Glossary

2.3 Metabolism

10 min readaugust 20, 2024

Metabolism is a crucial process in toxicology, determining how our bodies handle harmful substances. It involves two main phases: modify chemicals, while help eliminate them. Understanding these processes is key to grasping how toxins affect us.

The body's metabolic system, particularly the liver, plays a vital role in breaking down and removing toxins. Factors like , sex, and diet can influence metabolism, impacting how individuals respond to harmful substances. This knowledge is essential for predicting and managing toxic effects.

Phases of metabolism

  • Metabolism plays a crucial role in determining the fate and of xenobiotics in the body
  • reactions are divided into two main phases: Phase I and Phase II reactions
  • These reactions modify the chemical structure of xenobiotics to facilitate their elimination from the body

Phase I reactions

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  • Involve oxidation, reduction, or hydrolysis of the xenobiotic
  • Catalyzed by enzymes such as (CYP) monooxygenases and flavin-containing monooxygenases (FMOs)
  • Examples include hydroxylation of aromatic compounds (benzene) and oxidation of alcohols (ethanol)
  • Phase I reactions often result in the formation of reactive intermediates that can be more toxic than the parent compound
  • These reactions typically increase the polarity of the xenobiotic, making it more water-soluble

Phase II reactions

  • Involve conjugation of the xenobiotic or its Phase I metabolite with endogenous molecules
  • Catalyzed by transferase enzymes such as UDP-glucuronosyltransferases (UGTs) and sulfotransferases (SULTs)
  • Examples include glucuronidation of morphine and sulfation of acetaminophen
  • Phase II reactions generally increase the molecular weight and polarity of the xenobiotic, facilitating its
  • Conjugation reactions typically detoxify the xenobiotic, although some exceptions exist (acetaminophen-glucuronide)

Cytochrome P450 system

  • The cytochrome P450 (CYP) system is a superfamily of heme-containing enzymes that play a central role in xenobiotic metabolism
  • CYP enzymes are predominantly expressed in the liver but are also found in extrahepatic tissues (intestine, lung, brain)
  • These enzymes catalyze a wide range of Phase I reactions, including oxidation, reduction, and hydrolysis

Structure and function

  • CYP enzymes are membrane-bound proteins located in the endoplasmic reticulum
  • They contain a heme group that binds molecular oxygen and a substrate-binding site that determines substrate specificity
  • The catalytic cycle involves the activation of oxygen, leading to the insertion of one oxygen atom into the substrate and the formation of water
  • Examples of CYP-mediated reactions include the hydroxylation of steroids (testosterone) and the epoxidation of polycyclic aromatic hydrocarbons (benzo[a]pyrene)

Genetic polymorphisms

  • CYP enzymes exhibit significant genetic variability, resulting in interindividual differences in drug metabolism and toxicity
  • Polymorphisms can lead to altered enzyme activity, ranging from complete loss of function to increased activity
  • Examples include CYP2D6 polymorphisms affecting the metabolism of antidepressants (fluoxetine) and CYP2C19 polymorphisms influencing the response to proton pump inhibitors (omeprazole)
  • Genetic testing can help predict an individual's metabolic capacity and guide personalized drug therapy

Induction and inhibition

  • The activity of CYP enzymes can be modulated by various factors, including drugs, environmental pollutants, and dietary components
  • involves an increase in the expression or activity of CYP enzymes, leading to enhanced metabolism of substrates
  • Examples of CYP inducers include rifampicin (CYP3A4) and polycyclic aromatic hydrocarbons (CYP1A1)
  • results in decreased metabolism of substrates, potentially leading to drug-drug interactions and toxicity
  • Examples of CYP inhibitors include grapefruit juice (CYP3A4) and fluconazole (CYP2C9)

Conjugation reactions

  • Conjugation reactions are Phase II biotransformation reactions that involve the covalent attachment of endogenous molecules to xenobiotics or their Phase I metabolites
  • These reactions are catalyzed by transferase enzymes and require the presence of cofactors (UDP-glucuronic acid, 3'-phosphoadenosine-5'-phosphosulfate)
  • Conjugation reactions generally increase the polarity and molecular weight of the xenobiotic, facilitating its excretion via urine or bile

Glucuronidation

  • Catalyzed by UDP-glucuronosyltransferases (UGTs) in the endoplasmic reticulum
  • Involves the transfer of glucuronic acid from UDP-glucuronic acid to the xenobiotic or its Phase I metabolite
  • Examples include the glucuronidation of morphine and acetaminophen
  • Glucuronidation typically detoxifies xenobiotics, although some exceptions exist (morphine-6-glucuronide)

Sulfation

  • Catalyzed by sulfotransferases (SULTs) in the cytosol
  • Involves the transfer of a sulfonate group from 3'-phosphoadenosine-5'-phosphosulfate (PAPS) to the xenobiotic or its Phase I metabolite
  • Examples include the sulfation of steroid hormones (estradiol) and phenolic compounds (acetaminophen)
  • Sulfation can lead to the formation of reactive intermediates (N-sulfooxy-2-acetylaminofluorene)

Acetylation

  • Catalyzed by N-acetyltransferases (NATs) in the cytosol
  • Involves the transfer of an acetyl group from acetyl-coenzyme A to the amino group of the xenobiotic or its Phase I metabolite
  • Examples include the acetylation of isoniazid and sulfonamides
  • Acetylation exhibits genetic polymorphism, leading to slow and fast acetylator phenotypes

Methylation

  • Catalyzed by methyltransferases in the cytosol
  • Involves the transfer of a methyl group from S-adenosylmethionine (SAM) to the xenobiotic or its Phase I metabolite
  • Examples include the methylation of catecholamines (dopamine) and arsenic
  • Methylation can lead to the formation of toxic metabolites (monomethylarsonic acid)

Glutathione conjugation

  • Catalyzed by glutathione S-transferases (GSTs) in the cytosol
  • Involves the conjugation of the tripeptide glutathione to the xenobiotic or its Phase I metabolite
  • Examples include the conjugation of electrophilic compounds (aflatoxin B1) and reactive oxygen species
  • Glutathione conjugation is an important pathway, although some conjugates can be toxic (S-(1,2-dichlorovinyl)-L-cysteine)

Factors affecting metabolism

  • Various factors can influence the rate and extent of xenobiotic metabolism, leading to interindividual variability in toxicity and drug response
  • These factors include age, sex, nutritional status, disease states, and drug interactions
  • Understanding the impact of these factors is crucial for personalized medicine and risk assessment

Age and development

  • Metabolic capacity changes throughout the lifespan, with significant differences between neonates, children, adults, and the elderly
  • Neonates have immature enzyme systems, leading to reduced metabolism of certain drugs (theophylline)
  • Elderly individuals may have decreased liver mass and blood flow, resulting in altered drug clearance (benzodiazepines)
  • Developmental changes in enzyme expression can influence the susceptibility to toxicants (chlorpyrifos)

Sex differences

  • Sex-related differences in xenobiotic metabolism can be attributed to hormonal influences and genetic factors
  • Some CYP enzymes (CYP3A4) exhibit higher activity in females, while others (CYP1A2) have higher activity in males
  • Sex differences in metabolism can affect drug efficacy and toxicity (zolpidem)
  • Hormonal fluctuations during the menstrual cycle and pregnancy can alter metabolic capacity

Nutritional status

  • Diet and nutritional status can modulate the activity of drug-metabolizing enzymes
  • High-protein diets can induce CYP enzymes (CYP3A4), while malnutrition can lead to decreased enzyme activity
  • Specific dietary components can inhibit or induce enzyme activity (grapefruit juice, cruciferous vegetables)
  • Nutritional deficiencies (vitamin B6, iron) can impair the function of certain enzymes (cysteine conjugate β-lyase)

Disease states

  • Various disease states can alter the expression and activity of drug-metabolizing enzymes
  • Liver diseases (cirrhosis, hepatitis) can reduce the metabolic capacity of the liver
  • Inflammation and infection can downregulate CYP enzymes through the action of cytokines (interleukin-6)
  • Genetic diseases (Gilbert's syndrome) can lead to impaired conjugation reactions (glucuronidation)

Drug interactions

  • Drug-drug interactions can occur when one drug alters the metabolism of another drug
  • Enzyme induction by one drug can lead to increased metabolism and reduced efficacy of another drug (rifampicin and oral contraceptives)
  • Enzyme inhibition by one drug can result in decreased metabolism and increased toxicity of another drug (ketoconazole and midazolam)
  • Herbal supplements and dietary components can also interact with drugs by modulating enzyme activity (St. John's wort, grapefruit juice)

Metabolic activation vs detoxification

  • Xenobiotic metabolism can result in either detoxification or of the parent compound
  • Detoxification involves the conversion of the xenobiotic into less toxic or inactive metabolites, facilitating their elimination from the body
  • Bioactivation, or metabolic activation, involves the formation of reactive intermediates that can be more toxic than the parent compound
  • The balance between detoxification and bioactivation determines the ultimate toxicity of a xenobiotic

Bioactivation of toxicants

  • Many toxicants require metabolic activation to exert their toxic effects
  • Examples include the bioactivation of benzo[a]pyrene to diol epoxides that form DNA adducts and the activation of acetaminophen to N-acetyl-p-benzoquinone imine (NAPQI) that causes liver toxicity
  • Bioactivation often involves Phase I reactions catalyzed by CYP enzymes, leading to the formation of electrophilic intermediates
  • These reactive intermediates can bind to cellular macromolecules (DNA, proteins) and disrupt cellular function

Detoxification pathways

  • Detoxification pathways convert xenobiotics into less toxic or inactive metabolites that can be readily excreted from the body
  • Examples include the glucuronidation of morphine and the sulfation of acetaminophen
  • Detoxification often involves Phase II conjugation reactions that increase the polarity and water solubility of the xenobiotic
  • Glutathione conjugation is an important detoxification pathway for electrophilic compounds and reactive oxygen species

Balance and consequences

  • The balance between bioactivation and detoxification determines the net toxicity of a xenobiotic
  • Factors that influence this balance include the relative activities of Phase I and Phase II enzymes, the availability of cofactors, and genetic polymorphisms
  • When bioactivation overwhelms detoxification, the accumulation of reactive intermediates can lead to cellular damage and toxicity (acetaminophen overdose)
  • Interindividual differences in the balance between bioactivation and detoxification can contribute to variability in susceptibility to toxicants (aflatoxin B1)

Toxicokinetics of metabolism

  • Toxicokinetics describes the , , metabolism, and excretion (ADME) of xenobiotics in the body
  • Metabolism plays a crucial role in determining the fate and toxicity of xenobiotics
  • Understanding the toxicokinetics of metabolism is essential for predicting the exposure, bioavailability, and clearance of xenobiotics

Absorption and distribution

  • Absorption refers to the entry of a xenobiotic into the systemic circulation from the site of exposure (oral, dermal, inhalation)
  • Factors influencing absorption include the physicochemical properties of the xenobiotic (lipophilicity, molecular weight) and the route of exposure
  • Distribution describes the reversible transfer of the xenobiotic from the systemic circulation to various tissues and organs
  • The extent of distribution depends on factors such as plasma protein binding, tissue affinity, and the presence of tissue-specific transporters

Metabolic clearance

  • Metabolic clearance refers to the rate at which a xenobiotic is irreversibly removed from the body through metabolism
  • Clearance is determined by the activity of drug-metabolizing enzymes and the blood flow to the metabolizing organs (liver, kidneys)
  • High metabolic clearance can lead to rapid elimination of the xenobiotic, while low clearance can result in accumulation and prolonged exposure
  • Interindividual differences in metabolic clearance can contribute to variability in drug response and toxicity

Elimination half-life

  • The elimination half-life is the time required for the plasma concentration of a xenobiotic to decrease by 50% during the elimination phase
  • The half-life is determined by the clearance and the volume of distribution of the xenobiotic
  • Xenobiotics with short half-lives are rapidly eliminated from the body, while those with long half-lives can accumulate with repeated exposure
  • Knowledge of the half-life is important for determining dosing intervals and assessing the risk of toxicity

Bioavailability and bioaccumulation

  • Bioavailability refers to the fraction of the administered dose that reaches the systemic circulation unchanged
  • Factors influencing bioavailability include the extent of absorption, , and presystemic elimination
  • Bioaccumulation occurs when the rate of uptake of a xenobiotic exceeds the rate of elimination, leading to an increase in the body burden over time
  • Xenobiotics with high lipophilicity and low metabolic clearance are more likely to bioaccumulate (PCBs, dioxins)

Organ-specific metabolism

  • While the liver is the primary site of xenobiotic metabolism, other organs and tissues also possess metabolic capabilities
  • Organ-specific metabolism can influence the local toxicity of xenobiotics and contribute to the overall metabolic fate of the compound
  • Understanding the role of extrahepatic metabolism is important for predicting tissue-specific toxicity and drug-drug interactions

Liver as primary site

  • The liver is the principal organ responsible for xenobiotic metabolism due to its high expression of drug-metabolizing enzymes and its central role in blood circulation
  • Hepatocytes, the main cell type in the liver, express a wide range of Phase I and Phase II enzymes (CYP enzymes, UGTs, GSTs)
  • The liver's high metabolic capacity and blood flow make it a major site for first-pass metabolism and systemic clearance of xenobiotics
  • Liver-specific toxicity can occur when reactive metabolites are formed or when detoxification pathways are overwhelmed (acetaminophen-induced hepatotoxicity)

Extrahepatic metabolism

  • Extrahepatic tissues, such as the intestine, lung, kidney, and skin, also express drug-metabolizing enzymes
  • The intestine is a major site of first-pass metabolism for orally administered xenobiotics due to the presence of CYP enzymes and UGTs in enterocytes
  • The lung is exposed to inhaled xenobiotics and can metabolize compounds through CYP enzymes and phase II reactions (benzene, naphthalene)
  • The kidney plays a role in the metabolism and excretion of xenobiotics and can be a target for tissue-specific toxicity (chloroform)

Blood-brain barrier

  • The blood-brain barrier (BBB) is a selectively permeable barrier that regulates the entry of xenobiotics into the central nervous system (CNS)
  • The BBB is formed by tight junctions between endothelial cells and the presence of efflux transporters (P-glycoprotein)
  • Xenobiotics that are lipophilic and have low molecular weight can cross the BBB more readily (ethanol, caffeine)
  • Metabolism of xenobiotics by CYP enzymes and phase II reactions in the brain can influence their CNS effects and toxicity (nicotine, polycyclic aromatic hydrocarbons)

Placental transfer

  • The placenta is a selective barrier that regulates the transfer of xenobiotics from the maternal circulation to the fetal compartment
  • Placental transfer depends on factors such as the physicochemical properties of the xenobiotic, the stage of pregnancy, and the presence of placental transporters
  • Some xenobiotics can cross the placenta and expose the developing fetus to potential toxicity (thalidomide, alcohol)
  • The placenta expresses drug-metabolizing enzymes (CYP enzymes, UGTs) that can influence the extent of fetal exposure to xenobiotics and their metabolites

Metabolic disorders and toxicity

  • Metabolic disorders, whether inborn or acquired, can alter the body's ability to metabolize xenobiotics and endogenous compounds
  • These disorders can lead to the accumulation of toxic metabolites or the impaired detoxification of xenobiotics
  • Understanding the impact of metabolic disorders on toxicity is important for risk assessment and patient management

Inborn errors of metabolism

  • Inborn errors of metabolism are genetic disorders that affect the synthesis, degradation, or transport of specific molecules
  • Examples include phenylketonuria (PKU), which impairs the metabolism of phenylalanine, and galactosemia, which affects the metabolism of galactose
  • These

Key Terms to Review (23)

Absorption: Absorption is the process through which substances are taken up into the body, often after being introduced through various routes such as ingestion, inhalation, or dermal contact. This fundamental process determines how toxins and chemicals enter systemic circulation, influencing their subsequent distribution, metabolism, and overall toxicological effects within the body. Understanding absorption is crucial for evaluating how toxins behave once they enter the organism and how effectively they can be eliminated or neutralized.
Active Metabolite: An active metabolite is a product of drug metabolism that retains pharmacological activity, often contributing to the drug's therapeutic effects or toxicity. These metabolites can enhance, diminish, or alter the effects of the parent compound and may play a critical role in the overall pharmacokinetics and pharmacodynamics of the drug. Understanding active metabolites is essential for predicting drug interactions and individual responses to medications.
Age: Age refers to the length of time that a person has lived or a thing has existed. In the context of biological systems, age plays a critical role in how organisms metabolize substances and respond to toxic agents, as physiological processes can vary greatly across different life stages. Furthermore, age is a crucial factor in understanding cardiotoxicity, as the effects of drugs and environmental toxins on the cardiovascular system can differ significantly between younger and older populations.
Bioactivation: Bioactivation refers to the metabolic process through which a substance is converted into a more reactive or active form, often resulting in its increased toxicity or biological activity. This process is crucial in toxicology, as it helps to understand how various compounds, including drugs and environmental toxins, can transform within the body, leading to both therapeutic effects and potential harm.
Biotransformation: Biotransformation refers to the chemical modification made by an organism on a chemical compound. This process is crucial in toxicology as it can transform harmful substances into less toxic forms, impacting how these substances interact with biological systems. The ability to biotransform compounds varies widely across different organisms and can influence toxicity, metabolism, and the effects of natural toxins, making it a key concept in understanding how chemicals affect living beings over time.
Cytochrome P450: Cytochrome P450 is a large family of enzymes that play a critical role in the metabolism of various substances, including drugs and toxins, by facilitating their oxidation. These enzymes are primarily found in the liver and are involved in the biotransformation process, which alters the chemical structure of compounds to enhance their elimination from the body. Understanding cytochrome P450 is essential for toxicology as it impacts drug metabolism and the body's response to environmental chemicals.
Detoxification: Detoxification is the biochemical process by which harmful substances, including toxins and metabolic waste, are neutralized or eliminated from the body. This process is crucial for maintaining overall health as it helps prevent the accumulation of potentially dangerous compounds that can disrupt normal cellular functions and lead to disease. Detoxification primarily occurs in the liver but also involves other organs, such as the kidneys, lungs, and intestines, playing essential roles in ensuring that the body remains free from harmful substances.
Distribution: Distribution refers to the process by which a substance, such as a drug or toxin, is dispersed throughout the body after it enters the bloodstream. This involves the movement of substances from the site of absorption to various tissues and organs, influenced by factors like blood flow, tissue permeability, and the physicochemical properties of the substance. Understanding distribution is crucial for predicting how substances will behave in biological systems and their potential effects on health.
Environmental Factors: Environmental factors are external elements that can influence the development, metabolism, and overall health of organisms. These factors encompass a wide range of influences, including physical, chemical, biological, and social conditions in an organism's environment, which can significantly affect metabolic processes and the effects of toxins within the body.
Enzyme induction: Enzyme induction is a biological process where the synthesis of enzymes is increased, typically in response to the presence of a substrate or an external stimulus. This mechanism is essential for the regulation of metabolic pathways, allowing organisms to adapt to changes in their environment or to detoxify harmful substances more effectively. By enhancing the production of specific enzymes, the body can improve its ability to metabolize drugs and other xenobiotics, ultimately influencing overall metabolism.
Enzyme inhibition: Enzyme inhibition refers to the process by which a molecule, known as an inhibitor, decreases or halts the activity of an enzyme, which can impact various biochemical reactions. This is crucial in regulating metabolic pathways, drug development, and understanding the toxic effects of substances on biological systems. Inhibition can be reversible or irreversible and may involve competitive or non-competitive mechanisms, ultimately influencing physiological processes and therapeutic outcomes.
Excretion: Excretion is the biological process through which organisms eliminate waste products from their bodies. This process is vital for maintaining homeostasis and preventing the accumulation of toxic substances, which can interfere with metabolic functions and overall health. Excretion is closely linked to metabolism, as it is often the end result of metabolic processes that produce waste, and it plays a crucial role in toxicodynamics by determining how long a toxic substance remains in the body.
First-pass metabolism: First-pass metabolism is the process by which the concentration of a drug is significantly reduced before it reaches systemic circulation, primarily due to the metabolism that occurs in the liver. This phenomenon is crucial in pharmacokinetics, as it influences the bioavailability of orally administered medications and can determine their therapeutic effectiveness. The extent of first-pass metabolism can vary widely among different drugs and between individuals, impacting how much of the active substance reaches the bloodstream.
Genetics: Genetics is the branch of biology that studies heredity and variation in organisms, focusing on how traits are passed from parents to offspring through genes. It plays a crucial role in understanding metabolic processes, as genetic variations can influence enzyme production, drug metabolism, and the body's response to toxins, ultimately affecting an individual's susceptibility to various substances.
Glutathione s-transferase: Glutathione S-transferase (GST) is a family of enzymes that catalyze the conjugation of the antioxidant glutathione to various substrates, aiding in the detoxification process. These enzymes play a critical role in metabolism by facilitating the elimination of potentially harmful compounds, including drugs and environmental toxins, thus protecting cells from oxidative damage. The activity and expression of GSTs can vary among individuals due to genetic polymorphisms, making them an important focus in understanding individual responses to toxic exposures and drug metabolism.
Hepatic Metabolism: Hepatic metabolism refers to the biochemical processes that occur in the liver to convert various substances, including drugs and toxins, into metabolites that can be easily eliminated from the body. This process plays a crucial role in drug detoxification and elimination, as the liver acts as the primary site for drug metabolism. Understanding hepatic metabolism is essential for evaluating the efficacy and safety of pharmaceutical compounds, as well as understanding how different substances can affect liver function.
Inactive metabolite: An inactive metabolite is a chemical compound that is formed when a drug undergoes metabolism and loses its pharmacological activity. These metabolites are typically produced through biochemical processes, such as oxidation, reduction, or hydrolysis, and they usually do not exert therapeutic effects. Understanding inactive metabolites is essential in the study of drug metabolism, as they can influence the overall pharmacokinetics and safety profile of medications.
Inter-species variation: Inter-species variation refers to the differences in biological responses, including metabolic processes, toxicity levels, and susceptibility to chemicals, among different species. These variations can significantly influence how organisms metabolize substances, affecting the assessment of risks and toxicological outcomes when evaluating the effects of chemicals on human health and the environment.
Intra-species variation: Intra-species variation refers to the genetic, physiological, and behavioral differences that occur among individuals within the same species. This variation can significantly impact how organisms metabolize substances, respond to toxins, and adapt to their environments, making it a crucial factor in the study of metabolism and toxicology.
Phase I Reactions: Phase I reactions are biochemical processes that primarily involve the modification of drug molecules through oxidation, reduction, and hydrolysis. These reactions are crucial for increasing the polarity of compounds, making them more water-soluble and facilitating their elimination from the body. By introducing or exposing functional groups, Phase I reactions prepare compounds for subsequent Phase II reactions, where they can be further conjugated to enhance their excretion.
Phase II Reactions: Phase II reactions refer to the biochemical processes that involve the conjugation of small, polar molecules to metabolites that have been modified in Phase I reactions. These reactions serve to further detoxify and increase the water solubility of substances, facilitating their excretion from the body. The main goal is to prepare these metabolites for elimination through urine or bile, making them less toxic and easier to eliminate.
Toxic metabolite: A toxic metabolite is a chemical compound produced during the metabolism of a substance, which can have harmful effects on biological systems. These metabolites can result from the biotransformation of drugs, chemicals, or environmental pollutants, leading to unintended toxic effects that may contribute to cellular damage, organ dysfunction, or adverse health outcomes.
Toxicity: Toxicity refers to the degree to which a substance can cause harm to an organism. It encompasses how various factors such as dosage, exposure time, and individual susceptibility influence the adverse effects that can result from the intake of toxic substances. Understanding toxicity is crucial for evaluating the safety of chemicals, drugs, and environmental pollutants, particularly in how they interact with metabolic processes and accumulate in biological systems.
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