Fos metamorphoses: Lessons from mutants in model organisms

IF 2.6 Q2 Medicine
Carlos Alfonso-Gonzalez , Juan Rafael Riesgo-Escovar
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引用次数: 22

Abstract

The Fos oncogene gene family is evolutionarily conserved throughout Eukarya. Fos proteins characteristically have a leucine zipper and a basic region with a helix-turn-helix motif that binds DNA. In vertebrates, there are several Fos homologs. They can homo- or hetero-dimerize via the leucine zipper domain. Fos homologs coupled with other transcription factors, like Jun oncoproteins, constitute the Activator Protein 1 (AP-1) complex. From its original inception as an oncogene, the subsequent finding that they act as transcription factors binding DNA sequences known as TRE, to the realization that they are activated in many different scenarios, and to loss-of-function analysis, the Fos proteins have traversed a multifarious path in development and physiology. They are instrumental in ‘immediate early genes’ responses, and activated by a seemingly myriad assemblage of different stimuli. Yet, the majority of these studies were basically gain-of-function studies, since it was thought that Fos genes would be cell lethal. Loss-of-function mutations in vertebrates were recovered later, and were not cell lethal. In fact, c-fos null mutations are viable with developmental defects (osteopetrosis and myeloid lineage abnormalities). It was then hypothesized that vertebrate genomes exhibit partial redundancy, explaining the ‘mild’ phenotypes, and complicating assessment of complete loss-of-function phenotypes. Due to its promiscuous activation, fos genes (especially c-fos) are now commonly used as markers for cellular responses to stimuli. fos homologs high sequence conservation (including Drosophila) is advantageous as it allows critical assessment of fos genes functions in this genetic model. Drosophila melanogaster contains only one fos homolog, the gene kayak. kayak mutations are lethal, and allow study of all the processes where fos is required. The kayak locus encodes several different isoforms, and is a pleiotropic gene variously required for development involving cell shape changes. In general, fos genes seem to primarily activate programs involved in cellular architectural rearrangements and cell shape changes.

Fos变态:从模式生物的突变中得到的教训
Fos致癌基因家族在整个真核生物中都是进化保守的。Fos蛋白的特征是具有亮氨酸拉链和一个结合DNA的螺旋-螺旋-螺旋基序的基本区域。在脊椎动物中,有几种Fos同源物。它们可以通过亮氨酸拉链结构域同源或异二聚。Fos同源物与其他转录因子(如Jun癌蛋白)偶联,构成激活蛋白1 (AP-1)复合物。从最初作为致癌基因开始,随后发现它们作为结合DNA序列TRE的转录因子,到认识到它们在许多不同的情况下被激活,再到功能丧失分析,Fos蛋白在发育和生理上经历了多种途径。它们在“即时早期基因”反应中起着重要作用,并被看似无数的不同刺激组合激活。然而,这些研究中的大多数基本上是功能获得性研究,因为人们认为Fos基因会对细胞致命。脊椎动物的功能丧失突变后来才恢复,并且不是细胞致命的。事实上,c-fos零突变在发育缺陷(骨质疏松症和髓系异常)中是可行的。然后假设脊椎动物基因组表现出部分冗余,解释了“轻度”表型,并使完全功能丧失表型的评估复杂化。由于其混杂激活,fos基因(特别是c-fos)现在通常用作细胞对刺激反应的标记。fos同源物的高序列保守性(包括果蝇)是有利的,因为它允许在该遗传模型中对fos基因功能进行关键评估。黑腹果蝇只含有一个fos同源基因,即皮艇基因。Kayak突变是致命的,并且允许研究所有需要fos的过程。kayak基因座编码几种不同的同工异构体,是一种多效性基因,在涉及细胞形状变化的发育中有不同的要求。一般来说,fos基因似乎主要激活涉及细胞结构重排和细胞形状改变的程序。
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来源期刊
Mechanisms of Development
Mechanisms of Development 生物-发育生物学
CiteScore
3.60
自引率
0.00%
发文量
0
审稿时长
12.4 weeks
期刊介绍: Mechanisms of Development is an international journal covering the areas of cell biology and developmental biology. In addition to publishing work at the interphase of these two disciplines, we also publish work that is purely cell biology as well as classical developmental biology. Mechanisms of Development will consider papers in any area of cell biology or developmental biology, in any model system like animals and plants, using a variety of approaches, such as cellular, biomechanical, molecular, quantitative, computational and theoretical biology. Areas of particular interest include: Cell and tissue morphogenesis Cell adhesion and migration Cell shape and polarity Biomechanics Theoretical modelling of cell and developmental biology Quantitative biology Stem cell biology Cell differentiation Cell proliferation and cell death Evo-Devo Membrane traffic Metabolic regulation Organ and organoid development Regeneration Mechanisms of Development does not publish descriptive studies of gene expression patterns and molecular screens; for submission of such studies see Gene Expression Patterns.
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