2004
DOI: 10.1097/00004872-200401000-00030
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Analysis of arterial pressure regulating systems in renal post-transplantation hypertension

Abstract: None of the investigated mechanisms was altered in a way that might help to explain the rapid and consistent development of hypertension in recipients of an SHR kidney. We conclude that post-transplantation hypertension in recipients of an SHR kidney is due to mechanisms other than those investigated in the present study.

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Cited by 19 publications
(24 citation statements)
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“…Possible mechanisms include: (1) the reninangiotensin-aldosterone system, (2) renal sodium and volume handling, (3) sympathorenal interactions, and (4) (enhanced) production or inadequate excretion of a hitherto unknown hypertensinogenic substance. In several studies, 15,18,27,30,33,34 we were able to demonstrate that the renin-angiotensin-aldosterone system is not stimulated in recipients of an SHRSP or SHR kidney. Interestingly, recipients of an SHRSP kidney had a lower 24-hour urinary aldosterone secretion, 15 and recipients of an SHR kidney had lower plasma aldosterone concentrations than recipients of a kidney from normotensive donors.…”
Section: Renal Mechanisms Of Hypertensionmentioning
confidence: 86%
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“…Possible mechanisms include: (1) the reninangiotensin-aldosterone system, (2) renal sodium and volume handling, (3) sympathorenal interactions, and (4) (enhanced) production or inadequate excretion of a hitherto unknown hypertensinogenic substance. In several studies, 15,18,27,30,33,34 we were able to demonstrate that the renin-angiotensin-aldosterone system is not stimulated in recipients of an SHRSP or SHR kidney. Interestingly, recipients of an SHRSP kidney had a lower 24-hour urinary aldosterone secretion, 15 and recipients of an SHR kidney had lower plasma aldosterone concentrations than recipients of a kidney from normotensive donors.…”
Section: Renal Mechanisms Of Hypertensionmentioning
confidence: 86%
“…Interestingly, recipients of an SHRSP kidney had a lower 24-hour urinary aldosterone secretion, 15 and recipients of an SHR kidney had lower plasma aldosterone concentrations than recipients of a kidney from normotensive donors. 18 From these and other observations, we hypothesized that recipients of an SHRSP or SHR kidney, respectively, may have a primary defect in renal sodium handling. In fact, when we challenged our rats with a dietary sodium load, recipients of an SHRSP kidney showed a decreased renal capacity to excrete the load.…”
Section: Renal Mechanisms Of Hypertensionmentioning
confidence: 93%
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