GENETIC-LINKAGE STUDIES SUGGEST THAT ALZHEIMERS-DISEASE IS NOT A SINGLE HOMOGENEOUS DISORDER

被引：357

作者：

STGEORGEHYSLOP, PH

HAINES, JL

FARRER, LA

POLINSKY, R

VAN BROECKHOVEN, C

GOATE, A

MCLACHLAN, DRC

ORR, H

BRUNI, AC

SORBI, S

RAINERO, I

FONCIN, JF

POLLEN, D

CANTU, JM

TUPLER, R

VOSKRESENSKAYA, N

MAYEUX, R

GROWDON, J

FRIED, VA

MYERS, RH

NEE, L

BACKHOVENS, H

MARTIN, JJ

ROSSOR, M

OWEN, MJ

MULLAN, M

PERCY, ME

KARLINSKY, H

RICH, S

HESTON, L

MONTESI, M

MORTILLA, M

NACMIAS, N

GUSELLA, JF

HARDY, JA

机构：

[1] MASSACHUSETTS GEN HOSP, DEPT GEN INTERNAL MED, BOSTON, MA 02114 USA

[2] BOSTON UNIV, SCH MED, DEPT NEUROL, BOSTON, MA 02118 USA

[3] NINCDS, CLIN NEUROSCI BRANCH, BETHESDA, MD 20892 USA

[4] UNIV ANTWERP, BORN BUNGE FDN, DEPT NEUROGENET, ANTWERP, BELGIUM

[5] UNIV ANTWERP, BORN BUNGE FDN, DEPT NEUROL, ANTWERP, BELGIUM

[6] UNIV BRUSSELS, DEPT NEUROL, B-1090 BRUSSELS, BELGIUM

[7] ST MARYS HOSP, SCH MED, DEPT BIOCHEM, LONDON W2 1PG, ENGLAND

[8] ST MARYS HOSP, SCH MED, DEPT NEUROL, LONDON W2 1PG, ENGLAND

[9] UNIV TORONTO, TANZ NEUROSCI INST, CTR RES NEURODEGENERAT DIS, TORONTO M5S 1A8, ONTARIO, CANADA

[10] UNIV TORONTO, FAC MED, DEPT MED, TORONTO M5S 1A8, ONTARIO, CANADA

[11] UNIV TORONTO, FAC MED, DEPT PHYSIOL, TORONTO M5S 1A8, ONTARIO, CANADA

[12] UNIV TORONTO, FAC MED, DEPT PSYCHIAT, TORONTO M5S 1A8, ONTARIO, CANADA

[13] UNIV TORONTO, FAC MED, DEPT OBSTET, TORONTO M5S 1A8, ONTARIO, CANADA

[14] UNIV MINNESOTA, SCH MED, DEPT PSYCHIAT, MINNEAPOLIS, MN 55455 USA

[15] UNIV MINNESOTA, SCH MED, DEPT LAB MED, MINNEAPOLIS, MN 55455 USA

[16] STUDIO MULTICENT ITALIANO DEMENZA, CTR SUD, I-88046 LAMEZIA TERME, ITALY

[17] UNIV FLORENCE, DEPT NEUROL, I-50121 FLORENCE, ITALY

[18] UNIV TURIN, IST CLIN MALATTIE NERVOSE, I-10126 TURIN, ITALY

[19] HOP LA PITIE SALPETRIERE, ECOLE PRAT HAUTES ETUD, NEUROHISTOL LAB, F-75651 PARIS 13, FRANCE

[20] HOP LA PITIE SALPETRIERE, INSERM, U106, F-75651 PARIS 13, FRANCE

[21] UNIV MASSACHUSETTS, SCH MED, DEPT NEUROL, WORCESTER, MA 01605 USA

[22] INST MEXICANO SEGURO SOCIAL, DIV GENET, UNIDAD INVEST BIOMED OCCIDENTE, GUADALAJARA, JALISCO, MEXICO

[23] UNIV PAVIA, DIPARTIMENTO PATOL UMANA & EREDITARIA, I-27100 PAVIA, ITALY

[24] UNIV BRESCIA, NEUROL CLIN, I-25125 BRESCIA, ITALY

[25] RUSSIAN ACAD MED SCI, CTR MENTAL HLTH, MOSCOW 113152, RUSSIA

[26] COLUMBIA UNIV COLL PHYS & SURG, INST NEUROL, NEW YORK, NY 10032 USA

[27] KREISKRANKENHAUS LEMGO, NEUROL ABT, W-492 LEMGO, GERMANY

[28] LIFE TECHNOL INC, GAITHERSBURG, MD 20087 USA

来源：

NATURE | 1990年 / 347卷 / 6289期

关键词：

D O I：

10.1038/347194a0

中图分类号：

O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];

学科分类号：

07 ; 0710 ; 09 ;

摘要：

ALZHEIMER'S disease, a fatal neurodegenerative disorder of unknown aetiology, is usually considered to be a single disorder because of tbe general uniformity of the disease phenotype1,2. Two recent genetic linkage studies revealed co-segregation of familial Alzheimer disease with the D21S1/S11 and D21S16 loci on chromosome 21 (refs 3,4). But two other studies, one of pre-dominantly multiplex kindreds with a late age-of-onset5, the other of a cadre of kindreds with a unique Volga German ethnic origin6, found absence of linkage at least to D21S1/S11. So far it has not been possible to discern whether these conflicting reports reflect aetiological heterogeneity, differences in methods of pedigree selection, effects of confounding variables in the analysis (for example, diagnostic errors, assortative matings), or true non-replication. To resolve this issue, we have now examined the inheritance of five polymorphic DNA markers from the proximal long arm of chromosome 21 in a large unselected series of pedi-grees with familial Alzheimer's disease. Our data suggest that Alzheimer's disease is not a single entity, but rather results from genetic defects on chromosome 21 and from other genetic or nongenetic factors. © 1990 Nature Publishing Group.

引用

页码：194 / 197

页数：4

共 29 条

[1] PHENOTYPIC HETEROGENEITY IN FAMILIAL ALZHEIMERS-DISEASE - A STUDY OF 24 KINDREDS
BIRD, TD
SUMI, SM
NEMENS, EJ
NOCHLIN, D
SCHELLENBERG, G
LAMPE, TH
SADOVNICK, A
CHUI, H
MINER, GW
TINKLENBERG, J
[J]. ANNALS OF NEUROLOGY, 1989, 25 (01) : 12 - 25
[2] BONDAREFF W, 1987, ARCH GEN PSYCHIAT, V44, P412
[3] CASE-CONTROL STUDY OF LATE ONSET PROBABLE ALZHEIMERS-DISEASE
CHANDRA, V
PHILIPOSE, V
BELL, PA
LAZAROFF, A
SCHOENBERG, BS
[J]. NEUROLOGY, 1987, 37 (08) : 1295 - 1300
[4] CHUI HC, 1987, J NEURAL TRANSM, P57
[5] TRANSMISSION AND AGE-AT-ONSET PATTERNS IN FAMILIAL ALZHEIMERS-DISEASE - EVIDENCE FOR HETEROGENEITY
FARRER, LA
MYERS, RH
CUPPLES, LA
GEORGEHYSLOP, PHS
BIRD, TD
ROSSOR, MN
MULLAN, MJ
POLINSKY, R
NEE, L
HESTON, L
VAN BROECKHOVEN, C
MARTIN, JJ
CRAPPERMCLACHLAN, D
GROWDON, JH
[J]. NEUROLOGY, 1990, 40 (03) : 395 - 403
[6] ASSESSMENT OF GENETIC RISK FOR ALZHEIMERS-DISEASE AMONG 1ST-DEGREE RELATIVES
FARRER, LA
OSULLIVAN, DM
CUPPLES, LA
GROWDON, JH
MYERS, RH
[J]. ANNALS OF NEUROLOGY, 1989, 25 (05) : 485 - 493
[7] GOATE AM, 1989, LANCET, V1, P352
[8] NEOCORTICAL MORPHOMETRY, LESION COUNTS, AND CHOLINE-ACETYLTRANSFERASE LEVELS IN THE AGE SPECTRUM OF ALZHEIMERS-DISEASE
HANSEN, LA
DETERESA, R
DAVIES, P
TERRY, RD
[J]. NEUROLOGY, 1988, 38 (01) : 48 - 54
[9] HODGE SE, 1979, AM J HUM GENET, V31, pA135
[10] RISK OF DEMENTIA IN RELATIVES OF PATIENTS WITH ALZHEIMERS-DISEASE
HUFF, FJ
AUERBACH, J
CHAKRAVARTI, A
BOLLER, F
[J]. NEUROLOGY, 1988, 38 (05) : 786 - 790

← 1 2 3 →