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首页> 外文期刊>BioMed research international >Construction of a Novel Liver-Targeting Fusion Interferon by Incorporation of aPlasmodiumRegion I-Plus Peptide
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Construction of a Novel Liver-Targeting Fusion Interferon by Incorporation of aPlasmodiumRegion I-Plus Peptide

机译:融合疟原虫区域I加肽的新型肝靶向融合干扰素的构建。

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Interferon alpha (IFNα) exerts a multiplicity of biological actions including antiviral, immunomodulatory, and antiproliferative effects. Administration of IFNαis the current treatment for chronic hepatitis B; however, therapy outcome has not been completely satisfactory. The systemic effects of IFNαmay account for its lowin vivobiological activity and multiple adverse events. The purpose of this study was to design a novel liver-targeting fusion interferon (IFN-CSP) by fusing IFNα2b with aPlasmodiumregion I-plus peptide, thus targeting the drug specifically to the liver. The DNA sequence encoding IFN-CSP was constructed using improved splicing by overlapping extension-PCR method, and then cloned into the pET-21b vector for protein expression inE. coliBL21 (DE3). The recombinant protein was expressed as a His-tagged protein and purified using a combination of Ni affinity and HiTrap affinity chromatography at a purity of over 95%. The final yield of biologically active IFN-CSP was up to 270 mg/L culture. The purified recombinant protein showed anti-HBV activity and liver-targeting potentialityin vitro. These data suggests that the novel fusion interferon IFN-CSP may be an excellent candidate as a liver-targeting anti-HBV agent.
机译:干扰素α(IFNα)发挥多种生物学作用,包括抗病毒,免疫调节和抗增殖作用。 IFNα的给药是目前治疗慢性乙型肝炎的方法。然而,治疗结果还不能完全令人满意。 IFNα的全身作用可能是其体内生物学活性低和多种不良事件的原因。这项研究的目的是通过将IFNα2b与疟原虫区域I-plus肽融合,从而设计一种靶向肝脏的新型肝靶向融合干扰素(IFN-CSP)。利用重叠延伸PCR法通过改进的剪接构建编码IFN-CSP的DNA序列,然后将其克隆到pET-21b载体中以在E中表达蛋白。 coliBL21(DE3)。重组蛋白被表达为His标签蛋白,并使用Ni亲和力和HiTrap亲和层析相结合纯化,纯度超过95%。具有生物活性的IFN-CSP的最终产量可达270μmg/ L。纯化的重组蛋白在体外具有抗HBV活性和肝靶向性。这些数据表明,新型融合干扰素IFN-CSP可能是靶向肝的抗HBV药物的优秀候选者。

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