Department of Genetics, The University of North Carolina at Chapel Hill, Chapel Hill, North Carolina, USA.
UNCG Center for Translational Biomedical Research, North Carolina Research Campus, Kannapolis, North Carolina, USA.
J Virol. 2021 May 10;95(11):e0005821. doi: 10.1128/JVI.00058-21.
Iminosugar compounds are monosaccharide mimetics with broad but generally weak antiviral activities related to inhibition of enzymes involved in glycobiology. Miglustat (-butyl-1-deoxynojirimycin), which is approved for the treatment of lipid storage diseases in humans, and UV-4 [-(9-methoxynonyl)-1-deoxynojirimycin] inhibit the replication of hepatitis A virus (HAV) in cell culture (50% inhibitory concentrations [ICs] of 32.13 μM and 8.05 μM, respectively) by blocking the synthesis of gangliosides essential for HAV cell entry. We used a murine model of hepatitis A and targeted mass spectrometry to assess the capacity of these compounds to deplete hepatic gangliosides and modify the course of HAV infection . Miglustat, given by gavage to mice (4,800 mg/kg of body weight/day) depleted hepatic gangliosides by 69 to 75% but caused substantial gastrointestinal toxicity and failed to prevent viral infection. UV-4, similarly administered in high doses (400 mg/kg/day), was well tolerated but depleted hepatic gangliosides by only 20% after 14 days. UV-4 depletion of gangliosides varied by class. Several GM2 species were paradoxically increased, likely due to inhibition of β-glucosidases that degrade gangliosides. Both compounds enhanced, rather than reduced, virus replication. Nonetheless, both iminosugars had surprising anti-inflammatory effects, blocking the accumulation of inflammatory cells within the liver. UV-4 treatment also resulted in a decrease in serum alanine aminotransferase (ALT) elevations associated with acute hepatitis A. These anti-inflammatory effects may result from iminosugar inhibition of cellular α-glucosidases, leading to impaired maturation of glycan moieties of chemokine and cytokine receptors, and point to the potential importance of paracrine signaling in the pathogenesis of acute hepatitis A. Hepatitis A virus (HAV) is a common cause of viral hepatitis. Iminosugar compounds block its replication in cultured cells by inhibiting the synthesis of gangliosides required for HAV cell entry but have not been tested for their ability to prevent or treat hepatitis A . We show that high doses of the iminosugars miglustat and UV-4 fail to deplete gangliosides sufficiently to block HAV infection in mice lacking a key interferon receptor. These compounds nonetheless have striking anti-inflammatory effects on the HAV-infected liver, reducing the severity of hepatitis despite enhancing chemokine and cytokine expression resulting from hepatocyte-intrinsic antiviral responses. We propose that iminosugar inhibition of cellular α-glucosidases impairs the maturation of glycan moieties of chemokine and cytokine receptors required for effective signaling. These data highlight the potential importance of paracrine signaling pathways in the inflammatory response to HAV and add to our understanding of HAV pathogenesis in mice.
氨基糖化合物是单糖类似物,具有广泛但通常较弱的抗病毒活性,与参与糖生物学的酶的抑制有关。米格列醇(-丁基-1-去氧野尻霉素)已获批准用于治疗人类的脂质贮积病,而 UV-4 [-(9-甲氧基壬基)-1-去氧野尻霉素]通过阻断用于 HAV 细胞进入的神经节苷脂的合成来抑制甲型肝炎病毒(HAV)在细胞培养物中的复制(分别为 32.13 μM 和 8.05 μM 的 50%抑制浓度 [ICs])。我们使用甲型肝炎的小鼠模型和靶向质谱法来评估这些化合物耗尽肝神经节苷脂的能力,并改变 HAV 感染的过程。米格列醇通过灌胃给予小鼠(每天 4800mg/kg 体重),肝神经节苷脂减少了 69%至 75%,但引起了严重的胃肠道毒性,并未能预防病毒感染。UV-4 以高剂量(每天 400mg/kg)同样给予,耐受性良好,但 14 天后仅减少了 20%的肝神经节苷脂。UV-4 对神经节苷脂的消耗因类别而异。几种 GM2 物种被反常地增加,可能是由于抑制了降解神经节苷脂的β-葡萄糖苷酶。这两种化合物都增强了,而不是降低了病毒复制。尽管如此,两种氨基糖都具有令人惊讶的抗炎作用,可阻止肝脏内炎症细胞的积聚。UV-4 治疗还导致与急性甲型肝炎相关的血清丙氨酸氨基转移酶(ALT)升高的降低。这些抗炎作用可能是由于氨基糖抑制细胞内的α-葡萄糖苷酶,导致趋化因子和细胞因子受体的聚糖部分的成熟受损,并表明旁分泌信号在急性甲型肝炎发病机制中的潜在重要性。甲型肝炎病毒(HAV)是病毒性肝炎的常见原因。氨基糖化合物通过抑制 HAV 细胞进入所需的神经节苷脂的合成来阻止其在培养细胞中的复制,但尚未测试它们预防或治疗甲型肝炎的能力。我们表明,高剂量的氨基糖米格列醇和 UV-4 不足以耗尽神经节苷脂以阻止缺乏关键干扰素受体的小鼠中的 HAV 感染。尽管这些化合物对 HAV 感染的肝脏具有显著的抗炎作用,但尽管增强了由于肝细胞内抗病毒反应而导致的趋化因子和细胞因子的表达,仍降低了肝炎的严重程度。我们提出,氨基糖抑制细胞内的α-葡萄糖苷酶会损害有效信号所需的趋化因子和细胞因子受体的聚糖部分的成熟。这些数据突出了旁分泌信号通路在 HAV 炎症反应中的潜在重要性,并增加了我们对小鼠中 HAV 发病机制的理解。
