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淀粉样β肽中的金属结合呈现出肽内和肽间的配位模式。

Metal binding in amyloid beta-peptides shows intra- and inter-peptide coordination modes.

作者信息

Stellato Francesco, Menestrina Gianfranco, Serra Mauro Dalla, Potrich Cristina, Tomazzolli Rossella, Meyer-Klaucke Wolfram, Morante Silvia

机构信息

Dipartimento di Fisica, Università di Roma "Tor Vergata" INFM and INFN, Via della Ricerca Scientifica 1, 00133 Roma, Italy.

出版信息

Eur Biophys J. 2006 Apr;35(4):340-51. doi: 10.1007/s00249-005-0041-7. Epub 2006 Jan 11.

DOI:10.1007/s00249-005-0041-7
PMID:16404590
Abstract

X-ray absorption spectroscopy data show different metal binding site structures in beta-amyloid peptides according to whether they are complexed with Cu(2+) or Zn(2+) ions. While the geometry around copper is stably consistent with an intra-peptide binding with three metal-coordinated Histidine residues, the zinc coordination mode depends on specific solution conditions. In particular, different sample preparations are seen to lead to different geometries around the absorber that are compatible with either an intra- or an inter-peptide coordination mode. This result reinforces the hypothesis that assigns different physiological roles to the two metals, with zinc favoring peptide aggregation and, as a consequence, plaque formation.

摘要

X射线吸收光谱数据表明,β-淀粉样肽中不同的金属结合位点结构取决于它们是否与Cu(2+)或Zn(2+)离子络合。虽然铜周围的几何结构与三个金属配位组氨酸残基的肽内结合稳定一致,但锌的配位模式取决于特定的溶液条件。特别是,不同的样品制备方法会导致吸收体周围出现不同的几何结构,这些结构与肽内或肽间配位模式均兼容。这一结果强化了这样一种假设,即赋予这两种金属不同的生理作用,锌有利于肽聚集,进而导致斑块形成。

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Zinc ion rapidly induces toxic, off-pathway amyloid-β oligomers distinct from amyloid-β derived diffusible ligands in Alzheimer's disease.锌离子迅速诱导阿尔茨海默病中具有毒性的、非淀粉样蛋白途径的淀粉样-β寡聚体,而不是淀粉样-β衍生的可扩散配体。
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