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干扰素的糖基化。衣霉素对人免疫干扰素的影响。

Glycosylation of interferons. Effects of tunicamycin on human immune interferon.

作者信息

Mizrahi A, O'Malley J A, Carter W A, Takatsuki A, Tamura G, Sulkowski E

出版信息

J Biol Chem. 1978 Nov 10;253(21):7612-5.

PMID:701277
Abstract

Human immune interferon, induced in leukocytes by phytohemagglutinin, was prepared in the absence and presence of tunicamycin, an antibiotic which selectively inhibits the glycosylation of newly synthesized glycoproteins. Interferon preparations, produced in the absence of the antibiotic, displayed a considerable chromatographic heterogeneity on: (a) concanavalin A-agarose, (b) phenyl-agarose, (c) Cibacron Blue F3GA-agarose, and (d) polyuridylic acid-agarose. This heterogeneity was completely eliminated when tunicamycin (2 microgram/ml) was present during induction of interferon; all activity was then recovered in the breakthrough fractions from all sorbents. The level of interferon activity in leukocyte culture fluid was not affected by tunicamycin within the range of concentration 0.05 to 2.0 microgram/ml. These data indicate that (a) human immune interferon undergoes glycosylation, and tunicamycin is an effective inhibitor of this process. Thus, it appears that (b) at least some of the carbohydrates of human immune interferon are N-glycosidically linked. Moreover, it seems that (c) glycosylation is not necessary for an interferon molecule to either be secreted by the cell or (d) to express its antiviral function. Such properties of human immune interferon as (e) the apparent hydrophobicity and (f) an affinity for a polyribonucleotide are conferred only when its glycosylation is unimpaired.

摘要

人免疫干扰素是由植物血凝素在白细胞中诱导产生的,在有无衣霉素(一种能选择性抑制新合成糖蛋白糖基化的抗生素)的情况下制备。在无抗生素条件下产生的干扰素制剂在以下几种介质上表现出相当大的色谱异质性:(a)伴刀豆球蛋白A-琼脂糖、(b)苯基琼脂糖、(c)汽巴蓝F3GA-琼脂糖和(d)聚尿苷酸-琼脂糖。当在干扰素诱导过程中加入衣霉素(2微克/毫升)时,这种异质性完全消除;此时所有活性都在所有吸附剂的穿透组分中回收。在0.05至2.0微克/毫升的浓度范围内,衣霉素对白细胞培养液中的干扰素活性水平没有影响。这些数据表明:(a)人免疫干扰素会发生糖基化,衣霉素是这一过程的有效抑制剂。因此,似乎(b)人免疫干扰素的至少一些碳水化合物是以N-糖苷键连接的。此外,似乎(c)糖基化对于干扰素分子被细胞分泌或(d)发挥其抗病毒功能并非必需。人免疫干扰素的诸如(e)明显的疏水性和(f)对聚核糖核苷酸的亲和力等特性只有在其糖基化未受损害时才会赋予。

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