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人肿瘤坏死因子的分子克隆与表达及其与小鼠肿瘤坏死因子的比较

Molecular cloning and expression of human tumor necrosis factor and comparison with mouse tumor necrosis factor.

作者信息

Marmenout A, Fransen L, Tavernier J, Van der Heyden J, Tizard R, Kawashima E, Shaw A, Johnson M J, Semon D, Müller R

出版信息

Eur J Biochem. 1985 Nov 4;152(3):515-22. doi: 10.1111/j.1432-1033.1985.tb09226.x.

Abstract

U-937 cells, a monocytic line derived from a human histiocytic lymphoma, were induced for human tumor necrosis factor (TNF) secretion into the medium and were used for the preparation of TNF mRNA. Biological activity of the latter was quantified in a Xenopus laevis oocyte injection system. TNF mRNA was enriched by gradient centrifugation and this size-fractionated mRNA was used for synthesis of cDNA and inserted into the unique PstI site of pAT153. A recombinant plasmid containing human TNF cDNA was selected by colony hybridization using an internal fragment of a mouse TNF cDNA clone [Fransen, L., Mueller, R., Marmenout, A., Tavernier, J., Van der Heyden, J., Kawashima, E., Chollet, A., Tizard, R., Van Heuverswyn, H., Van Vliet, A., Ruysschaert, M. R. & Fiers, W. (1985) Nucleic Acids Res. 13, 4417-4429] as a probe. The sequence of this human TNF cDNA is in agreement with the one published by Pennica et al. [Pennica, D., Nedwin, G. E., Hayflick, J. S., Seeburg, P. H., Derynck, R., Palladino, M. A., Kohr, W. J., Aggarwal, B. B. & Goeddel, D. V. (1984) Nature (Lond.) 312, 724-729]. The 157-amino-acid-long mature sequence is about 80% homologous to mouse TNF and its hydrophilicity plot is also very similar, in spite of the apparent species specificity of TNF. In contrast to mouse TNF, it contains no potential N-glycosylation site. When compared to other cytokines, like IFN-beta, IFN-gamma, or IL-2, there is a remarkably high preference for G X C pairs in the third-letter positions. Expression of the TNF cDNA in monkey COS cells or in Escherichia coli gives rise to a protein having similar biological and serological properties as natural human TNF. A human genomic clone was also identified and sequenced; it was found to be in good agreement with the one recently published by Shirai et al. [Shirai, T., Yamaguchi, H., Ito, H., Todd, C. W. & Wallace, R. B. (1985) Nature (Lond.) 313, 803-806], except for some differences in the introns and 5'-untranslated region.

摘要

U - 937细胞系源自人类组织细胞淋巴瘤的单核细胞系,经诱导使其向培养基中分泌人肿瘤坏死因子(TNF),并用于制备TNF mRNA。后者的生物活性在非洲爪蟾卵母细胞注射系统中进行定量。TNF mRNA通过梯度离心进行富集,这种按大小分级分离的mRNA用于合成cDNA,并插入pAT153的独特PstI位点。使用小鼠TNF cDNA克隆的内部片段[弗兰森,L.,米勒,R.,马尔梅努特,A.,塔维尼耶,J.,范德海登,J.,川岛,E.,乔莱,A.,蒂扎德,R.,范赫弗斯温,H.,范弗利特,A.,鲁伊斯沙尔特,M. R.和菲尔斯,W.(1985年)《核酸研究》13卷,4417 - 4429页]作为探针,通过菌落杂交筛选出含有人TNF cDNA的重组质粒。这人TNF cDNA的序列与彭尼卡等人发表的序列一致[彭尼卡,D.,内德温,G. E.,海弗利克,J. S.,西伯尔格,P. H.,德里尼克,R.,帕拉迪诺,M. A.,科尔,W. J.,阿加瓦尔,B. B.和戈德尔,D. V.(1984年)《自然》(伦敦)312卷,724 - 729页]。157个氨基酸长的成熟序列与小鼠TNF约80%同源,尽管TNF有明显的物种特异性,但其亲水性图谱也非常相似。与小鼠TNF不同,它不含潜在的N - 糖基化位点。与其他细胞因子如IFN - β、IFN - γ或IL - 2相比,在第三字母位置上对GXC碱基对有明显较高的偏好。TNF cDNA在猴COS细胞或大肠杆菌中的表达产生一种具有与天然人TNF相似生物学和血清学特性的蛋白质。还鉴定并测序了一个人类基因组克隆;发现它与白井等人最近发表的克隆[白井,T.,山口,H.,伊藤,H.,托德,C. W.和华莱士,R. B.(1985年)《自然》(伦敦)313卷,803 - 806页]基本一致,只是在内含子和5' - 非翻译区存在一些差异。

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