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二巯基琥珀酸螯合疗法在降低啮齿动物模型脑铅含量方面的疗效。

Efficacy of succimer chelation for reducing brain Pb levels in a rodent model.

作者信息

Smith D, Bayer L, Strupp B J

机构信息

Department of Environmental Toxicology, University of California, Santa Cruz 95064, USA.

出版信息

Environ Res. 1998 Aug;78(2):168-76. doi: 10.1006/enrs.1998.3854.

Abstract

Increasing evidence indicates that early low-level lead (Pb) exposure produces enduring cognitive impairment in children, underscoring the need to develop improved therapeutic intervention. Although chelating agents have been shown to effectively reduce body Pb levels, it is not yet known whether this treatment ameliorates Pb-induced cognitive dysfunction. Clinical research in this area is hampered by the need to rely on reductions in blood Pb levels as the index of treatment efficacy, despite the fact that brain Pb level is the exposure parameter of greatest relevance to neurocognitive outcomes. The present studies were designed to provide information that will aid future research in this area in both human and animal models. The objectives of these studies were (1) to evaluate the efficacy of different doses and durations of succimer (meso-2,3-dimercaptosuccinic acid; DMSA) chelation for reducing brain and blood Pb levels and (2) to determine the extent to which blood Pb can serve as a surrogate of brain Pb following chelation. Long-Evans hooded rats were exposed to Pb from birth until day 31 (Study 1) or day 40 (Study 2) of life, followed by oral treatment with a vehicle or one of two succimer regimens for a duration of either 7 or 21 days. Results indicated that 7 days of succimer treatment produced a 1.5- to 2.5-fold greater reduction of Pb in blood than in brain, relative to time-matched vehicle groups. Prolonged treatment (21) days did not further reduce blood Pb levels (relative to 7-day succimer treatment), but did produce further reductions in brain Pb level compared to time-matched vehicle groups. Thus, chelation-mediated reductions in brain Pb did not parallel reductions in blood Pb over the course of treatment. While the relevance of these data to humans may be confounded by anatomical and physiological differences between rodents and primates, as well as differences in the metabolism of succimer (DMSA), they suggest that clinical studies should exercise caution when using blood Pb as an index of the efficacy of chelation treatment for reducing brain Pb levels.

摘要

越来越多的证据表明,儿童早期低水平铅(Pb)暴露会导致持久的认知障碍,这凸显了开发改进治疗干预措施的必要性。尽管螯合剂已被证明能有效降低体内铅水平,但这种治疗是否能改善铅诱导的认知功能障碍尚不清楚。该领域的临床研究因需要依赖血铅水平降低作为治疗效果指标而受到阻碍,尽管脑铅水平才是与神经认知结果最相关的暴露参数。本研究旨在提供有助于该领域未来人类和动物模型研究的信息。这些研究的目的是:(1)评估不同剂量和疗程的二巯基丁二酸(meso-2,3-二巯基丁二酸;DMSA)螯合对降低脑铅和血铅水平的疗效;(2)确定螯合后血铅可在多大程度上作为脑铅的替代指标。将Long-Evans有帽大鼠从出生暴露于铅直至生命的第31天(研究1)或第40天(研究2),随后用赋形剂或两种二巯基丁二酸方案之一进行口服治疗,持续7天或21天。结果表明,与时间匹配的赋形剂组相比,7天的二巯基丁二酸治疗使血铅降低幅度比脑铅大1.5至2.5倍。延长治疗(21天)并未进一步降低血铅水平(相对于7天的二巯基丁二酸治疗),但与时间匹配的赋形剂组相比,确实使脑铅水平进一步降低。因此,在治疗过程中,螯合介导的脑铅降低与血铅降低并不平行。虽然这些数据与人类的相关性可能因啮齿动物和灵长类动物之间的解剖学和生理学差异以及二巯基丁二酸(DMSA)代谢差异而受到混淆,但它们表明临床研究在将血铅用作螯合治疗降低脑铅水平疗效指标时应谨慎行事。

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