ACCELERATION OF HSP70 AND HSC70 HEAT-SHOCK GENE-EXPRESSION FOLLOWING TRANSIENT ISCHEMIA IN THE PRECONDITIONED GERBIL HIPPOCAMPUS

被引：82

作者：

AOKI, M

ABE, K

KAWAGOE, J

NAKAMURA, S

KOGURE, K

机构：

[1] Department of Neurology, Institute for Brain Diseases, Tohoku University School of Medicine, Sendai

[2] Department of Neurology, Institute for Brain Diseases, Toboku University School of Medicine, Aobaku, Sendai 980

来源：

JOURNAL OF CEREBRAL BLOOD FLOW AND METABOLISM | 1993年 / 13卷 / 05期

关键词：

HEAT SHOCK COGNATE PROTEIN 70; HEAT SHOCK PROTEIN 70; ISCHEMIA; TOLERANCE;

D O I：

10.1038/jcbfm.1993.99

中图分类号：

R5 [内科学];

学科分类号：

1002 ; 100201 ;

摘要：

To evaluate the mechanism of tolerance to ischemia, inductions of heat shock protein (HSP) 70 and heat shock cognate protein (HSC) 70 mRNAs in gerbil hippocampus were compared with in situ hybridization between cases of a single 3.5-min period of forebrain ischemia and a 3.5-min period of ischemia 2 days after 2-min pretreatment with ischemia. Immunohistochemistry for HSP70 protein and morphological studies were also performed in the same brains up to 7 days after the reperfusion. Following a single 3.5-min period of ischemia, HSP70 and HSC70 mRNAs were induced in all hippocampal cells. However, the hippocampal CA1 cells produced only a minimum of HSP70 protein, and the cells were almost lost by 7 days. Following 3.5 min of ischemia after 2-min pretreatment, large populations of the CA1 cells survived at 7 days. The peak time of the HSP70 and HSC70 mRNA induction shifted to an earlier period of reperfusion in all hippocampal cells as compared with the case of a single episode of ischemia. The peak of HSP70 and HSC70 mRNA induction shifted from 1 day to 3 h in the CA1 cells. The CA1 cells produced strongly immunoreactive HSP70 from 3 hr to 2 days. These results suggest that pretreatment with an initial period of ischemia (for 2 min) accelerated HSP70 and HSC70 gene expression at the transcriptional level, ameliorated the translational disturbance of HSP70 mRNA to protein, and saved the CA1 cells from subsequent lethal ischemia (for 3.5 min). These changes of heat shock gene expression might play important roles in the acquisition of ischemic tolerance of hippocampal CA1 neurons.

引用

页码：781 / 788

页数：8

共 30 条

[1] ABE K, 1989, ANN NY ACAD SCI, V559, P259
[2] INDUCTION OF HSP70 MESSENGER-RNA AFTER TRANSIENT ISCHEMIA IN GERBIL BRAIN
ABE, K
TANZI, RE
KOGURE, K
[J]. NEUROSCIENCE LETTERS, 1991, 125 (02) : 166 - 168
[3] TEMPORAL PROFILE OF THE INDUCTION OF HEAT-SHOCK PROTEIN-70 AND HEAT-SHOCK COGNATE PROTEIN-70 MESSENGER-RNAS AFTER TRANSIENT ISCHEMIA IN GERBIL BRAIN
AOKI, M
ABE, K
KAWAGOE, J
SATO, S
NAKAMURA, S
KOGURE, K
[J]. BRAIN RESEARCH, 1993, 601 (1-2) : 185 - 192
[4] REGIONAL IMPAIRMENT OF PROTEIN-SYNTHESIS FOLLOWING BRIEF CEREBRAL-ISCHEMIA IN THE GERBIL
ARAKI, T
KATO, H
INOUE, T
KOGURE, K
[J]. ACTA NEUROPATHOLOGICA, 1990, 79 (05) : 501 - 505
[5] MECHANISMS OF HEAT-SHOCK GENE ACTIVATION IN HIGHER EUKARYOTES
BIENZ, M
PELHAM, HRB
[J]. ADVANCES IN GENETICS INCORPORATING MOLECULAR GENETIC MEDICINE, 1987, 24 : 31 - 72
[6] INDUCTION OF A HEAT-SHOCK GENE AT THE SITE OF TISSUE-INJURY IN THE RAT-BRAIN
BROWN, IR
RUSH, S
IVY, GO
[J]. NEURON, 1989, 2 (06) : 1559 - 1564
[7] PROTECTION AGAINST HIPPOCAMPAL CA1 CELL LOSS BY POSTISCHEMIC HYPOTHERMIA IS DEPENDENT ON DELAY OF INITIATION AND DURATION
CARROLL, M
BEEK, O
[J]. METABOLIC BRAIN DISEASE, 1992, 7 (01) : 45 - 50
[8] TRAUMA-INDUCED PROTEIN IN RAT-TISSUES - A PHYSIOLOGICAL-ROLE FOR A HEAT-SHOCK PROTEIN
CURRIE, RW
WHITE, FP
[J]. SCIENCE, 1981, 214 (4516) : 72 - 73
[9] SYNTHESIS OF HEAT-SHOCK PROTEINS IN RAT-BRAIN CORTEX AFTER TRANSIENT ISCHEMIA
DIENEL, GA
KIESSLING, M
JACEWICZ, M
PULSINELLI, WA
[J]. JOURNAL OF CEREBRAL BLOOD FLOW AND METABOLISM, 1986, 6 (04) : 505 - 510
[10] INDUCED THERMAL RESISTANCE IN HELA-CELLS
GERNER, EW
SCHNEIDER, MJ
[J]. NATURE, 1975, 256 (5517) : 500 - 502

← 1 2 3 →