Effects of; Anesthesia, Spinal and Epidural, in Pregnancy Clinical Trial
Official title:
Does a Single Intravenous Dose of Ketamine Reduce the Need for Supplemental Opioids in Post-Cesarean Section Patients?
Pain control after cesarean delivery is associated with improved breastfeeding and infant
rooming-in times. In addition, inadequate analgesia leads to elevated plasma catecholamine
concentrations, which negatively affect every organ system. There is growing evidence that
ketamine, N-methyl-D-aspartate receptor antagonist, is efficacious when used as an adjuvant
in postoperative pain control. A 2006 Cochrane Collaboration systemic review and
meta-analysis concluded, "Ketamine in subanesthetic doses….is effective in reducing morphine
requirements in the first 24 hours after surgery."
Ketamine's prolonged analgesic effect, despite its short half-life and its use in low doses,
is theorized to be due to blockade of spinal cord central sensitization. Central
sensitization is a phenomenon whereby repeated painful stimulus leads to more severe pain
perception over time despite no change in the intensity of the painful stimulus.Ketamine may
also prevent the development of acute opioid tolerance. Ketamine's analgesic effects have
also demonstrated in the obstetric population. Post-cesarean delivery morphine requirements
in women who received ketamine as part of a general anesthesia technique were decreased.
Similary, low-dose ketamine in conjunction with bupivacaine-only spinal anesthesia reduced
postoperative analgesic requirements compared to bupivacaine-only spinal anesthesia and
bupivacaine-fentanyl spinal anesthesia.
In the United States, healthy women scheduled for elective cesarean delivery commonly
receive spinal anesthesia with bupivacaine-fentanyl-morphine. To our knowledge, IV ketamine
has not been studied as an adjuvant to this regimen in the analgesic management in
post-cesarean delivery patients. Multimodal therapy for postoperative pain control is widely
practiced due to the advantage it provides in blocking multiple pain pathways while
minimizing side effects of each individual pain medication. We hypothesize that low dose
intravenous ketamine will improve multi-modal post-cesarean analgesia compared to placebo.
The purpose of this study is to evaluate this hypothesis and study the possible side effects
of this regimen in combination with bupivacaine-fentanyl-morphine spinal anesthesia.
Eligible women for elective cesarean section admitted to the Labor and Delivery Unit of
Prentice Women's Hospital will be approached for study participation immediately after the
routine preanesthetic evaluation. This occurs shortly after admission to the Labor and
Delivery Unit. Women who agree to participate will give written, informed consent at this
time.
Subjects will be prepared preoperatively in the usual fashion with intravenous (IV) access,
aspiration prophylaxis and intraoperative monitoring. Preincision antibiotics will be given
and uterotonic medications will be used as per usual practice after delivery.
The anesthesiologist will perform a spinal anesthetic per routine with the subject in the
sitting position using sterile technique at the L3-4 interspace (± one vertebral
interspace). The spinal anesthetic will consist of 12 mg of hyperbaric bupivacaine + 15 μg
fentanyl + 150 μg of morphine. The subject will be placed supine with left lateral tilt to
alleviate aortocaval compression. Cesarean section will commence after adequate anesthesia
is assured to a T4 sensory level to pinprick. Vasopressors and IV fluids will be
administered at the anesthesiologist's discretion per usual practice.
At the time of delivery, subjects will be randomized to one of two groups using a computer
generated random number table. Randomization will be blocked based on whether the cesarean
procedure is a primary or a repeat procedure. Randomization assignments will be kept in
sequentially numbered opaque envelopes. The envelope will be opened by a research nurse who
will prepare a 20 mL syringe labeled "study drug". The syringe will be given to the
anesthesiologist blinded to the treatment group who will subsequently administer the study
drug. Subjects randomized to the treatment group will receive ketamine 10 mg (ketamine 10
mg/mL) diluted to 20 mL with 0.9% preservative free saline. Subjects randomized to the
placebo group will receive 20 mL preservative free saline.
The study drug will be administered into the intravenous line via an infusion pump over 10
minutes. Five minutes after placebo or drug administration, the anesthesiologist will ask
the subject if she has nausea, vomiting and pruritus. Nausea and pruritus will be graded as
none, mild, moderate or severe; and vomiting as present or absent. Any spontaneous
complaints of psychedelic effects will be noted at this time. Sedation will be assessed via
the Richmond agitation-sedation scale (RASS [see Appendix 1]).
Upon completion of the cesarean section, the subject will be transported to the post
anesthesia recovery unit. Patients will receive ketorolac 30 mg every 6 hours time 4 doses
beginning shortly after admission to the PACU.
At 1 h, 4 h, 8 h, 12 h and at 24 h after administration of the study drug, the subject's
pain will be assessed using the numeric rating scale for pain NRS 0-10 (see Appendix 2).
Patients may request rescue analgesia if they are experiencing discomfort. The time of first
rescue analgesia request will be noted, and the NRS will be determined at the time of
request for rescue analgesia.
Rescue medication will consist of hydrocodone 10 mg plus acetaminophen 325 mg per os. An
additional dose of hydrocodone 10 mg plus acetaminophen 325 mg will be provided after 1 hour
if the pain is not relieved to the subject's satisfaction. These are routine oral analgesic
medications for postoperative cesarean delivery analgesia. Standard orders will be written
for monitoring sedation and respiratory rate, and treatment of side effects (nausea,
vomiting, pruritus and respiratory depression). The total amount of rescue medication will
be determined for each subject after 24, 48 and 72 hours.
The presence of nausea, vomiting, and pruritus will be assessed at the same time intervals
as the NRS for pain: 1 h, 4 h, 8 h, 12 h and 24 h after IV infusion of ketamine or placebo.
The subjective psychedelic effects of ketamine and morphine will be assessed using a set of
true/false questions from the LSD and morphine short form of the Addiction Research Center
Inventory, ARCI (Appendix 3). These questions will be administered verbally by the
anesthesiologist or researcher blinded to the treatment group upon admission to the PACU and
at 4 h.
The following data will be collected in addition to the primary and secondary outcome data:
maternal age, height, weight, prepregnancy weight, gestational age and IV fluids
administered during cesarean section. In addition, all intraoperative and postoperative
medications will be recorded, including those administered for the treatment of side effects
listed above.
Protocol specific analgesia assessment ends 24 hours after administration of the study drug.
At 72 hours the subject will be asked about her satisfaction with postoperative analgesia
(100 mm scale, 0 mm = not satisfied at all, 100 mm = very satisfied). One telephone
follow-up evaluation 2 weeks after delivery will again, assess for satisfaction with
analgesia and average pain (NRS) since the procedure.
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Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
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