Heavy Metals

World Health Organization determined 13 heavy metals as the health harming compounds; arsenic, cadmium, cobalt, chromium, copper, mercury, manganese, nickel, lead, tin and titanium, initiating and exacerbating the pathologies. Some intoxication are due to the environmental pollutions, involves large populations and often not instantly might be recognized. Fast overview of the short clinical manifestations of such intoxications, epidemiological intoxication history facts as well as the possible new mechanism of the treatment might be beneficial for the readers.

years old have been killed from the outbreak and thousands of people affected, including >2000 children left with permanent disabilities [5][6][7] Dooyema, et al. [7] measured the concentrations of soil Pb and soil Hg which showed >100,000 ppm and about 4600 ppm for Pb and Hg, respectively.The study found that surviving children<five years of age had blood Pb levels (BLL) of about 370ug/dL which is above the CDC recommended BLL of 5ug/dL [8].It is necessarily to mention, the developing brain of children are very susceptible to the impact of the heavy metals.Heavy metals easily penetrate trough the hemato encephalic barriers and impair the physiological activity of the neuro-glial environment.
The developing brain is vulnerable to injury from toxic metals that interfere with the critical developmental processes, i.e., cellular proliferation, migration, differentiation, synaptogenesis myelination and apoptosis in the central nervous system (CNS) [9].The limited capacity of the developing CNS to compensate for the cell loss and the disruptions in neural networking results in compromised neuronal functions [10] and increased risk of neurodegeneration [11].Heavy metals including arsenic (As), cadmium (Cd), and lead (Pb) have received attention as both environmental contaminants and potential neurotoxicological hazards [12].Exposure to the metals in utero and in infancy is associated with risk of im-paired cognitive development [13], subclinical brain dysfunction [14] and behavioral anomalies [15].Heavy (Cd, Hg, Pb, and As) and transition metals (Fe, Cu, Co, and Cr), acting as powerful oxidative stress inducers and are responsible for various forms of nephropathy, as well as for some types of cancers [16].
Our laboratory investigates the one of the main initiators of the free radical's formation Xanthine Oxidoreductase, which is responsible for the purine catabolism final steps and standing in the mentioned pathway as the regulative enzymes.Under normal circumstances, most amount of this enzyme exists in the form of NAD-dependent cytosolic dehydrogenase (XDH).However, in pathological conditions Xanthine Oxidase (XO) might be formed due to the limited proteolysis [17].XO as well as the XDH are also responsible for the hydroxylation of a wide variety pyrimidine, pterin, and aldehyde substrates (EC: 1.17.1.4).We have proceeded the investigations related with the impact of the heavy metals on the activity of XOR in the rat's brain.The published results are evidencing, heavy metals are elevating XOR activity and, consequently, elevating the formation of free radicals.Cd 2+ elevated the activity of the XOR in comparison with the control 0,5338±0,1542 vs 0,6488±0,3635.Cr 6+ ions elevated the activity of XOR until 2,3996±0,3541 (p#<0.05),Pb 2+ -until 0,9492±0,3880 and Hg 2+ -until 1,1604±0,6918 [17].Also, in our previous investigations, we have shown, that pyridoxine or vitamin B6 is able to diminish the activity of XOR, in the low concentration (0.05mg/ml) [18].Pyridoxine was able mostly to diminish the activity of the XOR in the presence of the heavy metals.The impact of the ions of the Cd 2+ were switching the value until 0,8522±0,3461, for Cr 6+ until 0,1098±0,1098; for Pb 2+ -0,0130±7,9066e-3 and for Hg 2 +-0,6791±0,3572 (p#<0,037489 between the activation of Pb 2+ and that suppression under the impact of the pyridoxine; p#<0.05 between the activation of Cr 6+ and that suppression under the impact of the pyridoxine) in comparison with the controls, where there were added the substrate and [17].Thus, B6 is suggested for the use along with the other medications to cure heavy metals intoxication due to the inhibition of free radicals' formation (Figure 1).

Pb
The symptoms of acute lead poisoning are headache, irritability, abdominal pain and various symptoms related to the nervous system.Lead encephalopathy is characterized by sleeplessness and restlessness.Children may be affected by behavioral disturbances, learning and concentration difficulties.In severe cases of lead encephalopathy, the affected person may suffer from acute psychosis, confusion and reduced consciousness.People who have been exposed to lead for a long time may suffer from memory deterioration, prolonged reaction time and reduced ability to understand.Individuals with average blood lead levels under 3 µmol/l may show signs of peripheral nerve symptoms with reduced nerve conduction velocity and reduced dermal sensibility.If the neuropathy is severe the lesion may be permanent.In less serious cases, the most obvious sign of lead poisoning is disturbance of hemoglobin synthesis, and long-term lead exposure may lead to anemia [19].
Acute exposure to lead is known to cause proximal renal tubular damage [19].IARC classified lead as a 'possible human carcinogen' based on enough animal data and insufficient human data in 1987.
Since then a few studies have been published, the overall evidence for lead as a carcinogen being only weak, the most likely candidates are lung cancer, stomach cancer and gliomas [20].

Studies with single metal exposure have demonstrated that
As, Cd, or Pb infiltrate the immature blood-brain barrier (BBB) and accumulate in developing brain [21].Pb uptake through the BBB disrupts Ca2þ transport mechanism [22] and promotes activation of mitogen-activated protein (MAP) kinases in apoptotic glial cells [23].The sequestration of Pb at the level of the choroid plexus undermines brain growth and affects learning and cognitive functions of CNS [22], especially in children.Combination of 1-month pre-exposure of HgC l2 before MI changed the endothelial generation of oxidative stress induced by mercury exposure from NADPH oxidase pathway to XO (xanthine oxidase)-dependent ROS production [24].It has been suggested that reactive oxygen intermediates (ROIs) may have a role in the genotoxic effects of lead (Pb 2+ ) and mercury (Hg 2+ ).
Pb 2+ and Hg 2+ (0.1-1 μM) had no effect on the activities of partially purified catalase, glutathione peroxidase, or glutathione reductase, important enzymes involved with antioxidant defense, but these metals stimulated the activities of copper-zinc superoxide dismutase (CuZn-SOD) and xanthine oxidase (XO).Allopurinol (50μM), a specific inhibitor of xanthine oxidase, inhibited the induction of H 2 O 2 by Pb 2+ (0.8-1μM) and Hg 2+ (1μM) and inhibited Pb 2+ -and Hg 2+ -induced mutagenesis.These results demonstrate that Pb 2+ and Hg 2+ disrupt the redox status of AS52 cells by enhancing the activities of CuZn-SOD and XO [25].

Cd
In vivo and in vitro studies have revealed that acute or chronic Cd exposure enhances oxidative stress in astrocytes and accumulates reactive oxygen species (ROS) that induces astrocytic death [26].Perinatal exposure to Cd induces anxiety [27,28] and reduces learning ability of offspring [28].Cadmium is a toxic metal with negative effects on health [29].Previous studies have confirmed the pathogenic role of cadmium exposure in renal damage, bone destruction and cancer [30].To determine whether CdB in Chinese adults is associated with serum UA (Uric Acid) and hyperuricemia, 2996 participants from the cross-sectional SPECT-China study were recruited.A positive relationship between serum UA and CdB was found in Chinese men after adjusting for the estimated glomerular filtration rate (eGFR), current smoking status, diabetes, dyslipidemia, hypertension and body mass index and in participants with eGFR > 60mL/min per 1.73m 2 .Further, the odds ratio of hyperuricemia increased with increasing CdB quartiles (P for trend < 0.05) in men.In conclusion, CdB was positively related to the serum UA level [31].These data clearly evidencing about the activation of XOR and Cd intoxication process of the organism.
Inhalation of cadmium fumes or particles can be life threatening, and although acute pulmonary effects and deaths are uncommon, sporadic cases still occur [32,33].Cadmium exposure may cause kidney damage [34].IARC has classified cadmium as a human carcinogen (group I) based on enough evidence in both humans and experimental animals [35].Cadmium has been associated with prostate cancer, but both positive and negative studies have been published.Early data indicated an association between cadmium exposure and kidney cancer [36].

As
Chronic exposure to As, even at a sub micromolar concentration, promotes oxidative stress [37] and induces neuroglial damage in human brain [38].Intoxication with As presents deficits in spontaneous locomotor activity (SLA) and alterations in learningmemory task during postnatal development [39].Inorganic arsenic is acutely toxic and intake of large quantities leads to gastrointestinal symptoms, severe disturbances of the cardiovascular and central nervous systems, and eventually death.In survivors, bone marrow depression, hemolysis, hepatomegaly, melanosis, polyneuropathy and encephalopathy may be observed.Ingestion of inorganic arsenic may induce peripheral vascular disease, which in its extreme form leads to gangrenous changes (black foot disease, only reported in Taiwan).Populations exposed to arsenic via drinking water show excess risk of mortality from lung, bladder and kidney cancer, the risk increasing with increasing exposure.There is also an increased risk of skin cancer and other skin lesions, such as hyperkeratosis and pigmentation changes [40].

Hg
Acute mercury exposure may give rise to lung damage.Chronic poisoning is characterized by neurological and psychological symptoms, such as tremor, changes in personality, restlessness, anxiety, sleep disturbance and depression.The symptoms are reversible after cessation of exposure.Because of the bloodbrain barrier there is no central nervous involvement related to inorganic mercury exposure.Metallic mercury may cause kidney damage, which is reversible after exposure has stopped.It has also been possible to detect proteinuria at relatively low levels of occupational exposure.Metallic mercury is an allergen, which may cause contact eczema, and mercury from amalgam fillings may give rise to oral lichen.It has been feared that mercury in amalgam may cause a variety of symptoms.This so-called 'amalgam disease' is, however, controversial, and although some authors claim proof of symptom relief after removal of dental amalgam fillings [41], there is no scientific evidence of this [42].
Organic mercury Methyl mercury poisoning has a latency of 1 month or longer after acute exposure, and the main symptoms relate to nervous system damage [43].The earliest symptoms are paresthesia and numbness in the hands and feet.Later, coordination difficulties and concentric constriction of the visual field may develop as well as auditory symptoms.High doses may lead to death, usually 2-4 weeks after onset of symptoms.The Minamata catastrophe in Japan in the 1950s was caused by methyl mercury poisoning from fish contaminated by mercury discharges to the surrounding sea.In the early 1970s, more than 10,000 persons in Iraq were poisoned by eating bread baked from mercury-polluted grain, and several thousand people died because of the poisoning.However, the general population does not face significant health risks from methyl mercury exposure except for certain groups with high fish consumption.A high dietary intake of mercury from consumption of fish has been hypothesized to increase the risk of coronary heart disease [44].
Early recognition of the possible environmental pollutions and organism intoxication is the import environmental, political, health conserving and protecting primer duty for any and especially for the developing countries.

Figure 1 :
Figure 1: Reversed by B6 impact of heavy metals on XOR activity.