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Failure to vasodilate in response to salt loading blunts renal blood flow and causes salt-sensitive hypertension

Jing Wu, Larry N Agbor, Shi Fang, Masashi Mukohda, Anand R. Nair, Pablo Nakagawa, Avika Sharma, Donald A. Morgan, Justin L. Grobe, Kamal Rahmouni, Robert M. Weiss, James A. McCormick, Curt D. Sigmund

2020Cardiovascular Research29 citationsDOIOpen Access PDF

Abstract

AIMS: Salt-sensitive (SS) hypertension is accompanied by impaired vasodilation in the systemic and renal circulation. However, the causal relationship between vascular dysfunction and salt-induced hypertension remains controversial. We sought to determine whether primary vascular dysfunction, characterized by a failure to vasodilate during salt loading, plays a causal role in the pathogenesis of SS hypertension. METHODS AND RESULTS: Mice selectively expressing a peroxisome proliferator-activated receptor γ dominant-negative mutation in vascular smooth muscle (S-P467L) exhibited progressive SS hypertension during a 4 week high salt diet (HSD). This was associated with severely impaired vasodilation in systemic and renal vessels. Salt-induced impairment of vasodilation occurred as early as 3 days after HSD, which preceded the onset of SS hypertension. Notably, the overt salt-induced hypertension in S-P467L mice was not driven by higher cardiac output, implying elevations in peripheral vascular resistance. In keeping with this, HSD-fed S-P467L mice exhibited decreased smooth muscle responsiveness to nitric oxide (NO) in systemic vessels. HSD-fed S-P467L mice also exhibited elevated albuminuria and a blunted increase in urinary NO metabolites which was associated with blunted renal blood flow and increased sodium retention mediated by a lack of HSD-induced suppression of NKCC2. Blocking NKCC2 function prevented the salt-induced increase in blood pressure in S-P467L mice. CONCLUSION: We conclude that failure to vasodilate in response to salt loading causes SS hypertension by restricting renal perfusion and reducing renal NO through a mechanism involving NKCC2 in a mouse model of vascular peroxisome proliferator-activated receptor γ impairment.

Topics & Concepts

Renal blood flowMedicineInternal medicineBlood flowCardiologySalt (chemistry)EndocrinologyBlood pressureHeart failureChemistryPhysical chemistrySodium Intake and HealthNitric Oxide and Endothelin EffectsRenin-Angiotensin System Studies
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