Peer-reviewed veterinary case report
Prostaglandin E1 derivative widens nerve root arteries in dogs
By Shirasaka, Masayoshi et al.·Published in BMC musculoskeletal disorders·2008·Department of Pharmacy, Japan·View original on PubMed →
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Original publication title: Vasodilative effects of prostaglandin E1 derivate on arteries of nerve roots in a canine model of a chronically compressed cauda equina.
- Species:
- dog
Plain-English summary
A group of 14 dogs with chronic cauda equina compression, which can cause nerve pain and mobility issues, were given a medication derived from prostaglandin E1 (PGE1) to see if it could improve blood flow to their nerve roots. After taking the medication, the blood vessels supplying the nerves showed a significant increase in size and blood flow within an hour. This suggests that the PGE1 derivative could be a helpful treatment for dogs suffering from this condition, potentially improving their symptoms and overall comfort.
People also search for: dog cauda equina compression treatment · PGE1 for dogs · improving blood flow in dogs · dog nerve pain medication
Abstract
BACKGROUND: Reduction of blood flow is important in the induction of neurogenic intermittent claudication (NIC) in lumbar spinal canal stenosis. PGE1 improves the mean walking distance in patients with NIC type cauda equina compression. PGE1 derivate might be effective in dilating blood vessels and improving blood flow in nerve roots with chronically compressed cauda equina. The aim of this study was to assess whether PGE1 derivate has vasodilatory effects on both arteries and veins in a canine model of chronic cauda equina compression. METHODS: Fourteen dogs were used in this study. A plastic balloon inflated to 10 mmHg was placed under the lamina of the 7th lumbar vertebra for 1 week. OP-1206-cyclodextrin clathrate (OP-1206-CD: prostaglandin E1 derivate) was administered orally. The blood vessels of the second or third sacral nerve root were identified using a specially designed surgical microscope equipped with a video camera. The diameter of the blood vessels was measured on video-recordings every 15 minutes until 90 minutes after the administration of the PGE1 derivate. RESULTS: We observed seven arteries and seven veins. The diameter and blood flow of the arteries was significantly increased compared with the veins at both 60 and 75 minutes after administration of the PGE1 derivate (p < 0.05). Blood flow velocity did not change over 90 minutes in either the arteries or veins. DISCUSSION: The PGE1 derivate improved blood flow in the arteries but did not induce blood stasis in the veins. Our results suggest that the PGE1 derivate might be a potential therapeutic agent, as it improved blood flow in the nerve roots in a canine model of chronic cauda equina compression.
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Search related cases →Original publication on PubMed: https://pubmed.ncbi.nlm.nih.gov/18394203/