Edetic Acid | Genelabs.com

A chelating agent (chelating agents) that sequesters a variety of polyvalent cations. It is used in pharmaceutical manufacturing and as a food additive. [PubChem]
Brands	Cheladrate Endrate Havidote Titriplex Versenate
Categories	Anticoagulants Chelating Agents Food Additives
Manufacturers	Graceway pharmaceuticals llc Watson laboratories inc 3m pharmaceuticals inc
Packagers	Bioniche Pharma Graceway Pharmaceuticals Hospira Inc. Merit Pharmaceuticals North America Genescience LLC Septodont Inc. Torrance Co. V Sab Medical Labs Inc.
Synonyms	CaEDTA Calcium Disodium Edetate (JAN) Calcium Disodium Versenate Calcium disodium versenate (TN) Edetate Calcium Edetate calcium disodium (USP) EDT EDTA

indication

For the reduction of blood levels and depot stores of lead in lead poisoning (acute and chronic) and lead encephalopathy, in both pediatric populations and adults.

pharmacology

Edetate calcium is a heavy metal chelating agent. The calcium in edetate calcium can be displaced by divalent or trivalent metals to form a stable water soluble complex that can be excreted in the urine. In theory, 1 g of edetate calcium can theoretically bind 620 mg of lead, but in reality only about 5 mg per gram is actually excreted into the urine in lead poisoned patients. In addition to chelating lead, edetate calcium also chelates and eliminates zinc from the body. Edetate calcium also binds cadmium, copper, iron and manganese, but to a much lesser extent than either lead or zinc. Edetate calcium is relatively ineffective for use in treating mercury, gold or arsenic poisoning.

mechanism of action

The pharmacologic effects of edetate calcium disodium are due to the formation of chelates with divalent and trivalent metals. A stable chelate will form with any metal that has the ability to displace calcium from the molecule, a feature shared by lead, zinc, cadmium, manganese, iron and mercury. The amounts of manganese and iron metabolized are not significant. Copper is not mobilized and mercury is unavailable for chelation because it is too tightly bound to body ligands or it is stored in inaccessible body compartments. The excretion of calcium by the body is not increased following intravenous administration of edetate calcium disodium, but the excretion of zinc is considerably increased.

toxicity

Inadvertent administration of 5 times the recommended dose, infused intravenously over a 24 hour period, to an asymptomatic 16 month old patient with a blood lead content of 56 mcg/dl did not cause any ill effects. Edetate calcium disodium can aggravate the symptoms of severe lead poisoning, therefore, most toxic effects (cerebral edema, renal tubular necrosis) appear to be associated with lead poisoning. Because of cerebral edema, a therapeutic dose may be lethal to an adult or a pediatric patient with lead encephalopathy. Higher dosage of edetate calcium disodium may produce a more severe zinc deficiency.

biotransformation

Almost none of the compound is metabolized.

absorption

Poorly absorbed from the gastrointestinal tract. Well absorbed following intramuscular injection.

half life

The half life of edetate calcium disodium is 20 to 60 minutes.

route of elimination

It is excreted primarily by the kidney, with about 50% excreted in one hour and over 95% within 24 hours.2 Almost none of the compound is metabolized.

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