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Dr. RAGHU PRASADA M S
MBBS,MD
ASSISTANT PROFESSOR
DEPT. OF PHARMACOLOGY
SSIMS & RC.
Chele-claw- chelating agents usually contain polar
groups such as –SH or –OH which can bind a metal ion
as endogenous ligands bind to metal ion and form
stable non-toxic water soluble complexes
Relative affinity of chelator to heavy metal
Distribution of chelator in body
Capacity to mobilize the complex
Half life of heavy metal
Time after exposure
Heavy metals combines with
one or more reactive groups (Ligands)
Oxygen (-OH, -COO, -OPO)
Nitrogen (-NH2, -NH)
Sulphur (-SH, -S-S)
Hamper physiological function
Enzyme inhibition, Oxidative stress
Chelating agents useful as drugs are:
Dimercaprol (BAL)
Dimercaptosuccinic acid (DMSA)
Dimercaptopropane sulfonic acid (DMPS)
Disodium edetate
Calcium disodium edetate
Pencillamine
Desferrioxamine
Deferiprone
Drug
EDTA, DMSA ----------
Dimercaprol ---------------
Succimer (DMSA)
DMPS --------
Penicillamine, -------------
Trientine
Desferrioxamine -----------
Deferiprone -----------
Used against
Lead
Arsenic, copper, mercury
Lead, arsenic, mercury
Copper, mercury, lead
Copper
Iron
Iron
It was synthesized during the world war II by Britishers
as an antidote to arsenic war gas lewisite
Oily, pungent smelling, viscous fluid
It is administered i.m in oil (arachis oil)
-SH ligands of dimercaprol compete with –SH groups of
enzymes for heavy metal
Dimercaprol –metal complex is stable and excreted in
urine( urine should be kept alkaline to prevent
dissociation)
Uses:
For the treatment of arsenic and mercury poisoning
As adjuvant to Cal. disod. Edetate in lead poisoning
As an adjuvant to pencillamine in copper poisoning
and in Wilson’s disease
Contraindicated in iron and cadmium poisoning
As BAL-Fe-complex is toxic
Adverse effects:
Frequent, dose related, but generally not damaging
Rise in BP, tachycardia, tingling and burning sensations,
inflammation of mucous membranes, sweating,
cramps, headache and anxiety
Dose 5mg/kg followed by 2-3mg/kg 4hr/2days
2,3 Dimercapro Succinic acid
Dimercaprol analogue
Water soluble, less toxic and orally effective
Specific for the treatment of lead intoxication and
needs no combination with edetate calcium disodium
Effective in allevating acute toxicity and preventing
distribution of orally administered mercury
Side effects are nausea, anorexia, raised serum amino
transferases and loose motions
Dose-10mg/kg 8hrly/5days
Dimercaptopropane sulfonic Acid
Dimercaprol analogue
Water soluble, less toxic
Can be administered orally as well as IV
Used for severe acute poisoning by mercury and arsenic
Also effective in the treatment of lead poisoning
Dose-3-5mg/kg 4hrly by i.v in 20min
Adverse effects are low, except for mild self-limited
urticaria, IV infusion may cause hypotension
Ethylene Diamine tetra acetic acid disodium calcium salt
It is a disodium salt of EDTA
EDTA is a potent chelator for Ca+ and produces life
threatening tetany.
Causes tetany on i.v. injection (but not on slow infusion)
Can be used for emergency control of hypercalcaemia
(rare) 50mg/kg i.v. over 2-4hours
Ethylene Diamine tetra acetic acid disodium calcium salt
It is a disodium salt of EDTA
Potent chelator of many divalent(lead, zinc, cadmium,
manganese and mercury). In this exchange process, its own
calcium is displaced from the molecule
Calcium chelator of Na2 EDTA
Has a high affinity for lead
Most important use is lead poisoning
Poorly absorbed from GI –given i.m or i.v.
i.m is very painful –i.v. preferred
Not metabolized
Excreted by glomerular filtration and tubular secretion
DTPA-Diethylene Triamine Penta Acetic Acid
Is useful in removing radioactive uranium and
plutonium
Adverse reactions:
Does not produce tetany –relatively safe
Nephrotoxicity-Kidney damage with proximal tubular
necrosis –but dose related
An acute febrile reaction with chills, body ache,
malaise, tiredness occurs in some individuals
Dose- 50-75mg/kg /day i.v
Dimethylcysteine is a water soluble degradation
product of penicillin
D –isomer is used-relatively non toxic compared to l –
isomer (optic neuritis) is used in copper poisiining
Easily absorbed from GIT
Little metabolized, excreted in urine and faeces
It has strong copper chelating property and was used
in 1956 for Wilson’s disease
It selectively chelates Cu, Hg, Pb and Zn
Wilson’s disease (hepatolenticular degeneration)
Copper/ mercury (alternate to BAL & DMSA) poisoning
Adjuvant to cal. disod. Edetate in lead poisoning but
DMSA is preferred
Cystinuria and cystine stones-it complexes with cystine
and prevents precipitation in the urinary tract
Scleroderma –benefits by increasing the soluble
collagen
It was used as a disease modifying drug in rheumatoid
arthritis, but now replaced by safer drugs
Short term administration –does not cause much
problem (cutaneous reactions)
Long term use –produces pronounced toxicity
hypersensitivity
Dermatological, renal,
Hematological-leukopenia, aplastic anemia
and collagen tissue toxicities
Dose-0.5-1g daily in divided doses
Triethyl tetramine dihydrochloride
Less toxic alternative to pencillamine in copper
poisoning
Also effective orally
1gm BD on empty stomach
Adverse effect
Iron deficiency
Ferrioxamine derivative devoid of iron
Obtained from actinomycete
High affinity for Fe3+
1gm is capable of chelating 85mg of elemental iron
Unique property that it can remove iron from ferritin,
haemosiderin and to some extent from transferrin but not
from hemoglobin or cytochrome
Low affinity for calcium
Little of orally administered desferrioxamine is absorbed
Parenterally –partly metabolized, rapidly excreted in urine
Uses:
Acute iron poisoning: mostly in children, important
and life saving
Transfusion siderosis-blood transfusion to patients of
thalassemia
With hemodialysis in treatment of aluminium toxicity
in renal failure
Adverse effects:
Hypotensive shock due to histamine release
Abdominal pain, muscle cramps, fever and diarrhoea
Dose- i.v ,10-15mg/kg/hr infusion
Orally active iron chelator
Used in transfusion siderosis
Somewhat less effective, alternate to injected
desferrioxamine
Side effects and cost of treatment are reduced
Also indicated in iron poisoning (less effective than
desferrioxamine) and iron load in liver cirrhosis
Side effects are:
Anorexia, vomiting, altered taste, joint pain, reversible
neutropenia, rarely agranulocytosis
Long term safety is not yet known
Dose-50-100mg/kg
Oral iron chelator
For chronic iron overload- beta thalassemia
High affinity for iron, less affinity for zinc, copper
Iron deferasirox chelator complex is secreted through
bile and excreted in faeces
DEXRAZOXANE-used to protect against cardiotoxic
drugs—anthracyclines-doxorubicin, daunorubicin
Primary goals of chelation therapy:
To reduce metal retention
To decrease morbidity and mortality
To prevent complications
Administer less toxic chelator when possible
Unsolved issues:
Chelation of cadmium, chromium, platinum…
Chelation therapy in infants, children and during pregnancy
Combined chelation therapy
THANKYOU
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Chelating Agents in Heavy Metal Poisoning

  • 1. Dr. RAGHU PRASADA M S MBBS,MD ASSISTANT PROFESSOR DEPT. OF PHARMACOLOGY SSIMS & RC.
  • 2. Chele-claw- chelating agents usually contain polar groups such as –SH or –OH which can bind a metal ion as endogenous ligands bind to metal ion and form stable non-toxic water soluble complexes Relative affinity of chelator to heavy metal Distribution of chelator in body Capacity to mobilize the complex Half life of heavy metal Time after exposure
  • 3. Heavy metals combines with one or more reactive groups (Ligands) Oxygen (-OH, -COO, -OPO) Nitrogen (-NH2, -NH) Sulphur (-SH, -S-S) Hamper physiological function Enzyme inhibition, Oxidative stress
  • 4. Chelating agents useful as drugs are: Dimercaprol (BAL) Dimercaptosuccinic acid (DMSA) Dimercaptopropane sulfonic acid (DMPS) Disodium edetate Calcium disodium edetate Pencillamine Desferrioxamine Deferiprone
  • 5. Drug EDTA, DMSA ---------- Dimercaprol --------------- Succimer (DMSA) DMPS -------- Penicillamine, ------------- Trientine Desferrioxamine ----------- Deferiprone ----------- Used against Lead Arsenic, copper, mercury Lead, arsenic, mercury Copper, mercury, lead Copper Iron Iron
  • 6. It was synthesized during the world war II by Britishers as an antidote to arsenic war gas lewisite Oily, pungent smelling, viscous fluid It is administered i.m in oil (arachis oil) -SH ligands of dimercaprol compete with –SH groups of enzymes for heavy metal Dimercaprol –metal complex is stable and excreted in urine( urine should be kept alkaline to prevent dissociation)
  • 7. Uses: For the treatment of arsenic and mercury poisoning As adjuvant to Cal. disod. Edetate in lead poisoning As an adjuvant to pencillamine in copper poisoning and in Wilson’s disease Contraindicated in iron and cadmium poisoning As BAL-Fe-complex is toxic
  • 8. Adverse effects: Frequent, dose related, but generally not damaging Rise in BP, tachycardia, tingling and burning sensations, inflammation of mucous membranes, sweating, cramps, headache and anxiety Dose 5mg/kg followed by 2-3mg/kg 4hr/2days
  • 9. 2,3 Dimercapro Succinic acid Dimercaprol analogue Water soluble, less toxic and orally effective Specific for the treatment of lead intoxication and needs no combination with edetate calcium disodium Effective in allevating acute toxicity and preventing distribution of orally administered mercury Side effects are nausea, anorexia, raised serum amino transferases and loose motions Dose-10mg/kg 8hrly/5days
  • 10. Dimercaptopropane sulfonic Acid Dimercaprol analogue Water soluble, less toxic Can be administered orally as well as IV Used for severe acute poisoning by mercury and arsenic Also effective in the treatment of lead poisoning Dose-3-5mg/kg 4hrly by i.v in 20min Adverse effects are low, except for mild self-limited urticaria, IV infusion may cause hypotension
  • 11. Ethylene Diamine tetra acetic acid disodium calcium salt It is a disodium salt of EDTA EDTA is a potent chelator for Ca+ and produces life threatening tetany. Causes tetany on i.v. injection (but not on slow infusion) Can be used for emergency control of hypercalcaemia (rare) 50mg/kg i.v. over 2-4hours
  • 12. Ethylene Diamine tetra acetic acid disodium calcium salt It is a disodium salt of EDTA Potent chelator of many divalent(lead, zinc, cadmium, manganese and mercury). In this exchange process, its own calcium is displaced from the molecule Calcium chelator of Na2 EDTA Has a high affinity for lead Most important use is lead poisoning Poorly absorbed from GI –given i.m or i.v. i.m is very painful –i.v. preferred Not metabolized Excreted by glomerular filtration and tubular secretion
  • 13. DTPA-Diethylene Triamine Penta Acetic Acid Is useful in removing radioactive uranium and plutonium Adverse reactions: Does not produce tetany –relatively safe Nephrotoxicity-Kidney damage with proximal tubular necrosis –but dose related An acute febrile reaction with chills, body ache, malaise, tiredness occurs in some individuals Dose- 50-75mg/kg /day i.v
  • 14. Dimethylcysteine is a water soluble degradation product of penicillin D –isomer is used-relatively non toxic compared to l – isomer (optic neuritis) is used in copper poisiining Easily absorbed from GIT Little metabolized, excreted in urine and faeces It has strong copper chelating property and was used in 1956 for Wilson’s disease It selectively chelates Cu, Hg, Pb and Zn
  • 15. Wilson’s disease (hepatolenticular degeneration) Copper/ mercury (alternate to BAL & DMSA) poisoning Adjuvant to cal. disod. Edetate in lead poisoning but DMSA is preferred Cystinuria and cystine stones-it complexes with cystine and prevents precipitation in the urinary tract Scleroderma –benefits by increasing the soluble collagen It was used as a disease modifying drug in rheumatoid arthritis, but now replaced by safer drugs
  • 16. Short term administration –does not cause much problem (cutaneous reactions) Long term use –produces pronounced toxicity hypersensitivity Dermatological, renal, Hematological-leukopenia, aplastic anemia and collagen tissue toxicities Dose-0.5-1g daily in divided doses
  • 17. Triethyl tetramine dihydrochloride Less toxic alternative to pencillamine in copper poisoning Also effective orally 1gm BD on empty stomach Adverse effect Iron deficiency
  • 18. Ferrioxamine derivative devoid of iron Obtained from actinomycete High affinity for Fe3+ 1gm is capable of chelating 85mg of elemental iron Unique property that it can remove iron from ferritin, haemosiderin and to some extent from transferrin but not from hemoglobin or cytochrome Low affinity for calcium Little of orally administered desferrioxamine is absorbed Parenterally –partly metabolized, rapidly excreted in urine
  • 19. Uses: Acute iron poisoning: mostly in children, important and life saving Transfusion siderosis-blood transfusion to patients of thalassemia With hemodialysis in treatment of aluminium toxicity in renal failure Adverse effects: Hypotensive shock due to histamine release Abdominal pain, muscle cramps, fever and diarrhoea Dose- i.v ,10-15mg/kg/hr infusion
  • 20. Orally active iron chelator Used in transfusion siderosis Somewhat less effective, alternate to injected desferrioxamine Side effects and cost of treatment are reduced Also indicated in iron poisoning (less effective than desferrioxamine) and iron load in liver cirrhosis
  • 21. Side effects are: Anorexia, vomiting, altered taste, joint pain, reversible neutropenia, rarely agranulocytosis Long term safety is not yet known Dose-50-100mg/kg
  • 22. Oral iron chelator For chronic iron overload- beta thalassemia High affinity for iron, less affinity for zinc, copper Iron deferasirox chelator complex is secreted through bile and excreted in faeces DEXRAZOXANE-used to protect against cardiotoxic drugs—anthracyclines-doxorubicin, daunorubicin
  • 23. Primary goals of chelation therapy: To reduce metal retention To decrease morbidity and mortality To prevent complications Administer less toxic chelator when possible Unsolved issues: Chelation of cadmium, chromium, platinum… Chelation therapy in infants, children and during pregnancy Combined chelation therapy