Carcinogenesis: Mechanisms and Models Chapter | 20  343




  VetBooks.ir  Tumor Promotion Is a Nongenetic Process
             That Affects the Growth Kinetics of the Initiated
             Cells and It Can Be Reversible
             Tumor promoters alter the expression of genetic infor-
             mationofthe cell andinmanycasesinhibitpro-
             grammed cell death (Pitot, 2002). Tumor promoters are
             involved in mitogenic signaling to trigger increased cell
             proliferation, thereby influencing the proliferation of
             initiated cells as well. Irigaray and Belpomme (2010)
             defined tumor promoters as nongenotoxic carcinogens
             capable of causing clonal expansion of initiated cells,
             i.e., able to induce proliferation of mutated cells and to
             prevent these cells from apoptotic loss, so the possibility
             of additional genetic and/or epigenetic changes is
             preserved.
                The proliferation of preneoplastic cells leads to the
             formation of benign focal lesions, such as enzyme-altered
             foci in the liver, nodules in the mammary gland, polyps in
             the colon, papillomas in the skin. Because tumor promo-
             ters alter the expression of genetic information without
             changing the DNA sequence, tumor promotion is an epi-
             genetic process. In addition to causing cell proliferation,
             tumor promoters appear to block apoptosis, thus leading
             to the accumulation of preneoplastic cells within a tissue.
             Some of the lesions that develop due to promotion may
             regress, but others acquire additional mutations and prog-
             ress to malignant neoplasm. Tumor promotion is a
                                                                FIGURE 20.1 The target tissue must be exposed to an initiator first
             reversible process up to a certain stage if the promoter is
                                                                followed by repeated exposure to promoters in order for the tumors to
             withdrawn.
                                                                develop. If the time gap between the exposure to initiator and promoter
                In order for the tumors to develop, the target tissue  varies from a week to a year, tumors will still develop. However, if the
             must be exposed to an initiator first and then repeatedly  exposure to promoter is first and is followed by exposure to initiator,
             exposed to promoters. If the time gap between the  tumors will not develop. Also, if the exposure to promoter is not
                                                                repeated and spaced over time, tumors is not likely to develop even if
             exposure to initiator and promoter varies from a week
                                                                the exposure to promoter occurs after exposure to initiator.
             to a year, tumors will still develop. However, if the
             exposure to promoter is first and is followed by
             exposure to initiator, tumors will not develop. Fig. 20.1  cells. At the cytogenetic level, progression is associated
             shows the importance of the sequence of exposure   with additional mutations and a karyotypic change
             to tumor initiator and tumor promoter in tumor     because virtually all tumors are aneuploid (have the
             development. Table 20.4 shows some common tumor    wrong number of chromosomes). Additionally, chromo-
             promoters.                                         somal abnormalities, such as deletion, duplication,
                                                                or translocation of chromosomal fragments are hallmarks
                                                                of tumor progression. Additional mutations in the
             Tumor Progression Is a Genetic Process That        oncogenes and tumor suppressor genes also accumulate
             Involves Transformation of a Benign Tumor          during this phase. Because tumor progression is a genetic
             Into a Malignant Tumor and Metastasis              process that involves the accumulation of additional
             of the Malignant Neoplasm                          mutations (beyond the initiating mutation), tumor initia-
             The term tumor progression, coined by Leslie Foulds,  tors can also cause tumor progression (Qin et al., 2000;
             refers to the stepwise transformation of a benign tumor  Becker et al., 2003).
             into a malignant tumor and involves autonomous growth  Karyotypic instability and accumulation of additional
             and metastasis of the malignant neoplasm. Irigaray  mutations reflect an ongoing selection of cells suitable for
             and Belpomme (2010) defined tumor progressors as carci-  neoplastic growth and metastasis (Okey et al., 1998).
             nogens that advance mutated cells from promotion to pro-  Such increased fitness of a subset of cells for neoplastic
             gression, i.e., that allow premalignant mutated cells  growth and metastasis is thought to be conferred by
             to irreversibly acquire the phenotype of fully malignant  specific mutation(s) called driver mutations. The rest of