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Details

Autor(en) / Beteiligte
Titel
EFFECT OF NIMODIPINE ON SYSTEMIC, RENAL, AND CEREBRAL HAEMODYNAMICS AFTER A MILD HYPOXIC–ISCHAEMIC INSULT IN NEWBORN PIGLETS
Ist Teil von
  • Pharmacological Research, 1996, Vol.33 (1), p.5-12
Ort / Verlag
Netherlands: Elsevier Ltd
Erscheinungsjahr
1996
Link zum Volltext
Quelle
Elsevier Journal Backfiles on ScienceDirect (DFG Nationallizenzen)
Beschreibungen/Notizen
  • Because many Ca 2+channel blocking agents are known to cause adverse systemic effects, in this study we tested the haemodynamic side effects of nimodipine with and without a mild hypoxic–ischaemic (HI) insult in a newborn piglet model. Fifteen min after completing a brief period of asphyxia we gave i.v. nimodipine as 5μgkg −1bolus followed by 0.1μgkg −1min −1continuous infusion for 105 min in six piglets, while the same treatment was repeated in five animals without preceding HI insult. At third group of six served as sham operated controls. In the HI insult group by 105min of nimodipine infusion the mean BP dropped by 30% and the cardiac output dropped by 23% of respective baseline. In this group, the renal blood flow dropped between 65% and 77% of baseline and regional cerebral blood flow dropped between 28% and 55% of respective baseline by 45min and 105min of nimodipine fashion. In the group with no prior HI insult, 105min of nimodipine infusion caused no significant changes in these variables. Despite nimodipine infusion, HI insult caused a significant increase in the mean brain water content compared to the two control groups: 89±3.2% compared to 82.7±0.5% in the nimodipine control group, and 83.7±1.7% in the sham group ( P<0.0001). We conclude that while nimodipine therapy without prior asphyxial insult does not cause significant adverse haemodynamic effects, its infusion after even a mild HI insult could cause reduction in renal blood flow and moderate reduction in regional cerebral blood flow, BP, and cardiac output, suggesting a differential effect. A 15min lag between HI insult and nimodipine therapy may be too long to prevent cerebral oedema.

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