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用于在体内采集细胞外液和给药的改良型微透析探针。

Modified microdialysis probe for sampling extracellular fluid and administering drugs in vivo.

作者信息

Yadid G, Pacak K, Kopin I J, Goldstein D S

机构信息

Clinical Neuroscience Branch, National Institute of Neurological Disorders and Stroke, National Institutes of Health, Bethesda, Maryland 20892.

出版信息

Am J Physiol. 1993 Nov;265(5 Pt 2):R1205-11. doi: 10.1152/ajpregu.1993.265.5.R1205.

Abstract

In vivo microdialysis provides an important new tool for investigating changes in extracellular fluid levels of endogenous compounds in vivo. Delivery of drugs via the microdialysis probe can be used to study local release and metabolism of neurotransmitters, but the dialysis membrane limits diffusion of substances between the perfusate and the extracellular fluid. Thus there may be considerable delay in responses, drug concentrations at the effector sites are less than those in the probe, and high-molecular-weight substances cannot traverse the membrane at all. This report describes a simple modification of commercially available microdialysis probes. A cannula is glued to the external surface of the probe. When glycine was administered via the cannula into the striatum of conscious rats, increments in microdialysate concentrations of dopamine were at least 10 times greater than when glycine was administered via the dialysis fluid in the probe. The threshold glycine dose for behavioral (turning) effects was also decreased by approximately 60-fold, and the time to the peak neurochemical and behavioral effects was markedly decreased. The modified probe did not destroy local catecholaminergic cells, as indicated by tyrosine hydroxylase immunofluorescence. Use of the modified microdialysis probe should facilitate pharmacological and neuroendocrine studies in behaving animals.

摘要

体内微透析为研究体内内源性化合物细胞外液水平的变化提供了一种重要的新工具。通过微透析探针给药可用于研究神经递质的局部释放和代谢,但透析膜限制了物质在灌注液和细胞外液之间的扩散。因此,反应可能会有相当大的延迟,效应部位的药物浓度低于探针中的浓度,并且高分子量物质根本无法穿过膜。本报告描述了对市售微透析探针的一种简单改进。将一根套管粘在探针的外表面。当通过套管将甘氨酸注入清醒大鼠的纹状体时,微透析液中多巴胺浓度的增加至少比通过探针中的透析液给予甘氨酸时大10倍。行为(转向)效应的甘氨酸阈值剂量也降低了约60倍,神经化学和行为效应达到峰值的时间明显缩短。如酪氨酸羟化酶免疫荧光所示,改良后的探针并未破坏局部儿茶酚胺能细胞。使用改良后的微透析探针应有助于对行为动物进行药理学和神经内分泌研究。

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