Vaspin and its relation to cancer (Review)
- Authors:
- Published online on: September 23, 2021 https://doi.org/10.3892/wasj.2021.129
- Article Number: 58
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Copyright: © Agarwal et al. This is an open access article distributed under the terms of Creative Commons Attribution License.
Abstract
1. Introduction
Adipose tissue has been identified as a complex organ with endocrine, metabolic and immunoregulatory functions. Adipose tissue releases hormones and signaling molecules, known as adipokines, which function in an autocrine and paracrine manner (1). In obesity, adipocyte hypertrophy and hyperplasia alter the physiological microenvironment within adipocytes. This hyperadiposity causes a chronic low-grade inflammation resembling chronically injured tissue with immune cell infiltration and remodeling (2). In 1863, Virchow hypothesized that the origin of cancer was located at sites of chronic inflammation, partly based on the hypothesis that certain irritants cause tissue injury and cell proliferation occurs in the ensuing inflammatory environment. It has been observed that patients with obesity have a higher risk of developing cancer and also have increased mortality rates (3). One proposed mechanism is that of white adipose tissue hypertrophy and the adipocyte outgrowing its blood supply (4). The hypoxia of these cells leads to adipocyte stress, death and an adverse adipokine secretion profile. Adipocyte hypertrophy also leads to insulin resistance, and the established link is so substantial that an adipocyte size threshold has been identified for an increased risk of insulin resistance (5).
Hida et al (6) first identified a 47 kilodalton (kDa) molecule comprised of 415 amino acids termed vaspin (visceral adipose tissue-derived serpin) in the visceral adipose tissue of Otsuka Long-Evans Tokushima fatty rats at the age when obesity and insulin plasma concentrations peaked. This is a model of human type 2 diabetes that shares common components of the human metabolic syndrome, including abdominal obesity, insulin resistance, hypertension and dyslipidemia (6). From their experiments, Hida et al (6) concluded that vaspin exerts a protective effect against insulin resistance. Its increased levels suggest possible anti-protease properties, thereby improving insulin sensitivity (6). Adipokines may play a significant role in the regulation of cell growth, proliferation, cell cycle, angiogenesis, tumor growth and metastases. Vaspin is also known to cause an imbalance in favor of apoptosis inhibition via the phosphatidylinositol-3-kinase (PI3K)/protein kinase B (Akt) pathway (7). Several adipokines have been linked to various types of cancer with notable attempts made as regards their use as diagnostic tools, prognostic markers and therapeutic targets. The present review article aimed to shed light on available studies that have linked vaspin to various types of cancer.
2. Data collection methods
All articles reporting adipokines and various types of cancer were considered. The PubMed electronic database was searched using medical subject heading (MeSH) terms related to various adipokines, and benign and malignant tumors. Vaspin was first discovered in 2005(6). Hence, search results were considered from 2005 onwards to select relevant articles. Manually searching reference lists supplemented this for additional studies. Similarly, the Google Scholar database was also manually searched. Studies listing adipokines other than vaspin were excluded, since different adipokines use distinct mechanisms in exerting their effects. Review articles on other adipokines were also excluded. An initial search revealed 4,380 articles; finally, 11 clinical and translational studies were included (Fig. 1 and Table I).
Figure 1Flowchart of the study selection and criteria used for inclusion. |
Table ISummary of the studies comparing patients to healthy subjects and the inference of serum vaspin levels. |
3. Colorectal cancer
According to the study search performed, a total of three studies were found that attempted to highlight the association between vaspin and colorectal cancer. Fazeli et al (8) examined vaspin levels in 39 patients who had biopsy-confirmed colorectal cancer compared with those in control subjects. They found that the vaspin, visfatin and omentin-1 levels were significantly higher in patients with colorectal cancer (8). This result was obtained without adjusting for variables; following the adjustment for variables such as age, body mass index (BMI) and waist-to-hip ratio. Additionally, when examining the levels of vaspin in different groups according to sex, no significant difference was found between males and females. They also found that adipocytokines were not related to the stage of colorectal cancer in these patients (8).
Another study comprised 41 patients with confirmed colorectal cancer and 27 healthy controls (9). The included patients either had colon cancer or rectal/sigmoid cancer at various stages. Of note, no difference was observed between the serum levels of vaspin among the healthy volunteers and study subjects. However, there was a difference in the median age of the study subjects to controls (55 vs. 43 years) and the study subjects were enrolled 2-4 weeks following the surgical or colonoscopic removal of the tumor. It is possible that the therapeutic intervention and time interval may have altered the serum vaspin levels in the study subjects compared with the time point when the tumor burden was higher (9).
Kan et al (10) examined the effects of tumor burden on vaspin expression and cancer prognosis in 89 patients with confirmed colorectal cancer. In patients with disease progression, the vaspin levels at the time of initial diagnosis were 40.1 vs. 27.4 pg/ml (P=0.021) in patients who remained disease-free at the end of the study period. They also illustrated vaspin immunostaining imaging results in tumor burden subgroups according to disease progression and disease-free status. The results of their study revealed that patients with progressive disease had a higher vaspin expression at the start of the study irrespective of the tumor burden characteristics. That study highlighted that vaspin levels may be used as a potential marker for cancer progression and early cancer detection (10).
Although the underlying mechanisms remain to be fully elucidated, vaspin may possess anti-apoptotic properties (7). The lack of apoptosis of malignant cells may prevent them from dying. There are a number of mechanisms through which malignant cells can acquire a reduced apoptotic state. This can occur when there is an imbalance between pro- and anti-apoptotic proteins, as well as in instances where the reduced function of the caspase enzyme family, which is involved in the actual apoptosis of cells, provides the cells with their morphology, and impairs cell death signaling (11). Vaspin is known to cause an imbalance in favor of apoptosis inhibition via the PI3K/Akt pathway (Fig. 2) (7). This pathway has been implicated in the development of colorectal cancer (12).
Figure 2Insulin binds to the IR and activates IRS-1, which in turn activates PI3K. PI3K phosphorylates PIP2 to PIP3 which further activates Akt. Akt then regulates proteins involved in cell growth and proliferation. Vaspin inhibits the FFA-induced apoptosis via the PI3K/Akt pathway, increasing cell proliferation. FFA, free fatty acid, IR, insulin receptor; IRS-1, insulin receptor substrate 1; PI3K, phosphatidylinositol 3-kinase; PIP2, phosphatidylinositol-4,5-bisphosphate; PIP3, phosphatidylinositol-3,4,5-bisphosphate; Akt, protein kinase B |
4. Hepatocellular carcinoma
Adipokines have been linked to inflammation with eventual fibrotic, steatotic and angiogenic changes (13). These changes are mechanisms that underlie the development of chronic liver disease. Diseases, such as chronic hepatitis C induce metabolic alterations, including insulin resistance and contribute to hepatic steatosis. Kukla et al (14) demonstrated that vaspin was an independent predictor of the severity of liver fibrosis and positively correlated with the stage of fibrosis. In the case of no fibrosis or mild fibrosis limited to portal spaces, the serum vaspin level has been shown to be significantly decreased in patients with hepatitis C as compared with healthy controls. Insulin resistance, as noted with the homeostatic model assessment of insulin resistance (HOMA-IR) measurements, has also been shown to be significantly increased in patients with hepatitis C (14).
According to the search performed, two studies evaluated the relation of serum vaspin levels with hepatocellular carcinoma (HCC). The first study comprised 69 patients with cirrhosis and HCC. That study included patients with cirrhosis due to viral causes (81% had hepatitis C) and non-alcoholic fatty liver disease/non-alcoholic steatohepatitis with the majority of patients in Child-Pugh class A or B (15).
The serum vaspin levels were found to be higher in patients with HCC compared with healthy volunteers (0.18 vs. 0.10 ng/ml; P=0.05). Serum vaspin levels were also higher in patients with HCC due to viral causes compared with HCC due to non-viral causes (0.23 vs. 0.10 ng/ml; P=0.02). Vaspin levels were also higher in patients with chronic hepatitis C compared to those with liver disease due to non-viral causes (0.41 vs. 0.10 ng/ml, p=0.003). No difference was noted in the serum vaspin levels between different groups according to Child-Pugh scores or Barcelona clinic liver cancer scores. The authors of that study demonstrated that vaspin levels did not differ in patients with higher or lower HOMA-IR scores, indicating that the increase in vaspin levels was primarily from the cancer and not a compensatory mechanism for insulin resistance (15). The increase in vaspin levels may also be a result of liver fibrosis, as demonstrated by Kukla et al (14), or a direct result of hepatitis C virus infection, which causes insulin resistance by affecting the insulin signaling pathway and inhibiting signal transduction.
The second study was performed by Skonieczna et al (16), in which human HCC cells treated with vaspin were cytometrically evaluated. The researchers demonstrated that vaspin reduced apoptosis in a concentration-dependent manner in the cancer cells, thus promoting the proliferation of tumor cells. They also noted that the production of reactive oxygen species (ROS), specifically nitric oxide and superoxide anion, which are commonly elevated in apoptotic cells and implicated in the promotion of apoptosis, was decreased in the presence of vaspin. The levels of ROS were related to vaspin in a concentration-dependent manner with a significant reduction when vaspin was used at 5 ng/ml. The decreased levels of ROS observed with 5 ng/ml vaspin resulted from the suppression of physiological oxidative processes. The authors of that study suggested that an anti-apoptotic switch was activated at lower concentrations of vaspin and once initiated, the anti-apoptotic cascade was maintained with higher vaspin levels. The reduction in ROS generation could restrict pro-inflammatory processes in cancer cells, leading to increased viability and proliferation. Free radical scavenging in cells exposed to vaspin resulted in a reduction of pro-oxidative apoptotic signaling pathways (16).
5. Endometrial cancer
Chronic hyperinsulinemia is one of the main risk factors of endometrial cancer, and insulin is known to exhibit mitogenic and proliferative action through endometrial insulin receptors. Vaspin is known to play a role in augmenting tissue sensitivity to insulin, thereby protecting against one of the risk factors for endometrial cancer (6). It can be thus concluded that lower concentrations of vaspin would thus increase the risk of endometrial cancer development.
Following the search performed of the databases, two studies were found which investigated the relation of serum vaspin levels with endometrial cancer. In a previous study on 168 patients, including 92 patients with endometrial cancer and 76 patients with normal endometrium or benign polyps, no statistically significant differences in the mean values of vaspin levels were found in patients with endometrial cancer and patients with endometrial polyps or benign endometrium (17). However, significantly lower serum levels of vaspin were found in patients with lymph node or lymph vessel involvement. Lower levels were also observed in patients in whom the tumor had invaded deeper into the myometrium. The mean vaspin levels were examined between different tumor classification grades and were noted to be 1.1 ng/ml in patients with International Federation of Obstetrics and Gynecology (FIGO) stage I and II endometrial cancer, and 0.52 ng/ml in patients with FIGO stage III and IV endometrial cancer (17).
Another study by Erdogan et al examined at vaspin levels in 60 post-menopausal female patients with histologically confirmed endometrial cancer (18). The control group included 70 patients with benign endometrial conditions. The median vaspin levels were lower in patients with endometrial cancer compared with the controls (0.21 vs. 0.39 ng/ml; P<0.0001). A sub-group analysis of the various tertiles of vaspin levels also revealed that, when compared with the highest tertile of vaspin levels, the first tertile had an odds ratio of 17.04. This observation remained significant when the results were adjusted for BMI, HOMA-IR and the quantitative insulin-sensitivity check index (QUICKI) scores of the patients (18).
A possible mechanism of cancer development consists of understanding obesity and its implications. Obesity causes excess adipose tissue, which promotes the conversion of androgens to excess estrogen. Unopposed estrogen activity is known to be a risk factor of endometrial cancer. From cytological studies on vascular endothelial cells and smooth muscle cells, it is known that vaspin exerts an anti-inflammatory effect, thus protecting cells from tumorigenesis (19). This may explain why low vaspin levels were associated with a higher risk of developing endometrial cancer in both the studies on endometrial cancer mentioned above.
6. Other types of cancer
Jabbari et al (20) attempted to examined vaspin levels in medullary thyroid cancer in 45 patients with cancer and 45 healthy controls who were matched for age, sex and BMI. They found that the vaspin levels were elevated in patients with cancer compared with the healthy controls (0.52 vs. 0.45 ng/ml; P=0.0241).
Another study examined 42 patients who were diagnosed with prolactinomas and compared them with 30 controls (21). They further subdivided the patients with prolactinoma into 21 patients who underwent treatment with dopamine agonists and 21 patients who were newly diagnosed and were treatment-naive. Patients with prolactinomas had higher HOMA-IR and QUICKI scores compared with the healthy volunteers. The mean vaspin levels were lower in the untreated and treated patients with prolactinoma compared with the healthy controls. In a subset analysis of the healthy controls, after categorizing the controls into two groups with the median value of serum vaspin, lower vaspin levels were found to be associated with an increased risk of prolactinoma (odds ratio, 6.00). These results did not change after adjusting for confounding factors, such as BMI, HOMA-IR and QUICKI scores (21).
7. Other conditions
Zhu et al (22) examined the effect of vaspin on human osteoblasts in relation to apoptosis. They noted that there was a consistent decrease in apoptosis with increasing concentrations of vaspin at up to 100 ng/ml. Vaspin exposure also increased Bcl-2 protein expression and decreased Bax protein expression in a concentration-dependent manner. Bcl-2 protein is an inhibitor of apoptosis, while Bax protein is an inducer of apoptosis. With western blot analysis, the authors of that study were also able to demonstrate that vaspin exerted its anti-apoptotic effects by activating the mitogen-activated protein kinase (MAPK)/extracellular signal-regulated kinase (ERK) signaling pathway in human osteoblasts (22). Apoptosis is a natural phenomenon that occurs in aging cells. The anti-apoptotic activity of vaspin has been previously highlighted in HCC (16) and can be similarly responsible for the development of bone-related cancers.
Jung et al (7) established the anti-apoptotic nature of vaspin in endothelial cells. They studied the effects of vaspin on human aortic endothelial cells and discovered that free fatty acid-induced apoptosis was partly reversible with vaspin. In the vascular endothelium, there exists a signaling pathway that is very similar to that used by insulin to promote glucose transporter type 4 expression on the cell surface. The similar signaling pathway, when activated, increases nitric oxide production, which reduces endothelial dysfunction. Vaspin was noted to use the PI3K/Akt pathway to increase nitric oxide production. It also inactivated Bad protein (pro-apoptotic) and relieved the inhibitory effect on Bcl-2 protein (anti-apoptotic) with the increased expression of Akt and Bcl-2, as recorded in that study (7).
8. Conclusion
Vaspin appears to play a role in the promotion of tumor formation, possibly by inhibiting apoptosis via cellular mechanisms. In turn, it can promote the proliferation of cells with malignant potential. Mechanisms involved in insulin resistance may be involved. Thus far, an attempt has been made to establish its role in colorectal cancer and HCC, albeit in a limited number of studies. However, vaspin also appears to exert anti-inflammatory effects via similar cellular signaling pathways, as highlighted in the studies on endometrial cancer mentioned above. It is difficult to predict whether vaspin functions as a tumor promoter or a tumor inhibitor in other types of cancer, as only a limited number of studies have explored its role in various therapeutics. Further studies are thus warranted to fully elucidate its potential as a possible diagnostic tool, prognostic marker, or therapeutic target.
Acknowledgements
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Funding
No funding was received.
Availability of data and materials
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Authors' contributions
SA was involved in the conceptualization, methodology and literature search for the study, as well as in the writing of the original draft. SD was involved in the literature search for the study, and in writing, editing and revision of the manuscript. SA and SD confirm the authenticity of all raw data. Both authors have read and approved the final manuscript.
Ethics approval and consent to participate
Not applicable.
Patient consent for publication
Not applicable.
Competing interests
The authors declare that they have no competing interests.
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