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呋塞米抑制2型11β-羟类固醇脱氢酶。

Furosemide inhibits 11beta-hydroxysteroid dehydrogenase type 2.

作者信息

Fuster D, Escher G, Vogt B, Ackermann D, Dick B, Frey B M, Frey F J

机构信息

Department of Medicine, University Hospital of Berne, Inselspital, Switzerland.

出版信息

Endocrinology. 1998 Sep;139(9):3849-54. doi: 10.1210/endo.139.9.6175.

Abstract

11Beta-hydroxsteroid dehydrogenase 2 (11beta-OHSD2) protects the nonselective renal mineralocorticoid receptor from the endogenous glucocorticoid cortisol. Thus, drugs inhibiting 11beta-OHSD2 might enhance urinary loss of potassium. As diuretics influence the renal handling of potassium, we analyzed the impact of 13 commonly used diuretics on 11beta-OHSD2. Furosemide was the only inhibitor. Its inhibition constant (Ki) was 30 micromol when extracts from COS-1 cells transfected with human 11beta-OHSD2 were used as an enzyme source. The type of inhibition was competitive. To establish whether furosemide inhibits 11beta-OHSD2 and 11beta-OHSD1 in the renal target tissue, isolated tubular segments from rats were analyzed. Furosemide decreased the oxidative activity of 11beta-OHSD2 in intact distal tubules and 11beta-OHSD1 in proximal convoluted tubules. For the assessment of furosemide on the excretion of corticosterone metabolites in vivo, rats were given furosemide i.p., and the ratio of tetrahydrocorticosterone plus 5alpha-tetrahydrocorticosterone to 11-dehydrotetrahydrocorticosterone was determined in urine. This ratio increased after the administration of furosemide in all animals, indicating inhibition of the oxidative activity of 11beta-OHSD. Thus, furosemide inhibits the 11beta-OHSD2 enzyme in the target tissue and might by that mechanism enhance the mineralocorticoid effect of 11beta-hydroxyglucocorticoids.

摘要

11β-羟类固醇脱氢酶2(11β-OHSD2)可保护非选择性肾盐皮质激素受体免受内源性糖皮质激素皮质醇的影响。因此,抑制11β-OHSD2的药物可能会增加钾的尿排泄量。由于利尿剂会影响肾脏对钾的处理,我们分析了13种常用利尿剂对11β-OHSD2的影响。速尿是唯一的抑制剂。当用人11β-OHSD2转染的COS-1细胞提取物作为酶源时,其抑制常数(Ki)为30微摩尔。抑制类型为竞争性。为确定速尿是否抑制肾靶组织中的11β-OHSD2和11β-OHSD1,对大鼠分离的肾小管节段进行了分析。速尿降低了完整远曲小管中11β-OHSD2的氧化活性以及近曲小管中11β-OHSD1的氧化活性。为评估速尿对体内皮质酮代谢产物排泄的影响,给大鼠腹腔注射速尿,并测定尿中四氢皮质酮加5α-四氢皮质酮与11-脱氢四氢皮质酮的比值。在所有动物中,注射速尿后该比值均升高,表明11β-OHSD的氧化活性受到抑制。因此,速尿抑制靶组织中的11β-OHSD2酶,并可能通过该机制增强11β-羟基糖皮质激素的盐皮质激素作用。

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