ENERGY-METABOLISM AND SELECTIVE NEURONAL VULNERABILITY FOLLOWING GLOBAL CEREBRAL-ISCHEMIA

被引:45
|
作者
SIMS, NR [1 ]
机构
[1] FLINDERS UNIV S AUSTR,CTR NEUROSCI,ADELAIDE,SA 5001,AUSTRALIA
来源
NEUROCHEMICAL RESEARCH | 1992年 / 17卷 / 09期
关键词
ISCHEMIA; ENERGY METABOLISM; GLUCOSE METABOLISM; MITOCHONDRIA; NEURONAL DEGENERATION;
D O I
10.1007/BF00993269
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
A short period of global ischemia results in the death of selected subpopulations of neurons. Some advances have been made in understanding events which might contribute to the selectivity of this damage but the cellular changes which culminate in neuronal death remain poorly defined. This overview examines the metabolic state of tissue in the post-ischemic period and the relationship of changes to the development of damage in areas containing ischemia-susceptible neurons. During early recirculation there is substantial recovery of ATP, phosphocreatine and related metabolites in all brain regions. However, this recovery does not signal restitution of normal energy metabolism as reductions of the oxidative metabolism of glucose are seen in many areas and may persist for several days. Furthermore, decreases in pyruvate-supported respiration develop in mitochondria from at least one ischemia-susceptible region at times coincident with the earliest histological evidence of ischemia-induced degeneration. These mitochondrial changes could simply be an early marker of irreversible damage but the available evidence is equally consistent with these contributing to the degenerative process and offering a potential site for therapeutic intervention.
引用
收藏
页码:923 / 931
页数:9
相关论文
共 50 条
  • [41] SELECTIVE ALTERATIONS IN AMYLOID PRECURSOR PROTEIN FOLLOWING TRANSIENT CEREBRAL-ISCHEMIA
    HORSBURGH, K
    MCCULLOCH, J
    BRITISH JOURNAL OF PHARMACOLOGY, 1995, 116 : P350 - P350
  • [42] INHIBITION OF TYROSINE PHOSPHORYLATION PREVENTS DELAYED NEURONAL DEATH FOLLOWING CEREBRAL-ISCHEMIA
    KINDY, MS
    JOURNAL OF CEREBRAL BLOOD FLOW AND METABOLISM, 1993, 13 (03): : 372 - 377
  • [43] ENERGY-METABOLISM AND RENAL ISCHEMIA
    SOUTHARD, JH
    LINDELL, SL
    BELZER, FO
    RENAL FAILURE, 1992, 14 (03) : 251 - 255
  • [44] EFFECT OF FENTANYL ON THE ELECTROPHYSIOLOGICAL RECOVERY FOLLOWING INCOMPLETE GLOBAL CEREBRAL-ISCHEMIA
    VASTHARE, US
    RUBIN, S
    RIINA, HA
    ROSENWASSER, RH
    CARLSSON, C
    TUMA, RF
    DRUG DEVELOPMENT RESEARCH, 1991, 23 (03) : 227 - 232
  • [45] NEURONAL DAMAGE AND CALCIUM ACCUMULATION FOLLOWING REPEATED BRIEF CEREBRAL-ISCHEMIA IN THE GERBIL
    ARAKI, T
    KATO, H
    KOGURE, K
    BRAIN RESEARCH, 1990, 528 (01) : 114 - 122
  • [46] ADENOSINE AGONISTS AND GLOBAL CEREBRAL-ISCHEMIA
    KOLVENBACH, R
    FIGGE, C
    GODEHARDT, E
    SANDMANN, W
    BRITISH JOURNAL OF CLINICAL PHARMACOLOGY, 1993, 36 (02) : 134 - 135
  • [47] Bioactive glycerophospholipids and their role in modulating neuronal vulnerability following cerebral ischemia
    Xu, H.
    Valenzuela, N.
    Syrett, A.
    Graham, K.
    Fai, S.
    Bennett, S. A.
    STROKE, 2012, 43 (11) : E134 - E134
  • [48] Zinc neurotoxicity may contribute to selective neuronal death following transient global cerebral ischemia
    Choi, DW
    COLD SPRING HARBOR SYMPOSIA ON QUANTITATIVE BIOLOGY, 1996, 61 : 385 - 387
  • [49] CHEMICAL NEUROANATOMY OF ENERGY-METABOLISM - IMMUNOHISTOCHEMICAL STUDIES IN RELATION TO SELECTIVE VULNERABILITY
    KO, L
    SHEU, KFR
    BLASS, JP
    JOURNAL OF NEUROCHEMISTRY, 1993, 61 : S70 - S70
  • [50] EFFECTS OF PHENOBARBITAL IN CEREBRAL ISCHEMIA .1. CEREBRAL ENERGY-METABOLISM DURING PRONOUNCED INCOMPLETE ISCHEMIA
    NORDSTROM, CH
    SIESJO, BK
    STROKE, 1978, 9 (04) : 327 - 335
12345