Drug Discovery Antibody Platform Unit, RIKEN Center for Integrative Medical Sciences, Yokohama, Japan.
Laboratory for Inflammatory Regulation, RIKEN Center for Integrative Medical Sciences, Yokohama, Japan.
J Virol. 2022 Mar 9;96(5):e0168621. doi: 10.1128/JVI.01686-21. Epub 2022 Jan 5.
Hepatitis B virus (HBV) infects 240 million people worldwide. Current therapy profoundly suppresses HBV replication but requires long-term maintenance therapy. Therefore, there is still a medical need for an efficient HBV cure. HBV enters host cells by binding via the preS1 domain of the viral L protein to the Na/taurocholate cotransporting polypeptide (NTCP). Thus, NTCP should be a key target for the development of anti-HBV therapeutics. Indeed, myrcludex B, a synthetic form of the myristoylated preS1 peptide, effectively reduces HBV/hepatitis D virus (HDV) infection and has been approved as Hepcludex in Europe for the treatment of patients with chronic HDV infection. We established a monoclonal antibody (MAb), N6HB426-20, that recognizes the extracellular domain of human NTCP and blocks HBV entry into human liver cells but has much less of an inhibitory effect on bile acid uptake. , administration of the N6HB426-20 MAb prevented HBV viremia for an extended period of time after HBV inoculation in a mouse model system without strongly inhibiting bile acid absorption. Among the extracellular loops (ECLs) of NTCP, regions of amino acids (aa) 84 to 87 in ECL1 and aa 157 to 165 near ECL2 of transmembrane domain 5 are critically important for HBV/HDV infection. Epitope mapping and the three-dimensional (3D) model of the NTCP structure suggested that the N6HB426-20 MAb may recognize aa 276/277 at the tip of ECL4 and interfere with binding of HBV to the region from aa 84 to 87. In summary, we identified an neutralizing NTCP-targeting antibody capable of preventing HBV infection. Further improvements in efficacy of this drug will pave the way for its clinical applications. A number of entry inhibitors are being developed to enhance the treatment of HBV patients with oral nucleoside/nucleotide analogues (NA). To amplify the effectiveness of NA therapy, several efforts have been made to develop therapeutic MAbs with neutralizing activity against HBs antigens. However, the neutralizing effect of these MAbs may be muted by a large excess of HBsAg-positive noninfectious particles in the blood of infected patients. The advantage of NTCP-targeted HBV entry inhibitors is that they remain effective regardless of viral genotype, viral mutations, and the presence of subviral particles. Although N6HB426-20 requires a higher dose than myrcludex to obtain equivalent suppression of HBV in a model mouse system, it maintained the inhibitory effect for a long time postadministration in proportion to the half-life of an IgG MAb. We believe that further improvements will make this antibody a promising treatment option for patients with chronic hepatitis B.
乙型肝炎病毒(HBV)感染全球 2.4 亿人。目前的治疗方法可显著抑制 HBV 复制,但需要长期维持治疗。因此,仍然需要高效的 HBV 治愈方法。HBV 通过病毒 L 蛋白的前 S1 结构域与 Na/牛磺胆酸钠共转运多肽(NTCP)结合进入宿主细胞。因此,NTCP 应该是开发抗 HBV 治疗药物的关键靶点。事实上,合成的前 S1 肽(myristoylated preS1 peptide) 衍生物 myrcludex B 可有效降低 HBV/丁型肝炎病毒(HDV)感染,并已在欧洲被批准为 Hepcludex,用于治疗慢性 HDV 感染患者。我们开发了一种单克隆抗体(MAb)N6HB426-20,它识别人 NTCP 的细胞外结构域并阻断 HBV 进入人肝细胞,但对胆汁酸摄取的抑制作用要小得多。在小鼠模型系统中,HBV 接种后,N6HB426-20 MAb 的给药可在延长的时间内阻止 HBV 血症,而不会强烈抑制胆汁酸吸收。在 NTCP 的细胞外环(ECL)中,跨膜域 5 的 ECL1 中的氨基酸(aa)84 至 87 区域和 ECL2 附近的 aa157 至 165 区域对于 HBV/HDV 感染至关重要。表位作图和 NTCP 结构的三维(3D)模型表明,N6HB426-20 MAb 可能识别 ECL4 尖端的 aa276/277,并干扰 HBV 与 aa84 至 87 区域的结合。总之,我们鉴定出一种能够预防 HBV 感染的中和性靶向 NTCP 的抗体。进一步提高该药物的疗效将为其临床应用铺平道路。目前正在开发多种进入抑制剂以增强口服核苷/核苷酸类似物(NA)治疗 HBV 患者的效果。为了增强 NA 治疗的效果,已经做出了一些努力来开发具有中和 HBs 抗原活性的治疗性 MAb。然而,这些 MAb 的中和作用可能会因感染患者血液中大量 HBsAg 阳性无传染性颗粒而减弱。NTCP 靶向 HBV 进入抑制剂的优势在于,无论病毒基因型、病毒突变和亚病毒颗粒的存在如何,它们都能保持有效。虽然 N6HB426-20 在模型小鼠系统中获得与 myrcludex 相当的 HBV 抑制效果所需的剂量高于 myrcludex,但它在给药后的很长一段时间内保持抑制效果,与 IgG MAb 的半衰期成正比。我们相信,进一步的改进将使这种抗体成为慢性乙型肝炎患者的一种有前途的治疗选择。
