血红素加氧酶-1 多态性可能影响 HCV 复制，并且在人源化小鼠中对不同疗效的治疗反应也有影响。

Haem oxygenase-1 polymorphisms can affect HCV replication and treatment responses with different efficacy in humanized mice.

机构信息

I. Department of Medicine, Center for Internal Medicine, University Medical Center Hamburg-Eppendorf, Hamburg, Germany.

Institute of Experimental Immunology and Hepatology, University Medical Center Hamburg-Eppendorf, Hamburg, Germany.

出版信息

Liver Int. 2017 Aug;37(8):1128-1137. doi: 10.1111/liv.13347. Epub 2017 Jan 25.

DOI:10.1111/liv.13347

PMID:27992676

Abstract

BACKGROUND & AIMS: Enhancement of host anti-oxidant enzymes, such as haemoxygenase-1, may attenuate virus-mediated hepatocyte injury, while the induction of HO-1 by cobalt-protoporphyrin-IX (CoPP) administration, as the application of its haem degradation product biliverdin (BV), was shown to hinder HCV replication in vitro. In addition, (GT) -repeats length in the polymorphic region of the HO-1 promoter may affect HO-1 expression and responsiveness to infection and disease severity. Aim of this study was to investigate the antiviral and hepatoprotective effects of CoPP-mediated HO-1 induction, alone or in combination with interferon alpha (peg-IFNα), in HCV-infected mice harbouring hepatocytes from donors with different HO-1-promoter polymorphisms.

METHODS

Upon establishment of HCV infection, CoPP, BV and peg-IFNα were given alone or in combination. Viraemia changes and intrahepatic human gene expression were determined by qRT-PCR and immunohistochemistry.

RESULTS

CoPP administration increased human HO-1 expression and significantly reduced viraemia, although changes correlated with promoter length (Δ0.5log and Δ2log reduction with medium- and short-polymorphism respectively). Polymorphisms did not influence BV-mediated antiviral effects (Δ1log). Notably, HO-1 induction attenuated basal HCV-driven enhancement of interferon genes and pro-inflammatory cytokines, both in cells with short- or medium-polymorphisms. Moreover, simultaneous administration of CoPP and peg-IFNα reduced viraemia even stronger (median 3log), whereas 1log viraemia reduction was determined in mice receiving peg-IFNα monotherapy.

CONCLUSIONS

Although the protective function of HO-1 could be elicited in vivo with both host polymorphisms, the strength of HO-1 induction and suppression of HCV occurred in a polymorphism-dependent manner, indicating that host-genetic determinants may affect disease progression and infection outcome.

摘要

背景与目的

增强宿主抗氧化酶，如血红素加氧酶-1（HO-1），可能减轻病毒介导的肝细胞损伤，而钴原卟啉-IX（CoPP）给药诱导 HO-1 的产生，作为其血红素降解产物胆红素（BV）的应用，已被证明可抑制 HCV 在体外的复制。此外，HO-1 启动子多态性区域的（GT）-重复长度可能影响 HO-1 的表达以及对感染和疾病严重程度的反应性。本研究的目的是研究 CoPP 介导的 HO-1 诱导，单独或与干扰素 alpha（peg-IFNα）联合应用，对携带不同 HO-1 启动子多态性供体肝细胞的 HCV 感染小鼠的抗病毒和肝保护作用。

方法

在建立 HCV 感染后，单独或联合给予 CoPP、BV 和 peg-IFNα。通过 qRT-PCR 和免疫组织化学检测病毒血症变化和肝内人基因表达。

结果

CoPP 给药增加了人 HO-1 的表达，并显著降低了病毒血症，尽管变化与启动子长度相关（中-短多态性分别降低 0.5log 和 2log）。多态性不影响 BV 介导的抗病毒作用（1log）。值得注意的是，HO-1 诱导减弱了具有短或中多态性的细胞中基础 HCV 驱动的干扰素基因和促炎细胞因子的增强，同时给予 CoPP 和 peg-IFNα 甚至更强地降低了病毒血症（中位数 3log），而在接受 peg-IFNα 单药治疗的小鼠中则降低了 1log 病毒血症。