Apolipoprotein E isoform-specific differences in outcome from focal ischemia in transgenic mice

被引：129

作者：

Sheng, HX

Laskowitz, DT

Bennett, E

Schmechel, DE

Bart, RD

Saunders, AM

Pearlstein, RD

Roses, AD

Warner, DS

机构：

[1] Duke Univ, Med Ctr, Dept Anesthesiol, Durham, NC 27710 USA

[2] Duke Univ, Med Ctr, Dept Med Neurol, Durham, NC 27710 USA

[3] Duke Univ, Med Ctr, Dept Neurobiol, Durham, NC 27710 USA

[4] Duke Univ, Med Ctr, Dept Pediat, Durham, NC 27710 USA

[5] Duke Univ, Med Ctr, Dept Surg, Durham, NC 27710 USA

来源：

JOURNAL OF CEREBRAL BLOOD FLOW AND METABOLISM | 1998年 / 18卷 / 04期

关键词：

apolipoprotein E; brain; ischemia; mouse;

D O I：

10.1097/00004647-199804000-00003

中图分类号：

R5 [内科学];

学科分类号：

1002 ; 100201 ;

摘要：

Apolipoprotein E (apoE), a 34-kD glycosylated lipid-binding protein, is expressed as three common isoforms in humans (E2, E3, or E4). Clinical evidence suggests that the apoE genotype (APOE) may be a risk factor for poor outcome after acute central nervous system injury. This was examined further in transgenic mice constructed with the human APOE3 or APOE4 gene under the control of human promoter and tissue expression elements. Presence of human apoE3 and apoE4 proteins in brains of human APOE homozygous transgenic mice was confirmed by Western blotting. APOE3 (n = 12) and APOE4 (n = 10) mice underwent 60 minutes of middle cerebral artery occlusion. After 24-hour recovery, infarct size was measured. Infarct volumes (mean +/- standard deviation) were smaller in the APOE3 group (cortex: APOE3 = 18 +/- 4 mm(3); APOE4 = 30 +/- 11 mm(3), P = 0.04; subcortex: APOE3 = 12 +/- 4 mm(3); APOE4 = 18 +/- 4 mm(3); P = 0.003). Hemiparesis was less severe in APOE3 mice (P = 0.02). These data indicate that human isoform-specific effects of apoE are relevant to acute pathomechanisms of focal ischemic brain damage when examined in the mouse. APOE transgenic mice may provide an appropriate model to examine the mechanistic basis for the differential effects of human apoE isoforms in acute central nervous system injury.

引用

页码：361 / 366

页数：6

共 48 条

[31] PEPE MG, 1986, J IMMUNOL, V136, P3716
[32] SEVERE HYPERCHOLESTEROLEMIA AND ATHEROSCLEROSIS IN APOLIPOPROTEIN-E-DEFICIENT MICE CREATED BY HOMOLOGOUS RECOMBINATION IN ES CELLS
PLUMP, AS
SMITH, JD
HAYEK, T
AALTOSETALA, K
WALSH, A
VERSTUYFT, JG
RUBIN, EM
BRESLOW, JL
[J]. CELL, 1992, 71 (02) : 343 - 353
[33] ASTROCYTIC APOLIPOPROTEIN-E MESSENGER-RNA AND GFAP MESSENGER-RNA IN HIPPOCAMPUS AFTER ENTORHINAL CORTEX LESIONING
POIRIER, J
HESS, M
MAY, PC
FINCH, CE
[J]. MOLECULAR BRAIN RESEARCH, 1991, 11 (02): : 97 - 106
[34] EVOLUTION OF APOLIPOPROTEIN-E - MOUSE SEQUENCE AND EVIDENCE FOR AN 11-NUCLEOTIDE ANCESTRAL UNIT
RAJAVASHISTH, TB
KAPTEIN, JS
REUE, KL
LUSIS, AJ
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1985, 82 (23) : 8085 - 8089
[35] ATHEROSCLEROSIS IN MICE LACKING APO-E - EVALUATION OF LESIONAL DEVELOPMENT AND PROGRESSION
REDDICK, RL
ZHANG, SH
MAEDA, N
[J]. ARTERIOSCLEROSIS AND THROMBOSIS, 1994, 14 (01): : 141 - 147
[36] HEAD-INJURY, AMYLOID-BETA AND ALZHEIMERS-DISEASE
ROSES, AD
SAUNDERS, A
[J]. NATURE MEDICINE, 1995, 1 (07) : 603 - 604
[37] ASSOCIATION OF APOLIPOPROTEIN-E ALLELE EPSILON-4 WITH LATE-ONSET FAMILIAL AND SPORADIC ALZHEIMERS-DISEASE
SAUNDERS, AM
STRITTMATTER, WJ
SCHMECHEL, D
GEORGEHYSLOP, PHS
PERICAKVANCE, MA
JOO, SH
ROSI, BL
GUSELLA, JF
CRAPPERMACLACHLAN, DR
ALBERTS, MJ
HULETTE, C
CRAIN, B
GOLDGABER, D
ROSES, AD
[J]. NEUROLOGY, 1993, 43 (08) : 1467 - 1472
[38] Genetic determinants of susceptibility to excitotoxic cell death: Implications for gene targeting approaches
Schauwecker, PE
Steward, O
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1997, 94 (08) : 4103 - 4108
[39] Seliger Glenn, 1997, Neurology, V48, pA213
[40] DENERVATED SHEATH-CELLS SECRETE A NEW PROTEIN AFTER NERVE INJURY
SKENE, JHP
SHOOTER, EM
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA-BIOLOGICAL SCIENCES, 1983, 80 (13): : 4169 - 4173

← 1 2 3 4 5 →