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Teaching aims
By the end of the lecture, students would be able to : realize that humans are subjected to exposure to various foreign chemicals (xenobiotics) and understand how xenobiotics are handled at the cellular level
Core topics
Introduction Metabolism of xenobiotics Phase 1 Phase 2 Responses to xenobiotics
Introduction
A xenobiotic is a compound that is stranger to the body (xenobiotics xenos = stranger) Humans are subjected to exposure to various (maybe thousands) foreign chemicals e.g. drugs, good additives, pollutants, etc. Those relevance to medicine are drugs, chemical carcinogens, polychlorinated biphenyls (PCB) & certain insecticides
Introduction (cont.)
They must be metabolized (chemical alteration) before being excreted Knowledge of the metabolism of xenobiotics is basic to a rational understanding of pharmacology & therapeutics, pharmacy, toxicology, cancer research, drug addiction etc.
Metabolism of xenobiotics
Liver is the main organ involved in xenobiotics metabolism Occasionally, a xenobiotic may be excreted unchanged At least 30 different enzymes catalyze reactions involved in xenobiotics metabolism
It is convenient to consider the metabolism of xenobiotics in two phases: Phase 1 The major reaction involved is hydroxylation, catalyzed by members of a class of enzymes called monooxygenases or cytochrome P450s. In addition to hydroxylation, these enzymes catalyze wide range of reactions, including those involving deamination, dehalogenation, desulfuration,epoxidation, peroxygenation, & reduction
Reactions involving hydrolysis (eg. Catalyzed by esterases) & certain other non-P450-ctalyzed reactions Phase 2 Hydroxylated or other compounds produced in phase 1 are converted by specific enzymes to various polar metabolites by conjugation with glucuronic acid, sulfate, acetate, glutathione, or certain amino acids, or by methylation.
The overall purpose of the 2 phases is to increase their water solubility (polarity) and thus facilitate their excretion from the body
Very hydrophobic xenobiotics would persist in adipose tissue almost indefinitely unless they are converted to more polar forms
In certain cases, phase 1 metabolic reactions convert xenobiotics from inactive to biologically active compounds in these instances, the original xenobiotics are referred to as prodrugs or procarcinogens In other cases, additional phase 1 reaction (eg. further hydroxylation reactions) convert the active compounds to less active or inactive forms prior to conjugation.
In other cases, it is the conjugation reactions themselves that convert the active products of phase 1 reactions to less active or inactive products, which are subsequently excreted in the urine or bile. In a very few cases, conjugation may actually increase the biologic activity of a xenobiotic The term detoxification is sometimes used for many of the reactions involved in xenobiotics metabolism, but the term is not always appropriate
RH + O2 + NADPH + H+ R-OH + H2O + NADP or Reduced cyt. P-450 Oxidized cyt P-450
RH + O2 R OH + H2O RH can represent a variety of xenobiotics, including drugs, carcinogens, pesticides, petroleum products & pollutants (such as a mixture of PCBs)
Cyt.P-450
Endogenous compounds, such as certain steroids, eicosanoids, fatty acids & retinoids are also substrate (generally lipophilic) Cyt. P-450 is major monooxygenases in endoplasmic reticulum. It is important because approx. 50% of the drugs that humans ingest are metabolized by isoforms of cyt. P-450, and these enzymes also act on various carcinogens & pollutants
Cyt. 450 is considered the most versatile biocatalyst known Isoforms of cyt. P-450 make up a superfamily of heme-containing enzymes (they exhibit 40% or more sequence identity): Needs a systematic nomenclature (Arabic number followed by a capital letter indicating the subfamily & individual number) CYP1A1 is cyt. P-450,a member of family 1 & subfamily A & the first individual member. The gene encoding this enzyme is CYP1A1
They are hemoproteins They are widely distributed across species They are present in highest amount in liver & small intestine present mainly in membranes of the smooth endoplasmic reticulum. In the adrenal they are found in mitochondria as well as in the endoplasmic retic. Mitochondrial cyt. P-450 system differs from the macrosomal system in that it uses an NADPH-linked flavoprotein
There are at least six isoforms of cyt. P-450 present in the endopl. retic. of human liver, each with wide & somewhat overlapping substrate specificities & acting on both xenobiotics and endogenous compounds NADPH, not NADH is involved in the reaction mechanism of cyt. P-450 Lipids, particularly phosphatidylcholine are also components of cyt. P450 system
Most isoforms of cyt. P-450 are inducible (has important clinical implication due to biochemical mechanism of drug interaction. Certain isoforms of cyt. P-450 (eg. CYP2E1) are particularly involved in the metabolism of Polycyclic Aromatic Hydrocarbon (PAHs) & related molecules Certain cyt. P-450s exist in polymorphic forms (genetic isoforms), some of which exhibit low catalytic activity
b. Sulfation (Adenosine 3-phosphate-5phosphosulfate=PAPS as sulfate donor). Substrates: steroids, glycosaminoglycans, glycolipids & glycoproteins c. Conjugation with glutathione (tripeptide glutamylcysteinylglycine = GSH). Substrates: electrophilic xenobiotics R + GSH RSG R = an electrophilic xenobiotic and the enzymes catalysing the reaction are :
glutathione S-transferase.
Glutathione conjugates are subjected to further metabolism before excretion (eg. Mercapturic acid excreted in the urine)
d. Other reactions: 1. acetylation X + Acetyl-CoA acetyl-X + CoA (using acetyltransferases in the cytosol of various tissues, particularly liver, eg. Drug isoniazid for tuberculosis) 2. Methylation (using Sadenosylmethionine as methyl donor & methyltransferase as the enzyme)
Notes for glutathione: Other important function of glutathione: Participate in the decomposition of potentially toxic hydrogen peroxide catalyzed by glutathione peroxidase Intracellular reductant, helping to maintain essential SH groups of enzymes in their reduced state Transport of certain amino acids across membrane in the kidney
Diseases eg. cirrhosis of the liver can affect activities of drug metabolizing enzymes
Reactive metabolite
Nontoxic metabolite
Covalent bonding To macromolecules Cell injury Hapten Antibody production Cell injury Mutation
Cancer