Postoperative Pain Clinical Trial
Official title:
Intraperitoneal Atomization of Ropivacaine During Gynecologic Laparoscopic Surgery: Impact on Pain, Opioid Use and Length of Recovery Room Stay
Pain following laparoscopic surgery continues to be a clinically important problem with 80%
or more patients requiring opioid analgesia post-operatively to control their pain. By
reducing this surgical complication patients can experience less discomfort and be
discharged from the recovery room more rapidly leading to reduced resource utilization and
expense.
HYPOTHESIS: Post-operative pain after laparoscopic procedures could be treated by topical
anesthetics sprayed directly into the abdomen (inside the abdominal cavity, on the nerve
endings of the visceral peritoneal lining and diaphragm surface) via the surgical incision
METHODS: Randomized controlled trial on use of topical anesthetic (namely 0.25% ropivacaine)
delivered directly onto the target sites both at the beginning and the end of surgery in
patients undergoing laparoscopic gynecologic procedure for uterine or adnexal benign
pathology. The drug will be delivered using a CE approved delivery system that will direct a
fine mist of drug directly to the areas of the peritoneal cavity that are theoretically the
cause of post-op pain (diaphragms, peritoneal abdominal surface, surgical dissection site).
GOAL: to assess the efficacy of intraperitoneal topical anesthesia in reducing postoperative
pain, opioid requirements in patients undergoing laparoscopic gynecologic procedure for
uterine or adnexal benign pathology
Introduction:
Laparoscopic surgery has replaced open surgical techniques for a large number of abdominal
general surgical and gynecologic interventions. However pain following laparoscopic surgery
continues to be a clinically important problem with 80% or more patients requiring opioid
analgesia post-operatively to control their pain. Post-operative pain and to a lesser extent
post-operative nausea and vomiting (PONV) are the main factors leading to delayed discharge
from the surgical recovery room and from the hospital following most surgical cases. Hence,
post-operative pain and PONV lead to increased costs of care. By reducing these surgical
complications patients can be discharged from the recovery room more rapidly leading to
reduced resource utilization and expense. This is especially true for routine surgical cases
(laparoscopic cholecystectomy -gallbladder removal, gynecologic procedures, gastric surgery)
that have the potential for same day surgery and discharge to home if their pain can be
adequately treated. It also applies to inpatient cases where superior pain control and less
PONV require less nursing care and potentially earlier discharge.
The origin of pain after laparoscopic surgery is multifactorial with pain arising from the
incision site, direct trauma in the area of surgical dissection, peritoneal micro-tears and
inflammation due stretching during insufflation and peritoneal and diaphragm irritation of
from the residual CO2 remaining after the pneumoperitoneum is deflated. Because this pain is
multifactorial - a multifactorial approach is needed. Although the somatic pain associated
with the abdominal wall incision responds well to nerve blocks or opiate medications,
visceral pain due to pneumoperitoneum induced stretching, compression, oxygen deprivation
and inflammation during the surgery is less responsive to these interventions. However,
visceral pain can be treated by topical anesthetics sprayed directly onto the nerve endings
of the visceral peritoneal lining and diaphragm surface. This knowledge has resulted in
extensive research studying the effects of applying topical anesthetics to the peritoneal
surface during laparoscopic surgery in an effort to reduce post-operative pain and its
attendant complications. Fairly clear conclusions can be drawn from review of the research
investigating topical anesthetic application to the peritoneum, diaphragms and surgical
site: they effectively reduce postoperative pain and opioid use. They do not have any of the
adverse effects of systemically administered opioids such as sedation, respiratory
depression, nausea, or GI dysmotility. They are safe and relatively inexpensive. Their use
results in earlier progression to ambulation, less shoulder tip pain, less post-operative
nausea and vomiting, earlier discharge from the recovery room and in some studies earlier
discharge from the hospital.
Despite this research and international recommendations to use this therapy topical
anesthetic application during laparoscopic surgery is not routinely used by most general or
obstetrical surgeons. There are probably two inter-related reasons for this lack of adoption
of this simple concept. First, no simple method exists for delivering topical anesthetics to
the peritoneal surface. Most studies diluted the drug with large volumes of saline (making
it less potent and less likely to work), then injected it into a trocar where gravity took
the solution straight into the gravity dependent gutters. This type of delivery system would
not be expected to optimize results of any topically active medication since the majority of
the peritoneal surface is never exposed to the anesthetic. Secondly, the pain reductions
reported in most topical anesthetic studies were positive but not impressive enough for
surgeons to change practice. This marginal reduction in post-operative pain is probably due
to these poor delivery systems with non-directed application of the drug and the great
variations in drug concentrations, site of delivery, and timing of application. Studies that
used more directed spray seem to show better results. A 2010 metaanalysis concludes that
future studies should not be designed to determine if topical intraperitoneal local
anesthesia is effective (this is already proven), rather this research should focus on
optimization of the method of delivery (aerosolized), location of application, timing of
drug delivery, and drug dose and concentration.
This study is designed to address these issues. The investigators will use topical
anesthetic (namely 0.25% ropivacaine) delivered directly onto the target sites both at the
beginning and the end of surgery. The drug will be delivered using an inexpensive delivery
system that will direct a fine mist of drug directly to the areas of the peritoneal cavity
that are theoretically the cause of post-op pain (diaphragms, peritoneal abdominal surface,
surgical dissection site). Our primary goal is to assess the efficacy of intraperitoneal
topical anesthesia in reducing postoperative pain, opioid requirements in patients
undergoing laparoscopic gynecologic laparoscopic procedure for uterus or adnexal benign
pathology.
Materials and Methods:
Design:
Prospective, randomized, double-blinded, placebo controlled trial stratified by pathology
(uterus or adnexal benign).
Clinicaltrials.gov submission: This study design will be submitted to the clinicaltrials.gov
prospective trials registry as required by many journals.
Patients:
Women scheduled for elective gynecologic laparoscopic procedure for uterus or adnexal benign
pathology
Intervention:
Patients will be randomized to ropivicaine 0.25% 40 ml (100 mg) or placebo (NaCl 0.9%)
according to a randomization list stratified by pathology delivered in the following
fashion:
- the derma at the portal sites will each be injected with 2 ml of medication at the
onset of the surgery (total volume 6 ml).
- following insufflation of the abdomen, half of the remaining ropivacaine will be
atomized onto each subdiaphragmatic area (3.5ml + 3.5ml), onto the surgical dissection
site (3 ml) and diffusely across the peritoneal surface (dome of the abdomen and
surface of the visible bowel) (7ml). At the end of the case the remaining medication
with be atomized again onto the same areas, using the same volumes.
Primary Outcome Measured:
1. Post-operative pain intensity (NRS score. NRS; 0 = no pain and 10 = worse pain possible)
at 6h post-operatively.
Secondary Outcomes measured
1. Total post-operative opioid analgesic requirements in the first 48 hours
post-operatively or until discharge
2. Post-operative rescue opioid analgesic requirements in the first 6h post-operatively
3. Post-operative pain intensity scores during the first 48 hours post-operatively or
until discharge - measured at times 0, 1, 2, 4, 6, 10, 18, 24, 36, 48 hours
4. Post-operative shoulder pain (NRS score. NRS; 0 = no pain and 10 = worse pain possible)
intensity scores during the first 48 hours post-operatively or until discharge -
measured at times 0, 1, 2, 4, 6, 10, 18, 24, 36, 48 hours
5. Post-operative nausea and vomiting verbal description scores (0 = no symptoms, 1 =
nausea, 2 = nausea and vomiting) - measured at times 0, 1, 2, 4, 6, 10, 18, 24, 36, 48
hours
6. Post-operative sedation scores (Sedation will be evaluated using a 6 point Ramsay
sedation score: 1= anxious and agitated, 2 = cooperative, tranquil, oriented, 3 =
responds only to verbal commands, 4 = asleep with brisk response to light stimulation,
5 = asleep without response to light stimulation, 6 = non-responsive) measured at times
0, 1, 2, 4, 6 hours
7. Time until discharge from recovery room
8. Time until discharge from hospital
9. Time until first flatus or bowel movement
10. Time until ambulation.
Study Drug:
Study drug: ropivacaine 0.25% (2,5 mg/ml - 100 mg total) a local anesthetic manufactured by
Astra Zeneca (Basiglio, MI, Italy).
Placebo: Saline 0.9% (Fresenius Kabi, Isola della Scala, VR, Italy). Study Drug and Placebo
will be provided free of charge by the manufacturing companies, which will not have any
other role in the study.
Drug and placebo prepared under sterile conditions in a specific syringe in the O.R. by an
O.R. nurse, which thereafter will not be involved in the surgical operation nor in the
patient care in the recovery room.
Random sequence generation by a computer generated random number table will be used to
randomize each vial. Records of placebo versus active drug will be kept by the O.R.
coordinator, and not available to investigators until the end of study data analysis.
Study device:
Optispray surgical spray device [CE mark (0050)], manufactured by AbViser Medical, Salt Lake
City, UT, U.S.A. will be provided free of charge by the manufacturing company, which will
not have any other role in the study.
Procedure:
1. Potentially eligible patients will be screened and consented at the time of pre-operative
surgical evaluation (the night prior or morning of surgery).
2. A standard anesthetic procedure will be conducted for all patients.
- Pre-medication with midazolam 0.03mg/kg I.V.
- Induction with propofol 2 mg/kg. Maintenance with propofol 6mg/kg/h I.V.
- Muscle relaxation with cisatracurium, reversal with neostigmine and atropine
- Intra-operative analgesia will be standardized and administered by the anesthesiologist
to all patients:
- Fentanyl 2mcg/kg I.V. at induction, then 2mcg/kg 5 min before surgical incision
and 2mcg/kg 30 minutes prior to the end of surgery
- Remifentanil 0.1-0.3 mcg/kg/min I.V.
- Acetaminophen 1g I.V. and Ketoprofen 100 mg I.V. will be administered 30 minutes
prior to the end of surgery 4. A standard intra-operative antiemetic (Ondansetron
4 mg I.V.) will be administered by anesthesia 15 minutes prior to end of surgery.
5. All laparoscopies will be performed in a standardized fashion
1. Pneumoperitoneum by open technique (insufflation pressure 20 mmHg)
2. Insertion of 3 trocars
3. Intraabdominal pressure maintained at 12 mmHg
4. Uterine or ovarian surgical procedure in a standardized fashion
6. All study drug delivery will be performed in a standardized fashion
a. All port sites will be injected with 2 ml/each study drug prior to trocar
insertion b. Immediately following insufflation the Optispray surgical spray
device will be inserted into the abdomen and directed towards the diaphragms, dome
of inflated abdomen, bowel peritoneum and surgical dissection site and the study
drug will be delivered as an atomized spray in the following volumes:
- each subdiaphragmatic area 3.5 ml + 3.5ml
- surgical dissection site 3 ml
- diffusely across the peritoneal surface (dome of the abdomen and surface of the visible
bowel) 7 ml. At the end of the case the remaining medication with be atomized again
onto the same areas, using the same volumes.
c. At the end of the case - this process will be repeated with the remaining drug (no
repeat port site injections).
7. Postoperative analgesics:
- patients will receive Acetaminophen 1g I.V. 6h after surgery, then acetaminophen 1g per
os every 8h
- rescue analgesic will be Tramadol 100mg in 50 ml of 0.9% saline I.V., preceded by I.V.
0.01mg/kg droperidol.
8. Rescue post-operative antiemetics:
- ondansetron 4mg I.V. (Maximal for 3 times/day)
Data Collection procedure Data will be collected by investigator and stored in the
Dipartimento di Scienze Ginecologiche e della Riproduzione Umana. Electronic datasets will
be prepared including only anonymous data. Statistical analysis will be performed using SPSS
v.18 computer program (SPSS Inc., Chicago, IL, USA).
Risks to patient:
The only risk to the patient from this study is the risk of local anesthetic toxicity. The
toxicity of local anesthetics includes seizures and ventricular arrhythmias. At the
currently selected doses this is very low probability for the following reasons: the doses
selected are below the toxic doses described by the package insert for injected ropivacaine,
and yet this dose in not being injected rather it is being sprayed onto the peritoneal
surface. While there is no question some of the drug will be absorbed, this will occur over
time and the peak levels will not achieve that expected when a drug is injected I.V..
Finally, prior literature studies have used similar doses and do not describe any toxicity
in their patients nor toxic serum concentrations when applied to the peritoneal surface.
Benefits to patient This procedure is already proven to reduce postoperative pain in
numerous studies but is not routinely used. Therefore, the patient has a 50% probability of
being delivered the active anesthetic drug and can reasonably expect to have less pain if
they are in that arm of the study. Furthermore, if they have reduced pain and use fewer
opiates they may have less nausea and they may be discharged from recovery room and possible
from the hospital more rapidly.
Statistical Analysis The investigators will examine separately uterine surgical procedures
and adnexal surgical procedures.
Sample size determination:
Pain reduction: The study intention is to show a CLINICALLY significant reduction in pain
(not just statistically significant). This can be hard to define if they have relatively low
baseline pain, but most patients with anything but very minor laparoscopic surgeries who
have been studied in the past wake up with pain scores in the 4-6 range - 6 being more
typical. A pain score reduction of 1.5 would be 25% or more pain reduction (and the
investigators know from prior studies that 1.3 or 23% reduction is the lower limit of
clinically significant pain reduction).
A sample size of 45 in each group (treatment vs control) will have 80% power to detect a
difference in means of 1.500 (the difference between a Group 1 mean of 6.000 and a Group 2
mean of 4.500) assuming that the common standard deviation is 2.500 using a two group t-test
with a 0.050 two-sided significance level.
Due to potential drop-outs, the investigators will include 50 patients in each group, for a
total of 200 patients (100 undergoing uterine procedures and 100 undergoing adnexal
procedures). Statistical analysis will be performed as appropriate.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
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