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Solution structure of a conserved C-terminal domain of p73 with structural homology to the SAM domain.

机译:与SAM结构域具有结构同源性的p73保守C端结构域的溶液结构。

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摘要

p73 and p63 are two recently cloned genes with homology to the tumor suppressor p53, whose protein product is a key transcriptional regulator of genes involved in cell cycle arrest and apoptosis. While all three proteins share conserved transcriptional activation, DNA-binding and oligomerization domains, p73 and p63 have an additional conserved C-terminal region. We have determined the three-dimensional solution structure of this conserved C-terminal domain of human p73. The structure reveals a small five-helix bundle with striking similarity to the SAM (sterile alpha motif) domains of two ephrin receptor tyrosine kinases. The SAM domain is a putative protein-protein interaction domain found in a variety of cytoplasmic signaling proteins and has been shown to form both homo- and hetero-oligomers. However, the SAM-like C-terminal domains of p73 and p63 are monomeric and do not interact with one another, suggesting that this domain may interact with additional, as yet uncharacterized proteins in a signaling and/or regulatory role.
机译:p73和p63是两个最近克隆的与肿瘤抑制因子p53有同源性的基因,其蛋白产物是参与细胞周期阻滞和凋亡的基因的关键转录调节因子。尽管所有这三种蛋白质共享保守的转录激活,DNA结合和寡聚化域,但p73和p63具有一个额外的保守C端区域。我们已经确定了人p73的这个保守的C末端域的三维解决方案结构。该结构揭示了一个小的五螺旋束,与两个ephrin受体酪氨酸激酶的SAM(无菌α基序)结构域具有惊人的相似性。 SAM结构域是在各种细胞质信号蛋白中发现的一种推定的蛋白质-蛋白质相互作用结构域,并且已显示可形成同型和异型寡聚体。但是,p73和p63的SAM样C末端结构域是单体的,彼此不相互作用,表明该结构域可能与其他尚未表征的蛋白相互作用,起信号传导和/或调节作用。

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