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脲酶抑制剂乙酰氧肟酸在大鼠终末内髓集合管中通过尿素途径转运。

The urease inhibitor acetohydroxamic acid is transported by the urea pathway in rat terminal IMCD.

作者信息

Star R A, Gillin A D, Parikh V J, Sands J M

机构信息

Department of Internal Medicine, University of Texas Southwestern Medical Center, Dallas 75235-8856.

出版信息

Am J Physiol. 1993 Sep;265(3 Pt 2):F385-90. doi: 10.1152/ajprenal.1993.265.3.F385.

DOI:10.1152/ajprenal.1993.265.3.F385
PMID:8214097
Abstract

Acetohydroxamic acid (AHA), a urea analogue, is used clinically to dissolve struvite stones because it inhibits the urease produced by Proteus mirabilis. To be effective, the concentration of AHA must be high in the collecting duct system and final urine. Because AHA is structurally similar to urea, we investigated whether AHA is transported by the urea carrier found in the terminal inner medullary collecting duct (IMCD) and the erythrocyte. We examined AHA transport under four conditions known to affect urea movement across the terminal IMCD, i.e., stimulation by vasopressin (AVP) and hyperosmolality, and inhibition by phloretin and urea analogues. The AHA permeability was determined with a 10 mM bath-to-lumen AHA gradient. AHA was measured by ultramicrocolorimetry. Addition of 1 nM AVP to the bath increased the AHA permeability of the perfused terminal IMCD. Increasing perfusate and bath osmolality from 290 to 690 mosmol/kgH2O (by adding NaCl) also increased tubule permeability to AHA. Addition of either 0.25 mM phloretin to the bath or 200 mM thiourea to the lumen reversibly inhibited the AVP-stimulated AHA permeability. AHA-induced osmotic lysis of erythrocytes was inhibited by phloretin or thionicotinamide; AHA inhibited the osmotic lysis induced by the urea analogue acetamide. Thus, in the rat terminal IMCD, both urea and AHA transport are stimulated by AVP and hyperosmolality, and both are inhibited by phloretin and thiourea. In erythrocytes, both urea and AHA transport are inhibited by phloretin or thionicotinamide. Thus AHA is transported by the urea carrier in the terminal IMCD and erythrocyte.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

乙酰氧肟酸(AHA)是一种尿素类似物,临床上用于溶解鸟粪石结石,因为它能抑制奇异变形杆菌产生的脲酶。为了发挥作用,AHA在集合管系统和终尿中的浓度必须很高。由于AHA在结构上与尿素相似,我们研究了AHA是否通过终末内髓集合管(IMCD)和红细胞中的尿素载体进行转运。我们在已知影响尿素跨终末IMCD转运的四种条件下研究了AHA的转运,即抗利尿激素(AVP)刺激和高渗状态,以及根皮素和尿素类似物的抑制作用。通过10 mM浴液至管腔的AHA梯度测定AHA通透性。通过超微量比色法测量AHA。向浴液中添加1 nM AVP可增加灌注的终末IMCD对AHA的通透性。将灌注液和浴液渗透压从290 mosmol/kgH2O增加到690 mosmol/kgH2O(通过添加氯化钠)也增加了肾小管对AHA的通透性。向浴液中添加0.25 mM根皮素或向管腔中添加200 mM硫脲可可逆地抑制AVP刺激的AHA通透性。根皮素或硫代烟酰胺可抑制AHA诱导的红细胞渗透溶解;AHA可抑制尿素类似物乙酰胺诱导的渗透溶解。因此,在大鼠终末IMCD中,尿素和AHA的转运均受AVP和高渗状态刺激,且均受根皮素和硫脲抑制。在红细胞中,尿素和AHA的转运均受根皮素或硫代烟酰胺抑制。因此,AHA通过终末IMCD和红细胞中的尿素载体进行转运。(摘要截短于250字)

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The urease inhibitor acetohydroxamic acid is transported by the urea pathway in rat terminal IMCD.脲酶抑制剂乙酰氧肟酸在大鼠终末内髓集合管中通过尿素途径转运。
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