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高度糖基化的人α干扰素:一种新治疗候选药物的深入了解。

Highly glycosylated human alpha interferon: An insight into a new therapeutic candidate.

机构信息

Laboratorio de Cultivos Celulares, Facultad de Bioquímica y Ciencias Biológicas, Universidad Nacional del Litoral, Ciudad Universitaria, Paraje El Pozo-C.C. 242 (S3000ZAA) Santa Fe, Argentina.

出版信息

J Biotechnol. 2010 Mar;146(1-2):74-83. doi: 10.1016/j.jbiotec.2009.12.020. Epub 2010 Jan 11.

DOI:10.1016/j.jbiotec.2009.12.020
PMID:20067809
Abstract

The type I human interferon alpha (hIFN-alpha) family consists of small proteins that exert a multiplicity of biological actions including antiviral, antiproliferative and immunomodulatory effects. However, though administration of recombinant hIFN-alpha2b is the current treatment for chronic hepatitis B and C and for some types of cancers, therapy outcomes have not been completely satisfactory. The short serum half-life and rapid clearance of the cytokine accounts for its low in vivo biological activity. Here we describe and characterize a long-acting rhIFN-alpha2b mutein, 4N-IFN, which has been created by introducing four N-glycosylation sites via site-directed mutagenesis. The hyperglycosylated protein was found to have a 25-fold longer plasma half-life than the non-glycosylated rhIFN-alpha2b, even greater than the commercial pegylated derivative Intron-A PEG. In addition, glycosylation increased the in vitro stability of the mutein against serum protease inactivation. Interestingly, despite its lower in vitro activity, 4N-IFN showed a markedly enhanced in vivo antitumor activity in human prostate carcinoma implanted in nude mice. MALDI-TOF MS and HPAEC-PAD carbohydrate analyses revealed the presence of high amounts of tetrasialylated (40%) and trisialylated (28%) N-glycan structures, which are consequently responsible for the improved characteristics of the cytokine, making 4N-IFN a new therapeutic candidate for viral and malignant diseases.

摘要

I 型人干扰素 alpha(hIFN-alpha)家族由多种生物学功能的小蛋白组成,包括抗病毒、抗增殖和免疫调节作用。然而,尽管重组 hIFN-alpha2b 的给药是慢性乙型和丙型肝炎以及某些类型癌症的当前治疗方法,但治疗结果并不完全令人满意。细胞因子的血清半衰期短和快速清除导致其体内生物活性低。在这里,我们描述并表征了一种长效 rhIFN-alpha2b 突变体 4N-IFN,它是通过定点突变引入四个 N-糖基化位点而创建的。该高度糖基化的蛋白质被发现具有比非糖基化 rhIFN-alpha2b 长 25 倍的血浆半衰期,甚至超过了商业聚乙二醇化衍生物 Intron-A PEG。此外,糖基化增加了突变体对血清蛋白酶失活的体外稳定性。有趣的是,尽管其体外活性较低,但 4N-IFN 在植入裸鼠的人前列腺癌中的体内抗肿瘤活性明显增强。MALDI-TOF MS 和 HPAEC-PAD 碳水化合物分析显示存在大量四唾液酸化(40%)和三唾液酸化(28%)N-聚糖结构,这是细胞因子改善特性的原因,使 4N-IFN 成为病毒和恶性疾病的新治疗候选物。

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