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泛素交叉反应蛋白的缀合物呈细胞骨架模式分布。

Conjugates of ubiquitin cross-reactive protein distribute in a cytoskeletal pattern.

作者信息

Loeb K R, Haas A L

机构信息

Department of Biochemistry, Medical College of Wisconsin, Milwaukee 53226.

出版信息

Mol Cell Biol. 1994 Dec;14(12):8408-19. doi: 10.1128/mcb.14.12.8408-8419.1994.

Abstract

Ubiquitin cross-reactive protein (UCRP), a 15-kDa interferon-induced protein, is a sequence homolog of ubiquitin that is covalently ligated to intracellular proteins in a parallel enzymatic reaction and is found at low levels within cultured cell lines and human tissues not exposed to interferon. Ubiquitin and UCRP ligation reactions apparently target distinct subsets of intracellular proteins, as judged from differences in the distributions of the respective adducts revealed on immunoblots. In this study, successive passages of the human lung carcinoma line A549 in the presence of neutralizing antibodies against alpha and beta interferons had no effect on the levels of either free or conjugated UCRP, indicating that these UCRP pools are constitutively present within uninduced cells and are thus not a consequence of autoinduction by low levels of secreted alpha/beta interferon. In an effort to identify potential targets for UCRP conjugation, the immunocytochemical distribution of UCRP was examined by using affinity-purified polyclonal antibodies against recombinant polypeptide. UCRP distributes in a punctate cytoskeletal pattern that is resistant to extraction by nonionic detergents (e.g., Triton X-100) in both uninduced and interferon-treated A549 cells. The cytoskeletal pattern colocalizes with the intermediate filament network of epithelial and mesothelial cell lines. Immunoblots of parallel Triton X-100-insoluble cell extracts suggest that the cytoskeletal association largely results from the noncovalent association of UCRP conjugates with the intermediate filaments rather than direct ligation of the polypeptide to structural components of the filaments. A significant increase in the sequestration of UCRP adducts on intermediate filaments accompanies interferon induction. These results suggest that UCRP may serve as a trans-acting binding factor directing the association of ligated target proteins to intermediate filaments.

摘要

泛素交叉反应蛋白(UCRP)是一种15千道尔顿的干扰素诱导蛋白,是泛素的序列同源物,在平行酶促反应中与细胞内蛋白质共价连接,在未接触干扰素的培养细胞系和人体组织中含量较低。从免疫印迹上显示的各自加合物分布差异判断,泛素和UCRP连接反应显然针对细胞内蛋白质的不同亚群。在本研究中,人肺癌细胞系A549在存在抗α和β干扰素的中和抗体的情况下连续传代,对游离或结合型UCRP的水平均无影响,这表明这些UCRP库在未诱导的细胞中是组成性存在的,因此不是低水平分泌的α/β干扰素自动诱导的结果。为了确定UCRP结合的潜在靶点,使用针对重组多肽的亲和纯化多克隆抗体检测了UCRP的免疫细胞化学分布。在未诱导和经干扰素处理的A549细胞中,UCRP均以点状细胞骨架模式分布,这种模式对非离子去污剂(如Triton X-100)的提取具有抗性。细胞骨架模式与上皮和间皮细胞系的中间丝网络共定位。平行的Triton X-100不溶性细胞提取物的免疫印迹表明,细胞骨架关联主要是由于UCRP加合物与中间丝的非共价结合,而不是多肽直接与丝的结构成分连接。干扰素诱导后,中间丝上UCRP加合物的隔离显著增加。这些结果表明,UCRP可能作为一种反式作用结合因子,指导连接的靶蛋白与中间丝的关联。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4994/359380/55cc03faae61/molcellb00012-0742-a.jpg

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