Thirst and salt appetite responses in young and old Brown Norway rats

Thunhorst, Robert L.; Johnson, Alan Kim

doi:10.1152/ajpregu.00368.2002

Cited by 34 publications

(57 citation statements)

References 39 publications

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“…Consistent with our previous work (40), young rats drank about twice as much as middle-aged adult and old rats in response to hypertonic loads of NaCl. Middle-aged adult and old rats never differed in their drinking responses.…”

Section: Discussionsupporting

confidence: 91%

“…Most drinking occurred in the first 30 min of testing for all ages and, at each hypertonic concentration of NaCl, drinking in the first 30 min was proportional to the load. Together with previous work (40), the present results indicate that age-related reductions in osmotic drinking begin at least by 12 mo of age in the Brown Norway strain and are apparent using a dose (2 ml/kg body wt of 0.5 M) of NaCl solution calculated to produce a 1% increase in plasma osmolality. Notably, however, in the first 30 min of testing, all ages drank significantly more water in response to all hypertonic loads compared with basal intakes observed after isotonic saline.…”

Section: Discussionsupporting

confidence: 83%

“…The variability in responding by older rats, and presumably the stress involved in testing, can be reduced by extensive preexperimental handling (36). Similarly, we have observed highly variable daily water intakes in old rats compared with young rats upon initial receipt from the supplier, which we attributed to shipping stress or a response to the novel laboratory environment (40). For this reason, we allow 3-4 wk for adaptation to laboratory conditions before beginning aging studies rather than the 1-2 wk that we typically use in studies unrelated to aging.…”

Section: Discussionmentioning

confidence: 55%

“…We (40) and others (25) find that aged rats drink less than young rats to peripherally administered hypertonic NaCl solution, but this finding is also not consistent for all laboratories (25,34). Our previous work (40) indicated that 20-mo-old Brown Norway rats are refractory to osmotic loads producing 2-4% increases in estimated plasma osmolality, but we have not used smaller loads or older rats. To characterize declines in osmotic thirst with age more thoroughly, a further goal of the present work was to assess osmotically induced drinking over additional doses of NaCl and across a wider range of ages than in our previous tests.…”

mentioning

confidence: 70%

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Hypotension- and osmotically induced thirst in old Brown Norway rats

Thunhorst¹,

Beltz²,

Johnson³

2009

American Journal of Physiology-Regulatory, Integrative and Comp

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Thunhorst RL, Beltz TG, Johnson AK. Hypotension-and osmotically induced thirst in old Brown Norway rats. Am J Physiol Regul Integr Comp Physiol 297: R149 -R157, 2009. First published May 6, 2009 doi:10.1152/ajpregu.00118.2009.-Compared to young cohorts, old rats drink less water in response to several thirst-inducing stimuli. In these experiments, we characterized water drinking in response to hypotension and cellular dehydration in young (4 mo), middle-aged adult (12 mo) and old (29 -30 mo) male Brown Norway rats. We injected the vasodilator, minoxidil as an intravenous bolus in a range of doses (0 -20 mg/kg), so that drinking responses could be compared at equivalent reductions of arterial pressure. Old rats had greatly diminished reflex tachycardia and became significantly more hypotensive after minoxidil compared with young and middle-aged rats. When compared at equivalent reductions of arterial pressure, old rats drank one-third as much as middle-aged rats, and one-fifth as much as young rats. In addition, there were age-related deficits in drinking in response to a range of administered loads of sodium (0.15-2 M NaCl, 2 ml/100 g body wt). Urinary excretion of water and sodium in response to the loads was equivalent across ages. Both middle-aged and old rats were less able than young rats to repair their water deficits after sodium loading, attributable almost entirely to their reduced drinking responses compared with young rats. Lastly, agerelated declines in drinking appeared to be more severe in response to hypotension than in response to cellular dehydration. aging; drinking; diuresis; natriuresis; dehydration; blood pressure; heart rate ELDERLY PEOPLE AND OLD ANIMALS have impaired drinking responses to many thirst-inducing challenges (21, 23, 25, 28, 29, 33-35, 40, 41). However, the nature of the underlying causes of reduced drinking that accompanies old age, such as impaired neural or humoral signaling mechanisms, remain largely undetermined. Knowledge of the causes of age-related declines in drinking will increase our understanding of the ways to help the elderly maintain better fluid homeostasis. This is an important consideration for an increasingly aging population and for the relationship between hydrational status and disorders, such as heat-related injury.Hypotension is a potent stimulus of thirst in rats (e.g., 10,17,18,26,30,38). Thirst following hypotension is due mainly to release of renin and formation of ANG II in the circulation (26, 38; for a review, see Ref. 20) and is blocked by interfering with the actions of, or formation of, ANG II (10,26,33,38). There are conflicting reports about whether old rats drink less in response to hypotension. For example, old rats have been found to drink less after subcutaneous injections of isoproterenol compared with young rats (24, 34, 37), although not always (25,34). These previous studies did not record arterial pressure or control for differences in arterial pressure that may occur with aging (24,25,34,37). This information is important becau...

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Section: Discussionsupporting

confidence: 91%

Section: Discussionsupporting

confidence: 83%

Section: Discussionmentioning

confidence: 55%

mentioning

confidence: 70%

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Hypotension- and osmotically induced thirst in old Brown Norway rats

Thunhorst¹,

Beltz²,

Johnson³

2009

American Journal of Physiology-Regulatory, Integrative and Comp

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“…Interestingly, the effect of mineralocorticoids or salt depletion on salt appetite may be modified by glucocorticoids (18,34,50) and amphetamine (5). Moreover, salt appetite has been shown to be dependent on the age of the animal (54). It would be interesting to explore whether SGK1 participates in the modulation of salt appetite by other stimuli and by age.…”

Section: Discussionmentioning

confidence: 99%