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治疗性干扰素天然形式和变体形式的生物活性测定。

Bioactivity determination of native and variant forms of therapeutic interferons.

作者信息

Larocque Louise, Bliu Alex, Xu Ranran, Diress Abebaw, Wang Junzhi, Lin Rongtuan, He Runtao, Girard Michel, Li Xuguang

机构信息

Biologics and Genetic Therapies Directorate, Health Canada, Tunney's Pasture, Ottawa, ON, Canada K1A 0K9.

出版信息

J Biomed Biotechnol. 2011;2011:174615. doi: 10.1155/2011/174615. Epub 2011 Mar 3.

Abstract

The traditional antiviral assays for the determination of interferon potency are reported to have considerable variability between and within assays. Although several reporter gene assays based on interferon-inducible promoter activities have been reported, data from comprehensive validation studies are lacking and few studies have been conducted to analyze the variant forms of interferons, which could have undesirable clinical implications. Here, a reporter gene assay employing a HEK293 cell line stably transfected with luciferase gene under the control of interferon-stimulated response element promoter was developed and validated. The assay was found to be more sensitive, with a larger detection range than the antiviral assay. Several cytokines tested did not interfere with the test, suggesting the assay possesses a certain degree of selectivity. Moreover, the robustness of the assay was demonstrated by minimal variations in the results generated by different analysts and cell passage number (up to 52 passages). Finally, the method was employed to analyze several interferon variants (interferon-α 2a) and we found that the aggregated form has completely lost its potency; while a modest loss of bioactivity in oxidized interferon was observed (approx. 23%), the deamidated form essentially retained its activity.

摘要

据报道,用于测定干扰素效价的传统抗病毒检测方法在不同检测之间以及同一检测内部都存在相当大的变异性。尽管已经报道了几种基于干扰素诱导型启动子活性的报告基因检测方法,但缺乏来自全面验证研究的数据,并且很少有研究分析干扰素的变体形式,而这些变体可能具有不良的临床意义。在此,开发并验证了一种报告基因检测方法,该方法使用在干扰素刺激反应元件启动子控制下稳定转染荧光素酶基因的HEK293细胞系。结果发现该检测方法比抗病毒检测方法更灵敏,检测范围更大。测试的几种细胞因子不干扰该检测,表明该检测具有一定程度的选择性。此外,不同分析人员和细胞传代次数(高达52代)产生的结果变化极小,证明了该检测方法的稳健性。最后,该方法用于分析几种干扰素变体(干扰素-α 2a),我们发现聚集形式完全丧失了其效力;虽然观察到氧化型干扰素的生物活性有适度损失(约23%),但脱酰胺形式基本保留了其活性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e291/3051158/f23b87778a40/JBB2011-174615.001.jpg

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