OXIDATION CHEMISTRY OF INDOLES

吲哚的氧化化学

• 批准号: 3281132
• 负责人: GLENN DRYHURST
• 金额: $ 24.66万
• 依托单位: UNIVERSITY OF OKLAHOMA
• 依托单位国家: 美国
• 财政年份: 1983
• 资助国家: 美国
• 起止时间: 1983-09-15 至 1995-08-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/3281132
• 关键词: 5 hydroxytryptophan; Alzheimer's disease; autooxidation; brain mapping; brain metabolism; catecholamine inhibitor; cell components; disease /disorder model; dorsal raphe nucleus; drug screening /evaluation; electrical potential; electrochemistry; high performance liquid chromatography; histochemistry /cytochemistry; hydroxyindoleacetate; hydroxyl group; immunocytochemistry; indoles; infrared spectrometry; laboratory mouse; laboratory rat; locus coeruleus; mass spectrometry; neural degeneration; neurotoxins; neurotransmitter metabolism; neurotransmitter receptor; nuclear magnetic resonance spectroscopy; oxidation; peroxidases; receptor binding; serotonin; serotonin inhibitor; serotonin receptor; toxicant screening; tryptophan analog

The chemical or biochemical processes which cause degeneration of rather selective areas of the brain in Alzheimer's Disease (AD) are unknown. It is known, however, that there is a serious serotonergic dysfunction in AD. Furthermore, the indolic neurotransmitter 5-hydroxytryptamine (5-HT) and related central indoles are easily oxidized compounds. Some oxidation products when centrally administered to mice evoke profound behavioral responses, and cause transmitter depletions and/or metabolite disruptions in the catecholaminergic, serotonergic and cholinergic neuronal systems, i.e., systems most profoundly affected in AD. Unidentified but oxidized forms of 5-HT and other central indoles are present in cerebrospinal fluid of AD patients but not in that of age-matched controls. And, conditions appear to exist in Alzheimer brain tissue which should facilitate oxidation reactions. Taken together this evidence leads to a hypothesis that a defect in the serotonergic system in Alzheimer brain results in aberrant oxidations of central indoles forming toxins. The hypothesis further proposes that these toxins attack not only the parent serotonergic neurons, principally the raphe nuclei, but are released and attack the physically proximate noradrenergic locus coeruleus and the cholinergic nucleus basalis complex. These three structures originate in the isodendritic core and project to cortical regions of the brain and are rather selectively degenerated in AD. The specific aims of this proposal are to elucidate the oxidation chemistry and biochemistry of the central indoles under experimental conditions which might be relevant to those which exist in alzheimer brain tissue. Resulting products will be screened for toxicity and behavioral response following central administration to mice and rats. The effects of active drugs on the catecholaminergic serotonergic, and cholinergic neuronal systems will be investigated by neurotransmitter/metabolite analyses. In order to more fully understand the mode of action of active drugs, studies of transmitter uptake/release processes, effects on key biosynthetic and biodegradative enzymes, and on CNS receptors are planned. Histochemical and microscopic studies will be employed to assess specific regions of neuronal damage or destruction. Chemical mechanisms underlying the toxic effects of certain active drugs will be investigated. Evidence will also be sought to demonstrate that central indoles undergo oxidation reactions even under conditions of non-pathological aging, reactions which may be greatly accelerated in AD. Ultimately, it is expected that these studies might provide important insights into some aspects of the neuronal degeneration and biochemical defects underlying AD.

变质：导致细胞退化的化学或生物化学过程