| Literature DB >> 28534024 |
Sandeep K Singh1, Mehmet Tevfik Dorak2.
Abstract
The power of cancer immune surveillance has been documented beyond doubt, and the successful exploitation of immune response to cancer has started a new era in the war against cancer. Cancer biologists have recognized immunoevasion as an emerging hallmark in addition to the six hallmarks of cancer. Besides the natural connection between the immune system and cancer development, most established environmental risk factors are now known to interfere with immune surveillance mechanisms. Genetic variations regulating immunity may also modulate cancer susceptibility, but evidence for this is currently limited. Molecular cross talk linking "immune" and "genomic" surveillance pathways has been characterized. It appears that immune mechanisms may contribute to the effects of common cancer risk factors. We provide an updated overview of evidence for cancer immune surveillance, cancer risk factors interfering with it, and interventions to enhance cancer immune surveillance as tools to complement ongoing vaccine development efforts for cancer immunoprevention. Although there is a lot of support for cancer immunoprevention with simple lifestyle modifications from observational studies, there is an urgent need for clinical trials to establish the effectiveness of this approach for public health benefits.Entities:
Keywords: cancer immune surveillance; cancer immunology; cancer prevention; cancer risk factors; immunoprevention; public health
Year: 2017 PMID: 28534024 PMCID: PMC5421153 DOI: 10.3389/fpubh.2017.00101
Source DB: PubMed Journal: Front Public Health ISSN: 2296-2565
Immune regulatory gene polymorphisms and cancer susceptibility in GWAS and GRASP catalogs.
| Genetic variants | Main non-cancer associations | Cancer associations | Reference [PubMed ID number (PMID)] |
|---|---|---|---|
| Genetic variants regulating immune cell levels | Autoimmune disorders (type 1 diabetes, rheumatoid arthritis) | Neuroblastoma (rs6547705; | 21124317 |
| Genetic variants correlated with immune traits | Autoimmune disorders (ulcerative colitis); hemoglobin A2 level | Neuroblastoma (rs10917750; | 21124317 |
| Immunoregulatory gene variants associated with cancer risk in candidate gene studies | Autoimmune disorders (rheumatoid arthritis, Crohn disease) | Non-melanoma skin cancer (rs12203592; | 23548203 |
| Melanoma (rs12203592; | 20602913 | ||
| Neuroblastoma (rs12203592; | 21124317 | ||
| Breast cancer (rs12203592; | 20453838 | ||
| Hodgkin lymphoma (rs2395185; | 22286212 | ||
| Lung cancer (rs2395185; | 23143601 | ||
| Acute lymphoblastic leukemia (rs17007695; | 19176441 | ||
| Childhood acute lymphoblastic leukemia (rs5742909, | 20189245 | ||
| Breast cancer (rs2296135, | 23468962 | ||
| Non-Hodgkin lymphoma (rs1041981; | 21471979 | ||
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Evidence for immune surveillance against the development of cancer and for the control of existing cancer.
| Observation | Implication | Reference |
|---|---|---|
| Immunodeficient animals and humans developing more cancers; immunosuppression causing an increase in cancer incidence | Control of cancer development by the immune system | ( |
| Increased risk for cancer in people with lower natural cytotoxic activity in their peripheral blood | Control of cancer development by the immune system | ( |
| A high percentage of occult cancers in autopsy studies | Control of cancer at the preclinical stage by the immune system (equilibrium) | ( |
| Decades long time taken by pancreas cancer to become clinically overt | Control of cancer at the preclinical stage by the immune system | ( |
| Control of occult cancer at the equilibrium phase by adaptive immune system | Control of cancer at the preclinical stage by the immune system | ( |
| Development of donor-derived malignancies that have been kept under control in immunosuppressed transplant recipients | Control of cancer at the preclinical stage by the immune system | ( |
| More immunogenic tumors developing in more immunodeficient animals | Elimination of immunogenic tumors by immune competent hosts | ( |
| Cancer patients with antibodies against antigens of their tumors (e.g., carcinoembryonic antigen, mucin 1) having a better clinical outcome and even spontaneous regression | Existent antitumor immunity exerting a favorable effect on the outcome | ( |
| Successful chemopreventive agents (aspirin, metformin, tamoxifen, bisphosphonate) having immune enhancing effects | Contribution of the immune system to the preventive effects | ( |
| Successful cancer chemotherapeutic agents having immune modulatory effects favorable for anticancer immunity | Contribution of the immune system to the therapeutic effects | ( |
| The composition of tumor-infiltrating immune cells and indicators of immune system activity correlate with the clinical outcome | Existent antitumor immunity exerting a favorable effect on the outcome | ( |
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