Literature DB >> 22966789

Effect of amiloride and spironolactone on renal tubular function and central blood pressure in patients with arterial hypertension during baseline conditions and after furosemide: a double-blinded, randomized, placebo-controlled crossover trial.

Solveig K Matthesen1, Thomas Larsen, Henrik Vase, Thomas G Lauridsen, Janni M Jensen, Erling B Pedersen.   

Abstract

This study demonstrates that the increased potassium content in the body seems to change both the blood pressure and renal tubular function. We wanted to test the hypotheses that amiloride and spironolactone induced potassium retention reduces ambulatory blood pressure (ABP) and central blood pressure (CBP) during baseline conditions and after furosemide and that the tubular transport via the epithelial sodium channels (ENaCs) and aquaporin-2 (AQP2) water channels was increased by furosemide in arterial hypertension. Each of three 28-day treatment periods (placebo, amiloride, and spironolactone) was completed by a 4-day period with standardized diet regarding calories and sodium and water intake. At the end of each period, we measured pulse wave velocity (PWV), central systolic blood pressure (CSBP), central diastolic blood pressure (CDBP), glomerular filtration rate (GFR), free water clearance (CH2O), fractional excretion of sodium (FENa) and potassium (FEK), urinary excretion of AQP2 (u-AQP2), urinary excretion of γ-fraction of the ENaC (u-ENaCγ), and plasma concentrations of renin (PRC), angiotensin II (p-Ang II), and aldosterone (p-Aldo) at baseline conditions and after furosemide bolus. Ambulatory blood pressure and CBP were significantly lowered by amiloride and spironolactone. During 24-hour urine collection and at baseline, GFR, CH2O, FENa, FEK, u-AQP2 and u-ENaCγ were the same. After furosemide, CH2O, FENa, FEK, u-AQP2, u-ENaCγ, PRC, p-Ang II, p-Aldo, PWV and CDBP increased after all treatments. However, during amiloride treatment, FEK increased to a larger extent than after spironolactone and during placebo after furosemide, and CSBP was not significantly reduced. The increases in water and sodium absorption via AQP2 and ENaC after furosemide most likely are compensatory phenomena to antagonize water and sodium depletion. Amiloride is less effective than spironolactone to reduce renal potassium excretion.

Entities:  

Mesh:

Substances:

Year:  2012        PMID: 22966789     DOI: 10.3109/10641963.2012.721843

Source DB:  PubMed          Journal:  Clin Exp Hypertens        ISSN: 1064-1963            Impact factor:   1.749


  10 in total

1.  Changes in urinary excretion of water and sodium transporters during amiloride and bendroflumethiazide treatment.

Authors:  Janni M Jensen; Frank H Mose; Anna-Ewa O Kulik; Jesper N Bech; Robert A Fenton; Erling B Pedersen
Journal:  World J Nephrol       Date:  2015-07-06

2.  Central blood pressure for the management of hypertension: Is it a practical clinical tool in current practice?

Authors:  Hao-Min Cheng; Shao-Yuan Chuang; Tzung-Dau Wang; Kazuomi Kario; Peera Buranakitjaroen; Yook-Chin Chia; Romeo Divinagracia; Satoshi Hoshide; Huynh Van Minh; Jennifer Nailes; Sungha Park; Jinho Shin; Saulat Siddique; Jorge Sison; Arieska Ann Soenarta; Guru Prasad Sogunuru; Apichard Sukonthasarn; Jam Chin Tay; Boon Wee Teo; Yuda Turana; Narsingh Verma; Yuqing Zhang; Ji-Guang Wang; Chen-Huan Chen
Journal:  J Clin Hypertens (Greenwich)       Date:  2019-12-16       Impact factor: 3.738

3.  Epithelial sodium channel inhibition by amiloride on blood pressure and cardiovascular disease risk in young prehypertensives.

Authors:  Jigar Bhagatwala; Ryan A Harris; Samip J Parikh; Haidong Zhu; Ying Huang; Ishita Kotak; Nichole Seigler; Gary L Pierce; Brent M Egan; Yanbin Dong
Journal:  J Clin Hypertens (Greenwich)       Date:  2013-10-31       Impact factor: 3.738

4.  Nocturnal blood pressure decrease in patients with chronic kidney disease and in healthy controls - significance of obstructive sleep apnea and renal function.

Authors:  Bodil G Hornstrup; Pia H Gjoerup; Jost Wessels; Thomas G Lauridsen; Erling B Pedersen; Jesper N Bech
Journal:  Int J Nephrol Renovasc Dis       Date:  2018-11-08

5.  Effect of 3% saline and furosemide on biomarkers of kidney injury and renal tubular function and GFR in healthy subjects - a randomized controlled trial.

Authors:  F H Mose; A N Jörgensen; M H Vrist; N P Ekelöf; E B Pedersen; J N Bech
Journal:  BMC Nephrol       Date:  2019-06-03       Impact factor: 2.388

6.  Antioxidant, anti-apoptotic, and protective effects of myricitrin and its solid lipid nanoparticle on streptozotocin-nicotinamide-induced diabetic nephropathy in type 2 diabetic male mice.

Authors:  Akram Ahangarpour; Ali Akbar Oroojan; Layasadat Khorsandi; Maryam Kouchak; Mohammad Badavi
Journal:  Iran J Basic Med Sci       Date:  2019-12       Impact factor: 2.699

7.  Effect of furosemide on body composition and urinary proteins that mediate tubular sodium and sodium transport-A randomized controlled trial.

Authors:  Mose Frank Holden; Anna Ewa Oczachowska-Kulik; Robert Andrew Fenton; Jesper Nørgaard Bech
Journal:  Physiol Rep       Date:  2021-01

8.  Abnormal urinary excretion of NKCC2 and AQP2 in response to hypertonic saline in chronic kidney disease: an intervention study in patients with chronic kidney disease and healthy controls.

Authors:  Janni M Jensen; Frank H Mose; Anna-Ewa O Kulik; Jesper N Bech; Robert A Fenton; Erling B Pedersen
Journal:  BMC Nephrol       Date:  2014-06-26       Impact factor: 2.388

9.  Effect of volume expansion with hypertonic- and isotonic saline and isotonic glucose on sodium and water transport in the principal cells in the kidney.

Authors:  Janni M Jensen; Frank H Mose; Jesper N Bech; Soren Nielsen; Erling B Pedersen
Journal:  BMC Nephrol       Date:  2013-09-26       Impact factor: 2.388

Review 10.  How Do Antihypertensive Drugs Work? Insights from Studies of the Renal Regulation of Arterial Blood Pressure.

Authors:  Holly Digne-Malcolm; Matthew C Frise; Keith L Dorrington
Journal:  Front Physiol       Date:  2016-07-29       Impact factor: 4.566
  10 in total

北京卡尤迪生物科技股份有限公司 © 2022-2023.