Lecture #14 : INTRODUCTION TO TOXICOLOGY

  

Toxicology is the study of poisonous substances, their actions on the living organism, their detection by laboratory and other methods and measure taken to counteract their biologic effects.

Toxicology is the study of the adverse effects of chemical on living organisms. The toxicologist is especially trained to examine the nature of these adverse effects (including their cellular, biochemical and molecular mechanism of action) and to assess the probability of their occurrence. The variety of potential adverse effects and the diversity of chemicals present in our environment combine to make toxicology a very broad science.

Clinical toxicologists are physicians who receive specialized training in emergency medicine and poison management.

Concept of a poisonous substance

1.      Poison has been defined as any drug known to the pharmaceutical or medical profession, which is liable to be destructive to adult human life if taken in quantities of 60 grains or less.

2.      Poison in a strict sense is a substance which upon entering into solution in the blood or by chemically acting upon it, is capable of causing serious bodily injury, disease or death. In a broad sense, it is any substance which independent of any mechanical action causes serious bodily injury, disease or death when applied to, introduced into or developed within the body.

3.      Poison is any agent capable of producing a deleterious response in a biologic system, seriously injuring function or producing death. Paracelsius noted: “All substances are poisonous; there is none which is not a poison. The right dose differentiates a poison and a remedy.”

Different areas of toxicology

1.      Descriptive toxicology – concerned directly with toxicity testing, which provides necessary information for safety evaluation and regulatory requirements. The concern may be limited to effects on humans, as in the case of food additives.

2.      Mechanistic toxicology – is concerned directly with elucidating the mechanisms by which chemicals exert their toxic effects on living organisms.

3.      Regulatory toxicology – is concerned with the responsibility of deciding on the basis of data provided by the descriptive toxicologist if a drug or other chemical possess a sufficiently low risk to be marketed for a stated purpose.

Three specialized areas of toxicology

1.      Forensic toxicology – is a hybrid of analytical chemistry and fundamental toxicology principles. It is concerned with the medico–legal aspects of the harmful effects of chemical on human and animals. The expertise of the forensic toxicologist is primarily invoked to aid in establishing cause of death and elucidating its circumstances in a postmortem investigation.

2.      Clinical toxicology – designates an area of professional emphasis within the realm of medical science concerned with disease caused by, or uniquely with, toxic substances.

3.      Environmental toxicology – focuses on the impacts of chemical pollutants found in the environment on biological organisms. Although toxicologist concerned with the effect of environmental pollutants on human health fit within this definition, it is most commonly associated with studies on the impacts of chemicals on non – human organisms such as fish, birds, and other terrestrial animals.

Ecotoxicology – is a specialized area within environmental toxicology that focuses more specifically on the impacts of toxic substances on population, dynamics within an ecosystem. The transport, fate and interactions of chemicals in the environment constitute a critical component of both environmental toxicology and ecotoxicology.

Types of poison

1.      Corrosive poison – an agent whose content chemically causes local destruction of tissues.

2.      Cumulative poison – an agent which increases suddenly the intensity of action after the slow addition of poison.

3.      True poison – an agent which is still a poison no matter how diluted it is.

Type of poisoning

1.      Acute poisoning – one in which there is a prompt and marked disturbance of function or death within a short time and is due to:

a.      Excessive single dose

b.      Several small doses but frequent

2.      Chronic poisoning – there is a gradual deterioration of function of tissues and may or may not result in death. It may be produced by:

a.      Taking several small doses at long intervals

b.      Taking only toxic doses of the drug

GENERAL MECHANISM OF TOXICITY

All chemicals produce their toxic effects by alterations in normal cellular biochemistry and physiology. A thorough understanding of the biochemical and molecular sites and modes of action of specific drugs and chemicals is an essential part of toxicology.

Although many toxic responses are ultimately of cell death and loss of critical organ function, other responses may be the result of biochemical and pharmacological imbalances in normal physiological processes that do not result in cell death. There are many ways in which chemicals can interfere with normal biochemistry and physiology, and a brief overview of some general sites of toxic action is useful in appreciating the diversity of biochemical and cellular process that underlie toxic response.

General mechanism of toxic action

1.      Interference with normal receptor–ligand interactions

Receptors are macromolecular components of tissues with a drug or chemical (ligand) interacts to produce its characteristics biologic effects.

Receptor–ligand interactions are generally highly stereo specific and small changes in chemical structure can drastically reduce or eliminate the effect.

The adverse effects of many chemicals are related to their ability to interfere with normal receptor–ligand interactions. This is especially true with neurotoxicants, as the function of the nervous system is highly dependent on a diverse array of receptor–ligand interactions.

a.      Neuroreceptors  and neurotransmitter (e.g. atropine, strychnine, LSD, d– tubocurarine, organophosphates, anti–histamines)

b.      Hormone receptors (DES, TCDO, goitrogens)

c.       Enzyme activity (organophosphates, cyanide, sodium fluoroacetate)

d.     Transport proteins (carbon monoxide, nitrates)

2.      Interference with membrane function

The maintenance and stability of excitable membrane is essential to normal physiology. Chemicals can perturb excitable membrane function in many ways. For example, the flux of ions across neuronal axons is blocked by chemicals that act as ion channel blockers. The marine toxins, saxitonin, produce its paralyzing effects by blocking sodium channel in excitable membranes. Tetradotoxins, derived from the gonads and other organs of the puffer fish, is structurally quite different from saxitonin yet acts in essentially the same manner. The insecticide DDT produces the neurotoxic action by interfering with the closing of sodium channels, thus altering the rate of repolarization of excitable membranes. Organic solvents appear to produce their CNS depressant effects via non–specific alterations in membrane fluidity, largely as a property of their lipid solubility, rather than binding to specific macromolecular receptor.

3.      Interference with cellular energy productions

Many chemicals produce their adverse effects by interfering with the oxidation of carbohydrates to produce adenosine triphosphate (ATP). This interference can occur by blocking effective delivery of oxygen to tissues. For example, chemical oxidation of the iron hemoglobin (methemoglobin) by nitrates also interferes with oxygen delivery, as methemoglobin does not effectively bind oxygen. Utilization of oxygen in the tissues is blocked by cyanide, hydrogen sulfide and azide because of their affinity to cytochrome oxidase. The ultimate formation of ATP via oxidation of carbohydrates can be blocked by other sites as well.

The consequences of ATP depletion are many and include effects above, such as interference with membrane integrity, ion pumps and protein synthesis. Significant energy depletion will inevitably lead to loss of cell function and perhaps cell death.

Examples:

a.      Oxygen delivery to tissues (CO, nitrites)

b.      Uncoupling of oxidative phosphorylation (nitrophenols, organotins)

c.       Inhibition of electron transport (rotenone, antimycin A)

d.     Inhibition of carbohydrate metabolism (fluoroacetate)

4.      Binding to molecules

a.      Interference with enzyme functions

Many toxic substances exert their efforts via binding to the active sites of the enzymes, or proteins that are critical to cellular function. For example, hydrogen cyanide binds to the ferric ion atom in cytochrome a+a3 (cytochrome oxidase) which blocks the terminal event in electron transport. This single site of action responsible for the rapid and often fatal toxic effects of cyanide and understanding of this mechanism led to the development of specific antidotes to cyanide poisoning.

Carbon monoxide binds tightly to the reduced form of iron in hemoglobin, reducing the delivery of oxygen on tissues. Although this has for so many years been thought to be the sole mechanism of toxicity of carbon monoxide, there is evidence to suggest that CO also binds to cytochrome a+a3.

Many toxic trace metals such as lead, mercury, cadmium and arsenic bind to proteins with free sulfhydryl groups, which contribute to their toxicity. Chemical–induced porphyrias from lead, mercury and other metals, as well as certain halogenated hydrocarbons (e.g. hexachlorobenzene) result, in part, from the inhibition of specific enzyme in the heme biosynthetic pathway.

b.      Lipid peroxidation (CCl₄, paraquat, ozone)

Although some of the processes discussed above are capable of producing adverse physiological responses without the actual death of cells in any tissues or organ, other processes will eventually lead to loss of organ function and death of cell. This is especially true if exposure to the toxic substance occurs on chronic bases where tissue injury can accumulate from repeated cytotoxic episodes. The specific sequence of events leading to cell injury and death is complex and not fully understood. The most thorough understanding of the process leading to chemical induced cell death comes from studies on liver cells.

For most chemicals causing tissue necrosis, the initial step appears to be the formation of a reactive, electrophilic intermediate, often free radicals. Formation of free radicals may occur via enzyme–mediated one or two electron oxidations, as well as from the autooxidation of small molecules to such as reduced flaviness and thiols. Electron transfer from transition metals such iron to oxygen containing molecules can also initiate and propagate free radical reactions. The initiation of lipid peroxidation  via interaction of free radicals with polyunsaturated fatty acids to form lipid peroxyradicals (ROO), which then produce lipid cell injury and death. Peroxidative damage to membrane lipids could then lead to a loss membrane integrity and rupture of the cell membrane.

c.       Oxidative stress

It is now recognized that lipid peroxidation by itself may not be sufficient to induce cell death. In addition to inducing lipid peroxidation, electrophilic intermediates may also covalently interact with other nucleophilic sites in the cell, including glutathione (GSH) and thiol– containing protein which results in “oxidative stress” to the cell. Depletion of intracellular stores of glutathione appears to be required before significant oxidative stress occurs. As many critical enzymes in the cell require one or more reduced thiols (SH–group) to maintain their activity, oxidative stress in excess of that necessary to deplete intracellular GSH can lead to oxidation of protein thiols to form disulfide linkages, thereby destroying enzymatic activity. Although the direct covalent of electrophilic chemicals with protein thiols may contribute to enzyme inhibition, it appears that the majority of loss of activity of thiol–containing proteins is a result of reversible oxidation of the thiol groups that occurs as a result of oxidative stress. One group of thiol–containing enzymes that may play a critical role in cell injury and death as result of oxidative inactivation (oxidative stress) is calcium–transporting ATPases.

d.      Nucleic acid

There are numerous nucleophilic sites within DNA that may readily react with electrophilic chemicals. Alkylation of the O–6 position of guanine appears important in the mutagenicity and carcinogenicity of nitrosoamines and other chemicals that readily form methyl carbonium ions. However, other sites, such as N–7, N–2 and C–2 positions of guanine, may also be important sites of DNA adduct formation with other electrophilic chemicals. Adduction of DNA with exogenous chemicals may alter the expression of critical gene products necessary for survival of the cell and thus binding to DNA may lead to cell death. However, if perhaps more significant is the production of somatic mutation through chemical DNA adduct formation that may serve as the initiating event in chemical carcinogenesis. As with DNA, ribonucleic acid (RNA) also contains nucleophilic sites, and thus critical intracellular function of RNA, e.g., protein synthesis, maybe perturbed by covalent interaction of electrophilic chemicals with RNA.  

5.      Perturbation of calcium homeostasis

Interference with normal process responsible for intracellular calcium homeostasis appears to play a critical role in chemical mediated cell injury and death. Calcium accumulates in tissues following necrotic injury and death from ischemia, immunological response and a variety of toxic agents. Disruption on intracellular Ca²⁺ homeostasis can result from enhanced Ca²⁺ influx, release of Ca²⁺ from intracellular stores and inhibition of Ca²⁺ extrusion at the plasma membrane.

A wide variety of cytotoxic agents, including nitrophenols, quinones, peroxides, aldehydes, dioxins, halogenated alkanes and some metal ions, have been shown to disrupt Ca²⁺ homeostasis. Increased cellular calcium has been shown to disrupt Ca²⁺ homeostasis. Increased intracellular calcium has been associated with the development of membrane abnormalities (blebbing) in isolated cells, which appears to be a general phenomenon associated with the toxic and ischemic cell injury and death.

Ca²⁺ plays a key role as a second messenger in the regulation of many intracellular functions. For example, normal cytoskeletal organization is perturbed when intracellular Ca²⁺ increases apparently as a result of calcium– mediated dissociation of action of microfilaments and an activation of phospholipases and proteases. Although normally, the Ca²⁺ mediated activation of phospholipases plays a protective role of removing peroxidized phospholipids form damaged membranes. When activated by non– physiologic changes in Ca²⁺ concentration phospholipases may enhance membrane phospholipid breakdown, which may lead to cell injury and death. It is also known that an increase in intracellular Ca²⁺ can activate non– lysosomal proteases. Although the endogenous substrates for these proteases have not been fully characterized, they appear to act as cytoskeletal proteins. The importance of these proteases in the processes of cell death is demonstrated by the fact inhibitors of Ca²⁺ activated proteases delay or prevent the appearance of cytotoxic effects.

Ca²⁺ can also activate certain endonucleases, which result in DNA fragmentation and chromatin condensation. Although this process is an important physiological “programmed” cell death that occurs naturally as a part of tissue growth and differentiation (apoptosis) chemically mediated premature activation of this enzyme via a perturbation in Ca²⁺ homeostasis may contribute to the cytotoxic action of some toxic substances.

6.      Toxicity from selective cell loss

Selective death cell loss within an organ or tissue may also result in toxicologic effects that are quite specific and in some instances other disease processes. For example, high doses of manganese, or the illicit street drug 1– methyl–4–phenyl–1,2,5,6–tetrahydropyridine (MPTP), cause selective damage to dopaminergic cell in the basal ganglia in the brain, producing a neurological condition nearly indistinguishable from Parkinson’s disease. Some chemicals, both synthetic (e.g. Amitrole) and naturally occurring (e.g. 5 –vinyloxazolinethione from the rape seed plant), stimulate the growth of the thyroid gland and reduction of excess thyroid hormone, resulting in a pathological condition indistinguishable from goiter. Conversely, other chemicals may selectively accumulate in the thyroid gland, where they reach toxic concentrations and destroy the thyroid cells. (e.g. propylthiouracil).

The developing embryo is also quite sensitive to many toxic substances. Because in the early stages of embryonic growth cells may have pluripotent potential (can differentiate into a variety of mature cell types), loss of even a few cells can have major consequences, leading either to embryonic death (i.e., miscarriage) or some form of congenital malformation (birth defect). For example, the administration of the anti–nausea drug thalidomide to pregnant woman at a specific stage of fetal development resulted in the cytotoxic loss of early limb bud cells, with the consequence that children were born with severely underdeveloped or missing legs and or arms.

7.      Non–lethal genetic alterations in somatic cells

As noted above, the covalent interaction of xenobiotics with DNA can result directly in the death of the cell but may also result in the initiation of a complex series of events that may ultimately result in cancer. Chemicals that can produce a carcinogenic response via somatic mutations are called genotoxic carcinogens. The vast majority of chemically induced lesions in DNA are repaired but some may escape repair or be repaired incorrectly leading to the introduction of a mutated cell. If the mutation occurs in a somatic cell, then the genetic lesion cannot be passed onto future generations but could serve as a precursor for the eventual development of cancer.

It is currently thought that genotoxic chemicals can induce cancer by activating cellular “proto–oncogenes.” Proto–oncogenes, when aberrantly expressed, confer on a cell feature of a cancerous phenotype. Many of the gene products from oncogenes determine a cell response to growth– stimulating factor and or differentiation. In normal cells, the expression of proto–oncogenes is tightly controlled for the specific requirement for growth and or differentiation. In addition to the direct, covalent interaction of a xenobiotic with DNA, proto–oncogenes may be activated via a number of xenobiotic events, such as alterations in chromosome structure (e.g. rearrangement or deletions), interference with DNA replication, interference with DNA segregation or interference with DNA repair.

Although (alterations) activation of proto–oncogenes via or genotoxic event is one mechanism by which chemicals can induce cancer, it has been recognized for decades that cancer is a multi–step process and that some non–genotoxic chemicals may enhance the incidence of cancer, presumably through some mechanism other than by damaging DNA. Chemicals that are by themselves generally incapable of inducing cancer but enhance the development of tumors when given after an “initiator” are called tumor promoters.

Tumor promoters act by enhancing the probability of an initiated cell developing into tumor. Stimulation of an “initiated” cell into cell division and clonal expansion (e.g. mitogenic effect) appear to be a common feature of all tumor promoters. There is a variety of mechanism by which chemicals could act as tumor promoters. They could act directly as growth factors or interact with modified growth factor receptors, they could stimulate the production and release of endogenous growth factors; they could shift differentiated cells from a resting state (G_o) to a cell cycle phase (G₁), they could induce normal reparative cell growth to neighboring cells via a cytotoxic effect; they could inhibit normal cellular differentiation, which is necessary to ensure that mature cells stop dividing or they could interfere with normal cells–cell communication, which is important in regulation of normal cellular growth.

Although birth defects are most commonly induced via cytotoxic events are usually evident at birth, it is also possible to have delayed adverse effects developing in offspring that arise via genetic mutations induced in utero. For example, the synthetic estrogen diethylstilbesterol (DES) has b been claimed responsible for vaginal cancers in women who are exposed in uterus because their mother DES to reduce the chance of miscarriage. Fortunately, there are very few examples of such transplacental carcinogenesis.

CONCEPT OF AN ANTIDOTE

An antidote is any agent which neutralizes a poison or otherwise counteracts or opposes it or its effect.

Action of an antidote

1.      Removes the poison from the body – emetic and cathartic

2.      Mechanically prevent its absorption – demulcent

3.      Change the physical state or chemical composition – sodium sulfate for barium

4.      Act upon the functions of the body so as to overcome the effects of its absorption

Types of antidotes

a.      Chemical or true or specific antidote – is one which makes the poison harmless by chemically altering it.

b.     Mechanical antidote – is an agent that removes the poison without changing it, or so coats the surface of the organ so that absorption is prevented.

c.       Physiological antidote (antagonist) – is an agent that acts upon the system so as to counteract the effect of the poison.

Classification of toxic agents

1.      According to target organ

a.      Liver

b.      Kidney

c.       Hematopoietic system

2.      According to their use

a.      Pesticides

b.      Solvent

c.       Food additive

3.      According to their source

a.      Animal toxin

b.      Plant toxin

4.      According to their effects

a.      Cancer

b.      Mutation

c.       Liver injury

5.      According to physical state

a.      Gas

b.      Dust

c.       Liquid

6.      According to labelling requirement

a.      Explosive

b.      Flammable

c.       Oxidizer

7.      According to chemistry

a.      Aromatic amine

b.      Halogenated hydrocarbons

8.      According to their poisoning potential

a.      Extremely toxic

b.      Very toxic

c.       Slightly toxic

Classification of poison according to physical state

1.      Gases

a.      Carbon monoxide

2.      Volatitles

a.      Ethanol

b.      Other alcohols

3.      Non–volatile

a.      Pesticides

b.      Amphetamine group

c.       Cocaine

d.     Cannabinoids

e.      Methadone

f.        Methaqualone

g.      Opiates

h.      Phencyclidine

i.        Propoxyphene

j.        Phenothiazine

Manner or method of introduction

1.      Gastro–intestinal tract

2.      Rectal mucosa

3.      Sublingual administration

4.      Subcutaneous route

5.      Intramuscular route (intravenous / intraarterial)

6.      Thru lungs by inhalation

7.      Intrathecal

8.      Skin

Storage depot

Accumulation of the poison in the body is influenced by:

1.      Plasma protein binding usually to serum albumin

2.      Fat solubility

3.      Affinity for mucopolysaccharide of connective tissue

4.      Affinity for bones (calcium, lead, arsenic, tetracycline)

Route of excretion of poison

1.      Kidney – it the most important excretory organ. Most polar substances are excreted unchanged, while other substances must be metabolized and conjugated before they can be excreted.

2.      Hepatic and fecal excretion – metabolite secreted into the bile are usually reabsorbed in the gastrointestinal tract and excreted in the urine. Some pass into the feces.

3.      Milk (breast)

4.      Sweat (skin)

5.      Saliva (salivary gland)