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Shaping mechanisms of metal specificity in a family of metazoan metallothioneins: evolutionary differentiation of mollusc metallothioneins

机译:后生金属硫蛋白家族中金属特异性的形成机理:软体动物金属硫蛋白的进化分化

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摘要

Background: The degree of metal binding specificity in metalloproteins such as metallothioneins (MTs) can be crucial for their functional accuracy. Unlike most other animal species, pulmonate molluscs possess homometallic MT isoforms loaded with Cu+ or Cd2+. They have, so far, been obtained as native metal-MT complexes from snail tissues, where they are involved in the metabolism of the metal ion species bound to the respective isoform. However, it has not as yet been discerned if their specific metal occupation is the result of a rigid control of metal availability, or isoform expression programming in the hosting tissues or of structural differences of the respective peptides determining the coordinative options for the different metal ions. In this study, the Roman snail (Helix pomatia) Cu-loaded and Cd-loaded isoforms (HpCuMT and HpCdMT) were used as model molecules in order to elucidate the biochemical and evolutionary mechanisms permitting pulmonate MTs to achieve specificity for their cognate metal ion. Results: HpCuMT and HpCdMT were recombinantly synthesized in the presence of Cd2+, Zn2+ or Cu2+ and corresponding metal complexes analysed by electrospray mass spectrometry and circular dichroism (CD) and ultra violet-visible (UV-Vis) spectrophotometry. Both MT isoforms were only able to form unique, homometallic and stable complexes (Cd6-HpCdMT and Cu12-HpCuMT) with their cognate metal ions. Yeast complementation assays demonstrated that the two isoforms assumed metal-specific functions, in agreement with their binding preferences, in heterologous eukaryotic environments. In the snail organism, the functional metal specificity of HpCdMT and HpCuMT was contributed by metal-specific transcription programming and cell-specific expression. Sequence elucidation and phylogenetic analysis of MT isoforms from a number of snail species revealed that they possess an unspecific and two metal-specific MT isoforms, whose metal specificity was achieved exclusively by evolutionary modulation of non-cysteine amino acid positions. Conclusion: The Roman snail HpCdMT and HpCuMT isoforms can thus be regarded as prototypes of isoform families that evolved genuine metal-specificity within pulmonate molluscs. Diversification into these isoforms may have been initiated by gene duplication, followed by speciation and selection towards opposite needs for protecting copper-dominated metabolic pathways from nonessential cadmium. The mechanisms enabling these proteins to be metal-specific could also be relevant for other metalloproteins.
机译:背景:金属蛋白(例如金属硫蛋白(MTs))中金属结合特异性的程度对其功能准确性至关重要。与大多数其他动物物种不同,肺部软体动物具有负载Cu +或Cd2 +的同金属MT同工型。迄今为止,它们已作为天然金属-MT络合物从蜗牛组织中获得,它们参与与各自同工型结合的金属离子物种的代谢。但是,尚不清楚它们的特定金属占用是金属可用性的严格控制,宿主组织中同工型表达编程的结果还是决定不同金属离子配位选择的各个肽的结构差异的结果。在这项研究中,使用罗马蜗牛(Helix pomatia)负载铜和负载Cd的同工型(HpCuMT和HpCdMT)作为模型分子,以阐明允许肺MT对其同源金属离子实现特异性的生化和进化机制。结果:HpCuMT和HpCdMT在Cd2 +,Zn2 +或Cu2 +以及相应的金属配合物存在下重组合成,通过电喷雾质谱,圆二色性(CD)和紫外可见(UV-Vis)分光光度法进行分析。两种MT同工型均只能与其同源金属离子形成独特的,同金属的,稳定的络合物(Cd6-HpCdMT和Cu12-HpCuMT)。酵母互补分析表明,这两种同工型在异源真核环境中均具有金属特异性功能,与其结合偏好相吻合。在蜗牛生物中,HpCdMT和HpCuMT的功能金属特异性是由金属特异性的转录程序和细胞特异性的表达促成的。来自许多蜗牛物种的MT同工型的序列阐明和系统发育分析表明,它们具有非特异性和两种金属特异性的MT同工型,其金属特异性仅通过非半胱氨酸氨基酸位置的进化调节来实现。结论:罗马蜗牛HpCdMT和HpCuMT同工型可以被视为同工型家族的原型,这些同工型在肺部软体动物内进化出真正的金属特异性。这些同工型的多样化可能是通过基因复制开始的,然后是物种形成和选择,以保护铜为主的代谢途径免受不必要的镉的相反需求。使这些蛋白质具有金属特异性的机制也可能与其他金属蛋白质有关。

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