340 SECTION | III Nanoparticles, Radiation and Carcinogens




  VetBooks.ir  TABLE 20.1 Some Examples of Chemical Carcinogens

                                                    Aflatoxin (from the fungus Aspergillus flavus)
               Carcinogens occurring naturally
                                                    Aristolochic acid (in plant family Aristolochiaceae)
                                                    Toxic metals (e.g., As, Ni)
                                                    Safrole (from the root-bark or the fruit of sassafras plants)
                                                    Ionizing radiation
               Carcinogens produced by industrial and    Benzo[a]pyrene formed by incomplete combustion (e.g., vehicle emissions, tar and
               nonindustrial processes             asphalt fumes, meat barbeque)
                                                    Acrylamide formed during cooking French fries and potato chips
                                                    Tobacco smoke
                                                    Coal tar that is produced by the carbonization of coal, i.e., heating of coal in the
                                                   absence of air at very high temperatures
                                                    Benzene
                                                    Dyes (aromatic amines, such as 2-Naphthylamine)





             such as inorganic, organic, fibers, plastic, hormones, etc.  A genotoxic carcinogen can be a direct genotoxic car-
             Table 20.1 shows some chemical carcinogens.        cinogen or an indirect genotoxic carcinogen (procarcino-
                                                                gen). A direct genotoxic carcinogen is DNA-reactive
             Chemical Carcinogens Can Be Genotoxic              without metabolic activation, whereas an indirect geno-
             or Nongenotoxic                                    toxic carcinogen (procarcinogen) becomes DNA-reactive
                                                                following metabolic activation. Metabolic activation of
             Based on their biological activities, chemical carcinogens
                                                                the indirect genotoxic carcinogen (procarcinogen) gener-
             can be classified as genotoxic carcinogens that are DNA-
                                                                ates the ultimate carcinogen, which is DNA-reactive
             reactive, and nongenotoxic carcinogens that are not DNA-
                                                                (Table 20.2). The majority of genotoxic carcinogens are
             reactive.
                                                                indirect carcinogens because they need metabolic activa-
                                                                tion to form an electrophile that reacts with nucleophilic
             Genotoxic (DNA-Reactive) Carcinogens Interact      DNA (Marquardt, 1999).
             With DNA
             Most genotoxic carcinogens act as tumor initiators.
             Genotoxic carcinogens interact directly with DNA through  Nongenotoxic (Non DNA-Reactive) Carcinogens
             the formation of covalent bonds, resulting in DNA-  Do Not Directly Interact With DNA
             carcinogen complexes (DNA adducts). These complexes  Most nongenotoxic carcinogens act as tumor promoters
             lead to various types of DNA damage, such as point muta-  (Table 20.2). Nongenotoxic carcinogens do not directly
             tions, chromosome breakage, fusion, missegregation and  induce DNA damage. They can act through a number of
             nondisjunction, all of which result in modifications to the  different mechanisms, such as specific protein binding,
             information stored in DNA as well as genomic instability.  receptor interactions, hormonal and endocrine modifier
             Some of the mechanisms underlying structural alterations  effects, epigenetic changes in the DNA, etc. (Benigni
             include the formation of cross-links between the two heli-  et al., 2013). Thus, any genotoxic event in response to
             ces, chemical bonds between adjacent bases, removal of  challenge by nongenotoxic carcinogen is secondary to
             DNA bases (hydration) and cleavage of the DNA strands.  other biologic activity. For example, oxidative stress pro-
             Such mutations are typically fixed by DNA repair mechan-  duced by a nongenotoxic carcinogen as a primary effect
             isms; however, if DNA replication occurs prior to the action  can cause DNA damage as a secondary effect, but this
             of a repair mechanism, mutations can become permanent  secondary effect of DNA damage does not make the oxi-
             (Lee et al., 2013). In addition, DNA repair process is not  dative stress causing chemical a genotoxic carcinogen
             devoid of errors; therefore, mutations can be induced by the  (Trosko and Upham, 2005). Nongenotoxic carcinogens
             very repair processes cells use to rid themselves of DNA  usually exhibit tissue and species specificity.
             damage. An affected cell first tries to reverse the damage  Increasing evidence suggests that the demarcation
             by DNA repair. If DNA repair and removal of the damage  between genotoxic and nongenotoxic carcinogens may not
             fails the cell often undergoes programmed cell death (apo-  be as distinct as initially thought. For example, epigenetic
             ptosis). If the cell fails to undergo apoptosis, the result is a  changes may play a causative role in carcinogenic process
             permanent fixation of the damage in the DNA, which pro-  induced by genotoxic agents as well (Pogribny et al.,
             vides the first trigger of tumor development.      2008). Tumor initiators can both initiate and promote