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Review
. 2016 Dec;2(12):713-722.
doi: 10.1016/j.trecan.2016.11.003.

Cancer Prevention: Lessons Learned and Future Directions

Affiliations
Review

Cancer Prevention: Lessons Learned and Future Directions

Barbara K Dunn et al. Trends Cancer. 2016 Dec.

Abstract

In this review, we address selected areas that are central to the state-of-the-art of cancer prevention science. The emphasis on prevention as a viable and critical approach to decreasing cancer mortality has gained traction in recent years, evidenced by its inclusion in the US Vice President's Cancer Initiative (also termed 'Moonshot'). Cancer prevention occurs by arresting, slowing down, or reversing the carcinogenic process before invasion into surrounding tissue or by avoiding or blocking causative exposure. An important challenge is to identify individuals who will benefit most from preventive interventions with the least possible harm. Preventive interventions range from avoiding known carcinogens (e.g., tobacco or asbestos) to intervening with anticarcinogenic strategies (behavioral modifications , such as diet and exercise; medications; nutritional agents; and vaccination against causative agents). Here, we focus on active intervention with measures involving pharmaceutical and immunological agents.

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Figures

Figure 1
Figure 1
Evolution of a tumor from normal tissue through progressively advanced premalignant lesions to invasive cancer [going from left to right in (A)] is depicted by the cartoon in (B). Normal cells are shown in white. Progressively abnormal cells appear in gradually darker shades of blue, with dark-blue circles representing invasive cancer cells and red circles depicting cancer cells with metastatic potential. This progression results from the accumulation of oncogenic genetic mutations (C). The resulting mutational accumulation confers growth advantages, leading to clonal expansion over time of genetically more complex cells, as shown in cells spreading out along the Y axis (B). In parallel with the neoplastic progression (B), the microenvironment, in particular the immune environment (D), evolves. In normal-appearing or at-risk tissue, the immune component of the microenvironment is populated in large part by immunocompetent cells capable of fighting cancer cells; in (D), these are represented by TH/CD4 and cytolytic/CD8 T cells and antigen-presenting cells (APCs), such as dendritic cells (DCs). Among others, these cells are capable of carrying out immuno-surveillance and eliminating incipient premalignant cells. As lesions progress to more advanced premalignant and, ultimately, invasive malignant states, the immune environment becomes progressively suppressed and less able to eliminate the abnormal cells. This evolving immunosuppression is represented in (D) by increased abundance of T regulatory cells (Tregs) and myeloid-derived suppressor cells (MDSCs), which antagonize beneficial immune responses, allowing the tumor to grow. Administering anticancer drugs or vaccines before invasion (vertical red line) constitutes ‘preventive’ intervention. This approach, especially early during progression, is likely to be more effective than administering preventive agents late in premalignancy or ‘treatment’ interventions after invasion. The more intact state of the immune system early during premalignancy facilitates a robust response to cancer-preventive vaccination and may also enhance anticancer responses to chemopreventive agents. Additional factors contributing to the relative efficacy of preventive versus treatment interventions are shown in the large light-blue arrows. The progressive changes observed in the tumor microenvironment during carcinogenesis, including evolving immunosuppression, are reviewed in [93,138,139]. Key: formula image, normal-appearing/at-risk cell; formula image, formula image, progressively abnormal premalignant cells; formula image, invasive cancer cell; formula image, cancer cell with metastatic potential; formula image, helper T cell (TH/CD4]; formula image, cytolytic T cell (CTL/CD8]; formula image, APC, for example, DC.

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