首页> 外文期刊>Research Letters in Biochemistry >A Bioinformatics Analysis Reveals a Group of MocR Bacterial Transcriptional Regulators Linked to a Family of Genes Coding for Membrane Proteins
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A Bioinformatics Analysis Reveals a Group of MocR Bacterial Transcriptional Regulators Linked to a Family of Genes Coding for Membrane Proteins

机译:生物信息学分析揭示了一组MocR细菌转录调节因子,与编码膜蛋白的基因家族有关。

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The MocR bacterial transcriptional regulators are characterized by an N-terminal domain, 60 residues long on average, possessing the winged-helix-turn-helix (wHTH) architecture responsible for DNA recognition and binding, linked to a large C-terminal domain (350 residues on average) that is homologous to fold type-I pyridoxal 5′-phosphate (PLP) dependent enzymes like aspartate aminotransferase (AAT). These regulators are involved in the expression of genes taking part in several metabolic pathways directly or indirectly connected to PLP chemistry, many of which are still uncharacterized. A bioinformatics analysis is here reported that studied the features of a distinct group of MocR regulators predicted to be functionally linked to a family of homologous genes coding for integral membrane proteins of unknown function. This group occurs mainly in the Actinobacteria and Gammaproteobacteria phyla. An analysis of the multiple sequence alignments of their wHTH and AAT domains suggested the presence of specificity-determining positions (SDPs). Mapping of SDPs onto a homology model of the AAT domain hinted at possible structural/functional roles in effector recognition. Likewise, SDPs in wHTH domain suggested the basis of specificity of Transcription Factor Binding Site recognition. The results reported represent a framework for rational design of experiments and for bioinformatics analysis of other MocR subgroups.
机译:MocR细菌转录调节因子的特征是一个N末端结构域,平均长60个残基,具有负责DNA识别和结合的带翼螺旋-转-螺旋(wHTH)结构,并与一个大的C末端结构域相连(350平均残基)与I型吡ido醛5'-磷酸(PLP)依赖性酶(如天冬氨酸转氨酶(AAT))同源。这些调节剂参与参与直接或间接与PLP化学相关的几种代谢途径的基因表达,其中许多仍未表征。本文报道了一项生物信息学分析,研究了预测与功能上与编码未知功能的完整膜蛋白的同源基因家族功能连接的一组不同的MocR调节剂的功能。该组主要发生在放线菌和γ-变形杆菌门中。他们的wHTH和AAT域的多个序列比对的分析表明存在特异性决定位置(SDP)。 SDP映射到AAT域的同源性模型上暗示了效应子识别中可能的结构/功能作用。同样,wHTH域中的SDP提出了转录因子结合位点识别特异性的基础。报告的结果代表了合理设计实验和其他MocR子组的生物信息学分析的框架。

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