Serum cytokine profiles in patients with prostate carcinoma

  • Authors:
    • Eri Tazaki
    • Nobuaki Shimizu
    • Ryota Tanaka
    • Masakazu Yoshizumi
    • Hiroshi Kamma
    • Shigeru Imoto
    • Tomoyuki Goya
    • Kunihisa Kozawa
    • Atsuyoshi Nishina
    • Hirokazu Kimura
  • View Affiliations

  • Published online on: June 16, 2011     https://doi.org/10.3892/etm.2011.286
  • Pages: 887-891
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Abstract

It has been suggested that various cytokines are associated with the pathophysiology of prostate carcinoma (Pca). We profiled ten cytokines (IL-1β, IL-2, IL-4, IL-5, IL-6, IL-8, IL-10, IL-12, IFN-γ and TNF-α) in the serum levels of 11 patients with organ-confined Pca, 15 with advanced Pca without cachexia, 8 with advanced Pca with cachexia (cachexia group) and 5 healthy males as controls. Cytokines were measured using a highly sensitive fluorescence microsphere system. Compared to the control group, serum levels of all cytokines were significantly higher in the cachexia group, and six cytokines (IL-1β, IL-2, IL-8, IL-12, TNF-α and IFN-γ) were significantly higher in the group with advanced Pca without cachexia. In the group with organ-confined Pca, only IL-1β and IL-12 levels were significantly higher compared to the control group. In the cachexia group, levels of all cytokines apart from TNF-α were significantly higher compared to the group with organ-confined Pca, and levels of four cytokines (IL-2, IL-4, IL-8 and IL-10) were significantly higher compared to the group with advanced Pca without cachexia. These results indicate that i) an aberrance imbalance of cytokine production was associated with the pathophysiology of Pca and cachexia, ii) cytokine profiles in Pca patients were distinct by disease stage, and iii) IL-1β and IL-12 may be applicable as early diagnostic indicators.

Introduction

Prostate cancer (Pca) is a common cause of morbidity and mortality in the developed world, and is one of the major malignant neoplasms in males (13). Sixty to seventy percent of patients with advanced Pca suffer from cachexia (4). Cancer cachexia is one of the most devastating conditions of advanced malignant disease. It is characterized by weight loss and anorexia that involves the depletion of host adipose tissue and skeletal muscle (5). Cachexia brings a lower quality of life, a poorer response to chemotherapy and reduced survival (6). However, as in patients with other types of malignant diseases, the pathophysiology and etiology of cachexia in patients with Pca is not well understood, and intervention strategies to alleviate the condition are not yet available.

The pathophysiology of cachexia associated with the progression of malignant disease in patients is multifactorial. Several cytokines, such as tumor necrosis factor α (TNF-α), interleukin 1 (IL-1), IL-6 and IL-8, are known as agents that contribute to the condition (5). Cytokines are major homeostatic modulators in vivo and may be associated with the pathophysiology of various types of cancers (711). These cytokines are also reported to be associated with cachectic Pca (5,6,12,13). For example, the levels of pro-inflammatory cytokine, TNF-α, in cachectic Pca patients as well as organ-confined Pca patients were higher compared to the control (14). Another cytokine, IL-6, is also associated with the pathophysiology of cachexia in Pca (15). However, research into the relationships between other cytokines and the pathophysiology of cachexia is ongoing.

Previous studies have shown that more than thirty types of cytokines have been discovered and their biological functions studied (1418). Each cytokine forms a cytokine network, and these networks may synchronize various biological events, including immunity, cell differentiation, proliferation and cancer growth in humans. Thus, the evaluation of various cytokines could be critical to gaining a better understanding of the pathophysiology of Pca, including the complication of cachexia. In addition, it has been reported that ceratin cytokines in the serum may be distinct in the disease stages of Pca (11,13,14), although these reports involve less than five types of cytokines. Based on this background, we profiled ten types of cytokines in the sera levels of patients at various stages of Pca.

Materials and methods

Subjects

Thirty-nine subjects were categorized into four groups as previously described (14): patients with organ-confined Pca (n=11), patients of advanced Pca without cachexia (n=15), patients of advanced Pca with cachexia (n=8) and healthy male adults as controls (n=5) (Table I). Written informed consent was obtained from all patients. The study protocol was approved by the Ethics Committee on Human Research of Gunma Prefectural Cancer Center. The four groups were defined as follows.

Table I.

Clinical data of the subjects.

Table I.

Clinical data of the subjects.

Control (n=5)Organ-confined Pca (n=11)Advanced Pca without cachexia (n=15)Advanced Pca with cachexia (n=8)
Age (years)49.4±3.364.2±2.170.7±2.071.4±2.9
Radical prostectomy10
Hormone therapy1158
Stage I11
Stage IV158
Total serum protein (g/dl)7.4±0.27.2±0.16.3±0.25.6±0.3a
Serum albumin (g/dl)4.1±0.14.3±0.13.5±0.12.7±0.2a
Hb (104/μl)14.2±0.514.3±0.510.4±0.6a8.8±1.0a
PSA (ng/ml)1.7±0.511.6±3.01,206.2±374.0a1,390.5±705.6a
Life expectancyAll aliveAll alive8.4 months1.2 months

{ label (or @symbol) needed for fn[@id='tfn1-etm-02-05-0887'] } Pca, prostate carcinoma.

a p<0.05 vs. control or organ-confined Pca. Data are expressed as the means ± SE. Details of the statistical method are described in the text.

Organ-confined Pca group. This group consisted of 11 patients with newly diagnosed, organ-confined Pca, at stage 1. Radical prostectomy was performed on 10 of the 11 patients. The remaining patient underwent hormone therapy. Serum samples were obtained prior to primary therapy. The median age of this group was 64.2 years.

Advanced Pca without cachexia group. This group consisted of 15 advanced Pca patients without cachexia. They were all diagnosed with bone metastasis, but none of them suffered from peripheral edema, weight or appetite loss. The median age of this group was 70.7 years.

Advanced Pca with cachexia group (cachexia group). This group consisted of 8 advanced Pca patients with cachexia. They were all diagnosed with metastasis to other organs and suffered from appetite and weight loss. All patients died within 4 months (mean 1.2) after cachexia was diagnosed. The median age of this group was 71.4 years.

Control group. This group comprised 5 volunteers (healthy male adults) with no history of benign or malignant prostatic disease. The median age of this group was 49.4 years (Table I). Since high levels of prostate-specific antigen (PSA) in the serum due to benign prostatic hyperplasia (BPH) were found in individuals over the age of 51 years, we chose male subjects under 50 years of age as the control group (19,20).

Measurement of serum cytokines

Serum specimens were obtained from the patients or the normal controls at the Gunma Prefectural Cancer Center. We evaluated the levels of ten cytokines in a small volume (50 μl) of serum using a highly sensitive fluorescence microsphere system (Bio-Plex suspension array system, Hercules, CA, USA). Serum levels of the following cytokines were determined: IL-1β, IL-2, IL-4, IL-5, IL-6, IL-8, IL-10, IL-12, IFN-γ and TNF-α. Samples were processed following the Bio-plex cytokine assay instruction manual. Total protein, albumin and hemoglobin were measured in each blood sample.

Categorization of cytokines

The ten cytokines were categorized into four groups as previously described (21): proinflammatory cytokines (IL-1β, IL-6 and TNF-α; Fig. 1A–C), neutrophil recruitment-inducing chemokine (IL-8; Fig. 1D), Th1 cytokines (IL-2, IL-12 and IFN-γ; Fig. 1E-G) and Th2 cytokines (IL-4, IL-5 and IL-10; Fig. 1H–J).

Statistical analysis

Data were analyzed using the SAS JMP 8 software (Cary, NC, USA). All data were expressed as the means ± SE. Statistical analysis of the cytokine levels was performed by the Kruskal-Wallis method. Statistical significance was set at the level of p<0.05.

Results

Various cytokines (IL-1β, IL-2, IL-4, IL-5, IL-6, IL-8, IL-10, IL-12, IFN-γ and TNF-α) were profiled in the serum levels of patients with organ-confined Pca (n=11), advanced Pca without cachexia (n=15), advanced Pca with cachexia (cachexia group, n=8) and healthy males (control group, n=5). Fig. 1 shows the serum levels of the various cytokines quantitated in this study. Detailed statistical data with regard to cytokine concentrations in the sera are shown in Table II. Levels of all cytokines in the sera of the cachexia group were significantly higher than those in the control group. In the group with advanced Pca without cachexia, the levels of six cytokines (IL-1β, IL-2, IL-8, IL-12, TNF-α and IFN-γ) were significantly higher than those in the control group, and IL-1β and IL-12 were significantly higher in the sera of the group with organ-confined Pca. Levels of all cytokines except TNF-α were significantly higher in the sera of the cachexia group than in the organ-confined Pca group. In addition, the levels of four cytokines (IL-2, IL-4, IL-8 and IL-10) in the cachexia group were significantly higher than those in the group with advanced Pca without cachexia.

Table II.

Serum cytokine levels in the subjects (pg/ml).

Table II.

Serum cytokine levels in the subjects (pg/ml).

CytokineControl (A)Organ-confined Pca (B)Advanced Pca without cachexia (C)Advanced Pca with cachexia (D)p-values for (A) vs. (D)p-values for (A) vs. (C)p-values for (A) vs. (B)p-values for (B) vs. (D)p-values for (C) vs. (D)
IL-1βn.d.23.7±4.830.7±5.142.8±4.2<0.00010.00070.00930.0139n.s.
IL-2n.d.14.4±2.726.7±5.352.3±15.30.00050.0359n.s.0.00150.0189
IL-4n.d.4.4±1.18.9±2.322.8±6.20.0003n.s.n.s.0.00030.0027
IL-50.5±0.21.5±0.43.1±0.95.0±1.40.0099n.s.n.s.0.0118n.s.
IL-610.1±10.112.1±3.049.6±13.271.1±26.40.0279n.s.n.s.0.0116n.s.
IL-80.2±0.26.2±0.89.8±1.423.3±3.6<0.00010.0033n.s.<0.0001<0.0001
IL-100.2±0.11.1±0.42.3±0.54.6±1.60.0040n.s.n.s.0.00530.0400
IL-12n.d.10.7±1.816.1±3.022.4±1.2<0.00010.00050.02090.0047n.s.
TNF-α0.2±0.135.4±10.056.8±12.371.0±12.10.00280.0075n.s.n.s.n.s.
IFN-γn.d.17.9±4.826.4±5.941.3±12.10.00270.0305n.s.0.0424n.s.

[i] Pca, prostate carcinoma; n.s., not significant; n.d., not detected (lower than the limit of sensitivity). Data are expressed as the means ± SE. Details of the statistical method are described in the text. p<0.05 was considered statistically significant. All p-values for (B) vs. (C) are not significant.

Bood data were compared regarding serum total protein, serum albumin, serum PSA and hemoglobin concentrations in each group (Table I). The serum total protein and serum albumin in the cachexia group were lower than in the other groups. Hemoglobin concentrations of whole blood in the groups with advanced Pca without cachexia and cachexia were lower than those in both the organ-confined Pca and control groups. In addition, serum PSA levels in the group with advanced Pca without cachexia and cachexia group were higher than the level in the control group. However, no correlations between serum PSA and serum cytokine levels were found (p>0.05).

Discussion

We profiled serum cytokine levels (ten cytokines) in patients with organ-confined Pca, patients with advanced Pca without cachexia, patients with advanced Pca accompanied with cachexia (cachexia group) and healthy adults (control group). In the sera of the cachexia group, all cytokine levels were significantly higher than in the control group, nine cytokines (except TNF-α) were significantly higher than in the organ-confined Pca group and four cytokines (IL-2, IL-4, IL-8 and IL-10) were significantly higher than in the group with advanced Pca without cachexia. Compared to the controls, the levels of six cytokines (IL-1β, IL-2, IL-8, IL-12, TNF-α and IFN-γ) were significantly higher in the group with advanced Pca without cachexia, but only two cytokines (IL-1β and IL-12) were significantly higher in the organ-confined Pca group. In addition, hemoglobin concentrations in blood, serum protein and serum albumin were lower in the cachexia group than these concentrations in the control group. These results suggest that aberrant and imbalanced production of various cytokines in Pca patients with or without cachexia may be associated with the pathophysiology of Pca, and these cytokine profiles may represent distinct disease stages in patients with Pca. Furthermore, the serum levels of IL-1β and IL-12 may be applicable biomarkers of early-stage Pca, although larger scale studies are required.

Previous reports suggest that various cytokine levels in Pca sera are higher than those in normal adults. For example, IL-1, IL-6, IL-8 and TNF-α levels were found to be higher than normal in patients with advanced Pca (11,14). Indeed, our data are comparable to the data from these previous studies. Previous reports also discuss relationships between cytokinemia and the pathophysiology of Pca with or without cachexia. IL-6, IL-8 and TNF-α have been particularly well studied (5,14). The main symptoms of cachexia are weight loss and anorexia that involves the depletion of host adipose tissue and skeletal muscle. Both IL-8 and TNF-α are involved in the depletion of adipose tissue. In addition, IL-8 may be associated with tumor growth and the development of angiogenesis, tumorigenesis and metastasis (22,23). Another report showed that IL-1 may play a similar role to TNF-α (24).

Anemia is a well-known complication in cachectic patients (11). A previous study suggested that TNF-α inhibits normal hematopoietic progenitors, leading to both anemia and thrombocytopenia (25). Thus, in the present study, the high levels of these cytokines noted in cachectic patients may be associated with representative cachectic symptoms.

We also found that levels of other cytokines, such as IL-2, IL-4, IL-5, IL-10, IL-12 and IFN-γ, were higher than normal in cachexic patients. We explain the significances of these cytokines in Pca and cachexia as follows. First, IL-2, IL-12 and IFN-γ are Th1 cytokines and they may suppress cancer development and metastasis (26). These cytokines may be produced by phagocytic cells (monocytes, macrophages and neutrophils) and dendritic cells (DC), and activate natural killer (NK) cells (representative anticancer immune cells) leading to anticancer effects. IL-2 and IL-12 elicit IFN-γ from NK cells, CD4-positive cells and CD8 cells, and accordingly play crucial anticancer effects in vivo (27). IL-12 and IFN-γ may therefore be applicable to the development of therapies for various types cancers, including Pca (27). In the present study, the serum levels of IL-12 were significantly elevated in all groups with Pca, even in the organ-confined group (Table II). In addition, the serum levels of IFN-γ were also elevated in the advanced Pca groups. Based on these results, it is suggested that elevated levels of Th1 cytokines, such as IL-2, IL-12 and IFN-γ, in Pca acted as anticancer agents, and cytokine profiles by disease stage of Pca were distinct.

IL-4, IL-5 and IL-10 are representative Th2 cytokines, and may be associated with cancer development. In particular, IL-4, IL-5 and IL-10 act as immunosuppressors of cancer immunity and promote cancer development (28,29). In the present study, these immunosuppressive cytokines were significantly elevated in the cachexia group. Thus, these cytokines may have contributed to further cancer development.

More than 50 types of cytokines have been confirmed to date, and most of these are thought to be associated with cancer biology, such as cancer immunity and progression. Our preliminary results showed that many serum cytokine levels were elevated in patients with Pca, and cytokine profiles by disease stage of Pca were distinct. In addition, Th1 cytokines (IL-1β and IL-12) may be applicable diagnostic markers of early-stage Pca. Therefore, it is important to understand the diverse roles of various cytokines in order to further address the pathophysiology of various types of cancers, including Pca.

Acknowledgements

This study was supported in part by Research on Health and Welfare Programs from the Research Fund for Promoting Science and Technology of Gunma Prefecture, Japan.

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September-October 2011
Volume 2 Issue 5

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Spandidos Publications style
Tazaki E, Shimizu N, Tanaka R, Yoshizumi M, Kamma H, Imoto S, Goya T, Kozawa K, Nishina A, Kimura H, Kimura H, et al: Serum cytokine profiles in patients with prostate carcinoma. Exp Ther Med 2: 887-891, 2011
APA
Tazaki, E., Shimizu, N., Tanaka, R., Yoshizumi, M., Kamma, H., Imoto, S. ... Kimura, H. (2011). Serum cytokine profiles in patients with prostate carcinoma. Experimental and Therapeutic Medicine, 2, 887-891. https://doi.org/10.3892/etm.2011.286
MLA
Tazaki, E., Shimizu, N., Tanaka, R., Yoshizumi, M., Kamma, H., Imoto, S., Goya, T., Kozawa, K., Nishina, A., Kimura, H."Serum cytokine profiles in patients with prostate carcinoma". Experimental and Therapeutic Medicine 2.5 (2011): 887-891.
Chicago
Tazaki, E., Shimizu, N., Tanaka, R., Yoshizumi, M., Kamma, H., Imoto, S., Goya, T., Kozawa, K., Nishina, A., Kimura, H."Serum cytokine profiles in patients with prostate carcinoma". Experimental and Therapeutic Medicine 2, no. 5 (2011): 887-891. https://doi.org/10.3892/etm.2011.286