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Review

Nutrients Lowering Obesity-Linked Chemokines Blamable for Metastasis

by
Gabriela Ion
1,
Marinela Bostan
1,2,*,
Wanda Elaine Hardman
3,
Margaret Putt McFarland
3,
Coralia Bleotu
4,5,6,
Nicoleta Radu
7,8,
Carmen Cristina Diaconu
4,
Mirela Mihaila
1,9,*,
Mihai Dan Caramihai
10 and
Camelia Mia Hotnog
1,11
1
Center of Immunology, Stefan S. Nicolau Institute of Virology, Romanian Academy, 030304 Bucharest, Romania
2
Department of Immunology, ‘Victor Babes’ National Institute of Pathology, 050096 Bucharest, Romania
3
Department of Biomedical Sciences, Joan C. Edwards School of Medicine, Marshall University, Huntington, WV 25701, USA
4
Department of Cellular and Molecular Pathology, Stefan S. Nicolau Institute of Virology, Romanian Academy, 030304 Bucharest, Romania
5
Research Institute of the University of Bucharest (ICUB), University of Bucharest, 060023 Bucharest, Romania
6
The Academy of Romanian Scientist, 050711 Bucharest, Romania
7
Faculty of Biotechnology, University of Agronomic Sciences and Veterinary Medicine of Bucharest, 011464 Bucharest, Romania
8
Biotechnology Department, National Institute for Chemistry and Petrochemistry R&D of Bucharest, 060021 Bucharest, Romania
9
Faculty of Pharmacy, Titu Maiorescu University, 040314 Bucharest, Romania
10
Faculty of Automatic Control and Computer Science, National University of Science and Technology Politehnica Bucharest, 060042 Bucharest, Romania
11
Department of Biochemistry and Biophysics, Faculty of Midwives and Nursing, University of Medicine and Pharmacy “Carol Davila” Bucharest, 050474 Bucharest, Romania
 
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Int. J. Mol. Sci. 2025, 26(5), 2275; https://doi.org/10.3390/ijms26052275
Submission received: 28 January 2025 / Revised: 25 February 2025 / Accepted: 27 February 2025 / Published: 4 March 2025
(This article belongs to the Special Issue Natural Products in Cancer Prevention and Treatment)
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Abstract

:
Food intake is an essential contributor to both health and disease. Nutrients contribute to a beneficial metabolic equilibrium at the cellular level, preventing or delaying disease onset. Dietary intake contributes to obesity, and obesity supports further cancer and metastasis. Metastasis, a multifactorial and multistep process, is supported by the systemic inflammation of obesity. Spreading of the cancer cells requires the presence of a plethora of recruiter and regulator molecules. Molecules such as chemokines are provided at high levels by obesity-associated fat depots. Chemokine up-regulation in adipose tissue of obese individuals has been associated with different types of cancers such as breast, prostate, colon, liver, and stomach. Chemokines support all metastasis steps from invasion/migration to intravasation, circulation, extravasation, and ending with colonization. The obesity pool of chemokines supporting these processes includes CCL2, CCL3, CCL4, CCL5, CCL7, CCL8, CCL11, CCL18, CCL19, CCL20, CXCL1, CXCL5, CXCL 8, CXCL10, and CXCL12. Keeping obesity under control can be beneficial in reducing the levels of pro-inflammatory chemokines and the risk of poor cancer outcome. Nutrients can help, support, and boost cancer treatment effects or jeopardize the treatment. Constituents with anti-inflammatory and anti-obesity properties such as polyphenols, organosulfur components, fatty acids, curcumin, and vitamin E have a proven beneficial effect in lowering obesity and its contribution to metastasis.

1. Introduction

Obesity is a well-recognized risk factor for cancer development. The Centers for Disease Control and Prevention (CDC) listed 13 types of cancer associated with obesity [1]. Besides the growing evidence showing the positive impact of obesity metabolic disturbance on tumor development [2], emerging data support the chronic inflammation induced by obesity as an add-on to the negative effect of obesity on human health [3]. This review summarizes and synthesizes chemokines associated with obesity-related inflammation, cancer, and metastasis and their modulation by nutrients able to reduce the detrimental effect of excess adiposity.
Adipose tissue cells excrete soluble molecules such as cytokines, chemokines, adipokines, growth factors, and proteases that act on the neighboring cells to maintain the body’s physiological equilibrium. An imbalance in the signaling network can lead to and sustain inflammation. Thus, obesity sustaining inflammation is an important player in tumor development.
Epidemiological studies support the contribution of obesity to the increased rate of mortality in different cancers (colon, breast, esophagus, pancreas, kidney, and liver) [4]. Under physiological conditions, the role of inflammation is to restore homeostasis. However, an excessive inflammatory response has harmful effects. As a consequence, studies are showing that obesity can be responsible for kinase activation in the liver tissue, such as c-jun N-terminal kinase (JNK), which can be in charge of a high cytokine production [5]. High levels of circulating pro-inflammatory cytokines are associated not only with obesity per se but also with different associated diseases, including cancer [6]. Besides cytokines, obesity systemic inflammation provides a pool of chemokines favoring and supporting metastasis. Inflammation, as a deep-rooted path of obesity’s contribution to cancer progression [7,8], follows chemokines and chemokine receptor activation [9].
Chemokines produced by adipose tissue with a role in metastasis are chemokine (C-C motif) ligand (CCL) CCL2, CCL3, CCL4, CCL5, CCL7, CCL8, CCL11, CCL18, CCL19, CCL20, C-X-C motif chemokine ligand (CXCL) CXCL1, CXCL5, CXCL 8, CXCL10, CXCL12, and their receptors C-C chemokine receptor type (CCR) CCR1, CCR2, CCR3, and CCR5. Among the chemokines involved in all steps of the metastatic process (invasion/migration, intravasation, circulation, extravasation, and colonization) a very well established and depicted axis is CCL2/CCR2 [10] (Table 1).
CCL3 is another well-described chemokine involved in all metastasis steps (Table 1) by making pairs either with CCR5 [25] or CCR1 [26]. CCL4 involvement in cancer development has a long history. In spite of the fact that its contribution to cancer development was first mentioned in 1964 [27,28], like all other chemokines, the data linking CCL4 and metastasis only emerged in the last 2–3 decades.
In addition to excess food consumption, the quality of the food can make a difference between health and disease. Fruits, vegetables, and cooked food can improve obesity’s negative impact and decrease the inflammation interconnected with it. Organosulfur components, healthy fats, vitamin E, and polyphenols (curcumin, flavonoids, resveratrol, and stilbenes) have beneficial effects by reducing obesity, inflammation, and associated diseases, including the spread of cancer cells (Table 2). This effect is supported by a tremendous amount of literature data. Thus, organosulfur components lower adipogenesis, adipose tissue inflammation, cancer development, and CCL2 and CXCL12 release [29,30,31,32,33,34,35,36,37,38].
Vitamin E lowers CCL2 [39,40]. Curcumin is well recognized as decreasing adipogenesis, adipose tissue inflammation, and cytokine and chemokine (CCL2, CCL5, CCL7, CXCL1, CXCL2, CXCL10, CXCL12, and CXCL12/CXCR4) release [41,42,43,44,45,46,47,48,49,50,51,52,53,54,55,56,57,59,60,93,94]. Similarly, flavonoids (epicatechin, epigallocatechin-3-gallate, naringenin, genistein, quercetin, flavonoid fish-oil supplement, anthocyanins, baicalin, cirsimarin, and apigenin) lower adipogenesis, adipose tissue inflammation, and chemokine (CCL2, CCL5, CCL8, CCL19, CXCL8, CXCL12, and CXCR4) release [61,62,63,64,65,66,67,68,69,70,71,72,73,74,77,78,79].
Omega-3 polyunsaturated fatty acids (n-3 FAs) are important players in both obesity and cancer prevention. A well-balanced n-3–n-6 ratio is essential for good human health [95]. N-3 FAs have well-known anti-inflammatory properties [96]. A high n-3 diet decreases prostate [97], mammary [98,99,100], lung [101], and colorectal [102,103] carcinogenesis. N-3 FAs are present in foods such as fish (salmon, mackerel), nuts (walnuts), seeds (flaxseed) and their oils, and other plant oils (canola, soybean). Among n-3 FAs, α-linolenic acid (ALA), eicosapentaenoic acid (EPA), and docosahexaenoic acid (DHA) are the most used for human health. Since ALA is an essential fatty acid and cannot be synthetized by the body, it must be provided by food. The human body can synthetize EPA and DHA from their precursor, ALA, at a low rate. Therefore, a healthy status is supported by foods and supplements rich in ALA, EPA, and DHA.
Since obesity has become an epidemic, adipose tissue is now under extensive study, and new insights are being revealed regarding the complexity of its functionality. When healthy adipose tissue has a good balance of secreted products (e.g., chemokines), it can make a difference in the outcome of different diseases including cancer. Mechanisms involved in inflammatory processes induced by obesity that lead to tumor development need a more thorough understanding. In this regard, two points are pertinent: (i) how we can lower the inflammation induced by obesity in order to prevent or slow tumor progression and/or resistance to the classic chemotherapeutics; and (ii) how food intake can reduce the excess of adipose tissue, inflammation, and obesity-induced chemokine levels in the hope of lowering the risk of obesity-favored tumors.

2. Adipose Tissue in Obesity

Body fat is a widely spread organ with multiple functions (energy storage, thermogenesis, secretion of hormones, adipokines, cytokines, and chemokines). A simple classification of body fat is by morphology (white, brown, and beige) [104]. The most common classification is by localization (e.g., upper body, lower body, subcutaneous, visceral, and ectopic) [104,105,106,107]. Accumulation and enlargement of normally distributed adipose tissue and the ectopic localization of the fat depots are characteristic for obesity. The ectopic localization of adipose tissue affects tissues and organs such as the liver, muscles, vasculature, epicardium, and kidneys. The main cell type presented in adipose tissue is adipocytes. In addition, several other cell types are part of the tissue: preadipocytes, stromal/stem cells, fibroblasts, macrophages, and endothelial cells. Chronic inflammation benefits from the support of a widely distributed organ composed of different cell types that secrete a plethora of pro-inflammatory molecules.
Obesity-associated body fat influences not only the release of pro-inflammatory molecules but also directly interacts with tumor cells influencing their behavior. As a response to the changes in the microenvironment caused by obesity, tumor cells adjust the expression of chemokine receptors (such as CXCR4, CXCR7, and CCR2). This adjustment allows them to migrate to tissues (such as distant organs) where chemokines are elevated. Thus, tumor cells are intrinsically able to support both adipose tissue and tumor microenvironment inflammation. This leads to the recruitment of inflammatory cells generating a positive feedback loop that further support tumor progression and metastasis [108].

3. Chemokine Contribution to Obesity Chronic Inflammation and Metastasis

Chemokines (chemotactic cytokines) initially established as leukocyte recruiters [109] play a key role in tumor cell trafficking and metastasis [110]. In this context, a particular interest in the obesity systemic inflammation might focus on perivascular adipose tissue. The recent focus has mainly been on studies showing the role of perivascular adipose tissue cytokines/chemokines in the health of vasculature. A study published by Chatterjee TK et al. in 2009 supports the pro-inflammatory action of a high-fat diet on perivascular adipocytes. The authors showed that CCL2 (alias monocyte chemoattractant protein 1 (MCP-1)) is increased in perivascular adipocytes due to diet. Moreover, the amount of CCL2 is depot specific [11]. CCL2 as a pro-inflammatory molecule is an essential recruiter of macrophages to both adipose tissue and tumor microenvironment. Another study showed that, besides CCL2, the perivascular adipose tissue secretes CXCL8 (alias interleukin 8, IL-8) [12]. CXCL8 has a well-defined role in metastasis by facilitating tumor cell migration, increased vascular permeability, and new blood vessel formation [111]. Thus, high CXCL8 levels are associated with the presence of different cancers (oesophageal, gastric, pancreatic, breast, and kidney cancer) [112,113,114,115,116], metastasis, and drug resistance [116]. In order to support both metastasis and drug resistance, CXCL8 activates the serine/threonine kinase Akt pathway (protein kinase B) via CXCR2 [116].
The expression of CXCL8 alongside the chemokines CCL2, CCL5, CCL7, CCL19, CXCL1, CXCL5, and CXCL10 was found to be up-regulated in the subcutaneous adipose tissue of obese subjects [14] (Table 1). Moreover, the gene expression of CCL2, CCL3, CCL5, CCL7, CCL8, CCL11, and their receptors (CCR1, CCR2, CCR3, and CCR5) was found to be higher in both the subcutaneous and visceral adipose tissue of obese individuals [9].
CCL3 (alias macrophage inflammatory proteins-1α (MIP-1α)) and CCL4 (MIP-1β), secreted by macrophages and T cells and also by adipocytes [9,15,17], contribute to chronic inflammation by recruiting monocytes, T cells, and neutrophils to the inflammatory sites. In the tumor microenvironment, CCL3 and CCL4 help to establish a favorable niche for cancer cell dissemination.
CCL5 (alias regulated on activation normal T-cell expressed and secreted (RANTES)) associated with obesity is an important recruiter of monocytic myeloid-derived suppressor cells (MDSCs). Under obese conditions, CCL5/CCR5 signaling contributes to adipose tissue inflammation by enabling MDSC differentiation to tissue macrophages [117]. Moreover, CCL5 facilitates the migration and invasion of tumor cells through its interaction with CCR5 receptors present on these cells. Elevated concentrations of CCL5 within the tumor microenvironment contribute to immune evasion by recruiting immune cells that promote the survival and migration of cancer cells, thereby heightening the risk of metastasis [118,119,120,121].
CXCL1 (alias growth-regulated protein alpha Gro alpha, Gro1, melanoma growth-stimulating activity, alpha (MGSA-α)) released by adipocytes and preadipocytes [13] is associated with invasive breast cancer and metastasis. The process is supported by CXCL1 recruiting myeloid cells to tumors [122] through the nuclear factor kappa-light-chain-enhancer of activated B cells (NF-κB)/SRY (sex-determining region Y)-Box Transcription Factor 4 (SOX4) activation [123]. CXCL1 is a strategic player in bladder cancer, supporting repeated intravesical recurrence and disease progression [124].
CXCL12 (alias stromal cell-derived factor 1, SDF-1) is defined as a macrophage chemotactic factor released by adipocytes, stromal cells, and various cancer cells. It is a potent attractant for different cell types (immune, endothelial, and tumor cells), expressing its receptor, CXCR4. And its increased levels are observed in adipose tissue and tumors associated with obesity [23]. CXCL12 and its receptor CXCR4 are associated with the development of both different organ tumors and metastasis. Therefore, CXCL12 not only helps cancer cells find the nest, but also improves tumor-associated inflammation, facilitating the establishment of a metastatic niche [125,126,127].
Adipose tissue contributes not only to a local increase in chemokines, it can also contribute to a rise in serum chemokine levels. In this respect, high serum levels of chemokines have been found in different types of cancers. CCL2 is high in both serum and tumor tissue from patients with non-small-cell lung cancer [128]. Serum levels of CCL2 are also high in patients with ovarian cancer [129], nasopharyngeal carcinoma [130], and pancreatic cancer compared to healthy subjects [131]. CCL3 has been found to be high in the plasma of patients with non-small-cell lung carcinoma [132]. CCL4, CCL5, and CXCL5 are high in the serum of patients with hepatocellular carcinoma [133]. Human epidermal growth factor receptor 2 (Her2) (alias receptor tyrosine-protein kinase erbB-2 (ERBB2) or cluster of differentiation 340 (CD340))-positive breast cancer patients have high serum levels of CCL5 associated with poor prognosis [134]. CXCL8 has been found to be higher in the serum of patients with oesophageal, gastric, pancreatic, breast, or kidney cancer [112,113,114,115,116]. A high serum expression of CXCL8 is correlated with poor outcome of disease [116]. High plasma CXCL10 levels among other factors are associated with a poor outcome in metastatic renal cell carcinoma patients treated with antiangiogenic therapy [135]. CCL11 is elevated in the serum of patients with esophageal squamous cell carcinoma [136] or gastric cancer [137]. High serum CCL18 is associated with a poor prognosis in patients with different carcinoma such as laryngeal squamous cell [138], squamous cell carcinoma of the head and neck [139], breast cancer [140], non-small-cell lung carcinoma [141], and pancreatic ductal carcinoma [142].

4. Management of Obesity and Associated Tumor Processes

Adipose tissue in obesity provides a microenvironment characterized by endo/para and autocrine changes that may promote the initiation and/or progression of tumor processes. In this context, adipose tissue metabolic processes drive the long-term pro-inflammatory status. Among the processes supporting chronic inflammation is hypoxia. The partial pressure of oxygen in the adipose tissue of obese individuals is lower than in lean individuals [143]. Hypoxia occurring in the fat tissue of obese individuals is responsible for the increased expression of transcription factors: NF-κB and hypoxia-inducible factor-1α (HIF-1α). Both chronic and cyclic hypoxia maintain a high pro-inflammatory status [144]. Some studies emphasize that cyclic hypoxia might induce a higher expression of NF-κB and a greater pro-inflammatory response than chronic hypoxia [145]. Such a response triggers the release of CCL2, CXCL1, and CXCL8 [145] (Figure 1). CCL2 released by omental adipocytes facilitates the migration and omental metastasis of ovarian cancer through the activation of PI3K/AKT/mTOR followed by an increase in HIF-1α and vascular endothelial growth factor A (VEGF-A) [146]. The release of HIF-1α influences the synthesis of a large variety of proteins, such as collagen, metalloproteinase, metalloproteinases inhibitors, cytokines (interleukin 6 (IL-6), TNF), chemokines (CCL2, CXCL8, and CXCL12), and chemokine receptors (CXCR4) contributing to cell proliferation and metastasis [127,147,148,149,150,151]. High HIF-1α and CXCL8 are associated with the development of hepatocellular carcinoma and metastasis [151]. HIF also induces high CXCL12/CXCR4 responsible for breast cancer progression and metastasis [127]. CXCL12 is defined as a hypoxia-regulated gene strongly linked to carcinogenesis being responsible for drug resistance and metastasis [144].
Another process contributing to obesity systemic inflammation supporting metastasis is aerobic glycolysis. This process generates nutrients (lactate and pyruvate) required by tumor cells to complete mitochondrial oxidative metabolism. The process is known as the inverted Warburg effect, in which the mitochondria of tumor cells, via the process of beta-oxidation, use free fatty acids generated through lipolysis by stromal adipocytes [152,153]. Aerobic glycolysis is supported by the infiltration of macrophages into the white adipose tissue. Once activated, so-called M1 macrophages are pro-inflammatory and induce aerobic glycolysis [154]. Among the stimuli that activate M1 macrophages, there are CCL8, 19, 20, and CXCL10 [154]. These stimuli are released either by preadipocytes or adipocytes [13]. Glycolysis also requires the presence of hypoxia-activated glycolytic genes (aldolase, fructose-bisphosphate C (ALDOC), enolase 2 (ENO2), hexokinase (HK1, 2), and phosphofructokinase, platelet (PFKP)) [143,144].
NF-κB activation is present in animals fed with a high-fat diet, as well as in obese individuals [155,156,157]. It is responsible for maintaining an inflammatory environment by triggering chemokines CCL 3, 4, 5, 19, 20 and CXCL 1, 5, 8, 10 [158,159] (Figure 1), the survival of adipose tissue macrophages [160], and a positive feedback loop CXCL 1, 8 -NF-κB [159]. Moreover, NF-κB supports white adipose tissue (WAT) inflammation throughout cachexia. NF-κBp65 and its target CCL2 were found to be higher in adipose tissue of cancer cachectic patients compared to non-cachectic cancer or cancer-free patients [161].
Another contributor to tumor development and metastasis delivered by adipose tissue is adipose stromal/stem cells (ASCs). ASCs, largely present in WAT, have an obesity-associated high proliferative capability and can migrate from WAT to the tumor site, contributing to tumor progression [162,163,164]. The trafficking of ASCs is supported by chemokines that have a role in invasion/migration and colonization such as CXCL1 and CXCL8 [165,166]. There are studies showing that ASCs are able to differentiate into carcinoma-associated fibroblasts supporting tumor invasion [167]. The ASC tumor-promoting effect is documented for different cancers: breast [168], ovarian [22], and prostate [24]. The metastasis of breast cancer xenografts is induced by human ASCs [169]. Prostate cancer chemoresistance is associated with ASCs releasing CXCL12 [24]. Also, ASCs have a high expression of CCR5 and release CXCL-10 in ovarian cancer [22].
In a study conducted by Arendt LM, a so-called adipose stromal vascular fraction, comprising adipocytes (stem cells, pre- and mature adipocytes) and other stromal cells, recruits macrophages through CCL2/CXCL12 signaling [170]. The recruitment of macrophages, as was mentioned above, is a pillar in sustained inflammation and tumor progression supported by obesity.
In addition to ASCs, another set of interactions involves cancer-associated adipocytes (CAAs) as an interface between adipocytes and tumor cells. Compared to adipocytes, CAAs have a smaller size and lipid droplets, and a different pattern of differentiation markers [171]. To transform into CAAs, adipocytes need to go through lipolysis, which is induced by tumor cells [171]. CAAs are better equipped to support tumor invasion and metastasis by releasing CCL2, CCL5, CXCL8, IL-6, leptin, adiponectin, and VEGF [171,172]. CAAs are defined as high producers of CXCL8 [173], CCL2, and IL-6 [174] associated with breast cancer development. Also, the release of CCL2, CXCL1, and Il-6 by CAAs is associated with bladder cancer cell migration [175].

5. Adipose Tissue, Chemokines, and Chemo-Resistance

Chemoresistance benefits from the support of adipose tissue environment. Therefore, adipocytes are responsible for the resistance of acute lymphoblastic leukemia cells to daunorubicin and vincristine. One possible mechanism of daunorubicin resistance is the oxidative stress protection provided by adipocytes to leukemia cells [176]. Resistance to vincristine might be induced by adipocytes concealing the drug and increasing the expression of survival signaling [177]. Literature covering the support of adipose tissue in breast cancer development is very well documented. Studies are showing that adipocytes and adipose-derived stem cells are responsible for breast cancer cell resistance to tamoxifen and paclitaxel, respectively [178,179].
CCL2 has a proven role in drug resistance by activating the PI3K-Akt-mTOR signaling pathway in different cancers: breast [180], gastric [181], glioma [182], lung [183], and ovarian [184]. In order to exert its role in drug resistance, CCL2 is a part of different feedback loops such asNF-κB [181,184]; extracellular signal-regulated kinase (ERK)-ETS domain transcription factor 1 (ELK1)-early Growth Response 1 (EGR1) [185] (Figure 1).
CCL5 signaling through beta-catenin/signal transducers and activators of transcription 3 (STAT3) promotes both metastasis and drug resistance in prostate cancer [119,120]. A 2013 study on prostate cancer patients showed that the CCL5 serum levels were not different among patients groups: (i) negative prostate biopsy, (ii) initial diagnosis of prostate cancer, and (iii) taxane-resistant groups [186]. The study emphasizes the importance of CCR1 in the development of taxane-resistant prostate cancer. In a cell culture setup, the CCR1/CCL5 interaction supports the invasion of taxane-resistant prostate cancer cells through the activation of ERK and Rac signaling pathways [186]. Also, CCL5 signaling is associated with glioblastoma resistance to temozolomide [187]. CCL5 decreases breast cancer cell responsiveness to epirubicin. Moreover, CCL5 enhances breast cancer migration and invasion accompanied by increased vimentin and decreased e-cadherin expression [121]. High CCL5 expression has a role in breast cancer cell resistance to trastuzumab by ERK phosphorylation [134] and tamoxifen by STAT3 activation [188]. Platinum-based therapy-resistant ovarian cancer patients have a higher expression of CCL5 compared to chemo-sensitive patients [189]. High CCL5 expression promotes chemo-resistance through the STAT3 and PI3K/AKT signaling pathways [189]. Additionally, CCL5 supports the aggressiveness of ovarian cancer by attracting regulatory T cells [118]. Up-regulation of CCL5 is also present in bevacizumab-resistant head and neck squamous cell carcinoma [190].
CCL18 is associated with the chemo-resistance of lung cancer cells to cisplatin [191]. CCL20 has a role in crizotinib resistance in non-small-cell lung cancer. This drug resistance is induced by the activation of angiogenesis through Janus kinase 2 (JAK2)/STAT3-CCL20-VEGFA/IL6 [192]. High expression of CCL20 suppresses the response to immunotherapy and is linked to epithelial–mesenchymal transition and the TNF signal pathway in lung adenocarcinoma [193]. Similarly, in pancreatic ductal adenocarcinoma, CCL20 is associated with NF-κB-mediated TNF-related apoptosis-inducing ligand (TRAIL) resistance [194]. In ovarian cancer, it is associated with the resistance to paclitaxel via the Notch1 pathway [195] and the regulation of ABCB1 expression [196]. In chemo-resistant colorectal cancer, CCL20 recruits Tregs to support the process through the forkhead box protein O1 (FOXO1)/CCAAT/enhancer-binding protein beta (CEBPB)/NF-κB pathway [197] (Figure 1).
CXCL1 supports breast, bladder, and colorectal cancer cell survival under chemotherapy. A study published by Acharyya S. et al. in 2012 showed that breast cancer has high expression of CCL20 and CXCL3 as a response to drugs. The response to chemotherapy elicits the TNF-α-CXCL1/2-S100A8/9 paracrine pathway, leading to chemo-resistance and metastasis [122]. In colorectal cancer, a high CXCL1/5 expression is maintained via the CXCR/MMPI/epidermal growth factor (EGF) pathway [198]. Moreover, colon cancer patients under cetuximab therapy have the serum levels of CXCL1/5 correlated with the presence of Ras/Raf mutation [198].
CXCL5 high expression in bladder cancer is associated with mitomycin C resistance via NF-κB activation [199], and in kidney and breast cancer, it is associated with resistance to lysosomotropic drugs (sunitinib, lapatinib, and chloroquine) [200]. In lung cancer, CXCL5 induces resistance to checkpoint inhibitors [201].
CXCL8 is well recognized for its contribution to chemo-resistance and activation of pro-survival pathways. CXCL8 is associated with resistance to multiple chemotherapeutic approaches including platinum-based drugs in ovarian cancer [202], epidermal growth factor receptor (EGFR) inhibitors in lung cancer [203], cisplatin and doxorubicin in hepatocellular carcinoma [204], and gemcitabine in pancreatic cancer [205]. Pancreatic cells respond to gemcitabine treatment by a boosted expression of CXCL8 following ROS generation and NF-κB activation [206]. Similarly, melanoma cells respond to dacarbazine by a high level of CXCL8 in a NF-κB-dependent manner [207]. High expression of CXCL8 in colorectal cancer is part of the Myc/CXCL8/tissue inhibitor of metalloproteinase 1 (TIMP1) oncogenic mark [208]. Thus, it regulates resistance to cetuximab through the activation of the EGFR pathway [209] and doxorubicin by the modulation of multidrug resistance 1 (MDR1) via inhibitor of nuclear factor kappa-B kinase subunit beta 1 (IKK-β/p65) [210]. PI3K, Her2, JAK, and CXCL8 network signaling is responsible for the resistance to PI3K inhibitors [211]. The CXCL8 drug resistance system is supported by recent studies showing connector molecules like Src homology-2 domain-containing protein tyrosine phosphatase-2 (SHP2), which mediates the CXCL8-CXCR1/2 feedback loop through ERK-AKT-NFκB and Src homology-2 domain-containing protein tyrosine phosphatase-2 (GSK3β)-β-catenin signaling [212]. Her-2-positive breast cancer resistance to lapatinib is induced by CXCL8 through the activation of Src/STAT3/ERK1/2-mediated EGFR signaling [213]. CXCL8 exerts its action by triggering multidrug resistance genes like ABCB1 in tumor blood vessels [214], ABCB5 in mesothelioma [215], and ABCB 1 in gastric cancer [216] and increasing the expression of NF-κB-regulated antiapoptotic genes like B-cell lymphoma 2 (Bcl-2) and inhibitor of apoptosis (IAP) families [217].
CXCL10 is associated with breast cancer resistance to tamoxifen [218], pancreatic cancer resistance to gemcitabine [219], renal carcinoma resistance to sunitinib and pazopanib [135], and childhood acute lymphoblastic leukemia resistance to chemotherapy-induced apoptosis [220].
CXCL12 has a well-established role in gastrointestinal cancer resistance to chemotherapy, where it is linked to disease progression, anti-programmed cell death protein 1 (anti-PD-1) [221], and 5-fluorouracil resistance [222]. In pancreatic cancer, it is associated with gemcitabine resistance through the activation of FAK, ERK, AKT, β-catenin, and NF-κB [223] and the induction of special AT-rich sequence-binding protein-1 (SATB-1) [224]. Moreover, it is associated with ovarian cancer resistance to cisplatin via the Wnt/β-catenin pathway [225]. CXCL12 plays a role in the resistance of leukemia cells to tyrosine kinase inhibitors [226]. In colorectal cancer, CXCL12 mediates resistance to 5-fluorouracil by targeting miR-125b [227]. Glioblastoma cell resistance to temozolomide is mediated by CXCL12 by forkhead box protein M1 (FOXM1) up-regulation [228]. High expression of CXCL12 is linked with MDR1 overexpression in chronic myelogenous leukemia [229].

6. Nutrients Disabling the Detrimental Effect of Excess Adiposity

Nutrients can act as a support for body health or as a disease trigger. Components with excellent anti-inflammatory and antioxidant properties can lower obesity-related chemokine levels (Figure 2).

6.1. Vitamin E

CCL2 seems to be an essential target of vitamin E since CCL2 levels greatly decrease in individuals taking vitamin E supplements [39]. Vitamin E family members, such as tocotrienols, improve the adverse effect of TNF-α in adipocytes by lowering NF-κB activation and CCL2 secretion [40]. Besides supplements, good sources of vitamin E are plant-based oils (wheat germ, soybean, and sunflower), nuts (walnuts, peanuts, and almonds), and fruits and vegetables (mango, avocado, asparagus, and red bell pepper) (Table 2).

6.2. Curcumin

Curcumin reduces both adiposity and adipose tissue inflammation in mice [41]. Curcumin and white pepper lower high-fat-induced pro-inflammatory cytokines in subcutaneous adipose tissue [42]. The authors state that the effect is independent of adiposity, immune cell recruitment, and gut microbiota changes. A study performed on rats shows that curcumin protects against weight regain and limits adipose tissue growth [43]. Moreover, a study using a rat model for obesity-inducing multi-organ dysfunctionalities supports curcumin’s anti-obesity and anti-inflammatory effects [44]. The weight of epididymal adipose tissue in rats is reduced by curcuminoid intake in a dose-dependent manner [45]. In humans, overweight subjects taking curcumin showed a weight loss and reduction in body fat [46]. Advanced pancreatic cancer patients treated with curcumin had a greater loss of subcutaneous adipose tissue and muscle compared to untreated patients [47]. Curcumin inhibits the NF-κB pathway in adipocytes, reducing cytokine expression and chronic inflammation [48]. Curcumin blocks CCL2-induced adhesion, invasion, and motility of prostate cancer cells [49]. CCL2 expression in plasma and intestinal tissue in a mouse model of colon cancer is decreased by curcumin [50]. A curcumin-supplemented diet lowers the serum levels of CCL5 in rats [52]. Both CCL5 and CCL2 are down-regulated in mouse bone marrow stromal cells by curcumin [51]. CCL7 serum level and lung inflammation are lowered by curcumin [53].
Curcumin inhibits the up-regulation of CXCL1 and CXCL2 induced by 5-fluorouracil in the colon [54]. In breast and prostate cancer, both chemokines are down-regulated by curcumin via NF-κB signaling [55,56]. Another modulator of curcumin’s impact on CXCL1 and 2 levels in breast cancer is miR181b [93]. Curcumin is associated with reduced CXCL10 expression in hepatic tissue [57] and the brain [58]. Curcumin inhibits CXCL12-induced invasion of human esophageal carcinoma cells via the Rac1-PI3K signaling pathway [59]. New curcumin delivery systems act efficiently to suppress the CXCL12/CXCR4 axis and improve the gemcitabine effect on pancreatic cancer [94]. Curcumin weakens endometrial adenocarcinoma cell migration with the down-regulation of CXCL12 via Slit-2 mediation [60].

6.3. Flavonoids

Among flavonoids, epicatechin, which is largely present in fruits, acts as an anti-inflammatory on fat tissue by lowering NF-κB pro-inflammatory signals and CCL2 [61] and CCL19 [62] tissue chemokines (Table 2). Epigallocatechin-3-gallate (EGCG), highly present in green tea, reduces obesity and white adipose tissue gain in mice [63,64]. In humans, EGCG in the presence of resveratrol decreases adipogenesis, oxidative stress, and inflammation-related gene expression [65]. Besides its anti-inflammatory effect, EGCG is able to prevent the development of a CAA-like phenotypes in ASCs by inhibiting CCL2, CCL5, immunomodulators (HIF-1α, VEGFα), and NF-κB activation. The same study shows that EGCG hinders the chemotactic response of adipose-derived mesenchymal stem/stromal cells to the triple-negative breast cancer secretome [66].
In a model of obese ovariectomized mice, the flavanone naringenin managed to reduce adiposity and adipose tissue inflammation, and delayed the growth of mammary tumors [67]. The isoflavone genistein has well-recognized anti-obesity and anti-cancer properties. Accordingly, genistein down-regulates CXCL12, lowering the migratory and invasive potential of breast and ovarian cancer cells [72]. In an experimental design using human umbilical vascular endothelial cells stimulated with TNF-alpha, genistein was more efficient than daidzein in decreasing the CCL-2 in a dose-dependent manner [69]. In mice, dietary genistein inhibited TNF-alpha-induced CCL-2 and CXCL8 production [70]. Genistein also blocks the proliferation of melanoma cells by reducing CXCL8 levels [71]. On human synovial fibroblasts, genistein has adipogenic and anti-inflammatory effects. So it is able to reduce both endogenous and TNF-alpha-induced CXCL8 [68].
Quercetin alone or in the presence of green tea extract down-regulates the inflammatory response in adipose tissue of high-fat-diet mice [73]. In humans, a mixed flavonoid–fish oil supplement has an anti-inflammatory effect in obese and overweight women [74]. Tart cherry is presented as an important source of flavonoids such as anthocyanins. Obese rats fed with a diet rich in tart cherry showed a decrease in inflammatory markers in visceral (retroperitoneal and perigonadal) fat, which was not accompanied by changes in visceral fat accumulation [75]. A 2021 study emphasized that tart cherry supplements might have an anti-adipogenic effect by acting directly on the adipose tissue and down-regulating the high-fat-diet-induced mRNA expression of cannabinoid CB1 receptor, peroxisomeproliferator-activated receptor gamma (PPARγ), and sterol regulatory element-binding protein 1c (SREBP-1c) adipogenesis-related genes and transient receptor potential vanilloid subtype 1 (TRPV1) and 2 (TRPV2) channels [76]. Baicalin, a flavonoid extracted from Scutellaria baicalensis Georgi, decreases the cell migration induced by chemokines. In order to exert its anti-inflammatory action and limit chemokine activity, baicalin binds to different chemokines (CXCL12, CXCL8, CCL4, and CCL8) [77]. Cirsimarin, a flavonoid obtained from different species such as Cirsium japonicum var. ussuriense, Cirsium rhothophilum, Cirsium rhinoceros, and Microtea debilis, has anti-lipogenic activity and is able to decrease the intra-abdominal fat in mice by lowering the adipose cell diameter [78]. In the same line, apigenin, abundant in fruits and vegetables, is able to reduce the body weight and visceral fat in obese mice [79].

6.4. Organosulfur Components

Another group of food constituents with anti-inflammatory and anti-obesity properties is organosulfur components (Table 2). Vegetables such as garlic, onion, cabbage, cauliflower, and broccoli are excellent sources of organosulfur components. Garlic and onion oils have an anti-obesity effect on rats fed a high-fat diet [29]. Garlic constituents, diallyl disulfide and diallyl trisulfide, have emerged as new therapeutic agents to subdue drug resistance in breast cancer [30]. Diallyl disulfide can suppress the accumulation/activation of macrophages in adipose tissue and inhibit the release of CCL2 from adipocytes lowering the inflammatory status induced by obesity [31]. Diallyl trisulfide prevents adipogenesis in animal models of diet-induced obesity and cultured adipocytes [32,33,34]. Experiments performed on triple-negative breast cancer cells showed that diallyl trisulfide can target CCL2 and other molecules, inducing cell death and inhibiting cell migration [35]. In a pro-inflammatory experimental model, diallyl trisulfide inhibited the activation of CXCL12, showing its anti-chemo-attractive potential [36]. Sulforaphane, another promising compound in lowering obesity and its negative effects [37], is an isothiocyanate present in broccoli, cabbage, cauliflower, and kale [38]. Sulforaphane is able to reduce adipocyte lipid accumulation and lower cytokine production [80].

6.5. Fatty Acids

Fatty acids are key players in adipose tissue development and function. N-3 FAs have a very well-established beneficial effect on human wellbeing (Table 2). A study using keratinocytes and T cells shows that ALA is able to decrease levels of CCL2, CXCL1, CXCL10, and CXCL8 [81]. In an obesity model comprising rodents fed with ALA-rich flaxseed oil for 8 weeks, the CCL2 level was reduced, as well as adipocyte size and T-cell infiltration in adipose tissue [82]. In another study using a hybrid cell line, EPA and DHA lowered the production of CCL-2 and CXCL-8 [83]. Besides preventing high-fat-diet-induced obesity, EPA in mice is also able to reduce adipose tissue inflammation, adipogenesis, and adipocyte size [84]. In a mouse experimental model of prostate cancer, n-3 FAs lowered the infiltration of macrophages and CCL-2 expression [85]. Experiments using adipocytes generated from human subcutaneous adipose biopsies supported the n-3 FAs lowering CCL-2 levels [86]. CCL-2 and other pro-inflammatory molecules such as IL-6, NFkB, and Ptgs2 have a decreased level in mammary glands of mice fed with n-3 FAs. In these mice, mammary glands and abdominal fat have smaller adipocytes [87]. A co-culture experiment using adipocytes and murine splenic CD8+ T cells has shown that the levels of secreted CCL-3 and CCL-4 are reduced in the presence of n-3 FAs [88]. Conversely, a study using 60% calories from fat with low n-3 and high n-6 (n-6–n-3 ratio of 9:1) showed that this high-fat diet is responsible not only for increased body weight, fat mass, and pancreas weight but also for increased mesenteric adipose tissue and pancreas metaplasia [89].
N-3 fats exert their beneficial role acting on multiple levels, generating a network of interactions. In 2012, Philip Calder published a comprehensive review of n-3 FA mechanisms of action [90]. N-3 FAs can reduce obesity by keeping the systemic and tissue-specific lipid homeostasis under control via transcription factors (NFkB, SERBP, and PPAR) [90,91] and the tricarboxylic acid cycle [92]. Moreover, a well-balanced diet can support the psychophysical wellbeing of cancer patients, especially those being treated with chemotherapy. In this regard, n-3 FAs, along with antioxidants and fiber, may have a beneficial impact on cognitive function and reduce the prevalence of depression and anxiety in colorectal cancer patients [230].

7. Conclusions

Obesity is a preventable disease. The treatment approaches should take into consideration that a healthy diet not only promotes weight management but also mitigates the inflammatory processes associated with cancer progression. Dietary changes can significantly improve the overall quality of life for obese cancer patients, reducing treatment-related adverse effects and fostering both physical and mental health. Polyphenols, organosulfur components, and fatty acids are a few categories of active food elements that effectively support and improve human health. Unfortunately, in these times, we are more prone to study real foods than to eat them. So, how can we lower obesity supporting inflammation and metastasis? Besides allopathic, osteopathic, and homeopathic medicine, the new drug combinations and delivery systems, basically what is left to tackle is food intake. There is no magic pill to lower obesity and affect the systemic inflammation associated with it. To maintain a healthy state is a lifelong multi-step process and is beyond the individual (e.g., culinary traditions, life style, race, and ethnicity). Once the disease is present, to undo the damage is an intricate effort. To have a real impact on the prevalence of global obesity and to reduce the obesogenic environment, prevention should address not only the individual (e.g., nutrition and personalized diets, exercising and weight loss medication) but also, and especially, food systems. Food systems are essential to balancing the obesogenic environment with healthy choices. Policy changes should be implemented to lower the sugar content of the foods and to regulate taste enhancers, food colorants, and high-calorie and low-nutrient ultra-processed foods.

8. Future Perspectives

Future applications should address the efficiency of different dietary constituents in treating cancer. This might involve the utilization of vitamin E as a complementary therapy alongside conventional treatments, with the objective of enhancing therapeutic efficacy and minimizing the side effects associated with chemotherapy. Moreover, to maximize curcumin efficiency in cancer treatment, new perspectives are required to improve its bioavailability through innovative formulations or delivery systems. Integration of dietary compounds into established cancer treatment protocols could result in more compressive and holistic approaches, such as the development of flavonoid-rich supplements or foods, thus targeting specific cancers for a more personalized treatment approach [231]. It is essential to note that long-term and large-scale clinical trials are necessary to ascertain the efficiency and safety of these compounds in cancer therapy [232,233,234].

Author Contributions

Conceptualization, G.I.; data curation, M.M., C.M.H., N.R. and M.D.C.; writing—original draft preparation, G.I. and M.B.; writing—review and editing, W.E.H., M.P.M., C.B. and C.C.D.; visualization, M.M. and C.M.H.; supervision, G.I. All authors have read and agreed to the published version of the manuscript.

Funding

This research received no external funding.

Conflicts of Interest

The authors declare no conflicts of interest.

Abbreviations

The following abbreviations are used in this manuscript:
CDCCenters for Disease Control and Prevention
JNKc-jun N-terminal kinase
CCL chemokine (C-C motif) ligand
CXCL C-X-C motif chemokine ligand
CCR C-C chemokine receptor type
n-3 Fasomega-3 polyunsaturated fatty acids
ALAα-linolenic acid
EPAeicosapentaenoic acid
DHAdocosahexaenoic acid
CAAcancer-associated adipocytes
EGCGepigallocatechin-3-gallate
MIPmacrophage Inflammatory Proteins
MCP1 monocyte chemoattractant protein 1
RANTESregulated on activation, normal T-cell expressed and secreted
MDSCs monocytic myeloid-derived suppressor cells
Groα, Gro1growth-regulated protein alpha
MGSA-αmelanoma growth-stimulating activity-alpha
SDF-1 stromal cell-derived factor 1
NF-κB nuclear factor kappa-light-chain-enhancer of activated B cells
SRYSex-determining region Y
HIF-1αhypoxia-inducible factor-1a
VEGF-Avascular endothelial growth factor A
Her2 human epidermal growth factor receptor 2
ASCadipose stromal/stem cells
ALDOCaldolase, fructose-bisphosphate C
ENO2enolase 2
HK1, 2hexokinase
PFKPphosphofructokinase, platelet
CAAcancer-associated adipocytes
WATwhite adipose tissue
VEGFvascular endothelial growth factor
ERK extracellular signal-regulated kinase
ELK1ETS domain transcription factor 1
EGR1early Growth Response 1
STAT3signal transducer and activator of transcription 3
JAK2Janus kinase 2
TNFtumor necrosis factor
CEBPBCCAAT/enhancer-binding protein bet
EGFepidermal growth factor

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Ijms 26 02275 g001
Figure 1. Chemokines released by adipose tissue are part of multiple signaling loops that support inflammation, cancer, metastasis, and drug resistance.
Figure 1. Chemokines released by adipose tissue are part of multiple signaling loops that support inflammation, cancer, metastasis, and drug resistance.
Ijms 26 02275 g001
Ijms 26 02275 g002
Figure 2. The spread of tumor cells supported by obesity can be impaired by healthy foods. Through their beneficial effect, nutrients can reduce the release of pro-inflammatory chemokines from adipose tissue.
Figure 2. The spread of tumor cells supported by obesity can be impaired by healthy foods. Through their beneficial effect, nutrients can reduce the release of pro-inflammatory chemokines from adipose tissue.
Ijms 26 02275 g002
Table 1. Chemokines released by fat depots.
Table 1. Chemokines released by fat depots.
ChemokineFat DepotHigh Level Chemokines
(Obese vs. Lean) 		Where It Can ActReleased by
CCL2
(MCP-1)		Perivascular [11,12] Invasion/migration
Intravasation
Circulation
Extravasation
Colonization		Fibroblasts
Macrophages
Preadipocytes [13]
Adipocytes [13]
Epicardial [11]
Perirenal [11]
Subcutaneous [9,11,14,15][14,15]
Omental [11]
Intermuscular [16]
CCL3
(MIP-1α)		Subcutaneous [9,15][15]Invasion/migration
Intravasation
Circulation
Extravasation
Colonization
Visceral [9]
CCL4
(MIP-1β)		Subcutaneous [15][15]Invasion/migration
Circulation
Extravasation
Colonization
Pericardial [17]
CCL5
(Rantes)		Subcutaneous [9,14,15,18][14,15]Invasion/migration
Visceral [9,18]
Epicardial [18]
CCL7
(MCP-3)		Subcutaneous [9,14][14]Invasion/migration [19]
Intravasation
Circulation
Colonization		Preadipocytes [13]
Visceral [9]
CCL8
(MCP-2)		Subcutaneous [9] Invasion/migration
Intravasation
Extravasation
Colonization		Preadipocytes [13]
Visceral [9]
CCL11
(eotaxin-1)		Subcutaneous [9] Invasion/migrationPreadipocytes [13]
Visceral [9]
CCL18
(MIP-4)		Subcutaneous [15][15]Invasion/migration
Intravasation		Adipocytes [13]
CCL19
(MIP-3 β)		Subcutaneous [14,20][14,20]Invasion/migrationAdipocytes [13]
CCL20
(MIP-3 α; LARC)		Subcutaneous [15][15]Invasion/migration
Intravasation
Colonization
CXCL1
(Gro α)		Subcutaneous [14][14]Invasion/migration
Intravasation
Colonization		Preadipocytes [13]
Adipocytes [13]
CXCL2
(Gro β)		Omentum [21] Proliferation/migration/angiogenesisAdipocytes [21]
CXCL5
(ENA78)		Subcutaneous [14][14]Invasion/migration
Colonization
CXCL8
(IL-8)		Subcutaneous [14][14]Invasion/migration
Colonization
Perivascular [12]
CXCL10
(IP-10)		Subcutaneous [14][14]Invasion/migration
Colonization		Preadipocytes [13]
Adipose stem cells [22]
Omentum [22]
CXCL12
(SDF-1)		 Invasion/migration
Colonization		Adipocytes [23]
Adipose stromal cells [24]
CCR1
(CD191)		Subcutaneous [9] Invasion/migration
Visceral [9]
CCR2
(CD192)		Subcutaneous [9] Invasion/migration
Visceral [9]
CCR3
(CD193)		Subcutaneous [9] Invasion/migration
Visceral [9]
CCR5
(CD195)		Subcutaneous [9] Invasion/migrationAdipose stem cells [22]
Visceral [9]
Omentum [22]
Table 2. Nutrients lowering (Ijms 26 02275 i001) adiposity and chemokine release.
Table 2. Nutrients lowering (Ijms 26 02275 i001) adiposity and chemokine release.
NutrientsSourceEffect on Adipose Tissue
Viamin EPlant-based oils (wheat-germ,
soybean, sun flower);
Nuts (walnuts, peanuts, almonds);
Fruits and vegetables		CCL2 [39]
NF-κB [40]		Ijms 26 02275 i002
CurcuminRhizome Curcuma longaAdiposity and adipose tissue inflammation [41,42,43,44,45,46,47], NF-κB [48], CCL2 [49,50,51], CCL5 [51,52], CCL7 [53], CXCL1 and CXCL2 [54,55,56], CXCL10 [57,58], CXCL12 [59,60]Ijms 26 02275 i003
Flavonoids
EpicatechinFruitsAdipose tissue inflammation [61,62],
NF-κB [61], CCL2 [61], CCL19 [62]
Epigallocatechin-3-
gallate		Green teaAdipogenesis [63,64,65], NF-κB, CCL2 and CCL5 [66]
NaringeninCitrus fruits, tart cherries, tomatoesAdiposity and adipose tissue inflammation [67]Ijms 26 02275 i004
GenisteinSoy beans, soy-derived foodsAdipose tissue inflammation [68], CCL2 [69,70], CXCL8 [68,70,71], CXCL12 [72]
QuercetinFruits and vegetablesAdipose tissue inflammation [73]Ijms 26 02275 i005
Flavonoid fish-oil supplementAdipose tissue inflammation [74]
AnthocyaninsTart cherryAdipose tissue inflammation [75], adipogenesis [76]Ijms 26 02275 i006
BaicalinScutellaria baicalensis GeorgiAdipose tissue inflammation, chemokine activity [77]Ijms 26 02275 i007
Cirsimarin Cirsium japonicum var. ussuriense,
Cirsium rhothophilum, Cirsium rhinoceros, Microtea debilis		Lipogenesis, adipose cell diameter [78]
Apigenin Fruits and vegetablesAdipogenesis [79]Ijms 26 02275 i008
Organosulfur
components
Diallyl disulfideGarlicObesity [29], adipose tissue inflammation [31], CCL2 [31]Ijms 26 02275 i009
Diallyl trisulfideGarlicAdipogenesis [32,33,34], CCL2 [35], CXCL12 [36]Ijms 26 02275 i010
SulforaphaneBroccoli, cabbage, cauliflower, kaleObesity [37], adipocyte lipid accumulation [80], cytokine production [80]Ijms 26 02275 i011
Fatty acids
n-3 FAs: ALA, EPA, DHAFish, nuts, seeds, oils (canola, soybean)Adipose cell size; NF-κB; CCL2, CCL3, CCL4, CXCL1, CXCL10, CXCL8 [81,82,83,84,85,86,87,88,89,90,91,92]Ijms 26 02275 i012
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Ion, G.; Bostan, M.; Hardman, W.E.; Putt McFarland, M.; Bleotu, C.; Radu, N.; Diaconu, C.C.; Mihaila, M.; Caramihai, M.D.; Hotnog, C.M. Nutrients Lowering Obesity-Linked Chemokines Blamable for Metastasis. Int. J. Mol. Sci. 2025, 26, 2275. https://doi.org/10.3390/ijms26052275

AMA Style

Ion G, Bostan M, Hardman WE, Putt McFarland M, Bleotu C, Radu N, Diaconu CC, Mihaila M, Caramihai MD, Hotnog CM. Nutrients Lowering Obesity-Linked Chemokines Blamable for Metastasis. International Journal of Molecular Sciences. 2025; 26(5):2275. https://doi.org/10.3390/ijms26052275

Chicago/Turabian Style

Ion, Gabriela, Marinela Bostan, Wanda Elaine Hardman, Margaret Putt McFarland, Coralia Bleotu, Nicoleta Radu, Carmen Cristina Diaconu, Mirela Mihaila, Mihai Dan Caramihai, and Camelia Mia Hotnog. 2025. "Nutrients Lowering Obesity-Linked Chemokines Blamable for Metastasis" International Journal of Molecular Sciences 26, no. 5: 2275. https://doi.org/10.3390/ijms26052275

APA Style

Ion, G., Bostan, M., Hardman, W. E., Putt McFarland, M., Bleotu, C., Radu, N., Diaconu, C. C., Mihaila, M., Caramihai, M. D., & Hotnog, C. M. (2025). Nutrients Lowering Obesity-Linked Chemokines Blamable for Metastasis. International Journal of Molecular Sciences, 26(5), 2275. https://doi.org/10.3390/ijms26052275

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