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一种在人乳腺癌组织中表达的、缺乏串联重复序列的新型MUC1蛋白的特性鉴定与分子克隆。

Characterization and molecular cloning of a novel MUC1 protein, devoid of tandem repeats, expressed in human breast cancer tissue.

作者信息

Zrihan-Licht S, Vos H L, Baruch A, Elroy-Stein O, Sagiv D, Keydar I, Hilkens J, Wreschner D H

机构信息

Department of Cell Research and Immunology, George S. Wise Faculty of Life Sciences, Tel Aviv University, Ramat Aviv, Israel.

出版信息

Eur J Biochem. 1994 Sep 1;224(2):787-95. doi: 10.1111/j.1432-1033.1994.00787.x.

Abstract

The human breast cancer marker protein, MUC1, is a polymorphic transmembrane molecule containing a large extracellular domain that is primarily composed of a variable number of highly conserved 20-amino-acid tandem repeats. We report here the detection of a novel invariantly sized 1.2-kb MUC1 mRNA, in addition to the large polymorphic mRNAs, by probing Northern blots with MUC1-cDNA-unique-sequence probes. The nucleotide sequence of this novel MUC1 mRNA demonstrates that it is identical to the MUC1 cDNA sequences downstream and upstream to the tandem-repeat array of the transmembrane form of MUC1. However, it contains neither the central tandem repeat array itself nor its directly flanking sequences that are deleted by a differential splicing event utilizing splice acceptor and donor sequences 5' and 3' to the tandem-repeat array. The splice event retains, downstream to the splice acceptor site, an open reading frame identical to that of the repeat-array-containing MUC1 thereby generating the novel MUC1/Y protein. Cells transiently transfected with the novel MUC1/Y cDNA express the MUC1/Y protein that is modified by glycosylation. The MUC1/Y protein is also readily detected in human breast cancer cells grown in vitro. Furthermore, primary breast cancer tissue samples demonstrate significant levels of the MUC1/Y protein whereas expression in tissue adjacent to the tumor is undetectable. Molecular characterization presented here, of the novel MUC1/Y molecule lacking the repeat array, suggests that it is likely to play a role distinct to that of the polymorphic repeat-array-positive MUC1 protein and that it may act as a new marker protein for human breast cancer.

摘要

人乳腺癌标志物蛋白MUC1是一种多态性跨膜分子,其细胞外结构域较大,主要由数量可变的高度保守的20个氨基酸的串联重复序列组成。我们在此报告,通过用MUC1 - cDNA独特序列探针探测Northern印迹,除了检测到大量多态性mRNA外,还发现了一种大小恒定的新型1.2 kb MUC1 mRNA。这种新型MUC1 mRNA的核苷酸序列表明,它与MUC1跨膜形式串联重复序列阵列上下游的MUC1 cDNA序列相同。然而,它既不包含中央串联重复序列阵列本身,也不包含其直接侧翼序列,这些序列通过利用串联重复序列阵列5'和3'端的剪接受体和供体序列的差异剪接事件而缺失。剪接事件在剪接受体位点下游保留了一个与含重复序列阵列的MUC1相同的开放阅读框,从而产生了新型MUC1/Y蛋白。用新型MUC1/Y cDNA瞬时转染的细胞表达经糖基化修饰的MUC1/Y蛋白。在体外培养的人乳腺癌细胞中也很容易检测到MUC1/Y蛋白。此外,原发性乳腺癌组织样本中MUC1/Y蛋白水平显著,而肿瘤相邻组织中未检测到其表达。本文对缺乏重复序列阵列的新型MUC1/Y分子进行的分子特征分析表明,它可能发挥与多态性重复序列阵列阳性的MUC1蛋白不同的作用,并且可能作为人乳腺癌的一种新的标志物蛋白。

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