Your search keyword '"Bähring S"' showing total 3 results

1. Mutant phosphodiesterase 3A protects the kidney from hypertension-induced damage.

Author

Sholokh A, Walter S, Markó L, McMurray BJ, Sunaga-Franze DY, Xu M, Zühlke K, Russwurm M, Bartolomaeus TUP, Langanki R, Qadri F, Heuser A, Patzak A, Forslund SK, Bähring S, Borodina T, Persson PB, Maass PG, Bader M, and Klussmann E

Subjects

Humans, Cyclic Nucleotide Phosphodiesterases, Type 3, ErbB Receptors, Kidney, Epidermal Growth Factor, Hypertension complications

Published

2023

2. The Case| A handful of hypertension.

Author

van den Born BJ, Oskam LC, Zidane M, Schächterle C, Klussmann E, Bähring S, and Luft FC

Subjects

Adult, Brachydactyly genetics, Brachydactyly physiopathology, Cyclic Nucleotide Phosphodiesterases, Type 3 genetics, DNA Mutational Analysis, Female, Genetic Predisposition to Disease, Hand Bones diagnostic imaging, Humans, Hypertension diagnosis, Hypertension genetics, Hypertension physiopathology, Mutation, Phenotype, Blood Pressure genetics, Brachydactyly diagnosis, Hand Bones abnormalities, Hypertension congenital

Published

2016

3. A cross-over medication trial for patients with autosomal-dominant hypertension with brachydactyly.

Author

Schuster H, Toka O, Toka HR, Busjahn A, Oztekin O, Wienker TF, Bilginturan N, Bähring S, Skrabal F, Haller H, and Luft FC

Subjects

Adolescent, Adult, Cross-Over Studies, Double-Blind Method, Female, Humans, Hypertension genetics, Hypertension metabolism, Male, Potassium Channels physiology, Hypertension drug therapy, Limb Deformities, Congenital genetics

Abstract

We examined a family with autosomal-dominant hypertension and brachydactyly from northeastern Turkey. The hypertension was defined as severe, resulting in stroke before age 50 years, featuring normal renin, aldosterone, and catecholamine responses, and did not appear to be salt-sensitive. The responsible gene resides on chromosome 12p. To determine which medications were most effective, we performed a prospective clinical trial. We studied 13 affected individuals in a randomized double-blind, cross-over trial including a beta-blocker (BBL), alpha-blocker (ABL), calcium channel blocker (CCB), converting enzyme inhibitor (CEI), and hydrochlorothiazide (HCT) and placebo (PLA). We then added moxonidine (MOX) and continued the trial for an additional period in a single-blind fashion. Each drug was given for four weeks with an option to double the dose after two weeks; each washout period comprised two weeks. Blood, 24-hour urine, and saliva were studied at the outset, and blood and urine samples were obtained at the end of each phase. Blood pressure (BP) and heart rate measurements were with the patient ambulatory at 24 hours. All regimens required doubled doses at two weeks. Beta blocker, CCB, CEI, and ABL lowered BP (6 to 10 mm Hg) and BP load compared to PLA, while HCT and MOX did not. Converting enzyme inhibitor and HCT increased plasma renin activity (PRA), while BBL lowered PRA. The 24-hour urine analysis indicated a high dietary salt intake with a low potassium and calcium intake. The salivary electrolytes showed similar sodium and potassium concentrations, while chloride values were significantly higher in affected than nonaffected subjects. Thus, this monogenic form of hypertension resembles nonsalt-sensitive essential hypertension in that BBL, CCB, CEI, and ABL were effective, while HCT was not. The BP reduction was similar to other single drug trials in essential hypertension. The high salivary chloride values suggest an additional intermediary phenotype that may be related to electrolyte transport. These results raise the possibility that an as yet unknown hypertensive mechanism is operative in these subjects.

Published

1998