AGGREGATION STATE AND NEUROTOXIC PROPERTIES OF ALZHEIMER BETA-AMYLOID PEPTIDE

被引：181

作者：

HOWLETT, DR

JENNINGS, KH

LEE, DC

CLARK, MSG

BROWN, F

WETZEL, R

WOOD, SJ

CAMILLERI, P

ROBERTS, GW

机构：

[1] SMITHKLINE BEECHAM PHARMACEUT,WELWYN GARDEN CIT,HERTS,ENGLAND

[2] SMITHKLINE BEECHAM PHARMACEUT,KING OF PRUSSIA,PA 19406

来源：

NEURODEGENERATION | 1995年 / 4卷 / 01期

关键词：

ALZHEIMERS DISEASE; BETA-AMYLOID PROTEIN; ELECTRON MICROSCOPY; FIBRIL FORMATION; NEUROTOXICITY;

D O I：

10.1006/neur.1995.0003

中图分类号：

Q189 [神经科学];

学科分类号：

071006 ;

摘要：

The behaviour of synthetic batches of beta-amyloid (beta A) 1-40 peptide in solution has been studied. The effects of beta A1-40 on a PC12 cell toxicity assay was dependent upon the time of preincubation of an aqueous solution of the peptide before application to the cells. Fibrillization of the beta A1-40, quantitatively assessed by the binding of Congo red to amyloid fibrils, also increased in a time dependent manner over the 168 h incubation period studied. The degree of Congo red binding, in the absence of any preincubation, differed between two synthetically distinct batches of the peptide. The rate of development of fibril formation during subsequent incubation also differed between the two batches and appeared to parallel the effects on cell viability. Infra-red spectroscopic analysis revealed beta-sheet formation for both batches and other more subtle conformational differences between the peptides. Electron microscope examination of the batches of beta A1-40 confirmed the difference in occurrence and development of fibrils. At high magnification, fibrils of both batches exhibited a helical structure. The results suggest that the development of neurotoxicity of beta A1-40 is related to the fibrillar state of the peptide.

引用

页码：23 / 32

页数：10

共 35 条

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