Background
HBV infection is the most common cause of chronic liver injury and a major cause of liver cirrhosis, hepatocellular carcinoma, and liver failure [
1]. Liver failure is a severe clinical syndrome characterized by jaundice, ascites, hepatic encephalopathy, and a bleeding tendency due to impairment of liver function, leading to poor prognosis [
2]. According to World Health Organization estimates, approximately 240 million people around the world suffer from chronic HBV infection (
http://www.who.int/hiv/pub/hepatitis/hepatitis-b-guidelines/en/).
The outcomes of HBV infection depend on both viral and host factors, including genetic factors that determine a host’s immune mechanisms [
3]. It is generally accepted that HBV is not directly cytopathic; thus, HBV-related hepatocellular injuries are the results of the complex interplay among HBVs, hepatocytes, and host immune cells [
3,
4]. It has been widely recognized that host immunity contributes to the pathogenesis of liver injuries and even liver failure. The immune clearance of HBV can trigger extensive liver damage that results in fibrosis and cirrhosis. Cytotoxic T-lymphocytes (CTLs), the core of cellular immunity, play a key role in the clearance of intracellular viruses, which are the major cause of cell apoptosis or necrosis [
5]. Several studies have characterized intrahepatic CD4
+ and CD8
+ T lymphocytes in chronic hepatitis B (CHB) (as reviewed by Shimizu) [
6]. It is generally accepted that HBV-specific CD8
+ T cells have important functions in controlling HBV replication in the liver without causing hepatic necroinflammation, whereas non-specific CTLs may contribute to HBV-related intrahepatic inflammation [
7].
Macrophages Cells play a key role in the homeostasis of the liver, which undergo polarized activation to M1 or M2 or M2-like activation states in response to environmental signals. The M1 phenotype is characterized by the upregulation of proinflammatory cytokines and promotion of Th1 response, and strong microbicidal and tumoricidal activity. In contrast, M2 macrophages promote tissue remodeling and tumor progression, and have immunoregulatory functions (as reviewed by Antonio Sica, et al.) [
8]. It is general accepted that HBV promotes intrahepatic resident and recruited macrophages M2 polarization, leading to impairment of host immunity and progression of tissue fibrosis/remodeling [
9].
Th cells that produce IL-17 (Th17 cells) have recently been identified as the third subset of effector T cells, which produce IL-17A, IL-17 F, IL-22 and IL-21 [
10]. High numbers of IL-17-producing CD4
+ T cells have been observed in both the liver and the blood of CHB patients; and the elevation in this cell population has been correlated with a high serum level of IL-27 [
11]. An increase in circulating and intrahepatic IL-17-producing CD4
+ T cells is well correlated with ALT level and liver injury. CD4
+ T lymphocytes that produce IL-17 infiltrate into the livers of patients with CHB and increase the severity of liver damage [
12].
Prior studies on HBV-related hepatitis flares have demonstrated that, high ALT levels usually accompanied by increased serum levels of IL-12 and Th1 phenotypic cytokines (IL-2 and IFN-γ) [
13,
14], and the natural killer (NK)-cell mediated liver damage were found to be attributed to the increased serum IFN-a and IL-8 [
15]. Therefore, hepatitis B flares are results of complex interplay of the virus and the innate and adaptive immune responses, and the more vigorous immune response against HBV, the higher the serum ALT (as reviewed by Chang and Liaw) [
4].
Hepatic microcirculation disorders occur in all chronic liver diseases, which result in insufficient blood supply to hepatocytes. In addition, collateral circulation also depletes blood flow from the liver. As a result, a) nutrients absorbed from the intestines cannot nourish the liver; b) the therapeutic effects of certain drugs are decreased; and c) metabolic wastes accumulate. These events speed the progression of liver diseases.
Resistin is a 12.5-kd adipokine that belongs to a new family of small, cysteine-rich secretory proteins known as FIZZ (found in inflammatory zone) or resistin-like molecules [
16]. In rodents, resistin is highly expressed in adipose tissue, and circulating levels of resistin are increased during diet-induced or genetic obesity [
17]. It has been verified that resistin is expressed and upregulated under conditions of chronic injury in human liver tissue, and resistin can stimulate human hepatic stellate cells (HSCs) to secrete proinflammatory cytokines through activating the nuclear factor (NF)-κB signaling pathway [
18]. In patients with chronic hepatitis C virus infection, low serum levels of resistin are associated with the presence of fibrosis and may therefore be a biochemical marker of fibrosis [
19]. Moreover, Tsochatzis et al. found that in CHB and chronic hepatitis C (CHC) patients, resistin levels are independently associated with fibrosis severity [
20]. Another study found that elevated levels of resistin were prominent in patients with hepatobiliary inflammation and were associated with breach of self-tolerance; thus, resistin may be an important marker of disease severity in autoantibody-mediated gastrointestinal inflammatory diseases [
21]. Furthermore, increased serum resistin is known to be positively correlated with histological inflammatory score in nonalcoholic fatty liver disease (NAFLD), suggesting that increased resistin in NAFLD patients is related to the histological severity of this disease [
22].
In the present study, patients with chronic HBV infection were retrospectively selected. The serum resistin levels and serum levels of the cytokines IL-1, IL-6, IL-17, IL-23, TNF-α, and TGF-β1 were assayed. The association between serum resistin levels and serum cytokine levels, liver biochemical indices, and fibrosis severity were analyzed. The possible role of resistin as a marker of the inflammatory process in patients with CHB was investigated in detail.
Discussion
This study revealed that patients with chronic HBV infection had significantly elevated serum resistin levels; this finding is consistent with previously reported data [
20]. Patients with LC-B or LF-B had significantly higher serum resistin levels than CHB patients (
p < 0.01), whereas LC-B patients and LF-B patients did not significantly differ with respect to serum resistin levels (
p > 0.05). These results suggest that serum resistin could play a role as an indicator of disease severity and/or degeneration in patients with hepatitis B. Moreover, high serum levels of IL-1, IL-6, IL-17, TNF-α, and TGF-β1 but not IL-23 were detected in CHB, LC-B, and LF-B patients. Serum IL-1 levels were higher in LC-B patients than in CHB and LF-B patients, whereas serum IL-6 and TNF-α levels were much higher for LC-B patients and LF-B patients than for CHB patients; these findings are consistent with the inflammatory roles of the proinflammatory cytokines IL-1, IL-6, and TNF-α [
25].
In this study, serum resistin levels were weakly correlated with LS values determined by FibroScan among CHB patients but not among LC-B patients or LF-B patients. This result can be explained by the fact that LS depends on the extent of fibrosis due to prior intrahepatic deposits [
26]. Serum markers such as procollagen peptide, matrix metalloproteinases (MMPs), tissue inhibitors of matrix metalloproteinases (TIMPs), laminins, and TGF-β1, are correlated with molecules derived directly from the ECM or produced by activated HSCs. Thus, the elevation of these serum markers suggests the activation of fibrogenesis [
27,
28]. Interestingly, serum resistin levels were positively correlated with serum TGF-β1 levels, particularly among LC-B patients (Fig.
4). Furthermore, among CHB patients, serum resistin levels were positively correlated with serum AST levels (Fig.
5). These results are consistent with the general notion that resistin can act as an intrahepatic cytokine with proinflammatory activity in HSCs via a Ca2
+/NF-κB-dependent pathway and involvement in the pathophysiology of liver fibrosis [
18].
IL-17 is a major effector cytokine secreted by Th17 cells, which play a proinflammatory role in the pathogenesis of hepatitis B and promote HBV infection-related injury [
29]. In this study, all patients with CHB, LC-B, or LF-B exhibited similarly elevated serum IL-17 levels (Fig.
2c). There were no significant correlations between serum IL-17 and serum ALT, AST, or TBil (data not shown). Serum IL-17 was positively correlated with serum resistin among LC-B patients and LF-B patients but not among CHB patients (Fig.
3); these findings provide additional evidence supporting the proinflammatory role of IL-17, especially in the context of advanced liver injury.
Recently, Ming et al. found that the upregulation of the TGF-β1/IL-31 pathway is associated with disease severity in LC-B, since elevated serum TGF-β1 and IL-31 levels were positively associated with albumin, alpha-fetoprotein, creatinine, white blood cell, and platelet levels among LC-B patients [
30]. Furthermore, TGF-β1/IL-31 pathway may also play an important role in the pathogenesis of liver injury during chronic HBV infection, since increased activity of the TGF-β1/IL-31 pathway has been found well correlated with the extent of liver injury, disease severity, and nonsurvival among ACLF patients, whereas reduced activity of this pathway has been detected during the recovery from liver injury in CHB cases [
31]. In the current study, patients with HBV chronic infection exhibited elevated serum TGF-β1, and serum TGF-β1 levels were significantly higher in LF-B patients than in CHB patients or LC-B patients. CHB and LC-B patients did not significantly differ with respect to serum TGF-β1, although average serum TGF-β1 levels were slightly higher in LC-B patients than in CHB patients. These results provided additional data to support the potential role of TGF-β1 in the pathogenesis of liver injury in patients with chronic HBV infection, particularly patients with LF-B.
IL-23 has recently been identified as playing a critical role in a number of chronic inflammatory diseases. Xia et al. reported that both serum IL-23 level and hepatic IL-23 were positively correlated with liver injury in CHB patients [
32]. In this study, average serum IL-23 levels were higher in patients than in HCs and were markedly higher in CHB patients than in HCs (8.149 vs. 4.589), with no significant differences in serum IL-23 levels among CHB patients, LC-B patients, and LF-B patients. This lack of significance may be attributable to the large deviations detected in serum IL-23 levels (which ranged from 0.49 to 118.92).
Taken together, the findings of this study demonstrated that high serum resistin was positively correlated with serum IL-17 and TGF-β1. Elevated resistin is associated with the inflammation and necrosis of liver cells and could therefore potentially be used as an index of disease severity and degeneration in patients with chronic HBV infection. However, the mechanism of resistin in the inflammatory process of chronic hepatitis B is unclear, further studies are needed to elucidate how resistin works in the progress of liver injury, and the cross-talk between resistin and IL-17 or TGF-β signaling pathways.
Acknowledgements
The authors thank Yuling He and Yingqi Huang for excellent technical assistance.