Milich D R, Schödel F, Hughes J L, Jones J E, Peterson D L
Department of Molecular Biology, The Scripps Research Institute, La Jolla, California 92037, USA.
J Virol. 1997 Mar;71(3):2192-201. doi: 10.1128/JVI.71.3.2192-2201.1997.
Secretion of the hepatitis B virus (HBV) e antigen (HBeAg) has been conserved throughout the evolution of hepadnaviruses. However, the function of this secreted form of the viral nucleoprotein remains enigmatic. It has been suggested that HBeAg functions as an immunomodulator. We therefore examined the possibility that the two structural forms of the viral nucleoprotein, the particulate HBV core (HBcAg) and the nonparticulate HBeAg, may preferentially elicit different T helper (Th) cell subsets. For this purpose, mice were immunized with recombinant HBcAg and HBeAg in the presence and absence of adjuvants, and the immunoglobulin G (IgG) isotype profiles of anti-HBc and anti-HBe antibodies were determined. Second, in vitro cytokine production by HBcAg- and HBeAg-primed Th cells was measured. The immunogenicity of HBcAg, in contrast to that of HBeAg, did not require the use of adjuvants. Furthermore, HBcAg elicited primarily IgG2a and IgG2b anti-HBc antibodies, with a low level of IgG3, and no IgG1 anti-HBc antibodies. In contrast, the anti-HBe antibody response was dominated by the IgG1 isotype; low levels of IgG2a or IgG2b anti-HBe antibodies and no IgG3 anti-HBe antibodies were produced. Cytokine production by HBcAg- and HBeAg-primed Th cells was consistent with the IgG isotype profiles. HBcAg-primed Th cells efficiently produced interleukin-2 (IL-2) and gamma interferon (IFN-gamma) and low levels of IL-4. Conversely, efficient IL-4 production and lesser amounts of IFN-gamma were elicited by HBeAg immunization. The results indicate that HBcAg preferentially, but not exclusively, elicits Th1-like cells and that HBeAg preferentially, but not exclusively, elicits Th0 or Th2-like cells. Because HBcAg and the HBeAg are cross-reactive in terms of Th cell recognition, these findings demonstrate that Th cells with the same specificity can develop into different Th subsets based on the structural form of the immunogen. These results may have relevance to chronic HBV infection. Circulating HBeAg may downregulate antiviral clearance mechanisms by virtue of eliciting anti-inflammatory Th2-like cytokine production. Last, the influence of antigen structure on Th cell phenotype was not absolute and could be modulated by in vivo cytokine treatment. For example, IFN-alpha treatment inhibited HBeAg-specific Th2-mediated antibody production and altered the IgG anti-HBe isotype profile toward the Th1 phenotype.
乙型肝炎病毒(HBV)e抗原(HBeAg)的分泌在嗜肝DNA病毒的整个进化过程中一直保留。然而,这种病毒核蛋白分泌形式的功能仍然是个谜。有人提出HBeAg作为一种免疫调节剂发挥作用。因此,我们研究了病毒核蛋白的两种结构形式,即颗粒状的HBV核心(HBcAg)和非颗粒状的HBeAg,是否可能优先诱导不同的辅助性T(Th)细胞亚群。为此,在有佐剂和无佐剂的情况下,用重组HBcAg和HBeAg免疫小鼠,并测定抗HBc和抗HBe抗体的免疫球蛋白G(IgG)同种型谱。其次,测量由HBcAg和HBeAg致敏的Th细胞在体外产生的细胞因子。与HBeAg相比,HBcAg的免疫原性不需要使用佐剂。此外,HBcAg主要诱导产生IgG2a和IgG2b抗HBc抗体,IgG3水平较低,且不产生IgG1抗HBc抗体。相反,抗HBe抗体反应以IgG1同种型为主;产生低水平的IgG2a或IgG2b抗HBe抗体,不产生IgG3抗HBe抗体。由HBcAg和HBeAg致敏的Th细胞产生的细胞因子与IgG同种型谱一致。由HBcAg致敏的Th细胞有效产生白细胞介素-2(IL-2)和γ干扰素(IFN-γ),IL-4水平较低。相反,HBeAg免疫诱导产生高效的IL-4和少量的IFN-γ。结果表明,HBcAg优先但非唯一地诱导Th1样细胞,而HBeAg优先但非唯一地诱导Th0或Th2样细胞。由于HBcAg和HBeAg在Th细胞识别方面具有交叉反应性,这些发现表明具有相同特异性的Th细胞可根据免疫原的结构形式发育成不同的Th亚群。这些结果可能与慢性HBV感染有关。循环中的HBeAg可能通过诱导产生抗炎性Th2样细胞因子而下调抗病毒清除机制。最后,抗原结构对Th细胞表型的影响不是绝对的,可通过体内细胞因子治疗进行调节。例如,IFN-α治疗可抑制HBeAg特异性Th2介导的抗体产生,并使抗HBe IgG同种型谱向Th1表型改变。
