Reduced levels of amyloid β-peptide antibody in Alzheimer disease

被引:223
作者
Du, Y
Dodel, R
Hampel, H
Buerger, K
Lin, S
Eastwood, B
Bales, K
Gao, F
Moeller, HJ
Oertel, W
Farlow, M
Paul, S
机构
[1] Indiana Univ Sch Med, Dept Pharmacol & Toxicol, Indianapolis, IN 46285 USA
[2] Indiana Univ Sch Med, Dept Neurol, Indianapolis, IN 46285 USA
[3] Indiana Univ Sch Med, Dept Psychiat, Indianapolis, IN 46285 USA
[4] Univ Marburg, Dept Neurol, Marburg, Germany
[5] Univ Munich, Dementia Res Sect, Munich, Germany
[6] Univ Munich, Memory Clin, Munich, Germany
[7] Eli Lilly & Co, Lilly Res Labs, Dept Stat & Math Sci, Neurosci Discovery Res, Indianapolis, IN 46285 USA
来源
NEUROLOGY | 2001年 / 57卷 / 05期
关键词
D O I
10.1212/WNL.57.5.801
中图分类号
R74 [神经病学与精神病学];
学科分类号
摘要
Objective: To investigate whether it was possible to detect the presence and different levels of naturally occurring anti-beta -amyloid (A beta) antibodies in the CSF of patients with AD and age-matched controls by employing a sensitive ELISA. Background: Immunization with preaggregated amyloid beta -peptide (A beta (1-42)) and administration of antibodies against A beta into amyloid precursor protein APP(V717F)-transgenic mice (an animal model of AD) have recently been reported to dramatically reduce amyloid plaque deposition, neuritic dystrophy, and astrogliosis, most likely by enhancing A beta clearance from brain. Methods: A sensitive ELISA was performed to detect levels of naturally occurring anti-A beta antibodies in the CSF of patients with AD and age-matched controls. Additionally, an immunoprecipitation assay was performed to confirm that naturally occurring anti-A beta antibodies also exist in the human blood. Result: Naturally occurring antibodies directed against A beta were found in the CSF and plasma of patients with AD and healthy control subjects. Moreover, CSF anti-A beta antibody titers are significantly lower in patients with AD compared with healthy control subjects. Conclusion: Naturally occurring antibodies directed against A beta exist in human CSF and plasma. The CSF anti-A beta antibody titers may be helpful in better understanding the effects of future immunologic therapies for AD.
引用
收藏
页码:801 / 805
页数:5
相关论文
共 18 条
[1]  
ARMITAGE P, 1994, STAT METHODS MED RES, P389
[2]   Peripherally administered antibodies against amyloid β-peptide enter the central nervous system and reduce pathology in a mouse model of Alzheimer disease [J].
Bard, F ;
Cannon, C ;
Barbour, R ;
Burke, RL ;
Games, D ;
Grajeda, H ;
Guido, T ;
Hu, K ;
Huang, JP ;
Johnson-Wood, K ;
Khan, K ;
Kholodenko, D ;
Lee, M ;
Lieberburg, I ;
Motter, R ;
Nguyen, M ;
Soriano, F ;
Vasquez, N ;
Weiss, K ;
Welch, B ;
Seubert, P ;
Schenk, D ;
Yednock, T .
NATURE MEDICINE, 2000, 6 (08) :916-919
[3]   Alzheimer's disease - The ins and outs of amyloid-beta [J].
Beyreuther, K ;
Masters, CL .
NATURE, 1997, 389 (6652) :677-678
[4]   A presenilin-1-dependent γ-secretase-like protease mediates release of Notch intracellular domain [J].
De Strooper, B ;
Annaert, W ;
Cupers, P ;
Saftig, P ;
Craessaerts, K ;
Mumm, JS ;
Schroeter, EH ;
Schrijvers, V ;
Wolfe, MS ;
Ray, WJ ;
Goate, A ;
Kopan, R .
NATURE, 1999, 398 (6727) :518-522
[5]   ALZHEIMER-TYPE NEUROPATHOLOGY IN TRANSGENIC MICE OVEREXPRESSING V717F BETA-AMYLOID PRECURSOR PROTEIN [J].
GAMES, D ;
ADAMS, D ;
ALESSANDRINI, R ;
BARBOUR, R ;
BERTHELETTE, P ;
BLACKWELL, C ;
CARR, T ;
CLEMENS, J ;
DONALDSON, T ;
GILLESPIE, F ;
GUIDO, T ;
HAGOPIAN, S ;
JOHNSONWOOD, K ;
KHAN, K ;
LEE, M ;
LEIBOWITZ, P ;
LIEBERBURG, I ;
LITTLE, S ;
MASLIAH, E ;
MCCONLOGUE, L ;
MONTOYAZAVALA, M ;
MUCKE, L ;
PAGANINI, L ;
PENNIMAN, E ;
POWER, M ;
SCHENK, D ;
SEUBERT, P ;
SNYDER, B ;
SORIANO, F ;
TAN, H ;
VITALE, J ;
WADSWORTH, S ;
WOLOZIN, B ;
ZHAO, J .
NATURE, 1995, 373 (6514) :523-527
[6]   ALZHEIMERS-DISEASE - INITIAL REPORT OF THE PURIFICATION AND CHARACTERIZATION OF A NOVEL CEREBROVASCULAR AMYLOID PROTEIN [J].
GLENNER, GG ;
WONG, CW .
BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 1984, 120 (03) :885-890
[7]   AMYLOID BETA-PEPTIDE IS PRODUCED BY CULTURED-CELLS DURING NORMAL METABOLISM [J].
HAASS, C ;
SCHLOSSMACHER, MG ;
HUNG, AY ;
VIGOPELFREY, C ;
MELLON, A ;
OSTASZEWSKI, BL ;
LIEBERBURG, I ;
KOO, EH ;
SCHENK, D ;
TEPLOW, DB ;
SELKOE, DJ .
NATURE, 1992, 359 (6393) :322-325
[8]   THE PRECURSOR OF ALZHEIMERS-DISEASE AMYLOID-A4 PROTEIN RESEMBLES A CELL-SURFACE RECEPTOR [J].
KANG, J ;
LEMAIRE, HG ;
UNTERBECK, A ;
SALBAUM, JM ;
MASTERS, CL ;
GRZESCHIK, KH ;
MULTHAUP, G ;
BEYREUTHER, K ;
MULLERHILL, B .
NATURE, 1987, 325 (6106) :733-736
[9]   BETA-AMYLOID NEUROTOXICITY REQUIRES FIBRIL FORMATION AND IS INHIBITED BY CONGO RED [J].
LORENZO, A ;
YANKNER, BA .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1994, 91 (25) :12243-12247
[10]   NEURONAL ORIGIN OF A CEREBRAL AMYLOID - NEUROFIBRILLARY TANGLES OF ALZHEIMERS-DISEASE CONTAIN THE SAME PROTEIN AS THE AMYLOID OF PLAQUE CORES AND BLOOD-VESSELS [J].
MASTERS, CL ;
MULTHAUP, G ;
SIMMS, G ;
POTTGIESSER, J ;
MARTINS, RN ;
BEYREUTHER, K .
EMBO JOURNAL, 1985, 4 (11) :2757-2763
12