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阿尔茨海默病β肽组装的立体化学特异性。

Stereochemical specificity of Alzheimer's disease beta-peptide assembly.

作者信息

Esler W P, Stimson E R, Fishman J B, Ghilardi J R, Vinters H V, Mantyh P W, Maggio J E

机构信息

Department of Biological Chemistry and Molecular Pharmacology, Harvard Medical School, Boston, MA 02115, USA.

出版信息

Biopolymers. 1999 May;49(6):505-14. doi: 10.1002/(SICI)1097-0282(199905)49:6<505::AID-BIP8>3.0.CO;2-I.

DOI:10.1002/(SICI)1097-0282(199905)49:6<505::AID-BIP8>3.0.CO;2-I
PMID:10193196
Abstract

The formation and growth of insoluble amyloid deposits composed primarily of the human beta-amyloid peptide (A beta) in brain is an essentially invariant feature of Alzheimer's disease (AD) and is widely believed to contribute to the progressive neurodegeneration of the disorder. To probe the specificity of amyloid formation and growth, we synthesized and examined the self-assembly of D- and L-stereoisomers of A beta in vitro. While both enantiomers formed insoluble aggregates at similar rates with amyloid-like fibrillar morphology, deposition of soluble A beta peptide onto preexisting A beta aggregates was stereospecific. Although the L-peptide deposited readily onto immobilized L-A beta aggregates with first-order kinetic dependence on soluble peptide concentration, essentially no association between the D-peptide and L-template was observed. Similarly, the D-peptide deposited with first-order kinetics onto a D-A beta aggregate template but did not deposit onto a similar template composed of aggregates of the L-enantiomer. Furthermore, although the L-A beta isomer deposited onto authentic AD amyloid in preparations of unfixed AD brain, no focal association between the D-peptide and brain amyloid was detected. These results establish that deposition of soluble A beta onto preexisting amyloid template is stereospecific, likely involving direct docking interactions between peptide backbone and/or side chains rather than simple hydrophobic association.

摘要

由人类β淀粉样肽(Aβ)在大脑中形成并生长的不溶性淀粉样沉积物,是阿尔茨海默病(AD)的一个基本不变的特征,并且人们普遍认为这会导致该疾病的进行性神经退行性变。为了探究淀粉样蛋白形成和生长的特异性,我们在体外合成并检测了Aβ的D型和L型立体异构体的自组装情况。虽然两种对映体以相似的速率形成具有淀粉样纤维形态的不溶性聚集体,但可溶性Aβ肽在预先存在的Aβ聚集体上的沉积具有立体特异性。尽管L肽很容易沉积在固定化的L-Aβ聚集体上,且对可溶性肽浓度呈一级动力学依赖性,但未观察到D肽与L模板之间有明显的结合。同样,D肽以一级动力学沉积在D-Aβ聚集体模板上,但不沉积在由L对映体聚集体组成的类似模板上。此外,尽管L-Aβ异构体在未固定的AD脑制备物中沉积在真实的AD淀粉样蛋白上,但未检测到D肽与脑淀粉样蛋白之间有局灶性结合。这些结果表明,可溶性Aβ在预先存在的淀粉样模板上的沉积具有立体特异性,可能涉及肽主链和/或侧链之间的直接对接相互作用,而不是简单的疏水结合。

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Stereochemical specificity of Alzheimer's disease beta-peptide assembly.阿尔茨海默病β肽组装的立体化学特异性。
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