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对细菌中PII信号转导蛋白新靶点的研究确定了乙酰辅酶A羧化酶的生物素羧基载体蛋白组分是一种PII结合伴侣。

Search for novel targets of the PII signal transduction protein in Bacteria identifies the BCCP component of acetyl-CoA carboxylase as a PII binding partner.

作者信息

Rodrigues Thiago E, Gerhardt Edileusa C M, Oliveira Marco A, Chubatsu Leda S, Pedrosa Fabio O, Souza Emanuel M, Souza Gustavo A, Müller-Santos Marcelo, Huergo Luciano F

机构信息

Instituto Nacional de Ciência e Tecnologia da Fixação Biológica de Nitrogênio, Departamento de Bioquímica e Biologia Molecular, UFPR, Curitiba, PR, Brazil.

出版信息

Mol Microbiol. 2014 Feb;91(4):751-61. doi: 10.1111/mmi.12493. Epub 2014 Jan 6.

Abstract

The PII family comprises a group of widely distributed signal transduction proteins. The archetypal function of PII is to regulate nitrogen metabolism in bacteria. As PII can sense a range of metabolic signals, it has been suggested that the number of metabolic pathways regulated by PII may be much greater than described in the literature. In order to provide experimental evidence for this hypothesis a PII protein affinity column was used to identify PII targets in Azospirillum brasilense. One of the PII partners identified was the biotin carboxyl carrier protein (BCCP), a component of the acetyl-CoA carboxylase which catalyses the committed step in fatty acid biosynthesis. As BCCP had been previously identified as a PII target in Arabidopsis thaliana we hypothesized that the PII -BCCP interaction would be conserved throughout Bacteria. In vitro experiments using purified proteins confirmed that the PII -BCCP interaction is conserved in Escherichia coli. The BCCP-PII interaction required MgATP and was dissociated by increasing 2-oxoglutarate. The interaction was modestly affected by the post-translational uridylylation status of PII ; however, it was completely dependent on the post-translational biotinylation of BCCP.

摘要

PII家族由一组广泛分布的信号转导蛋白组成。PII的典型功能是调节细菌中的氮代谢。由于PII能够感知一系列代谢信号,有人提出PII调节的代谢途径数量可能比文献中描述的要多得多。为了为这一假设提供实验证据,使用PII蛋白亲和柱来鉴定巴西固氮螺菌中的PII靶标。鉴定出的PII相互作用蛋白之一是生物素羧基载体蛋白(BCCP),它是乙酰辅酶A羧化酶的一个组分,催化脂肪酸生物合成中的关键步骤。由于BCCP先前已在拟南芥中被鉴定为PII靶标,我们推测PII -BCCP相互作用在整个细菌中是保守的。使用纯化蛋白进行的体外实验证实,PII -BCCP相互作用在大肠杆菌中是保守的。BCCP与PII的相互作用需要MgATP,并通过增加2-酮戊二酸而解离。该相互作用受到PII翻译后尿苷酰化状态的适度影响;然而,它完全依赖于BCCP的翻译后生物素化。

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