Phosducin influences sympathetic activity and prevents stress-induced hypertension in humans and mice
Nadine Beetz, … , Ulrich Broeckel, Lutz Hein
Nadine Beetz, … , Ulrich Broeckel, Lutz Hein
Published November 23, 2009
Citation Information: J Clin Invest. 2009;119(12):3597-3612. https://doi.org/10.1172/JCI38433.
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Phosducin influences sympathetic activity and prevents stress-induced hypertension in humans and mice

Abstract

Hypertension and its complications represent leading causes of morbidity and mortality. Although the cause of hypertension is unknown in most patients, genetic factors are recognized as contributing significantly to an individual’s lifetime risk of developing the condition. Here, we investigated the role of the G protein regulator phosducin (Pdc) in hypertension. Mice with a targeted deletion of the gene encoding Pdc (Pdc–/– mice) had increased blood pressure despite normal cardiac function and vascular reactivity, and displayed elevated catecholamine turnover in the peripheral sympathetic system. Isolated postganglionic sympathetic neurons from Pdc–/– mice showed prolonged action potential firing after stimulation with acetylcholine and increased firing frequencies during membrane depolarization. Furthermore, Pdc–/– mice displayed exaggerated increases in blood pressure in response to post-operative stress. Candidate gene–based association studies in 2 different human populations revealed several SNPs in the PDC gene to be associated with stress-dependent blood pressure phenotypes. Individuals homozygous for the G allele of an intronic PDC SNP (rs12402521) had 12–15 mmHg higher blood pressure than those carrying the A allele. These findings demonstrate that PDC is an important modulator of sympathetic activity and blood pressure and may thus represent a promising target for treatment of stress-dependent hypertension.

Authors

Nadine Beetz, Michael D. Harrison, Marc Brede, Xiangang Zong, Michal J. Urbanski, Anika Sietmann, Jennifer Kaufling, Michel Barrot, Mathias W. Seeliger, Maria Augusta Vieira-Coelho, Pavel Hamet, Daniel Gaudet, Ondrej Seda, Johanne Tremblay, Theodore A. Kotchen, Mary Kaldunski, Rolf Nüsing, Bela Szabo, Howard J. Jacob, Allen W. Cowley Jr., Martin Biel, Monika Stoll, Martin J. Lohse, Ulrich Broeckel, Lutz Hein

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Figure 2

Pdc-deficient mice have increased blood pressure.

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Pdc-deficient mice have increased blood pressure. (A and B) Midequatoria...
(A and B) Midequatorial cross-sections through the hearts of wild-type (A, inset) or Pdc–/– mice (B, inset) did not reveal microscopic alterations in Pdc–/– hearts (H&E staining). Scale bars: 50 μm (A and B); 0.5 mm (insets). (C) Heart weight/tibia length ratios did not differ between Pdc+/+ and Pdc–/– mice (age 1.5–2 months, n = 6–10 per genotype; P = 0.213). (DG) During isoflurane anesthesia, arterial and left ventricular catheterization with a microtip catheter revealed increased SBP and DBP and dP/dtmax in Pdc–/– mice (n = 8 per genotype group). *P < 0.05, **P < 0.01, ***P < 0.001. (HJ) Infusion i.v. of norepinephrine or dobutamine in anesthetized mice did not reveal differences in hemodynamic response between genotypes (n = 6–11 per genotype).