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利尿剂和抗利尿剂对锂清除率的影响作为近端输送的标志物。

Effect of diuretic and antidiuretic agents on lithium clearance as a marker for proximal delivery.

作者信息

Kirchner K A

机构信息

Department of Medicine, University of Mississippi Medical Center, Jackson 39216-4505.

出版信息

Kidney Int Suppl. 1990 Mar;28:S22-5.

PMID:2182927
Abstract

Diuretic drugs have marked effects on lithium clearance. The magnitude and mechanism of the effect depend not only on the site of action of the diuretic but also on the sodium intake of the subject as well. In sodium restricted rats all diuretics except the thiazides increase FeLi and abolish distal lithium uptake. The increase in FeLi produced by proximal and loop diuretics are associated with changes in proximal delivery. Amiloride, on the other hand, increases FeLi solely through inhibition of distal lithium uptake. Therefore, this agent is useful to detect lithium reabsorption beyond the proximal tubule. Additionally the values for FeLi obtained after amiloride administration may provide the best quantitative estimate for proximal delivery in conditions where distal lithium uptake is a consideration. Antidiuretic agents, especially those which potentiate ADH activity, may also have marked effects on lithium clearance. NSAID's and dDAVP are able to significantly reduce FeLi even in sodium loaded animals. As this occurs without a change in proximal delivery, these agents increase lithium reabsorption in distal nephron segments preferentially. Thus, estimates of proximal delivery determined by lithium clearance are not valid in the presence of these agents. Experimental conditions which produce high levels of endogenous ADH or potentiate the action of endogenous ADH may also adversely effect FeLi as a quantitative marker for proximal delivery. Whether there are other drugs which disrupt the ability of lithium clearance to function as a marker for proximal delivery requires further study.

摘要

利尿药对锂清除率有显著影响。这种影响的程度和机制不仅取决于利尿药的作用部位,还取决于受试者的钠摄入量。在限钠大鼠中,除噻嗪类药物外,所有利尿药都会增加锂排泄分数(FeLi)并消除远端锂摄取。近端和襻利尿药引起的FeLi增加与近端输送的变化有关。另一方面,阿米洛利仅通过抑制远端锂摄取来增加FeLi。因此,该药物可用于检测近端小管以外的锂重吸收。此外,在考虑远端锂摄取的情况下,服用阿米洛利后获得的FeLi值可能为近端输送提供最佳的定量估计。抗利尿药,尤其是那些增强抗利尿激素(ADH)活性的药物,也可能对锂清除率有显著影响。即使在钠负荷动物中,非甾体抗炎药(NSAID)和去氨加压素(dDAVP)也能够显著降低FeLi。由于这种情况发生时近端输送没有变化,这些药物优先增加远端肾单位节段的锂重吸收。因此,在这些药物存在的情况下,通过锂清除率确定的近端输送估计值是无效的。产生高水平内源性ADH或增强内源性ADH作用的实验条件,也可能对作为近端输送定量标志物的FeLi产生不利影响。是否有其他药物会干扰锂清除率作为近端输送标志物的功能,还需要进一步研究。

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