DEGENERATION OF SKELETAL-MUSCLE, PERIPHERAL-NERVES, AND THE CENTRAL-NERVOUS-SYSTEM IN TRANSGENIC MICE OVEREXPRESSING WILD-TYPE PRION PROTEINS

被引：305

作者：

WESTAWAY, D

DEARMOND, SJ

CAYETANOCANLAS, J

GROTH, D

FOSTER, D

YANG, SL

TORCHIA, M

CARLSON, GA

PRUSINER, SB

机构：

[1] UNIV CALIF SAN FRANCISCO,DEPT PATHOL,SAN FRANCISCO,CA 94143

[2] UNIV CALIF SAN FRANCISCO,DEPT BIOCHEM & BIOPHYS,SAN FRANCISCO,CA 94143

[3] MCLAUGHLIN RES INST,GREAT FALLS,MT 59405

来源：

CELL | 1994年 / 76卷 / 01期

关键词：

D O I：

10.1016/0092-8674(94)90177-5

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：

Prion diseases of humans and animals are known to be caused by infection with prions containing PrP(Sc) or mutation of the prion protein (PrP) gene. During transgenetic studies, we discovered that uninoculated older mice harboring high copy numbers of wild-type (wt) PrP transgenes derived from Syrian hamsters (SHa), sheep (She), and PrP-B mice developed truncal ataxia, hindlimb paralysis, and tremors. These transgenic (Tg) mice exhibited a profound necrotizing myopathy involving skeletal muscle, a demyelinating polyneuropathy, and focal vacuolation of the central nervous system. Development of disease was dependent on transgene dosage. For example, half of all Tg(SHaPrP+/+)7 mice homozygous for the SHaPrP transgene array developed disease by approximately 460 days of age, while no hemizygous Tg(SHaPrP+/0)7 mice became ill before 650 days. The novel neurologic syndrome found in older Tg(wtPrP) mice implies that overexpression of wtPrP(C) is pathogenic and widens the spectrum of prion diseases.

引用

页码：117 / 129

页数：13

共 50 条

[1] PREDICTED SECONDARY STRUCTURE AND MEMBRANE TOPOLOGY OF THE SCRAPIE PRION PROTEIN
BAZAN, JF
FLETTERICK, RJ
MCKINLEY, MP
PRUSINER, SB
[J]. PROTEIN ENGINEERING, 1987, 1 (02): : 125 - 135
[2] DEGENERATION OF CEREBELLAR + HYPOTHALAMO-NEUROHYPOPHYSIAL SYSTEMS IN SHEEP WITH SCRAPIE - + ITS RELATIONSHIP TO HUMAN SYSTEM DEGENERATIONS
BECK, E
PARRY, HB
DANIEL, PM
[J]. BRAIN, 1964, 87 (01) : 153 - &
[3] BEER J, 1991, ALZHEIMERS DISEASE : BASIC MECHANISMS, DIAGNOSIS AND THERAPEUTIC STRATEGIES, P473
[4] NEARLY UBIQUITOUS TISSUE DISTRIBUTION OF THE SCRAPIE AGENT PRECURSOR PROTEIN
BENDHEIM, PE
BROWN, HR
RUDELLI, RD
SCALA, LJ
GOLLER, NL
WEN, GY
KASCSAK, RJ
CASHMAN, NR
BOLTON, DC
[J]. NEUROLOGY, 1992, 42 (01) : 149 - 156
[5] BOSANQUET FD, 1956, LANCET, V2, P737
[6] NORMAL DEVELOPMENT AND BEHAVIOR OF MICE LACKING THE NEURONAL CELL-SURFACE PRP PROTEIN
BUELER, H
FISCHER, M
LANG, Y
BLUETHMANN, H
LIPP, HP
DEARMOND, SJ
PRUSINER, SB
AGUET, M
WEISSMANN, C
[J]. NATURE, 1992, 356 (6370) : 577 - 582
[7] CARLSON GA, 1993, GENETICS, V133, P979
[8] CELLULAR ISOFORM OF THE SCRAPIE AGENT PROTEIN PARTICIPATES IN LYMPHOCYTE-ACTIVATION
CASHMAN, NR
LOERTSCHER, R
NALBANTOGLU, J
SHAW, I
KASCSAK, RJ
BOLTON, DC
BENDHEIM, PE
[J]. CELL, 1990, 61 (01) : 185 - 192
[9] CHOMCZYNSKI P, 1987, ANAL BIOCHEM, V162, P156, DOI 10.1016/0003-2697(87)90021-2
[10] PROGRESSIVE NEURONOPATHY IN TRANSGENIC MICE EXPRESSING THE HUMAN NEUROFILAMENT HEAVY GENE - A MOUSE MODEL OF AMYOTROPHIC-LATERAL-SCLEROSIS
COTE, F
COLLARD, JF
JULIEN, JP
[J]. CELL, 1993, 73 (01) : 35 - 46

← 1 2 3 4 5 →