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大鼠钙调蛋白结合肽酶 19 蛋白及其长型 PEP-19 同工型的 RNA 结合活性。

RNA-binding activity of the rat calmodulin-binding PEP-19 protein and of the long PEP-19 isoform.

机构信息

Dipartimenti di Scienze e Tecnologie Molecolari e Biomolecolari, Università degli Studi di Palermo, Palermo, Italy.

出版信息

Int J Mol Med. 2012 Feb;29(2):141-5. doi: 10.3892/ijmm.2011.819. Epub 2011 Oct 20.

Abstract

Synthesis of H1˚ histone protein, in the developing rat brain, seems to be regulated mainly at the post-transcriptional level. Since regulation of RNA metabolism depends on a series of RNA-binding proteins, we have been searching for RNA-binding proteins involved in the post-transcriptional regulation of the H1˚ gene. We recently reported isolation, from a cDNA expression library, of an insert encoding a novel protein, the C-terminal half of which is identical to that of PEP-19, a brain-specific protein involved in calcium metabolism. The novel protein was called long PEP-19 isoform (LPI). Herein we show that LPI, as well as PEP-19, can bind H1˚ RNA. Moreover, in order to improve production of functional LPI/PEP-19, we modified the protocol normally adopted for preparing histidine tagged-proteins from bacteria, by adding an additional purification step. We also found that both LPI and PEP can compete for H1˚ RNA binding with PIPPin (CSD-C2), another RNA-binding protein previously discovered in our laboratory. Since PEP19/LPI contain a calmodulin binding domain, we finally investigated whether their ability to bind RNA is affected by calmodulin. Our results show that calmodulin interferes with binding of H1˚ RNA to both PEP-19 and LPI, while it is not able to bind RNA on its own. This finding suggests that calcium/calmodulin may have a role in controlling H1˚ mRNA metabolism in the developing brain.

摘要

H1˚组蛋白蛋白的合成,在发育中的大鼠脑中,似乎主要受转录后水平调控。由于 RNA 代谢的调节依赖于一系列 RNA 结合蛋白,我们一直在寻找参与 H1˚基因转录后调控的 RNA 结合蛋白。我们最近报道了从 cDNA 表达文库中分离出一个插入片段,该插入片段编码一种新的蛋白质,其 C 末端与参与钙代谢的脑特异性蛋白 PEP-19 相同。这种新的蛋白质被称为长 PEP-19 同种型(LPI)。在此,我们表明 LPI 与 PEP-19 一样可以结合 H1˚ RNA。此外,为了提高功能性 LPI/PEP-19 的产量,我们修改了通常用于从细菌中制备组氨酸标记蛋白的方案,增加了一个额外的纯化步骤。我们还发现,LPI 和 PEP 都可以与我们实验室先前发现的另一种 RNA 结合蛋白 PIPPin(CSD-C2)竞争结合 H1˚ RNA。由于 PEP19/LPI 含有钙调蛋白结合结构域,我们最终研究了它们结合 RNA 的能力是否受钙调蛋白的影响。我们的结果表明,钙调蛋白干扰 H1˚ RNA 与 PEP-19 和 LPI 的结合,而自身不能结合 RNA。这一发现表明,钙/钙调蛋白可能在控制发育中大脑 H1˚ mRNA 代谢中发挥作用。

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