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发育和疾病中的可变内含子启动子。

Alternative intronic promoters in development and disease.

作者信息

Vacik Tomas, Raska Ivan

机构信息

Institute of Biology and Medical Genetics, First Faculty of Medicine, Charles University and General University Hospital in Prague, Albertov 4, Praha 2, Czech Republic.

出版信息

Protoplasma. 2017 May;254(3):1201-1206. doi: 10.1007/s00709-016-1071-y. Epub 2017 Jan 11.

Abstract

Approximately 20,000 mammalian genes are estimated to encode between 250 thousand and 1 million different proteins. This enormous diversity of the mammalian proteome is caused by the ability of a single-gene locus to encode multiple protein isoforms. Protein isoforms encoded by one gene locus can be functionally distinct, and they can even have antagonistic functions. One of the mechanisms involved in creating this proteome complexity is alternative promoter usage. Alternative intronic promoters are located downstream from their canonical counterparts and drive the expression of alternative RNA isoforms that lack upstream exons. These upstream exons can encode some important functional domains, and proteins encoded by alternative mRNA isoforms can be thus functionally distinct from the full-length protein encoded by canonical mRNA isoforms. Since any misbalance of functionally distinct protein isoforms is likely to have detrimental consequences for the cell and the whole organism, their expression must be precisely regulated. Misregulation of alternative intronic promoters is frequently associated with various developmental defects and diseases including cancer, and it is becoming increasingly clear that this phenomenon deserves more attention.

摘要

据估计,大约2万个哺乳动物基因可编码25万至100万个不同的蛋白质。哺乳动物蛋白质组的这种巨大多样性是由单个基因座编码多种蛋白质异构体的能力所导致的。由一个基因座编码的蛋白质异构体在功能上可能不同,甚至可能具有拮抗功能。造成这种蛋白质组复杂性的机制之一是可变启动子的使用。可变内含子启动子位于其典型对应物的下游,并驱动缺乏上游外显子的可变RNA异构体的表达。这些上游外显子可以编码一些重要的功能域,因此,由可变mRNA异构体编码的蛋白质在功能上可能与由典型mRNA异构体编码的全长蛋白质不同。由于功能不同的蛋白质异构体的任何失衡都可能对细胞和整个生物体产生有害影响,因此它们的表达必须受到精确调控。可变内含子启动子的失调常常与包括癌症在内的各种发育缺陷和疾病相关,而且越来越明显的是,这一现象值得更多关注。

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