Pentosan polysulfate preserves renal microvascular P2X 1 receptor reactivity and autoregulatory behavior in DOCA-salt hypertensive rats
Inflammation contributes to ANG II-associated impairment of renal autoregulation and microvascular P2X 1 receptor signaling, but its role in renal autoregulation in mineralocorticoid-induced hypertension is unknown. Autoregulatory behavior was assessed using the blood-perfused juxtamedullary nephron...
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Veröffentlicht in: | American journal of physiology. Renal physiology 2016-03, Vol.310 (6), p.F456-F465 |
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Sprache: | eng |
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Zusammenfassung: | Inflammation contributes to ANG II-associated impairment of renal autoregulation and microvascular P2X
1
receptor signaling, but its role in renal autoregulation in mineralocorticoid-induced hypertension is unknown. Autoregulatory behavior was assessed using the blood-perfused juxtamedullary nephron preparation. Hypertension was induced in uninephrectomized control rats (UNx) by subcutaneous implantation of a DOCA pellet plus administration of 1% NaCl in the drinking water (DOCA-salt) for 3 wk. DOCA-salt rats developed hypertension that was unaltered by anti-inflammatory treatment with pentosan polysulfate (DOCA-salt+PPS) but was suppressed with “triple therapy” (hydrochlorothiazide, hydralazine, and reserpine; DOCA-salt+TTx). Baseline arteriolar diameters were similar across all groups. UNx rats exhibited pressure-dependent vasoconstriction with diameters declining to 69 ± 2% of control at 170 mmHg, indicating intact autoregulation. DOCA-salt treatment significantly blunted this pressure-mediated vasoconstriction. Diameters remained between 91 ± 4 and 98 ± 3% of control over 65–170 mmHg, indicating impaired autoregulation. In contrast, pressure-mediated vasoconstriction was preserved in DOCA-salt+PPS and DOCA-salt+TTx rats, reaching 77 ± 7 and 75 ± 3% of control at 170 mmHg, respectively. ATP is required for autoregulation via P2X
1
receptor activation. ATP- and β,γ-methylene ATP (P2X
1
receptor agonist)-mediated vasoconstriction were markedly attenuated in DOCA-salt rats compared with UNx ( P < 0.05), but significantly improved by PPS or TTx ( P < 0.05 vs. DOCA-salt) treatment. Arteriolar responses to adenosine and UTP (P2Y
2
receptor agonist) were unaffected by DOCA-salt treatment. PPS and TTx significantly reduced MCP-1 and protein excretion in DOCA-salt rats. These results support the hypothesis that hypertension triggers inflammatory cascades but anti-inflammatory treatment preserves renal autoregulation in DOCA-salt rats, most likely by normalizing renal microvascular reactivity to P2X
1
receptor activation. |
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ISSN: | 1931-857X 1522-1466 |
DOI: | 10.1152/ajprenal.00110.2015 |