Downregulation of Immunosuppressive Environment in Patients with Chronic HBV Hepatitis on Maintained Remission

Recent years have witnessed the development of highly effective immunomodulatory therapies, especially for treating cancers and autoimmune diseases. The most promising targets include immunosuppressive Tregs, characterized by FoxP3 expression, and the inhibitory pathways involving CTLA-4 and PD-1/PD-L1 molecules. A recent paper by Germanidis et al. provides interesting insights into the relevance of these immunosuppressive pathways for treating chronic hepatitis B virus (HBV) hepatitis (CHB) (1). CHB is characterized by chronic liver damage, inflammation, and fibrosis, eventually leading to cirrhosis and hepatic carcinoma. The HBV life cycle is not cytolytic to infected hepatocytes, and the liver damage is caused by a prolonged immune response induced by the expression of HBsAg on infected hepatocytes. The immune response involves HBsAg-specific CD8 CTLs and to a lesser extent CD4 T effector cells (Teff) (2). CHB is managed with either interferon-based therapies that act by enhancing anti-viral immune responses or nucleos(t)ide analogs (NAs), such as entecavir, which inhibit HBV replication (3). Successful anti-viral therapy is characterized by (i) restored anti-viral immune response, (ii) HBsAg seroconversion, (iii) a decrease in covalently closed circular DNA (cccDNA), and (iv) a decrease in circulating HBV DNA (3–5). However, most patients initially experience “remission,” followed by HBV reactivation after treatment withdrawal (3). cccDNA is the HBV transcription template, it is highly stable and persists even following resolution of CHB or acute HBV infection. It enables HBV reactivation and it is a key hurdle for achieving complete remission (3). Elevated levels of intra-hepatic and circulating FoxP3 Tregs have been described in CHB and chronic hepatitis C (CHC) (6– 8). In this study, Germanidis et al. reported down-regulated liver mRNA expression of FoxP3 and suppressive cytokines, IL-10, and TGF-β, in patients maintained ontreatment following 5 years of remission compared to patients with active disease and no prior treatment (1). CD8 was also decreased in patients on-treatment and in remission. This data suggest a decrease in both intra-hepatic FoxP3 Tregs and CTLs following CHB resolution. Interestingly, IL-2 and IFN-γ expressions were not restored during remission; this could indicate long-term CTL impairment or else it could be due to a reduction in intra-hepatic CTLs preventing any immune response from being restored to pre-infection intensity. The role of Tregs in CHB and other chronic viral infections is not fully clear and further analyses are required (9, 10). In vitro Treg depletion can restore the functional activity of virus-specific CTLs (11, 12). In addition, Tregs are expanded in severe CHB, but correlate with serum viral load rather than impaired HBV-specific immune responses (6, 7). In this study, Germanidis et al. proposed that FoxP3 Tregs might be expanded non-specifically in response to chronic liver inflammation rather than as HBV-specific Tregs (1). In a previous study, the same group reported that liver FoxP3 expression is closely linked to liver inflammation regardless of the underlying cause; viral, toxic, or autoimmunity (13). The current findings confirm FoxP3 is strongly correlated with inflammation in CHB, in addition to PD-1, PD-L1, and CD8. FoxP3 expression also correlated closely with serum viral load, ALT, and AST (markers of liver injury). Apoptosis-induced inflammation is observable in CHB and other liver diseases due to sustained liver injury (14), and Tregs could prevent catastrophic pathology due to apoptosis-induced inflammation. During inflammatory expansion, HBVspecific Tregs might also be generated in response to HBsAg on infected hepatocytes explaining differing reports regarding HBV-specific and non-specific Tregs from CHB patients. FoxP3 is essential for Treg development and it is used as the hallmark marker to identify Tregs in most studies. However, FoxP3 can be upregulated on nonsuppressive Teff during inflammation and activation. More specific Treg markers have