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Abstract

Antioxidants play important roles in the maintenance of cellular integrity and thus are critical in maintaining the homeostasis of the host immune system. A balance between the levels of pro-oxidants and antioxidants defines the cellular fate of genomic integrity via maintaining the redox status of the cells. An aberration in this balance modulates host immunity that affects normal cellular signaling pathways resulting in uncontrolled proliferation of cells leading to neocarcinogenesis. For decades, there have been scientific debates on the use of antioxidants for the treatment of human cancers. This review is focused on current updates on the implications of antioxidant use as adjuncts in cancer therapy with an emphasis on immunomodulation and radiosensitization.

Keywords

antioxidants cancer therapy immunosuppression oxidized glycerophosphocholines platelet-activating factor–receptor immunomodulation radiosensitization

Introduction

The involvement of the reactive oxygen species (ROS) is well documented in various disease processes, including cancers.^1-3 Under normal circumstances, the redox status of cells is maintained by a balance between ROS production and its sequestration by antioxidants.¹ While ROS is used as an innate mechanism of host immunity to fight against extracellular pathogens, including bacterial and viral infections, an exacerbated generation causes imbalance in cellular redox potential leading to alterations in signaling pathways and neocarcinogenesis.^1-8 ROS release can be affected by several cellular compartments.^9,10 As changes in the mitochondrial electron transport activity result in the production of ROS (mROS), heteroplasmic mutations in the mitochondrial DNA have been shown to increase the tumorigenicity of cancer cells via overproduction of mROS.^8,11,12 Several cellular antioxidant systems, including superoxide dismutase and thioredoxin play crucial roles in counteracting the damaging effects of increased ROS.^10,13 Cancer cells, particularly in the tumor microenvironment exhibit higher basal oxidative stress compared to normal cells and thus take advantage of the upregulated antioxidant system to circumvent ROS-mediated tumor cell damage.^10,14,15

Antioxidants and Immunity

The development of cancer has been linked to an inability of the host immune system to respond appropriately to tumor antigens, which leads to tumor immune evasion.^16,17 The recognition and eradication of cancer cells by the immune system are categorized as elimination, equilibrium, and escape phases, referred to as the 3Es of immunoediting, which are governed by various factors.^18-21 Briefly, in elimination phase, the host immune cells via the surveillance process recognize and try to eliminate nascent tumors.²¹ Whereas the equilibrium phase starts when a few tumor cells become resistant enough to sustain immune surveillance mechanisms and enter into the dormant stage, where equilibrium exists between tumor cell proliferation and immune cell–mediated apoptosis.^21,22 An escape phase is established when tumor cells override their destruction by the immune system, an immunosuppressive environment is maintained, which favors tumor cell proliferation, and the development of clinically detectable tumors is finally achieved.^21,23 A direct link between antioxidants and modulation of cancer immunoediting has not been fully established. Nevertheless, curcumin has been shown to modulate immunoediting processes including resurrecting immune surveillance mechanisms to help eradicate cancer cells via (a) restoration of CD4+/CD8+ T cells, (b) suppression of T cell apoptosis, and (c) inhibition of immunosuppression through attenuation of immunosuppressive regulatory T cells (Tregs) (Table 1).^24-28 Curcumin is a yellow-colored curcuminoid of turmeric of the family Zingiberaceae that is used as an herbal supplement, food flavoring and food coloring agent and is known to possess medicinal and anticarcinogenic properties that are attributed to its antioxidant and anti-inflammatory activities.^29-31 In addition, the antioxidant ascorbic acid (vitamin C) has been demonstrated to play an important role in stimulating the immune system via attenuating chronic inflammatory responses, the persistence of which is implicated in the etiology of various diseases, including cancer.³² Of note, chronic inflammation in tumors mediated via tumor infiltrating leucocytes (TIL) has been shown to induce immunosuppression and promote cancer growth.³³

Table 1.

Effect of Antioxidants on Host Antitumor Immunity: Evidences From Preclinical Studies.

Treatment	Experimental Model	Results	References
Curcumin	Swiss albino mice with Ehrlich ascites carcinoma cells	Restoration of tumor-induced depletion of host CD4+/CD8+ T cell proliferation, inhibition of thymocytes and splenocytes apoptosis, expansion of central memory and effector memory T cells and inhibition of suppressive activity of Tregs	27, 28
Resveratrol	BALB/c mice with 4T1 breast carcinoma cells	Inactivation of Stat3, prevention of tumor-evoked regulatory B cells (tBregs) generation and function and restricting the tBreg-induced conversion of FoxP3+ Tregs	34
Resveratrol	C57BL/6 and BABL/c mice with EG6 lymphoma and CT26 colon carcinoma cell lines	Suppression of tumor-derived Tregs	35
Fish oil and selenium yeast	BALB/cByJ mice with Line-1 and YAC-1 lymphoma cells	Decreased populations of immunosuppressive Tregs and myeloid-derived suppressor cells	36

Immunosuppression (ie, inhibition of the host immune system) via diverse environmental agents (such as ultraviolet radiation) acting on the skin is classically divided into local (localized to the site of application) and systemic immunosuppression.³⁷ Of importance, systemic immunosuppression has been implicated in human malignancies such as melanoma and glioblastoma.^38-40 In most cancer models, tumor-dependent immune suppression has been recognized as one of the major events in promoting immune evasion of malignant cells from the host’s antitumor immunity.^41-44 While tumor antigen-induced effector T-cells are required in inducing antitumor immunity, suppressor cells such as Tregs and myeloid-derived suppressor cells (MDSCs) promote tumor escape mechanisms.^41-47 Importantly, immune checkpoint inhibitors such as cytotoxic T lymphocyte associated protein 4 (CTLA-4) and programmed cell death protein 1 (PD-1) have been shown to mediate Tregs-induced immunosuppression and promote cancer growth. The blockade of these immune checkpoint inhibitors via anti-CTLA-4 and anti-PD-1 antibodies attenuates tumor growth as well as augments the effectiveness of cancer therapy approaches.^47-50 Notably, Tregs and MDSCs have been shown to be associated with poor prognosis and cancer treatment failure, including immunotherapy and vaccination approaches.^51-53 Therefore, agents/anti-cancer drugs that target these immunosuppressive cell types are being explored in several preclinical and clinical cancer models and also in combination with known anti-cancer drugs against various malignancies.^54-57 With regard to antioxidant use in attenuating the enhanced tumor growth mediated by these immunosuppressive cells, studies by Lee-Chang et al³⁴ have shown that administration of resveratrol, a dietary polyphenol compound possessing antioxidant properties at low doses that are nontoxic to immune cells, inhibits lung metastasis of breast cancer tumor. This resveratrol-induced effect was mediated via Stat3 inactivation, resulting in an inhibition of the generation and function of tumor-evoked regulatory B cells (tBregs) and their conversion into Tregs. In support of these findings, studies by Yang et al³⁵ have demonstrated that suppression of tumor-derived Tregs mediates resveratrol-induced inhibition of syngeneic murine EG7 lymphoma and CT26 colon carcinoma tumors in C57BL/6 and BALB/c mice models.³⁵ Of importance, resveratrol can exert both antioxidant and pro-oxidant properties depending on its concentration and cell types used.⁵⁸ Along similar lines, Wang et al³⁶ have demonstrated that a combination of fish oil and selenium that possesses anti-inflammatory and antioxidant activities exerted synergistic effects in suppressing lung tumor growth mediated via decreasing the population of splenic Tregs and MDSCs and thus augmented host anti-tumor immunity against lung carcinoma.

Exposure to pro-oxidative stressors generating ROS, including ultraviolet B (UVB) radiation and cigarette smoke (CS), is associated with the modulation of host immunity. Studies including ours have demonstrated the beneficial effects of antioxidant administration, including vitamin C and N-acetyl cysteine (NAC) in attenuating the systemic immunosuppressive effects of various environmental pro-oxidative agents, including UVB and CS in animal models.^59-65 Of significance, UVB and CS generate a class of oxidized lipid mediators nonenzymatically via free radical mediated attack on membrane phospholipid glycerophosphocholines (ox-GPCs).^59-65 In contrast, enzymatic synthesis of platelet-activating factor (PAF, 1-hexadecyl-2-acetyl-glycerophosphocholine) is a tightly regulated process, which requires cytoplasmic phospholipase A₂ (cPLA₂) that acts on 1-alkyl glycerophosphocholines (GPC) with sn-2 long-chained unsaturated fatty acids (eg, arachidonate) forming the lyso species which then is acetylated, forming PAF.^66,67 These ox-GPCs possess PAF and PAF-like agonist activities, which bind to and activate a 7-transmembrane G-protein coupled receptor, the PAF-receptor (PAF-R) which is expressed on various cell types (immune and nonimmune) including keratinocytes and tumor cells.^59-68 Our group uses 2 functional assays to quantify total PAF-agonists by very specific interleukin 8 (IL-8) protein or Ca²⁺ mobilization using stably PAF-R expressing (KBP) and deficient (KBM) cells generated retrovirally from human epidermal KB cells.^{59-62,65,69-71} The activity of Ox-GPCs/PAF is regulated by PAF-acetyl hydrolases (PAF-AH; PLA2G7).^66-68 Of 3 types, PAF-AHI is the major plasma isoform. PAF-R activation mediates various biological activities including early pro-inflammatory and delayed systemic immunosuppressive effects.^59-64 Our research group and others have shown that ox-GPCs/PAF-R agonists mediate UVB- and CS-induced systemic immunosuppression in a PAF-R dependent manner which is measured by inhibition of contact hypersensitivity (CHS) or delayed type hypersensitivity (DTH) responses to an eliciting allergen, dinitrofluorobenzene (DNFB) or an antigen, Candida albicans.^59-64 In using this methodology, for example, to measure UVB-mediated systemic immunosuppression, the shaved dorsal back skin of mice were exposed to UVB. A group of mice injected intraperitoneally with either PBS or the PAF-R agonist, CPAF served as negative and positive controls. Five days later, a 2x2 cm area of the back skin (approximately 2.5 cm distant from the UVB-radiated site) was sensitized with 0.5% DNFB topically. After 9 days, postelicitation changes in CHS were assessed by measuring changes in ear thickness. With similar methodology, the local immunosuppressive effect of UVB is assessed when dorsal skin of mice is sensitized with DNFB onto the UVB-exposed area (a model of local immunosuppression) and usually required lower UVB doses. Using this methodology we have demonstrated that PAF-R does not mediate UVB-induced local immunosuppressive effects,⁶⁵ despite its effect in mediating systemic immunosuppression. This PAF-R-dependent systemic immunosuppression is mediated via upregulation of COX-2 enzyme and COX-2-generated prostanoids, immunosuppressive cytokine interleukin 10 (IL-10) and the Tregs cell type, in a process blocked by antioxidants.^59-64 As both environmental and therapeutic pro-oxidative stressors generate ROS and thus ox-GPCs/PAF-R agonists, we have shown that supplementation of vitamin C and NAC in drinking water prophylactically suppressed generation of ox-GPCs/PAF-R agonists mediated by UVB, chemotherapy, and radiation therapy—as well as diminishing the augmentation of tumor growth induced by systemic immunosuppression.^69-71 Several standard chemotherapeutic agents, including dacarbazine and melphalan generate PAF-R agonists from both murine and human melanoma cells in vitro and intratumorally treated melanoma tumor xenografts in vivo.⁷⁰ Using a dual tumor model, we demonstrated that intratumoral melphalan (MELP) chemotherapy (of one tumor) augments the growth of secondary (untreated) B16F10 melanoma tumor in a PAF-R dependent manner.⁷⁰ Systemic antioxidants, COX-2 inhibitors or depleting Treg Abs attenuated this MELP-mediated enhanced growth of secondary tumors in WT mice,⁷⁰ indicating the role of oxidatively generated PAF-R agonists and downstream COX-2 and Tregs in modulating MELP efficacy. Nevertheless, antioxidant use postchemotherapy or to augment cancer therapy effectiveness in preclinical cancer models with regard to immunosuppression requires further investigation.

Antioxidants in Cancer Therapy

Despite recent advances in local and systemic treatment modalities, chemotherapy, radiation therapy and immunotherapy are widely considered either alone or in combinations for a variety of cancers. In chemotherapy, cancer cells are targeted by chemically modified agents/natural compounds with cytotoxic properties; radiation therapy uses high-energy particles/waves, including x-rays and gamma rays, to kill tumor cells; and immunotherapy treatments are designed to stimulate the host’s own immune system to attack cancer cells. One of the consequences of chemotherapy and radiation therapy is the generation of ROS which via its direct and indirect effects on tumor cells, induces DNA damage and/or affects DNA replication machinery, leading to aberrations in several cellular signaling pathways resulting in chemotherapy- or radiation therapy-induced cell death.^72-74 Most of these therapies are not considered a good option as a single agent to treat advanced-stage/metastatic cancers, in part due to the development of therapy-induced innate and/or acquired tumor resistance or local/systemic toxicities leading to either reduced response, nonresponsiveness or tumor relapse after an initial antitumor response.^75,76 Therefore, potentially new therapeutic approaches with agents that exhibit anticancer properties and can potentiate chemotherapy- or radiation therapy–mediated antitumor responses are required for inducing optimal and long-term benefits in cancer patients.

Several nutritional cancer chemopreventive compounds having antioxidant properties have been documented to potentiate radiation therapy–induced cytotoxic effects on cancer cells while reducing its toxicity on normal surrounding tissues.^77-86 In this regard, multiple studies by Raffoul et al⁷⁸ have shown that phytochemical soy isoflavones (genistein, daidzein, and glycitein), which exhibit anticarcinogenic properties in part via their antioxidant activities, could be used as potent radiosensitizers to enhance the efficacy of radiotherapy-mediated suppression of the growth and metastatic ability of cancers, including prostate cancer.^78-80 A study comparing the effects of the soy isoflavone component genistein on prostate cancer demonstrated that both soy and genistein inhibited the growth of in vitro human PC-3 prostate cancer cells and in vivo orthotopic PC-3 tumors and that these effects were enhanced when soy or genistein was combined with radiotherapy.⁷⁹ Mechanistically, soy isoflavones attenuated the radiation-induced increase in expression of apurinic/apyrimidinic endonuclease 1/redox factor-1 (APE1/Ref-1) and activation of NF-kB and its DNA-binding activity, resulting in potentiating radiotherapy-mediated effects and their use as radiosensitizers.⁷⁹ In addition, soy isoflavones have been shown to augment radiation-induced suppression of in vitro growth of human A549 non–small cell lung cancer cells via inducing increased DNA damage, inhibition of APE1/Ref-1 mediated DNA repair and decreased expression of the transcription factors NF-κB and HIF-1α.⁸² Importantly, agents possessing proteotoxic stress activities have been shown to enhance radiosensitization. In this regard, Pruitt et al⁸³ have demonstrated that dietary polyphenols known as hydroxychalones augmented radiation-mediated death of human colorectal adenocarcinoma HT-29 and pancreatic cancer Panc 1 cells. These effects were mediated via activation of the heat shock factor 1 (Hsf1) in a process blocked by prophylactic treatment with α-napthoflavone (ANF), a specific inhibitor of cytochrome P450 1A2 (CYP1A2).⁸³ Along similar lines, resveratrol and piperine, which possess properties including antitumor activities, have been shown to augment ionizing radiation (IR)-induced apoptosis and loss of mitochondrial membrane potential in murine colon carcinoma CT26 and melanoma B16F10 cells via enhancing IR-induced ROS generation.⁸⁴ Moreover, pentoxifylline (PTX), a methylxanthine that possesses antioxidant properties is known to improve tumor tissue oxygenation in murine hypoxic tumors as well as inhibiting post radiation-induced normal tissue injury in mice.^85-88 Importantly, PTX has been shown to enhance radiation-mediated effects in human breast MCF-7 and colon HT-29 carcinoma cells in vitro and murine mammary adenocarcinoma SCK tumors in A/J mice in-vivo.^85-88 In in vitro studies, PTX treatment has been shown to enhance radiotherapy-mediated effects in a dose and time dependent manner in post-irradiated cells, and did not change the cellular response to radiation in pre-irradiated cells.⁸⁶

Several chemotherapeutic agents used for the treatment of human malignancies generate ROS as one of the potent mechanisms to eradicate tumor cells via targeting multiple oncogenic signaling pathways. Hence, targeting ROS by antioxidants not surprisingly has yielded mixed results in the therapeutic efficacy of chemotherapy.^89-91 Importantly, in a systematic review, Block et al^92,93 have summarized the impact of antioxidant supplementation on the efficacy and toxicity of chemotherapeutic agents from several randomized controlled trials (RCTs). Antioxidants such as glutathione, melatonin, vitamin A and E, NAC, selenium, l-carnitine, Co-Q10, ellagic acid, an antioxidant mixture such as vitamin C and E with beta-carotene or selenium supplementation were evaluated on the efficacy of chemotherapeutic regimens, including oxaliplatin and cisplatin in combinations with agents such as etoposide, gemcitabine for several malignancies including breast, lung and gastric cancers.⁹⁰ Survival of patients and tumor response were the primary outcomes of these trials.⁹⁰ While a statistically significant improved survival rate either at 1 year or 5 years was associated with melatonin supplementation, vitamin A exerted mixed responses on therapy outcomes and no significant differences in the tumor response or survival were reported with other antioxidants.⁹⁰ Of significance, 24 RCTs reported significantly decreased toxicities with concurrent supplementation of antioxidants (mentioned above) with chemotherapy in cancer patients compared to patients who were not on systemic antioxidants (controls).⁹¹ On the other hand, 9 RCTs reported no differences in the toxicities by antioxidants supplementation and 1 RCT with vitamin A reported increased toxicity.⁹¹ Along similar lines, a systematic review on RCTs by Yasueda et al⁹⁴ summarized that it is difficult to determine whether antioxidant supplements affect treatment outcomes or ameliorate adverse effects induced by chemotherapy and radiotherapy. The authors concluded that harm caused by antioxidant supplementation remained unclear for patients during cancer therapy, except for smokers undergoing radiotherapy.⁹⁴ As cancer patients experience therapy-induced adverse side effects, including weight loss due to low nutritional intake and/or loss of appetite, individualized counsel for the use of antioxidants or supplements with antioxidant properties during treatment is important to circumvent its detrimental effects and/or therapy outcome.

Conclusion

While the safety and benefits of antioxidants use during cancer treatment are limited, their indispensable role in the maintenance of immune system homeostasis cannot be overruled. A large percentage of cancer patients undergoing active treatments uses antioxidants and not all antioxidants are likely to be beneficial; as well, their mode of action on cellular systems and interaction with anticancer drugs remained largely unexplored. Therefore, further preclinical and clinical studies are needed to establish the clinical implications of antioxidant doses and timings based on treatment regimens, disease stage, and especially immune suppression status.

Footnotes

Acknowledgements

The authors thank Dr Jeffrey Travers for critically reading the manuscript and providing inputs.

Declaration of Conflicting Interests

The author(s) declared no potential conflicts of interest with respect to the research, authorship, and/or publication of this article.

Funding

The author(s) disclosed receipt of the following financial support for the research, authorship, and/or publication of this article: RPS acknowledges the support from National Institutes of Health grant K22 ES023850.

References

Halliwell

. Reactive oxygen species in living systems: source, biochemistry, and role in human disease. Am J Med. 1991;91(3C):14S-22S.

Sreevalsan

Safe

. Reactive oxygen species and colorectal cancer. Curr Colorectal Cancer Rep. 2013;9:350-357.

Marinescu

Anghel

Gruia

Beuran

. Involvement of reactive oxygen species in the mechanisms associated with cervical cancer specific treatment. Chirurgia (Bucur). 2014;109:806-811.

Paiva

Bozza

. Are reactive oxygen species always detrimental to pathogens? Antioxid Redox Signal. 2014;20:1000-1037.

Bahia

Oliveira

Kubota

et al . The role of reactive oxygen species in Anopheles aquasalis response to Plasmodium vivax infection. PLoS One. 2013;8:e57014.

Cui

Chen

Wang

. Mechanisms and pathways of innate immune activation and regulation in health and cancer. Hum Vaccin Immunother. 2014;10:3270-3285.

Acharya

Das

Chandhok

Saha

. Redox regulation in cancer: a double-edged sword with therapeutic potential. Oxid Med Cell Longev. 2010;3:23-34.

Sullivan

Chandel

. Mitochondrial reactive oxygen species and cancer. Cancer Metab. 2014;2:17.

Panieri

Gogvadze

Norberg

Venkatesh

Orrenius

Zhivotovsky

. Reactive oxygen species generated in different compartments induce cell death, survival, or senescence. Free Radic Biol Med. 2013;57:176-187.

10.

Raninga

Trapani

Tonissen

. Cross talk between two antioxidant systems, thioredoxin and DJ-1: consequences for cancer. Oncoscience. 2014;1:95-110.

11.

Murphy

. How mitochondria produce reactive oxygen species. Biochem J. 2009;417:1-13.

12.

Sena

Chandel

. Physiological roles of mitochondrial reactive oxygen species. Mol Cell. 2012;48:158-167.

13.

Oyewole

Birch-Machin

. Mitochondria-targeted antioxidants. FASEB J. 2015;29:4766-4771.

14.

Bernardes

de Souza-Neto

Ramalho

et al . Systemic oxidative profile after tumor removal and the tumor microenvironment in melanoma patients. Cancer Lett. 2015;361:226-232.

15.

Satoh

Moriguchi

Taguchi

et al . Nrf2-deficiency creates a responsive microenvironment for metastasis to the lung. Carcinogenesis. 2010;31:1833-1843.

16.

Yan

Pan

et al . Lewis lung cancer cells promote SIGNR1 (CD209b)-mediated macrophages polarization induced by IL-4 to facilitate immune evasion. J Cell Biochem. 2016;117:1158-1166.

17.

Vences-Catalán

Rajapaksa

Srivastava

et al . Tetraspanin CD81 promotes tumor growth and metastasis by modulating the functions of T regulatory and myeloid-derived suppressor cells. Cancer Res. 2015;75:4517-4526.

18.

Teng

Galon

Fridman

Smyth

. From mice to humans: developments in cancer immunoediting. J Clin Invest. 2015;125:3338-3346.

19.

Bhatia

Kumar

. Cancer stem cells and tumour immunoediting: putting two and two together. Expert Rev Clin Immunol. 2016;12:605-607.

20.

Jones

Broz

Ranger

et al . STAT3 establishes an immunosuppressive microenvironment during the early stages of breast carcinogenesis to promote tumor growth and metastasis. Cancer Res. 2016;76:1416-1428.

21.

Schreiber

Old

Smyth

. Cancer immunoediting: integrating immunity’s roles in cancer suppression and promotion. Science. 2011;331:1565-1570.

22.

Koebel

Vermi

Swann

et al . Adaptive immunity maintains occult cancer in an equilibrium state. Nature. 2007;450:903-907.

23.

Quintana

Shackleton

Foster

et al . Phenotypic heterogeneity among tumorigenic melanoma cells from patients that is reversible and not hierarchically organized. Cancer Cell. 2010;18:510-523.

24.

Bose

Panda

Mukherjee

. Curcumin and tumor immune-editing: resurrecting the immune system. Cell Div. 2015;10:6.

25.

Ranjan

Johnston

Elliott

Bondada

Nagabhushan

. Curcumin blocks cyclosporine A–resistant CD28 costimulatory pathway of human T-cell proliferation. J Surg Res. 1998;77:174-178.

26.

Jagetia

Aggarwal

. “Spicing up” of the immune system by curcumin. J Clin Immunol. 2007;27:19-35.

27.

Pal

Bhattacharyya

Choudhuri

Datta

Das

. Amelioration of immune cell number depletion and potentiation of depressed detoxification system of tumor-bearing mice by curcumin. Cancer Detect Prev. 2005;29:470-478.

28.

Bhattacharyya

Md Sakib Hossain

Mohanty

et al . Curcumin reverses T cell-mediated adaptive immune dysfunctions in tumor-bearing hosts. Cell Mol Immunol. 2010;7:306-315.

29.

Sahu

Agarwal

. Structure activity relationship, cytotoxicity and evaluation of antioxidant activity of curcumin derivatives. Bioorg Med Chem Lett. 2016;26:1342-1347.

30.

Anuradha

Bai

Sailaja

Sudhakar

Priyanka

Deepika

. Evaluation of anti-inflammatory effects of curcumin gel as an adjunct to scaling and root planing: a clinical study. J Int Oral Health. 2015;7:90-93.

31.

Kumaravel

Sankar

Latha

Benson

Rukkumani

. Antiproliferative effects of an analog of curcumin in Hep-2 cells: a comparative study with curcumin. Nat Prod Commun. 2013;8:183-186.

32.

Sorice

Guerriero

Capone

Colonna

Castello

Costantini

. Ascorbic acid: its role in immune system and chronic inflammation diseases. Mini Rev Med Chem. 2014;14:444-452.

33.

Umansky

Sevko

. Overcoming immunosuppression in the melanoma microenvironment induced by chronic inflammation. Cancer Immunol Immunother. 2012;61:275-282.

34.

Lee-Chang

Bodogai

Martin-Montalvo

et al . Inhibition of breast cancer metastasis by resveratrol-mediated inactivation of tumor-evoked regulatory B cells. J Immunol. 2013;191:4141-4151.

35.

Yang

Paik

Cho

et al . Resveratrol induces the suppression of tumor-derived CD4+ CD25+ regulatory T cells. Int Immunopharmacol. 2008;8:542-547.

36.

Wang

Chan

et al . Reduction of splenic immunosuppressive cells and enhancement of anti-tumor immunity by synergy of fish oil and selenium yeast. PLoS One. 2013;8:e52912.

37.

Ullrich

. Mechanisms underlying UV-induced immune suppression. Mutat Res. 2005;571:185-205.

38.

Finlay-Jones

Hart

. Ultraviolet irradiation, systemic immunosuppression and skin cancer: role of urocanic acid. Australas J Dermatol. 1997;38(suppl 1):S7-S12.

39.

Schoof

Iles

Bishop

et al . Genomel Consortium. Pathway-based analysis of a melanoma genome-wide association study: analysis of genes related to tumour-immunosuppression. PLoS One. 2011;6:e29451.

40.

Gustafson

Lin

New

et al . Systemic immune suppression in glioblastoma: the interplay between CD14+HLA-DRlo/neg monocytes, tumor factors, and dexamethasone. Neuro Oncol. 2010;12:631-644.

41.

Youn

Nagaraj

Collazo

Gabrilovich

. Subsets of myeloid-derived suppressor cells in tumor-bearing mice. J Immunol. 2008;181:5791-5802.

42.

Nagaraj

Collazo

Corzo

et al . Regulatory myeloid suppressor cells in health and disease. Cancer Res. 2009;69:7503-7506.

43.

Nagaraj

Gabrilovich

. Myeloid-derived suppressor cells in human cancer. Cancer J. 2010;16:348-353.

44.

Gabrilovich

Velders

Sotomayor

Kast

. Mechanism of immune dysfunction in cancer mediated by immature Gr-1+ myeloid cells. J Immunol. 2001;166:5398-5406.

45.

Schlecker

Stojanovic

Eisen

et al . Tumor-infiltrating monocytic myeloid-derived suppressor cells mediate CCR5-dependent recruitment of regulatory T cells favoring tumor growth. J Immunol. 2012;189:5602-5611.

46.

Steitz

Brück

Lenz

Knop

Tüting

. Depletion of CD25⁺ CD4⁺ T cells and treatment with tyrosinase-related protein 2-transduced dendritic cells enhance the interferon α-induced, CD8⁺ T-cell-dependent immune defense of B16 melanoma. Cancer Res. 2001;61:8643-8646.

47.

Wang

Lau

Zhu

Korman

Weber

. PD1 blockade reverses the suppression of melanoma antigen-specific CTL by CD4+ CD25(Hi) regulatory T cells. Int Immunol. 2009;21:1065-1077.

48.

van Elsas

Sutmuller

Hurwitz

et al . Elucidating the autoimmune and antitumor effector mechanisms of a treatment based on cytotoxic T lymphocyte antigen-4 blockade in combination with a B16 melanoma vaccine: comparison of prophylaxis and therapy. J Exp Med. 2001;194:481-489.

49.

Weber

. Immune checkpoint proteins: a new therapeutic paradigm for cancer–preclinical background: CTLA-4 and PD-1 blockade. Semin Oncol. 2012;37:430-439.

50.

Curran

Montalvo

Yagita

Allison

. PD-1 and CTLA-4 combination blockade expands infiltrating T cells and reduces regulatory T and myeloid cells within B16 melanoma tumors. Proc Natl Acad Sci U S A. 2012;107:4275-4280.

51.

Flammiger

Weisbach

Huland

et al . High tissue density of FOXP3+ T cells is associated with clinical outcome in prostate cancer. Eur J Cancer. 2013;49:1273-1279.

52.

Sun

et al . A study of circulating anti-CD25 antibodies in non-small cell lung cancer. Clin Transl Oncol. 2013;15:633-637.

53.

Zhou

Ding

Pan

Zhu

Zheng

. Increased intratumoral regulatory T cells are related to intratumoral macrophages and poor prognosis in hepatocellular carcinoma patients. Int J Cancer. 2009;125:1640-1648.

54.

Curiel

. Regulatory T cells and treatment of cancer. Curr Opin Immunol. 2008;20:241-246.

55.

Son

Bae

Shin

et al . Combination effect of regulatory T-cell depletion and ionizing radiation in mouse models of lung and colon cancer. Int J Radiat Oncol Biol Phys. 2015;92:390-398.

56.

Rossowska

Pajtasz-Piasecka

Anger

et al . Cyclophosphamide and IL-12-transduced DCs enhance the antitumor activity of tumor antigen-stimulated DCs and reduce Tregs and MDSCs number. J Immunother. 2014;37:427-439.

57.

Maskey

et al . Decreased intratumoral Foxp3 Tregs and increased dendritic cell density by neoadjuvant chemotherapy associated with favorable prognosis in advanced gastric cancer. Int J Clin Exp Pathol. 2014;7:4685-4694.

58.

de la Lastra

Villegas

. Resveratrol as an antioxidant and pro-oxidant agent: mechanisms and clinical implications. Biochem Soc Trans. 2007;35(pt 5):1156-1160.

59.

Zhang

Yao

Konger

et al . UVB radiation-mediated inhibition of contact hypersensitivity reactions is dependent on the platelet-activating factor system. J Invest Dermatol. 2008;128:1780-1787.

60.

Konger

Marathe

Yao

Zhang

Travers

. Oxidized glycerophosphocholines as biologically active mediators for ultraviolet radiation-mediated effects. Prostaglandins Other Lipid Mediat. 2008;87:1-8.

61.

Yao

Wolverton

Zhang

et al . Ultraviolet B radiation generated platelet-activating factor receptor agonist formation involves EGF-R-mediated reactive oxygen species. J Immunol. 2009;182:2842-2848.

62.

Sahu

Petrache

Van Demark

et al . Cigarette smoke exposure inhibits contact hypersensitivity via the generation of platelet activating factor agonists. J Immunol. 2013;190:2447-2454.

63.

Lehr

Weyrich

Saetzler

et al . Vitamin C blocks inflammatory platelet-activating factor mimetics created by cigarette smoking. J Clin Invest. 1997;99:2358-2364.

64.

Ullrich

. Mechanisms underlying UV-induced immune suppression. Mutat Res. 2005;571:185-205.

65.

Sahu

Yao

Konger

Travers

. Platelet-activating factor does not mediate UVB-induced local immune suppression. Photochem Photobiol. 2012;88:490-493.

66.

Braquet

Touqui

Shen

Vargaftig

. Perspectives in platelet-activating factor research. Pharmacol Rev. 1987;39:97-145.

67.

Stafforini

McIntyre

Zimmerman

Prescott

. Platelet-activating factor, a pleiotrophic mediator of physiological and pathological processes. Crit Rev Clin Lab Sci. 2003;40:643-672.

68.

Travers

Huff

Rola-Pleszczynski

Gelfand

Morelli

Murphy

. Identification of functional platelet-activating factor receptors on human keratinocytes. J Invest Dermatol. 1995;105:816-823.

69.

Sahu

Turner

DaSilva

et al . The environmental stressor ultraviolet B radiation inhibits murine antitumor immunity through its ability to generate platelet-activating factor agonists. Carcinogenesis. 2012;33:1360-1367.

70.

Sahu

Ocana

Harrison

et al . Chemotherapeutic agents subvert tumor immunity by generating agonists of platelet-activating factor. Cancer Res. 2014;74:7069-7078.

71.

Sahu

Harrison

Weyerbacher

et al . Radiation therapy generates platelet-activating factor agonists. Oncotarget. 2016;7:20788-20800.

72.

Glebova

Veiko

Kostyuk

Izhevskaya

Baranova

. Oxidized extracellular DNA as a stress signal that may modify response to anticancer therapy. Cancer Lett. 2015;356:22-33.

73.

Wang

. Cancer cell killing via ROS: to increase or decrease that is the question. Cancer Biol Ther. 2008;7:1875-1884.

74.

Vikram

Coleman

Deye

. Current status and future potential of advanced technologies in radiation oncology. Part 1. Challenges and resources. Oncology (Williston Park). 2009;23:279-283.

75.

Shaked

. Balancing efficacy of and host immune responses to cancer therapy: the yin and yang effects. Nat Rev Clin Oncol. 2016;13:611-626. doi:10.1038/nrclinonc.2016.57.

76.

Khan

Karmokar

Howells

et al . Targeting cancer stem-like cells using dietary-derived agents—where are we now? Mol Nutr Food Res. 2016;60:1295-1309.

77.

Mut-Salud

Álvarez

Garrido

Carrasco

Aránega

Rodríguez-Serrano

. Antioxidant intake and antitumor therapy: toward nutritional recommendations for optimal results. Oxid Med Cell Longev. 2016;2016:6719534.

78.

Raffoul

Sarkar

Hillman

. Radiosensitization of prostate cancer by soy isoflavones. Curr Cancer Drug Targets. 2007;7:759-765.

79.

Raffoul

Banerjee

Singh-Gupta

et al . Down-regulation of apurinic/apyrimidinic endonuclease 1/redox factor-1 expression by soy isoflavones enhances prostate cancer radiotherapy in vitro and in vivo. Cancer Res. 2007;67:2141-2149.

80.

Raffoul

Banerjee

Che

et al . Soy isoflavones enhance radiotherapy in a metastatic prostate cancer model. Int J Cancer. 2007;120:2491-2498.

81.

Ahmad

Forman

Sarkar

et al . Soy isoflavones in conjunction with radiation therapy in patients with prostate cancer. Nutr Cancer. 2010;62:996-1000.

82.

Singh-Gupta

Joiner

Runyan

et al . Soy isoflavones augment radiation effect by inhibiting APE1/Ref-1 DNA repair activity in non–small cell lung cancer. J Thorac Oncol. 2010;6:688-698.

83.

Pruitt

Sasi

Freeman

Sekhar

. Radiosensitization of cancer cells by hydroxychalcones. Bioorg Med Chem Lett. 2010;20:5997-6000.

84.

Tak

Lee

Park

. Resveratrol and piperine enhance radiosensitivity of tumor cells. BMB Rep. 2012;45:242-246.

85.

Song

Hasegawa

Kwon

Lyons

Levitt

. Increase in tumor oxygenation and radiosensitivity caused by pentoxifylline. Radiat Res. 1992;130:205-210.

86.

Kim

Khil

Ryu

Kim

. Enhancement of radiation response on human carcinoma cells in culture by pentoxifylline. Int J Radiat Oncol Biol Phys. 1992;25:61-65.

87.

Horvath

Marton

Halmosi

et al . In vitro antioxidant properties of pentoxifylline, piracetam, and vinpocetine. Clin Neuropharmacol. 2002;25:37-42.

88.

Zhang

Sharma

Agarwal

Falcone

. Effect of pentoxifylline in reducing oxidative stress-induced embryotoxicity. J Assist Reprod Genet. 2005;22:415-417.

89.

Tong

Chuang

Zuo

. Reactive oxygen species in redox cancer therapy. Cancer Lett. 2015;367:18-25.

90.

Glasauer

Chandel

. Targeting antioxidants for cancer therapy. Biochem Pharmacol. 2014;92:90-101.

91.

Watson

. Oxidants, antioxidants and the current incurability of metastatic cancers. Open Biol. 2013;3:120144.

92.

Block

Koch

Mead

Tothy

Newman

Gyllenhaal

. Impact of antioxidant supplementation on chemotherapeutic efficacy: a systematic review of the evidence from randomized controlled trials. Cancer Treat Rev. 2007;33:407-418.

93.

Block

Koch

Mead

Tothy

Newman

Gyllenhaal

. Impact of antioxidant supplementation on chemotherapeutic toxicity: a systematic review of the evidence from randomized controlled trials. Int J Cancer. 2008;123:1227-1239.

94.

Yasueda

Urushima

Ito

. Efficacy and interaction of antioxidant supplements as adjuvant therapy in cancer treatment: a systematic review. Integr Cancer Ther. 2016;15:17-39.

Potential Contributions of Antioxidants to Cancer Therapy: Immunomodulation and Radiosensitization

Abstract

Keywords

Introduction

Antioxidants and Immunity

Antioxidants in Cancer Therapy

Conclusion

Footnotes

Acknowledgements

Declaration of Conflicting Interests

Funding

References