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Influence of oral administration of kukoamine A on blood pressure in a rat hypertension model.

Christine A ButtsDuncan I HedderleySheridan MartellHannah DinnanSusanne Middlemiss-KraakBarry J BunnTony K McGhieRoss E Lill
Published in: PloS one (2022)
The benefits of lowering blood pressure (BP) are well established for the prevention of cardiovascular disease. While there are a number of pharmaceuticals available for lowering BP, there is considerable interest in using dietary modifications, lifestyle and behaviour changes as alternative strategies. Kukoamines, caffeic acid derivatives of polyamines present in solanaceous plants, have been reported to reduce BP. We investigated the effect of orally administered synthetic kukoamine A on BP in the Spontaneously Hypertensive Rat (SHR) laboratory animal model of hypertension. Prior to the hypertension study, we determined the safety of the synthetic kukoamine A in a single oral dose (5 or 10 mg kg-1 bodyweight) 14-day observational study in mice. No negative effects of the oral administration of kukoamine A were observed. We subsequently investigated the effect of daily oral doses of kukoamine A (0, 5, 10 mg kg-1 bodyweight) for 35 days using the SHR rat model of hypertension. The normotensive control Wistar Kyoto (WKY) strain was used to provide a baseline for normal BP in rats. We observed no effect of orally administered synthetic kukoamine A on arterial hypertension in this laboratory animal model of hypertension.
Keyphrases
  • blood pressure
  • hypertensive patients
  • cardiovascular disease
  • heart rate
  • arterial hypertension
  • type diabetes
  • physical activity
  • blood glucose
  • weight loss
  • atomic force microscopy
  • skeletal muscle
  • insulin resistance