PRODUCTION OF INTRACELLULAR AMYLOID-CONTAINING FRAGMENTS IN HIPPOCAMPAL-NEURONS EXPRESSING HUMAN AMYLOID PRECURSOR PROTEIN AND PROTECTION AGAINST AMYLOIDOGENESIS BY SUBTLE AMINO-ACID SUBSTITUTIONS IN THE RODENT SEQUENCE

被引：165

作者：

DESTROOPER, B

SIMONS, M

MULTHAUP, G

VANLEUVEN, F

BEYREUTHER, K

DOTTI, CG

机构：

[1] EUROPEAN MOLEC BIOL LAB, CELL BIOL PROGRAM, D-69012 HEIDELBERG, GERMANY

[2] CATHOLIC UNIV LEUVEN, CTR HUMAN GENET, B-3000 LOUVAIN, BELGIUM

[3] UNIV HEIDELBERG, CTR BIOL MOLEC, D-69120 HEIDELBERG, GERMANY

来源：

EMBO JOURNAL | 1995年 / 14卷 / 20期

关键词：

AMYLOID PRECURSOR PROTEIN; ALZHEIMERS DISEASE; HIPPOCAMPAL NEURONS;

D O I：

10.1002/j.1460-2075.1995.tb00176.x

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

A distinguishing feature of Alzheimer's disease (AD) is the deposition of amyloid plaques in brain parenchyma. These plaques arise by the abnormal accumulation of beta A4, a proteolytic fragment of amyloid precursor protein (APP). Despite the fact that neurons are dramatically affected in the course of the disease, little is known about the neuronal processing of APP. To address this question we have expressed in fully mature, synaptically active rat hippocampal neurons, the neuronal form of human APP (APP695), two mutant forms of human APP associated with AD, and the mouse form of APP (a species known not to develop amyloid plaques). Protein expression was achieved via the Semliki Forest Virus system. Expression of wild type human APP695 resulted in the secretion of beta A4-amyloid peptide and the intracellular accumulation of potential amyloidogenic and non-amyloidogenic fragments. The relative amount of amyloid-containing fragments increased dramatically during expression of the clinical mutants, while it decreased strongly when the mouse form of APP was expressed. 'Humanizing' the rodent APP sequence by introducing three mutations in the beta A4-region also led to increased production of amyloid peptide to levels similar to those obtained with human APP. The single Gly601 to Arg substitution alone was sufficient to triple the ratio of beta A4-peptide to non-amyloidogenic p3-peptide. Due to the capacity of these cells to secrete and accumulate intracellular amyloid fragments, we hypothesize that in the pathogenesis of AD there is a positive feed-back loop where neurons are both producers and victims of amyloid, leading to neuronal degeneration and dementia. Moreover, our observations may explain why aging rodents (in contrast to other species such as human, polar bear, dog and monkey), never develop amyloid deposits.

引用

页码：4932 / 4938

页数：7

共 48 条

[1] PROTEIN-PHOSPHORYLATION INHIBITS PRODUCTION OF ALZHEIMER AMYLOID-BETA/A4 PEPTIDE
BUXBAUM, JD
KOO, EH
GREENGARD, P
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1993, 90 (19) : 9195 - 9198
[2] RELEASE OF EXCESS AMYLOID BETA-PROTEIN FROM A MUTANT AMYLOID BETA-PROTEIN PRECURSOR
CAI, XD
GOLDE, TE
YOUNKIN, SG
[J]. SCIENCE, 1993, 259 (5094) : 514 - 516
[3] GENERATION OF AMYLOID-BETA PROTEIN FROM ITS PRECURSOR IS SEQUENCE-SPECIFIC
CITRON, M
TEPLOW, DB
SELKOE, DJ
[J]. NEURON, 1995, 14 (03) : 661 - 670
[4] MUTATION OF THE BETA-AMYLOID PRECURSOR PROTEIN IN FAMILIAL ALZHEIMERS-DISEASE INCREASES BETA-PROTEIN PRODUCTION
CITRON, M
OLTERSDORF, T
HAASS, C
MCCONLOGUE, L
HUNG, AY
SEUBERT, P
VIGOPELFREY, C
LIEBERBURG, I
SELKOE, DJ
[J]. NATURE, 1992, 360 (6405) : 672 - 674
[5] INTRACELLULAR ROUTING OF WILD-TYPE AND MUTATED POLYMERIC IMMUNOGLOBULIN RECEPTOR IN HIPPOCAMPAL-NEURONS IN CULTURE
DEHOOP, M
VONPOSER, C
LANGE, C
IKONEN, E
HUNZIKER, W
DOTTI, CG
[J]. JOURNAL OF CELL BIOLOGY, 1995, 130 (06) : 1447 - 1459
[6] THE INVOLVEMENT OF THE SMALL GTP-BINDING PROTEIN RAB5A IN NEURONAL ENDOCYTOSIS
DEHOOP, MJ
HUBER, LA
STENMARK, H
WILLIAMSON, E
ZERIAL, M
PARTON, RG
DOTTI, CG
[J]. NEURON, 1994, 13 (01) : 11 - 22
[7] SITE-DIRECTED MUTAGENESIS OF VIRTUALLY ANY PLASMID BY ELIMINATING A UNIQUE SITE
DENG, WP
NICKOLOFF, JA
[J]. ANALYTICAL BIOCHEMISTRY, 1992, 200 (01) : 81 - 88
[8] THE AMYLOID BETA-PROTEIN PRECURSOR OR PROTEINASE NEXIN-II FROM MOUSE IS CLOSER RELATED TO ITS HUMAN HOMOLOG THAN PREVIOUSLY REPORTED
DESTROOPER, B
VANLEUVEN, F
VANDENBERGHE, H
[J]. BIOCHIMICA ET BIOPHYSICA ACTA, 1991, 1129 (01) : 141 - 143
[9] STUDY OF THE SYNTHESIS AND SECRETION OF NORMAL AND ARTIFICIAL MUTANTS OF MURINE AMYLOID PRECURSOR PROTEIN (APP) - CLEAVAGE OF APP OCCURS IN A LATE COMPARTMENT OF THE DEFAULT SECRETION PATHWAY
DESTROOPER, B
UMANS, L
VANLEUVEN, F
VANDENBERGHE, H
[J]. JOURNAL OF CELL BIOLOGY, 1993, 121 (02) : 295 - 304
[10] BASOLATERAL SECRETION OF AMYLOID PRECURSOR PROTEIN IN MADIN-DARBY CANINE KIDNEY-CELLS IS DISTURBED BY ALTERATIONS OF INTRACELLULAR PH AND BY INTRODUCING A MUTATION ASSOCIATED WITH FAMILIAL ALZHEIMERS-DISEASE
DESTROOPER, B
CRAESSAERTS, K
DEWACHTER, I
MOECHARS, D
GREENBERG, B
VANLEUVEN, F
VANDENBERGHE, H
[J]. JOURNAL OF BIOLOGICAL CHEMISTRY, 1995, 270 (08) : 4058 - 4065

← 1 2 3 4 5 →