The characteristic dimension in scraped surface heat transfer

SUMMARY1. The effect on renal Na and water excretion of increasing the NaCl concentration of blood supplying the brain was investigated in conscious water-loaded sheep. Intracarotid infusion of 4 m-NaCl at 0-8 ml./min for 60 min was compared with equivalent intrajugular infusion.2. A more rapid increase in renal Na excretion and urine osmolality occurred with the intracarotid infusions than with intrajugular infusions.3. Intracarotid infusions of 2 M sucrose or fructose at 1-6 ml./min for 30 min compared with equivalent intrajugular infusions also caused a greater increase in renal Na excretion, urine osmolality and a decrease in urine flow rate.4. The results suggest that there are receptors in the brain sensitive to changes in extracellular tonicity which influence renal Na excretion. It is possible that changes in ADH secretion alone mediate the early natriuresis seen with intracarotid hypertonic infusions although an alternative concurrent mechanism cannot be ruled out.

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Mechanism of natriuresis during intrarenal infusion of prostaglandins

Haas¹,

Hammond²,

Granger³

et al. 1984

American Journal of Physiology-Renal Physiology

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Intrarenal infusion of the natural prostaglandin PGE2 increases renal blood flow, renal interstitial hydrostatic pressure, and urinary sodium excretion. A newly synthesized prostaglandin analogue, 4-3-[3-[2-(1-hydroxycyclohexyl)- ethyl]-4-oxo-2-thiazolidinyl]propyl benzoic acid, increases renal blood flow without increasing sodium excretion. To investigate the role of renal interstitial hydrostatic pressure in this dissociation, comparisons were made between PGE2 and the prostaglandin analogue. Intrarenal infusion of PGE2 increased renal blood flow, renal interstitial hydrostatic pressure, and urinary sodium excretion. Following a similar increase in renal blood flow with intrarenal infusion of prostaglandin analogue, renal interstitial hydrostatic pressure and urinary sodium excretion were not changed. To determine whether increases in urinary sodium excretion due to PGE2 infusion are causally related to the increase in renal interstitial hydrostatic pressure rather than to the increase in renal blood flow, responses to PGE2 were obtained in the absence of increases in interstitial pressure. When renal interstitial hydrostatic pressure was held constant, urinary sodium excretion did not change although there was a marked increase in renal blood flow. We conclude that increased renal interstitial hydrostatic pressure is necessary to produce an increase in urinary sodium excretion with prostaglandin-mediated renal vasodilation.

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Brain osmoreceptors, cerebrospinal fluid electrolyte composition and thirst

1974

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E H Blaine

Evidence for a renal vascular receptor in control of renin secretion

A central osmosensitive receptor for renal sodium excretion.

Mechanism of natriuresis during intrarenal infusion of prostaglandins

Brain osmoreceptors, cerebrospinal fluid electrolyte composition and thirst

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