RESCUE OF NEUROPHYSIOLOGICAL PHENOTYPE SEEN IN PRP NULL MICE BY TRANSGENE ENCODING HUMAN PRION PROTEIN

被引：127

作者：

WHITTINGTON, MA

SIDLE, KCL

GOWLAND, I

MEADS, J

HILL, AF

PALMER, MS

JEFFERYS, JGR

COLLINGE, J

机构：

[1] UNIV LONDON IMPERIAL COLL SCI TECHNOL & MED,ST MARYS HOSP,SCH MED,DEPT BIOCHEM & MOLEC GENET,LONDON W2 1PG,ENGLAND

[2] UNIV LONDON IMPERIAL COLL SCI TECHNOL & MED,ST MARYS HOSP,SCH MED,DEPT PHYSIOL & BIOPHYS,LONDON W2 1PG,ENGLAND

[3] ST MARYS HOSP,DEPT NEUROL,LONDON W2 1NY,ENGLAND

来源：

NATURE GENETICS | 1995年 / 9卷 / 02期

基金：

英国惠康基金;

关键词：

D O I：

10.1038/ng0295-197

中图分类号：

Q3 [遗传学];

学科分类号：

071007 ; 090102 ;

摘要：

The prion protein (PrP) is central to the aetiology of the prion diseases, transmissible neurodegenerative conditions of humans and animals. PrP null mice show abnormalities of synaptic neurophysiology, in particular weakened GABA(A) receptor-mediated fast inhibition and impaired long-term potentiation in the hippocampus. Here we demonstrate that this PrP null phenotype is rescued in mice with a high copy number of a transgene encoding human PrP but not in low copy number mice, confirming the specificity of the phenotype for loss of function of PrP. The ability of human PrP to compensate for loss of murine PrP will allow direct study of the functional consequences of the 18 human PrP mutations, which cause the inherited prion diseases; this phenotype can now form the basis of the first functional assay for PrP.

引用

页码：197 / 201

页数：5

共 33 条

[1] AMINO-ACID POLYMORPHISM IN HUMAN PRION PROTEIN AND AGE AT DEATH IN INHERITED PRION DISEASE [J].

BAKER, HF ;

POULTER, M ;

CROW, TJ ;

FRITH, CD ;

LOFTHOUSE, R ;

RIDLEY, RM ;

COLLINGE, J .

LANCET, 1991, 337 (8752) :1286-1286

[2] SCRAPIE AND CELLULAR PRION PROTEINS DIFFER IN THEIR KINETICS OF SYNTHESIS AND TOPOLOGY IN CULTURED-CELLS [J].

BORCHELT, DR ;

SCOTT, M ;

TARABOULOS, A ;

STAHL, N ;

PRUSINER, SB .

JOURNAL OF CELL BIOLOGY, 1990, 110 (03) :743-752

[3] NORMAL DEVELOPMENT OF NERVE MUSCLE SYNAPSES IN MICE LACKING THE PRION PROTEIN GENE [J].

BRENNER, HR ;

HERCZEG, A ;

OESCH, B .

PROCEEDINGS OF THE ROYAL SOCIETY B-BIOLOGICAL SCIENCES, 1992, 250 (1328) :151-155

[4] NORMAL DEVELOPMENT AND BEHAVIOR OF MICE LACKING THE NEURONAL CELL-SURFACE PRP PROTEIN [J].

BUELER, H ;

FISCHER, M ;

LANG, Y ;

BLUETHMANN, H ;

LIPP, HP ;

DEARMOND, SJ ;

PRUSINER, SB ;

AGUET, M ;

WEISSMANN, C .

NATURE, 1992, 356 (6370) :577-582

[5]

CATHALA F, 1987, P467

[6] SYNAPTIC DEGENERATION IS THE PRIMARY NEUROPATHOLOGICAL FEATURE IN PRION DISEASE - A PRELIMINARY-STUDY [J].

CLINTON, J ;

FORSYTH, C ;

ROYSTON, MC ;

ROBERTS, GW .

NEUROREPORT, 1993, 4 (01) :65-68

[7] GENETIC PREDISPOSITION TO IATROGENIC CREUTZFELDT-JAKOB DISEASE [J].

COLLINGE, J ;

PALMER, MS ;

DRYDEN, AJ .

LANCET, 1991, 337 (8755) :1441-1442

[8] PRION DEMENTIA WITHOUT CHARACTERISTIC PATHOLOGY [J].

COLLINGE, J ;

OWEN, F ;

POULTER, M ;

LEACH, M ;

CROW, TJ ;

ROSSOR, MN ;

HARDY, J ;

MULLAN, MJ ;

JANOTA, I ;

LANTOS, PL .

LANCET, 1990, 336 (8706) :7-9

[9] PRION PROTEIN IS NECESSARY FOR NORMAL SYNAPTIC FUNCTION [J].

COLLINGE, J ;

WHITTINGTON, MA ;

SIDLE, KCL ;

SMITH, CJ ;

PALMER, MS ;

CLARKE, AR ;

JEFFERYS, JGR .

NATURE, 1994, 370 (6487) :295-297

[10] Prion diseases [J].

Collinge, John ;

Palmer, Mark S. .

CURRENT OPINION IN GENETICS & DEVELOPMENT, 1992, 2 (03) :448-454

← 1 2 3 4 →