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Principles of toxicology

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Amna Medani
Amna Medani

This document discusses the key principles of toxicology including: - Toxicology is the science of the adverse effects of chemicals on living organisms. Different types of toxicologists study toxicity through tests, mechanisms of action, and risk assessment. - Descriptive toxicologists perform toxicity tests to evaluate risk, while mechanistic toxicologists determine how chemicals cause effects. Regulatory toxicologists judge risks to make chemicals available. - Toxicity depends on dose and can be acute or chronic. Factors like chemical forms, metabolites, interactions, and individual susceptibility influence effects. - Toxicity tests in animals are used to estimate risks before human exposure. Acute, subacute and chronic tests provide information on signs, organs and

Education
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04/27/15 Dr. Medani A.B. ,2006 Principles of toxicologyPrinciples of toxicology -It is the science of the adverse effects of chemicals on-It is the science of the adverse effects of chemicals on living organisms.living organisms. -A descriptive toxicologist performs toxicity tests toA descriptive toxicologist performs toxicity tests to obtain information that can be used to evaluate the riskobtain information that can be used to evaluate the risk of exposure to a chemical pose to human beings and theof exposure to a chemical pose to human beings and the enviroment.enviroment. -Amechanistic toxicologist attempts to determine howAmechanistic toxicologist attempts to determine how chemicals exert deleterious effects on living organisms .chemicals exert deleterious effects on living organisms . -A regulatory toxicologist judges whether or not a drugA regulatory toxicologist judges whether or not a drug or other chemicals has a low enough risk to justify makingor other chemicals has a low enough risk to justify making it available for its intended purpose .it available for its intended purpose .
04/27/15 Dr. Medani A.B. ,2006 Con. • An acceptable daily intake (ADI) is the input of a chemical that can be consumed over an entire life-time without any apprciable risk. • A threshold limit value (TLV) is the maximum concentration of each chemical that does not harm the enviroment . • Forensic toxicology that combines analytical chemistry and the fundimental toxicology in a medicolegal concept that assisst in postmorteum investigations to establish the cause of a stage of a crime up to the level of death crimes.
04/27/15 Dr. Medani A.B. ,2006 Con. • Clinical toxicology focuses on disease that are caused or are uniquely associated with toxic substances to help in diagnosis through new techniques and treatment of such intoxications.
04/27/15 Dr. Medani A.B. ,2006 Dose-response curve • It is crucially important as it is graded in individuals quantal in population . • Gradedd doses given to an individual may result in a greater reponse as it increases. • Quantal doses given to a population affect a larger percentage as they are raised . This is used to determine the median lethal dose(LD50) of drugs and other chemicals.
04/27/15 Dr. Medani A.B. ,2006 Risk and its assessment • There is marked differences in LD50 of drugs , some may be harmful in a fraction of micrograms and others may be relatively less harmful in doses of several grams or even more. • Inspite of the advanced technology , it is not easy to distinguish between toxic and non-toxic drugs.
04/27/15 Dr. Medani A.B. ,2006 Con. • Pracelsus statement” All substances are poisons , but the right dose differentiate the remedy from the poison” . • In risk assessment one should consider the direct and indirect harmful effects of a chemical on the enviroment when used in the quantity and manner proposed. • In a chemical delivered to humans and enviroment in association with food ,one should be very careful. • In those given as drugs , one should weigh the benefit vs harm.
04/27/15 Dr. Medani A.B. ,2006 Acute versus chronic exposure • Acute Chronic *Dose delivered *small doses over a as a single event long period of time allow slow accumulation.
04/27/15 Dr. Medani A.B. ,2006 Chemical forms of drugs that produce toxicity • Deleterious effects of any drug are due to the chemical structure of the parent drug and its metabolites that are produced by enzymes , light and reactive oxygen species.
04/27/15 Dr. Medani A.B. ,2006 Toxic metabolites • Chemical metabolites of drugs are mainly the cause of their toxicities. • Unstable metabolites are called reactive metabolites. • Both stable and unsatble metabolites are more toxic in cases where CYP450 is increased.
04/27/15 Dr. Medani A.B. ,2006 Phototoxic and photoallergic reactions • Many chemicals are biotransformed into their toxic metabolite by hepatic enzymes. • Some chemicals are activated in the skin by ultraviolet &/or visible radiation. • Inphotoallergy, drugs may absorp the light ,then converted to a product that is more potent as an allergen than the parent drug.
04/27/15 Dr. Medani A.B. ,2006 Con. • Drugs on reaching the skin , either locallyor systemically, may undergo photochemical reactions within the skin to induce directly photosensitivity or enhance the usual sunlight effects.
04/27/15 Dr. Medani A.B. ,2006 Reactive oxygen species • Paraquat and its metabolites lose one electron paired in electron donation with oxygen forming a reactive oxygen species leading to severe lung injury.
04/27/15 Dr. Medani A.B. ,2006 Spectrum of undesired effects • A drug may produce many types of effects, but only one remains the goal of treatment. • Side effects of a drug are usually non- deleterious. • Undesirable toxic effects include most of the other effects.
04/27/15 Dr. Medani A.B. ,2006 Types of toxic reactions • Toxic effects are either pharmacological, pathological or genotoxic. • Depending on the concentration of the chemical ,toxic effects are usually reversible. • Pharmacological effects discontinue due to biotransformation,while pathological and genotoxic effects need repair
04/27/15 Dr. Medani A.B. ,2006 Local versus systemic toxicity • Local toxicity occurs at the site of first contact between the toxicant and the biological system. • Systemic toxicity requires absorption and distribution of the toxicant. • A toxicant may produce both effects . • Severity of local toxicity depends on the portal of entry.
04/27/15 Dr. Medani A.B. ,2006 Reverible and irreversible toxic effects • Prohibitively toxic drugs cause irreversible toxicity. • Ability of the tissue to reverse the drug toxicity depends on the tissue capacity to regenerate.
04/27/15 Dr. Medani A.B. ,2006 Delayed toxicity • Most toxic drug effects occur at predictable time. • Aplastic anemia occur after weeks of chloramphenicol treatment stops. • Carcinogenic effects of chemicals are also delayed type of toxicity.
04/27/15 Dr. Medani A.B. ,2006 Chemical carcinogens • Either genotoxic or non-genotoxic. • Most gentoxic carcinogen are inactive which turn in the body into the primary or ultimate ones by drug metabolizing to reactive electron defficient intermediates ( electrophiles) . • These electrophiles interact with electron-rich centers in DNA to produce mutation.
04/27/15 Dr. Medani A.B. ,2006 Con. • DNA can reverse this effects if DNA repair mechanism are normal . • Nongenotoxic carcinogen are promoters that do not produce a tumor alone, but can potentiate the effects of genotoxic carcinogens by facilitation of the growth and development of dormant or latent tumor cells.
04/27/15 Dr. Medani A.B. ,2006 Laboratory tests i/ Mutagenicity testing of the carcinogens using Ames test of Salmonella typhimurium for genotoxic carcinogens. ii/ Using laboratory animals feeding with the carcinogen for the entire life-span , then do autopsies and histopathological testing comparing with control animals. This test is for genotoxic and promotor carcinogens.
04/27/15 Dr. Medani A.B. ,2006 Allergic reactions • An adverse reaction that result from previous exposure to a particular chemical or to one that is structurally similar. • Hapten + endogenous protien antigen complex + antibody complex subsequent eposure {allergy}
04/27/15 Dr. Medani A.B. ,2006 Idiosyncratic reactions • Are the genetically determined abnormal reactivity to a test. • This response could be in a form of extreme sensitivity to low doses or increased insensitivity to high doses of a chemical. • These genetic polymorphisms can be due to inter-individual differences in drug pharmacokinetics or pharmacodynamics . • This knowledge is used toindividulize dosages in a science known as pharmacogenomics.
04/27/15 Dr. Medani A.B. ,2006 Interactions between chemicals •Concurrent exposure to more than one chemical may alter the pharmaacokinetics of one or both interacting drugs. •The pharmacodynamics of drugs may be altered due to the competition on receptors. •Functional non-receptor drug interaction occur when two drugs have different mechanisms of action. •The combined toxicant therapy may be equql to,less than or greater than the sum of effects of the individual agents.
04/27/15 Dr. Medani A.B. ,2006 Classification of chemical interations between drugs • Additive effect= combined effects of two chemicals is equal to the effect of each toxican if given alone. • Potentiation= increased effect of a toxicant acting simultaneously with a non-toxic one. • Antagonism=interferance of one chemical with the action of another (antagonistic agent = antidote).
04/27/15 Dr. Medani A.B. ,2006 Descriptive toxicity tests in animals • Principles: -When followed properly the application to human beings. -Exposure of lab. Animals to toxic agents in much lower dose than expected in humans.
04/27/15 Dr. Medani A.B. ,2006 Con. • Experimental animals are tested for: i/Acute toxicity by estimating the LD50 in two different animal species by two different routes of adminstration, death number in two weeks are recorded, signs of intoxications,lethergy, behavioural modifications and morbidity.
04/27/15 Dr. Medani A.B. ,2006 Con. ii/Subacute is then tested for 90 days by using laboratory species in the same route intende to be used by humans (3 doses) ,detect the needed parameters and test organs by a pathologist.
04/27/15 Dr. Medani A.B. ,2006 Con. iii/ Chronicity is tested for short term drugs for 6 month and for long term drugs for two years.
04/27/15 Dr. Medani A.B. ,2006 Incidence of acute poisoning • Incidence of acute poisoningecreased highly due to good packing of drugs,drain cleaners,turpentine and other house hold chemicals,improved medical training and care and increased public awareness of potential poisons. • Although the most common causes are house hold cleaners and cosmetics ,drugs are the most common causes of death.
04/27/15 Dr. Medani A.B. ,2006 Con. • Most of death cases occurs intentionally in adults and accidentally in kids. • Accidental poisoning in kids accounts to 53% of the incidence of poisoning.
04/27/15 Dr. Medani A.B. ,2006 Sources of information on poisoning i/ Books.. ii/ Computerized sources. iii/ Poison centers.
04/27/15 Dr. Medani A.B. ,2006 Prevention & treatment of poisoning • Many acute poisoning incidences by common sense advice from a physician. • Toxic agents are either having specific antidote or not .The majority of toxicants do not have antidote ,so : -Maintain respiration and circulation. -Do serial measurements of vitalsigns and reflexes. -Observe response to therapy and need for additional treatment.
04/27/15 Dr. Medani A.B. ,2006 Con. • In acute poisoning treatment you maintain vital functions, keep the concentration of toxicants in tissue as low as possible by decreasing its absorption and enhancing its elimination, then combat toxicological signs at effecter sites.
04/27/15 Dr. Medani A.B. ,2006 Prevention of further absorption i/Emesis : this used for oral poisoning .It is contraindicated in case of case of corrosives for the fear of gastric perforation and further necrosis of the oesophagus, aspiration in cases of coma, delirium or stupor ,in case of ingestion of CNS stimulants for the fear of convulsion and in case of ingestion of petrolium distellates for the fear of peritonitis.It is indicated in case of dangerous chemicals like pesticides.
04/27/15 Dr. Medani A.B. ,2006 Con. •ii/ Gastric lavage is the administration of a tube into the stomach to wash it with water ,normal saline or half normal saline before the absorption of poisons.This need experts for the fear of gastric injury, but its contraindications are similar to those of emesis.
04/27/15 Dr. Medani A.B. ,2006 Con. iii/Chemical adsorption of many chemicals to the surface of activated charcoal avidyl to reduce the enterohepatic circulation of the drug and enhance its excretion.
04/27/15 Dr. Medani A.B. ,2006 Con. •Chemical inactivation is the changeof the chemical nature of a poison rendering it less toxic or decrease its absorption.This needs time and the use of neutralizing agents is contraversal.
04/27/15 Dr. Medani A.B. ,2006 Con. •Purgation : The rashionale for using osmotic harmless cathratic is to minimize absorption by hastening the passage of toxicants through the GIT, usually after the ingestion of enteric coated tablets by more than one hour.

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Principles of toxicology

  • 1. 04/27/15 Dr. Medani A.B. ,2006 Principles of toxicologyPrinciples of toxicology -It is the science of the adverse effects of chemicals on-It is the science of the adverse effects of chemicals on living organisms.living organisms. -A descriptive toxicologist performs toxicity tests toA descriptive toxicologist performs toxicity tests to obtain information that can be used to evaluate the riskobtain information that can be used to evaluate the risk of exposure to a chemical pose to human beings and theof exposure to a chemical pose to human beings and the enviroment.enviroment. -Amechanistic toxicologist attempts to determine howAmechanistic toxicologist attempts to determine how chemicals exert deleterious effects on living organisms .chemicals exert deleterious effects on living organisms . -A regulatory toxicologist judges whether or not a drugA regulatory toxicologist judges whether or not a drug or other chemicals has a low enough risk to justify makingor other chemicals has a low enough risk to justify making it available for its intended purpose .it available for its intended purpose .
  • 2. 04/27/15 Dr. Medani A.B. ,2006 Con. • An acceptable daily intake (ADI) is the input of a chemical that can be consumed over an entire life-time without any apprciable risk. • A threshold limit value (TLV) is the maximum concentration of each chemical that does not harm the enviroment . • Forensic toxicology that combines analytical chemistry and the fundimental toxicology in a medicolegal concept that assisst in postmorteum investigations to establish the cause of a stage of a crime up to the level of death crimes.
  • 3. 04/27/15 Dr. Medani A.B. ,2006 Con. • Clinical toxicology focuses on disease that are caused or are uniquely associated with toxic substances to help in diagnosis through new techniques and treatment of such intoxications.
  • 4. 04/27/15 Dr. Medani A.B. ,2006 Dose-response curve • It is crucially important as it is graded in individuals quantal in population . • Gradedd doses given to an individual may result in a greater reponse as it increases. • Quantal doses given to a population affect a larger percentage as they are raised . This is used to determine the median lethal dose(LD50) of drugs and other chemicals.
  • 5. 04/27/15 Dr. Medani A.B. ,2006 Risk and its assessment • There is marked differences in LD50 of drugs , some may be harmful in a fraction of micrograms and others may be relatively less harmful in doses of several grams or even more. • Inspite of the advanced technology , it is not easy to distinguish between toxic and non-toxic drugs.
  • 6. 04/27/15 Dr. Medani A.B. ,2006 Con. • Pracelsus statement” All substances are poisons , but the right dose differentiate the remedy from the poison” . • In risk assessment one should consider the direct and indirect harmful effects of a chemical on the enviroment when used in the quantity and manner proposed. • In a chemical delivered to humans and enviroment in association with food ,one should be very careful. • In those given as drugs , one should weigh the benefit vs harm.
  • 7. 04/27/15 Dr. Medani A.B. ,2006 Acute versus chronic exposure • Acute Chronic *Dose delivered *small doses over a as a single event long period of time allow slow accumulation.
  • 8. 04/27/15 Dr. Medani A.B. ,2006 Chemical forms of drugs that produce toxicity • Deleterious effects of any drug are due to the chemical structure of the parent drug and its metabolites that are produced by enzymes , light and reactive oxygen species.
  • 9. 04/27/15 Dr. Medani A.B. ,2006 Toxic metabolites • Chemical metabolites of drugs are mainly the cause of their toxicities. • Unstable metabolites are called reactive metabolites. • Both stable and unsatble metabolites are more toxic in cases where CYP450 is increased.
  • 10. 04/27/15 Dr. Medani A.B. ,2006 Phototoxic and photoallergic reactions • Many chemicals are biotransformed into their toxic metabolite by hepatic enzymes. • Some chemicals are activated in the skin by ultraviolet &/or visible radiation. • Inphotoallergy, drugs may absorp the light ,then converted to a product that is more potent as an allergen than the parent drug.
  • 11. 04/27/15 Dr. Medani A.B. ,2006 Con. • Drugs on reaching the skin , either locallyor systemically, may undergo photochemical reactions within the skin to induce directly photosensitivity or enhance the usual sunlight effects.
  • 12. 04/27/15 Dr. Medani A.B. ,2006 Reactive oxygen species • Paraquat and its metabolites lose one electron paired in electron donation with oxygen forming a reactive oxygen species leading to severe lung injury.
  • 13. 04/27/15 Dr. Medani A.B. ,2006 Spectrum of undesired effects • A drug may produce many types of effects, but only one remains the goal of treatment. • Side effects of a drug are usually non- deleterious. • Undesirable toxic effects include most of the other effects.
  • 14. 04/27/15 Dr. Medani A.B. ,2006 Types of toxic reactions • Toxic effects are either pharmacological, pathological or genotoxic. • Depending on the concentration of the chemical ,toxic effects are usually reversible. • Pharmacological effects discontinue due to biotransformation,while pathological and genotoxic effects need repair
  • 15. 04/27/15 Dr. Medani A.B. ,2006 Local versus systemic toxicity • Local toxicity occurs at the site of first contact between the toxicant and the biological system. • Systemic toxicity requires absorption and distribution of the toxicant. • A toxicant may produce both effects . • Severity of local toxicity depends on the portal of entry.
  • 16. 04/27/15 Dr. Medani A.B. ,2006 Reverible and irreversible toxic effects • Prohibitively toxic drugs cause irreversible toxicity. • Ability of the tissue to reverse the drug toxicity depends on the tissue capacity to regenerate.
  • 17. 04/27/15 Dr. Medani A.B. ,2006 Delayed toxicity • Most toxic drug effects occur at predictable time. • Aplastic anemia occur after weeks of chloramphenicol treatment stops. • Carcinogenic effects of chemicals are also delayed type of toxicity.
  • 18. 04/27/15 Dr. Medani A.B. ,2006 Chemical carcinogens • Either genotoxic or non-genotoxic. • Most gentoxic carcinogen are inactive which turn in the body into the primary or ultimate ones by drug metabolizing to reactive electron defficient intermediates ( electrophiles) . • These electrophiles interact with electron-rich centers in DNA to produce mutation.
  • 19. 04/27/15 Dr. Medani A.B. ,2006 Con. • DNA can reverse this effects if DNA repair mechanism are normal . • Nongenotoxic carcinogen are promoters that do not produce a tumor alone, but can potentiate the effects of genotoxic carcinogens by facilitation of the growth and development of dormant or latent tumor cells.
  • 20. 04/27/15 Dr. Medani A.B. ,2006 Laboratory tests i/ Mutagenicity testing of the carcinogens using Ames test of Salmonella typhimurium for genotoxic carcinogens. ii/ Using laboratory animals feeding with the carcinogen for the entire life-span , then do autopsies and histopathological testing comparing with control animals. This test is for genotoxic and promotor carcinogens.
  • 21. 04/27/15 Dr. Medani A.B. ,2006 Allergic reactions • An adverse reaction that result from previous exposure to a particular chemical or to one that is structurally similar. • Hapten + endogenous protien antigen complex + antibody complex subsequent eposure {allergy}
  • 22. 04/27/15 Dr. Medani A.B. ,2006 Idiosyncratic reactions • Are the genetically determined abnormal reactivity to a test. • This response could be in a form of extreme sensitivity to low doses or increased insensitivity to high doses of a chemical. • These genetic polymorphisms can be due to inter-individual differences in drug pharmacokinetics or pharmacodynamics . • This knowledge is used toindividulize dosages in a science known as pharmacogenomics.
  • 23. 04/27/15 Dr. Medani A.B. ,2006 Interactions between chemicals •Concurrent exposure to more than one chemical may alter the pharmaacokinetics of one or both interacting drugs. •The pharmacodynamics of drugs may be altered due to the competition on receptors. •Functional non-receptor drug interaction occur when two drugs have different mechanisms of action. •The combined toxicant therapy may be equql to,less than or greater than the sum of effects of the individual agents.
  • 24. 04/27/15 Dr. Medani A.B. ,2006 Classification of chemical interations between drugs • Additive effect= combined effects of two chemicals is equal to the effect of each toxican if given alone. • Potentiation= increased effect of a toxicant acting simultaneously with a non-toxic one. • Antagonism=interferance of one chemical with the action of another (antagonistic agent = antidote).
  • 25. 04/27/15 Dr. Medani A.B. ,2006 Descriptive toxicity tests in animals • Principles: -When followed properly the application to human beings. -Exposure of lab. Animals to toxic agents in much lower dose than expected in humans.
  • 26. 04/27/15 Dr. Medani A.B. ,2006 Con. • Experimental animals are tested for: i/Acute toxicity by estimating the LD50 in two different animal species by two different routes of adminstration, death number in two weeks are recorded, signs of intoxications,lethergy, behavioural modifications and morbidity.
  • 27. 04/27/15 Dr. Medani A.B. ,2006 Con. ii/Subacute is then tested for 90 days by using laboratory species in the same route intende to be used by humans (3 doses) ,detect the needed parameters and test organs by a pathologist.
  • 28. 04/27/15 Dr. Medani A.B. ,2006 Con. iii/ Chronicity is tested for short term drugs for 6 month and for long term drugs for two years.
  • 29. 04/27/15 Dr. Medani A.B. ,2006 Incidence of acute poisoning • Incidence of acute poisoningecreased highly due to good packing of drugs,drain cleaners,turpentine and other house hold chemicals,improved medical training and care and increased public awareness of potential poisons. • Although the most common causes are house hold cleaners and cosmetics ,drugs are the most common causes of death.
  • 30. 04/27/15 Dr. Medani A.B. ,2006 Con. • Most of death cases occurs intentionally in adults and accidentally in kids. • Accidental poisoning in kids accounts to 53% of the incidence of poisoning.
  • 31. 04/27/15 Dr. Medani A.B. ,2006 Sources of information on poisoning i/ Books.. ii/ Computerized sources. iii/ Poison centers.
  • 32. 04/27/15 Dr. Medani A.B. ,2006 Prevention & treatment of poisoning • Many acute poisoning incidences by common sense advice from a physician. • Toxic agents are either having specific antidote or not .The majority of toxicants do not have antidote ,so : -Maintain respiration and circulation. -Do serial measurements of vitalsigns and reflexes. -Observe response to therapy and need for additional treatment.
  • 33. 04/27/15 Dr. Medani A.B. ,2006 Con. • In acute poisoning treatment you maintain vital functions, keep the concentration of toxicants in tissue as low as possible by decreasing its absorption and enhancing its elimination, then combat toxicological signs at effecter sites.
  • 34. 04/27/15 Dr. Medani A.B. ,2006 Prevention of further absorption i/Emesis : this used for oral poisoning .It is contraindicated in case of case of corrosives for the fear of gastric perforation and further necrosis of the oesophagus, aspiration in cases of coma, delirium or stupor ,in case of ingestion of CNS stimulants for the fear of convulsion and in case of ingestion of petrolium distellates for the fear of peritonitis.It is indicated in case of dangerous chemicals like pesticides.
  • 35. 04/27/15 Dr. Medani A.B. ,2006 Con. •ii/ Gastric lavage is the administration of a tube into the stomach to wash it with water ,normal saline or half normal saline before the absorption of poisons.This need experts for the fear of gastric injury, but its contraindications are similar to those of emesis.
  • 36. 04/27/15 Dr. Medani A.B. ,2006 Con. iii/Chemical adsorption of many chemicals to the surface of activated charcoal avidyl to reduce the enterohepatic circulation of the drug and enhance its excretion.
  • 37. 04/27/15 Dr. Medani A.B. ,2006 Con. •Chemical inactivation is the changeof the chemical nature of a poison rendering it less toxic or decrease its absorption.This needs time and the use of neutralizing agents is contraversal.
  • 38. 04/27/15 Dr. Medani A.B. ,2006 Con. •Purgation : The rashionale for using osmotic harmless cathratic is to minimize absorption by hastening the passage of toxicants through the GIT, usually after the ingestion of enteric coated tablets by more than one hour.