is because most forms of mercury in the blood decrease by one-half every three days if exposure has been stopped. Thus, mercury levels in the blood provide more useful information after recent exposures than after long-term exposures. (6) Human Biomonitoring Range: Normal (unexposed population): < 5.8 [micro]g/L (US Environmental Protection Agency) Normal (unexposed population): < 8 [micro]g/L (University of lowa, USA) Normal (unexposed population): < 2 [micro]g/L (Environmental Protection Agency, Germany) Levels of Acute Exposure as Utilized in Occupational Medicine: BEI Bei (pā, bā), river, c.200 mi (320 km) long, formed by the union of two headstreams in the Nanling Mts., N Guangdong prov., S China. It flows S into the Xi River, E of Guangzhou, to form the Pearl River delta. (Biological Exposure Index): 15 [micro]g/L (total inorganic, end of shift, end of work week) BAT (Biological Tolerance Value): 50[micro]g/L (organic and inorganic) BAT (Biological Tolerance Value): 100[micro]g/L (organic) Treatment Options for Mercury When a blood test no longer reflects a mercury exposure, a DMPS DMPS dimercaptopropane sulfonate DMPS Defense Meteorological Satellite Program DMPS Dual Modular Power System DMPS Device Manager Proxy Stub challenge test may be performed to confirm or rule out mercury intoxication. DMSA DMSA dimercaptosuccinic acid. can also be used provoke mercury binding and excretion, though the binding ability of intravenously administered DMPS is much stronger. Note: many physicians assume that oral DMPS has the same binding capacity as IV DMPS. The fact is, the mercury-binding ability of oral DMSA and oral DMPS is similar, and both of these oral chelators have a lower mercury-binding capability than IV DMPS. Blood Metal Analysis Diagnosing Chronic (Over) Exposure Biomonitoring ranges apply for a population considered "nonexposed." Ironically and sadly, the long-term exposed are often chronically ill people with sad histories of "unexposed" until the diagnosis indicates a blood or urine value above the biomonitoring range. Table 2 shows human biomonitoring ranges as set by the German Environmental Agency. These ranges apply to people not working in industries that may lead to occupational exposure. People with past exposures or those exposed to low levels on a daily basis may or may not show blood levels above these ranges. Most importantly, unremarkable results do not rule out chronic exposure.
Table 2: Biomonitoring Ranges, Last Updated by German Environmental
Agency 2005 References Values for Arsenic (As) and Metals (Pb, Cd, Hg,
Pt, Ni) in Blood or Urine
Parameter and Population Year of Reference Value
Matrix Group/Period of Life Study
[Bibliographical]
Arsenic in urine Children (6 to 12 2001/2003 15.0 [micro]g/l
[39. 50] years) without fish
consumption 48 hours
before sample
collection (1), (2)
Adults (18 to 69 1997/99
years) without fish
consumption 48 hours
before sample
collection (3)
Lead in blood [6, Children (6 to 12 2001/2003 15.0
34, 42, 50] years) (1), (2) [micro]g/l (a)
Females (18 to 69 1997/99 70
years) (3) [micro]g/l (a)
Males (18 to 69 1997/99 90
years) (3) [micro]g/l (a)
Cadmium in urine Non-smoking children 2001/2003 0.5
[11, 42, 50] (6 to 12 years) (1) [micro]g/l (a)
Non-smoking adults 1197/99 1.0 [micro]g/l
(18 to 69 years) (3)
Mercury in blood Children (6 to 12 2001/2002 1.5
[13, 42, 50] years), fish [micro]g/l (a)
consumption [less
than or equal to]
times per month (1)
Adults (18 to 69 1997/99 2.0 [micro]g/l
years) fish
consumption [less
than or equal to]
times per month (3)
Nickel in urine Adults (but not a 4 3 [micro]g/l
[32] strictly
representative
reference sample)
(4)
Platinum in urine Adults (18 to 69 1997/99 10 ng/l
[13, 42] years) without teeth
with dental inlays,
crowns, bridge
elements of precious
metal (3)
Notes: [xy] bibliographical data publication:
http://www.umweltbundesamt.de/uba-info-daten-e/daten-e/monitor/pub.htm
(1) Source: Pilot study for the German Environmental Survey on Children
2001/2002 (GerES IV).
(2) Source: Project of the "Sentinel Health Department of Baden-
Wurttemberg" 2002/2003 (BW-EHS).
(3) Source: German Environmental Survey 1998 (GerES III).
(4) Source: based on publicatical data.
(a) An analytical uncertainty of [+ or -] 20% has to be considered.
When we suspect past or chronic exposure, but blood tests are negative, we consider a "challenge test," also referred to a "provocation test provocation test Medtalk 1 Any of a number of tests used to deliberately induce a suspected pathologic derangement–eg, provocation of ↑ intraocular pressure by ingestion of excess water 2 Neutralization, see there Orthopedics Any of a number of tests ." By introducing a chelating substance into the bloodstream, we force metal binding and excretion. Results are often astonishing. Depending on how much of a metal has been stored in the body, urine excretion levels may rise well above the expected range. In most cases, patients respond favorably, if not unexpectedly. Symptoms, even unrelated ones, may disappear. Every doctor practicing chelation therapy has such case histories. Case History Beate, a 45-year-old biologist, works in our laboratory. She is extremely disciplined and efficient, but rheumatoid arthritis rheumatoid arthritis Chronic, progressive autoimmune disease causing connective-tissue inflammation, mostly in synovial joints. It can occur at any age, is more common in women, and has an unpredictable course. (with a high positive RA factor) has proven to be a challenge since her early twenties. She had been on cortisone cortisone (kôr`tĭsōn'), steroid hormone whose main physiological effect is on carbohydrate metabolism. It is synthesized from cholesterol in the outer layer, or cortex, of the adrenal gland under the stimulation of adrenocorticotropic , but stopped after experiencing strong side effects Side effects Effects of a proposed project on other parts of the firm. . During her frequent rheumatic rheu·mat·ic adj. Relating to or characterized by rheumatism. n. One who is affected by rheumatism. rheumatic pertaining to or affected with rheumatism. attacks, strong pain medication was her only alternative. Beate has suffered from asthma since childhood and also suffers from Hashimoto disease. She currently takes thyroxin Thyroxin The hormone secreted by the thyroid gland. Mentioned in: Goiter thyroxine, thyroxin a hormone of the thyroid gland that contains iodine and is a derivative of the amino acid tyrosine. , 175 mcg daily. During history taking, it became apparent that the Hashimoto appeared after the removal of her many amalgam fillings, which her dentist took out "all at once and without any precautions." At that time, she experienced multiple food sensitivities and an allergy to penicillin. Migraine became another problem. Mercury overexposure overexposure too long an exposure time or too high a milliamperage causing too black a picture, loss of detail and some anomalies of translucency. seemed a reasonable diagnosis. Hair mercury levels were at 1.89 mg/kg (= ppm), far exceeding the upper range of 0.6 ppm. Medical analysis showed a normal renal function and blood pressure. We first tested her reaction to DMSA by giving her 500 mg under close supervision. Her urine mercury excretion level was a modest 3.37 mcg/g creatinine. Other than feeling weak and light-headed, she noticed no side effects. The next day, she felt amazingly well. Joint swelling and pain were noticeably decreased. We supported her nutritionally before the next "challenge test" two weeks later. Again, she felt weak and light-headed, urine results showed a slight increase in urine mercury at 5.36 [micro]g/g crea, and again, the day after, she was without pain and felt energetic. We have continued this treatment cycle, and so far results have been amazing. After three months of biweekly treatment, DMSA was increased to 1000 mg and urine mercury excretion rose to a significant 36.2 [micro]g/g crea. She continued to be symptom-free. A repeat RA factor turned out to be normal. Two weeks later, she experienced a monosodium glutamate monosodium glutamate: see glutamic acid. monosodium glutamate (MSG) White crystalline substance, a sodium salt of the amino acid glutamic acid. MSG is used to intensify the natural flavour of meats and vegetables. (MSG MSG: see glutamic acid. ) reaction after eating at an Italian restaurant. A severe migraine was followed by another rheumatic attack. The treatment cycle was temporarily stopped. Choosing the Most Appropriate Chelator chelator A chemical–eg, EDTA that binds metal ions from solutions. See Chelation therapy. Why did we, in Beate's case, not use IV DMPS, which is a stronger mercury chelator? We didn't do so for two reasons: 1. Beate is hypersensitive hy·per·sen·si·tive adj. Responding excessively to the stimulus of a foreign agent, such as an allergen; abnormally sensitive. hy and afraid of experiencing reactions. A softer approach seemed warranted. 2. DMPS injectables were unavailable at the time. We could have used oral DMPS, but it has a similar binding as DMSA. We did not use oral DMPS, because it has a stronger affinity to bind zinc, and Beate's hair analysis showed borderline zinc levels. Unlike oral DMPS, DMSA does not bind zinc in any significant way. Every chelating agent has a specific binding capacity to certain metals, and we can enhance the effectiveness of chelation therapy by paying attention to those chemical specificities. Similarly, we reduce the chelation benefit by ignoring "finer points." Diagnostically, it is important to find out the type and severity of the existing metal intoxication. In addition, it is important to identify existing deficiencies and pay attention to borderline deficiencies. If we would use DMPS (or EDTA) on a borderline zinc-deficient patient, we could create an acute deficiency. Consequently, we must initiate a nutritional program before chelation is started to prevent potential problems. Zinc deficiency zinc deficiency (zinkˑ d  ·fiˑ ·sh symptoms are not
unknown among patients who have undergone chelation therapy and who have
experienced side effects after DMPS or EDTA treatment. A proper
supplementation schedule could have avoided the problems.
Before any chelation treatment is started, we must know renal function and order additional diagnostic tests, depending on the patient's health problems. A cardiac patient will require a different diagnostic schedule than a neurological patient. After we diagnostically define the patient's general health status, we can select the appropriate and most effective chelating agent. Are So-Called Unexposed Patients in Need of Chelation? The term "unexposed" is used for people who do not work in a hazardous working environment and have not been exposed to environmental-or industry-related accidents. Unfortunately, chronic metal intoxication exists more than we are willing to admit. The following excerpt from the New York City New York City: see New York, city. New York City City (pop., 2000: 8,008,278), southeastern New York, at the mouth of the Hudson River. The largest city in the U.S. Health Report of July 23, 2007 should be a warning. It indicates that one in four New Yorkers has elevated blood mercury levels, a clear sign of mercury overexposure: Today's findings are the latest presented from New York New York, state, United States New York, Middle Atlantic state of the United States. It is bordered by Vermont, Massachusetts, Connecticut, and the Atlantic Ocean (E), New Jersey and Pennsylvania (S), Lakes Erie and Ontario and the Canadian province of City's Health and Nutrition Examination Survey (NYC-HANES), the first such survey ever conducted by a US city. It's possible that other cities have similarly high levels, or higher ones, but haven't yet documented them. Because mercury is a concern for the health of newborns, recommendations on mercury exposure are most important for pregnant and breastfeeding women. * Among women 20-49 years old in New York City, the average blood mercury level is 2.64 [micro]g/L (micrograms per liter), three times that of similarly-aged women nationally (0.83 [micro]g/L). * Approximately one-quarter of New York City women in this age group have a blood mercury level at or above 5 [micro]g/L, the New York State reportable level. * People who eat fish three or fewer times each week have, on average, levels of mercury below the reportable level, while average readings exceed the reportable level among those who eat fish four or more times. * Higher-income New Yorkers have higher mercury levels; New Yorkers in the highest income bracket average 3.6 [micro]g/L, compared to 2.4 [micro]g/L among the lowest income group. * Average blood mercury levels are considerably higher among New York City Asian women (4.1 [micro]g/L); nearly half (45%) have blood mercury levels at or above the State reportable level. * Among Asians, foreign-born Chinese women have particularly high levels compared to the rest of New York City. Two-thirds (66%) have mercury at or above the reportable level. * Foreign-born Chinese New Yorkers eat an average of three fish meals per week, compared to about one among New Yorkers overall. About one-quarter of Chinese New Yorkers eat fish five or more times each week, compared to fewer than one in 15 overall. Should we routinely check whole blood metals? Do one in four New Yorkers need chelation? The New York City Health Report speaks for itself. Is the mercury problem unique to New Yorkers? It would be naive to believe that. Notes (1.) Committee on Human Biomonitoring for Environmental Toxicants, National Research Council; Human Biomonitoring for Environmental Chemicals (2006), Board on Environmental Studies and Toxicology (BEST) (2.) Dept. of Ecology, State of Washington. Available at: http://www.ecy.wa.gov/programs/hwtr/demodebris/pages2/lbloodtest.html (3.) CDC Weekly, December 22,2000;49(50):1133-7. Available at: www.cdc.gov/mmwr/preview/mmwrhtml/mm4950a3.htm (4.) Australian Government. Dept. of Environmental, Water, Heritage and the Art. Available at: http://www.deh.gov.au/settlements/chemicals/index.html. (5.) Agency for Toxic Substances and Disease Registry (ATSDR). 1999. Toxicological profile for Cadmium. Atlanta, GA: US Department of Health and Human Services Noun 1. Department of Health and Human Services - the United States federal department that administers all federal programs dealing with health and welfare; created in 1979 Health and Human Services, HHS , Public Health Service. (6.) Ibid. (7.) Van der Schaar P. IBCMT Textbook of Clinical Metal Toxicology. 2008. Available at: www.ibcmt.com.
Children (USA) < 100 [micro]g/L = 10[micro]g/dl
Adults (USA) < 250 [micro]g/L
Children and adults (Germany) < 50 (Table 1)
Females (18-69yrs) (Germany) < 70 (Table 1)
Males (18-69yrs) (Germany) < 90 (Table 1)
Adults (occupational exposure US ranges)
OSHA action level > 40 ug/dl = 400[micro]g/L
BEI (Biological Exposure) > 30 ug/dl = 300[micro]g/L
BAT (Biological Tolerance) > 70 ug/dl = 700[micro]g/L
German agencies have set stricter standards:
Non-smoking children 6-12 years < 0.5[micro]g/L
Non-smoking adults, 18-69 years < 1.0[micro]g/L
Blood Sampling Specifics
Collection Metal free royal blue EDTA tube Please note that
Medium: Heparin or regular EDTA tubes are no longer used
for metal testing due to contamination.
Minimum: 3mL whole blood
Analysis: Must be AA hydrid method or ICP-MS with collision
or cell reaction technique. All other ICP-MS
instruments are too much affected by interferences
and are unable to have the needed sensitivity to
detect low levels. False highs may be a problem.
Analytical Two days to one week
Time:
by E.Blaurock-Busch, PhD E. Blaurock-Busch, PhD, founded the German analytical laboratory service Micro Trace Minerals (MTM MTM Medication Therapy Management MTM Minutes to Midnight (Linkin Park album) MTM Mary Tyler Moore (actress) MTM Made to Measure MTM Motoren-Technik-Mayer MTM Methods Time Measurement ) in 1975, and the Coloradobased laboratory Trace Minerals International in 1984, which was sold to King James Medical Laboratory in 2000. She now works exclusively at MTM, Germany and is advisor to the scientific board of IBCMT. She has written several books in German and numerous articles. [ILLUSTRATION OMITTED] |
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