Epidural analgesia in the management of severe vaso-occlusive sickle cell crisis

Epidural analgesia in the management of severe vaso-occlusive sickle cell crisis

To determine whether continuous epidural analgesia could effectively decrease pain and thereby improve the management of severe vaso-occlusive crisis in children with sickle cell disease who were unresponsive to conventional analgesic therapy. Retrospective observational study. A tertiary care hospi...

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Bibliographic Details
Published in:Pediatrics (Evanston) Vol. 93; no. 2; pp. 310 - 315
Main Authors: YASTER, M, TOBIN, J. R, BILLETT, C, CASELLA, J. F, DOVER, G
Format: Journal Article
Language:English
Published: Elk Grove Village, IL American Academy of Pediatrics 01-02-1994
Subjects:
Analgesia
Analgesia, Epidural
Analgesics
Anemia, Sickle Cell - complications
Anemias. Hemoglobinopathies
Biological and medical sciences
Child
Diseases of red blood cells
Drug therapy
Emergencies
Female
Fentanyl - therapeutic use
Hematologic and hematopoietic diseases
Humans
Lidocaine - administration & dosage
Lidocaine - therapeutic use
Male
Medical research
Medical sciences
Methods
Pain
Pain - drug therapy
Pain - etiology
Pain in children
Pediatric diseases
Pediatric pain
Pediatrics
Retrospective Studies
Sickle cell anemia
Sickle cell anemia in children
Treatment Outcome
Human
Hemoglobinopathy
Sickle cell anemia
Continuous
Treatment efficiency
Hemopathy
Obstruction
Thrombosis
Genetic disease
Crisis
Analgesia
Hemolytic anemia
Analgesic
Pain
Treatment
Blood vessel
Extradural administration
Child
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Description
Summary:To determine whether continuous epidural analgesia could effectively decrease pain and thereby improve the management of severe vaso-occlusive crisis in children with sickle cell disease who were unresponsive to conventional analgesic therapy. Retrospective observational study. A tertiary care hospital with a large pediatric sickle cell patient referral population. The study describes nine children in 11 painful vaso-occlusive crises, unresponsive to high-dose systemic opioids, nonsteroidal anti-inflammatory drugs, and adjunctive measures, who underwent continuous epidural analgesia to control pain. Subjective pain scores, arterial oxygen saturation monitoring, and plasma lidocaine levels. Placement of an epidural catheter for the administration of a continuous infusion of local anesthetic, alone, or in combination with fentanyl, in the management of vaso-occlusive crisis. An initiation of epidural analgesic therapy, 8 of 9 patients reported severe pain (8 to 10 on a scale of 0 to 10, 0 = no pain, 10 = the worst pain they ever experienced). Analgesic was immediate (pain score 0 to 2) in 8 of 9 patients, and continuously effective in 9 of 11 crises. Five patients required either the addition of fentanyl or changing the local anesthetic from lidocaine to bupivacaine to maintain analgesia for 2 to 5 days. In 7 of 9 patients, oxygen saturation dramatically increased from 87 to 95% to 99 to 100% after epidural analgesia was initiated. In all patients, plasma lidocaine levels ranged from 1.1 to 4.6 mg/L and dose-related toxicity did not occur. One patient developed hypotension secondary to high sympathetic blockade (T-4), one had an inadvertent dural puncture during insertion of the catheter, one had the epidural catheter removed for fever, and one achieved analgesia only transiently. There were no other complications, and epidural analgesia was not associated with sedation, respiratory depression, or limitation of movement. All epidural catheters were cultured on removal, and colonization did not occur. Epidural analgesia with local anesthetics administered alone or in combination with fentanyl effectively and safely treats the pain of sickle cell vaso-occlusive crisis unresponsive to conventional pain management and does so without causing sedation, respiratory depression, or significant limitation on ambulation. Furthermore, early treatment of painful crisis with this technique may improve oxygenation, a critical factor in the evolution of further sickling.
ISSN:0031-4005
1098-4275
DOI:10.1542/peds.93.2.310