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代谢性、机械性、热性或化学性损伤恢复过程中脑鸟氨酸脱羧酶的诱导。

Induction of brain ornithine decarboxylase during recovery from metabolic, mechanical, thermal, or chemical injury.

作者信息

Dienel G A, Cruz N F

出版信息

J Neurochem. 1984 Apr;42(4):1053-61. doi: 10.1111/j.1471-4159.1984.tb12710.x.

Abstract

Metabolic, mechanical, thermal, and chemical injury induced ornithine decarboxylase (ODC) activity in rat brain. A two- to sixfold increase in ODC activity was measured at 5-9 h after different modes of injury to the brain. During the early phase of recovery from transient ischemia, when average protein synthesis was less than 50% of control, ODC activity was increased nearly fivefold. The rise in activity could be blocked by anisomycin, or reduced by intracerebral injections of actinomycin D. Drilling burr holes into the skull, injection of the vehicle for actinomycin D, hyperthermia, and freezing lesions all caused increased ODC activity. Neurotoxic chemicals (ammonia, methionine sulfoximine, acrylamide, carbon tetrachloride, and anisomycin) also increased brain ODC activity, whereas other chemicals (mannitol and valine) did not. Treatments known to stimulate the synthesis of heat shock proteins (carotid occlusion, hyperthermia, Cd2+, canavanine, and ethanol) induced ODC activity in the liver, whereas only hyperthermia and ethanol caused significant increases in spleen ODC activity. All increases in ODC activity were blocked by difluoromethylornithine, an irreversible inhibitor of ODC. The cellular response to noxious or stressful stimuli includes the synthesis of a small number of proteins of unknown functions; ODC may be one of these "heat shock" or "trauma" proteins.

摘要

代谢、机械、热和化学损伤可诱导大鼠脑内鸟氨酸脱羧酶(ODC)的活性。在对脑进行不同方式的损伤后5 - 9小时,可检测到ODC活性增加了2至6倍。在短暂性脑缺血恢复的早期阶段,当平均蛋白质合成低于对照的50%时,ODC活性增加了近5倍。活性的升高可被茴香霉素阻断,或通过脑内注射放线菌素D而降低。在颅骨上钻孔、注射放线菌素D的溶剂、热疗和冷冻损伤均导致ODC活性增加。神经毒性化学物质(氨、蛋氨酸亚砜亚胺、丙烯酰胺、四氯化碳和茴香霉素)也会增加脑内ODC活性,而其他化学物质(甘露醇和缬氨酸)则不会。已知能刺激热休克蛋白合成的处理(颈动脉闭塞、热疗、Cd2 +、刀豆氨酸和乙醇)可诱导肝脏中的ODC活性,而只有热疗和乙醇会使脾脏ODC活性显著增加。ODC活性的所有增加均被二氟甲基鸟氨酸阻断,二氟甲基鸟氨酸是ODC的不可逆抑制剂。细胞对有害或应激刺激的反应包括合成少量功能未知的蛋白质;ODC可能是这些“热休克”或“创伤”蛋白之一。

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