Acute Pain Clinical Trial
Official title:
A Blinded, Randomized Controlled Trial of Opioid Analgesics for the Management of Acute Fracture Pain in Adults Discharged From the Emergency Department
Background: Emergency department (ED) providers are frequently challenged with how best to
treat acute pain, specifically when non-opioid analgesics are insufficient or
contraindicated. Studies have documented older patients presenting to the ED with painful
conditions are less likely to receive pain medications than younger patients, and this
inadequate pain control has been associated with increased risk of delirium and longer
hospital stays. Given the concerns for drug interactions, adverse side effects, over-sedation
and addiction; emergency physicians often report uncertainty regarding the ideal choice of
opioid analgesic in older adults. There are no guidelines informing best practice for the
management of acute pain in this population.
Objective: The primary objective is to compare the efficacy of codeine, oxycodone and
hydromorphone for acute fracture pain in patients discharged from the ED.
Methods: This will be a blinded, randomized controlled trial of adults (age ≥ 18) discharged
home from the ED with acute pain secondary to an upper extremity, lower extremity, rib,
pelvic or vertebral compression fracture. Patients will be randomized to receive a 3-day
supply of codeine, oxycodone or hydromorphone. Patients will also be given acetaminophen.
Patients will be contacted by phone or email 3 days following their ED visit. The primary
outcome will be differences in pain scores at 3 days assessed using the validated Brief Pain
Inventory (Short Form). Secondary outcomes will include side effects (ie: confusion,
constipation), adverse events (i.e, falls, healthcare visits) and pain interference with
daily activity. Patients, physicians and all research staff will be blinded to group
allocation.
Importance: All analgesics (including opioids) prescribed to adults are associated with an
increased risk of adverse events. This study seeks to inform ED providers of opioid efficacy,
side effects and patient-important, functional outcomes in this growing patient population.
Introduction :Pain is a major symptom of many patients presenting to the emergency department
(ED), with up to 42% of ED visits being related to painful conditions. ED providers are
challenged with how best to treat acute pain, specifically when non-opioid analgesics are
ineffective or contraindicated. There is considerable debate regarding most appropriate
choice of analgesic when treating acute pain. Providers seek to prescribe the most effective
analgesic with the least side effects, including the least risk of opioid dependence. Factors
contributing to debate around the most appropriate opioid analgesic have also been influenced
by pharmaceutical industry marketing and health care systems' efforts to improve clinicians'
treatment of pain.
Ontario's most commonly prescribed opioid is codeine. Yet, its utilization as an analgesic is
debated in the analgesic literature. Codeine is a prodrug that is metabolized to morphine in
the liver. In most people, 5% to 10% of codeine is converted to morphine. Thus, some experts
suggest that a 30 mg dose of codeine is considered equivalent to a 3 mg dose of morphine.
However, other experts in this area suggest equi-analgesic doses of opioids are equally
efficacious in relieving pain. In fact, codeine has been compared to hydrocodone using
morphine-equivalent doses and were found equally efficacious at relieving pain the ED in a
randomized controlled trial. Two additional randomized controlled trials have compared short
acting hydrocodone and short acting oxycodone found them to be equally effective to relieve
pain.
Another recent study by Chang et al., reported no statistically significant or clinically
important differences in pain reduction at 2 hours after single-dose treatment with ibuprofen
and acetaminophen or with 3 different opioid and acetaminophen combination analgesics for
patients presenting to the ED with acute extremity pain. The largest difference in decline in
mean pain score between any two treatments was 0.9 at the 2-hour time point, a difference
that was not statistically significant and was less than 1.3, which was the author's a priori
criterion to define a minimal clinically important difference in pain. This study had several
limitations including the limited follow-up time of 2 hours, lack of adverse event reporting,
and the exclusion of patients over the age of 65 years. This study is one of the only
published randomized trials evaluating analgesic efficacy of opioid and non-opioid analgesics
for an acutely painful condition.
There is a surprising paucity of studies evaluating analgesic efficacy, particularly after ED
discharge, and there are no guidelines informing best practice for the management of acute
pain following ED disposition for acute pain. To date, there have not been studies directly
comparing the 3 most commonly prescribed opioids in Canadian EDs: codeine, hydromorphone and
oxycodone. In light of mounting concern about the misuse of oral opioids, studies are needed
to inform policy makers and to assist physicians in making evidence-based decisions about
optimal short-term outpatient pain management.
There remains a paucity of data informing ED providers of opioid efficacy and patient
important, functional outcomes in adults. Therefore, the objective of this study is to
identify a preferred prescribed oral opioid analgesic for outpatient pain management among
adults presenting to the ED with an acutely painful condition.
reater pharmacodynamic sensitivity to analgesic central nervous system effects. Objectives
Primary:
To identify the most effective prescribed oral opioid analgesic for outpatient pain
management among adults presenting to the emergency department with an acutely painful
condition.
Secondary:
To describe analgesic use, side effects, adverse events and patient-important, functional
outcomes in adults.
METHODS:
Study Setting This will be a pragmatic, blinded, randomized controlled trial (RCT) conducted
in the ED of Mount Sinai Hospital, in Toronto, Ontario, Canada. This is a tertiary care,
urban teaching hospital with approximately 65,000 ED visits per year.
Inclusion Criteria Patients will be considered for inclusion if they are 18 years and older,
live independently, present to the ED with an acutely painful condition occurring within 7
days prior to ED visit, and if their treating ED physician intends to prescribe opioid
analgesic upon ED discharge.
Exclusion Criteria Patients will be excluded from this study if they have an allergy to any
of the study drugs (acetaminophen, polyethylene glycol 3350 (PEG), codeine, oxycodone or
hydromorphone), are non-English speaking without an adequate interpreter available, are
already on prescribed chronic opioid pain medication, have ongoing use of sedating
medications (ie. benzodiazepines, antipsychotics), have current substance use disorder
(excluding tobacco), are on opioid substitution therapy, comorbidity representing an absolute
or relative contraindication to acute opioid prescribing (ie. any medical condition requiring
home oxygen, Addison's disease, dialysis dependence, obstructive sleep apnea on non-invasive
positive pressure ventilation, body mass index > 45, Cushing's Disease), have moderate or
severe dementia, inability to follow-up, or reside in a nursing home or location where a
professional dispenses medications.
Study Protocol Attending physicians will identify eligible patients prior to ED discharge,
and informed written consent for trial participation will be obtained by trained research
personnel. Research personnel will not approach physicians for fractures or painful
conditions alone, rather they approached on the basis of the treating physician's intent to
prescribe opioids for home use. After providing informed written consent, patients will be
randomized to either receive oxycodone, hydromorphone or codeine for analgesia for home use
using a fixed 1:1:1 allocation ratio produced by a computer-based random number generator.
Block sizes of 6 will be used to ensure equal allocation to each group. MSH pharmacy will
prepare study drugs in opaque vials with identical labels based on a randomization scheme
provided by the trial methodologist. The opaque vials will be included in sealed,
sequentially numbered study packets that will be replaced as they are used. To avoid
potential patient selection and allocation bias, all physicians, nurses, RAs and patients
will be blinded to the randomization schedule. Study investigators will be permitted to
un-blind the study medication in the event of allergic reaction, consisting of rash and/or
airway compromise.
Each research packet to be dispensed to patients at ED discharge will contain 3 medication
vials and medication instructions as below:
1. Acetaminophen 500 mg Instructions: Take 1 - 2 tablets by mouth every 8 hours as needed
for pain.
2. Polyethylene Glycol 3350 (PEG) 17 g sachets Instructions: Dissolve in 120 to 240 mL (4
to 8 ounces) of beverage and drink. Use one sachet daily as needed to prevent
constipation if you are taking the opioid study drug.
3. Blinded Opioid Study Medication in an opaque vial (5 mg morphine equivalent tablets of
either codeine, oxycodone or hydromorphone) Codeine: 30 mg tablets Oxycodone: 5 mg
tablets Hydromorphone: 1 mg tablets Instructions: Take 1 tablet every 4 hours as needed
for moderate to severe pain if you continue to have pain despite taking acetaminophen.
The research packet will be kept in the locked narcotic cupboard of the ambulatory care
assessment are in the ED in a box labeled "Study Drugs". At any given time, 3 packets will be
maintained, and the temperature of this cupboard will be monitored by the study RA. The room
temp logs will be maintained on a daily basis with a calibrated thermometer. The key to this
cupboard is kept by the nurse on duty in this area.
Once a patient is randomized, the physician will order a study medication packet with a paper
order for prescribing the study drug (designed and provided by MSH pharmacy). The nurse in
the ambulatory care area will remove this packet from the cupboard, log its removal on a
study specific narcotic sheet for inventory in ED. As in any other narcotic stored in the ED,
the study packets will be counted daily at the end of the day as per narcotic regulations.
The RA will record the patient's name, MRN, and other info on label that is dispensed with
study medication (follow labeling requirements). The RA will inform the patient of medication
instructions, possible side effects and medication reconciliation procedures.
Trained research personnel will collect demographic and clinical parameters (medical history,
physical examination findings, diagnostic testing, ED management) from the patient and from
paper and electronic charts using a standardized data collection tool.
Discharge instructions will be read by the attending physician. Patients will be provided a
printed copy of the discharge instructions. The RA will discuss each of the medications
provided to the patient and read the specific instructions and potential side effects for
each medication. The RA will also instruct the patient how to complete the Medication Diary.
Prior to ED discharge, the RA will schedule the telephone follow-up assessment and will
administer the BPI. Patients will be provided a pre-addressed envelope to return study
medications and the completed Medication Diary to the research team at study completion. At
the time of discharge, a time will be scheduled for a courier to pick up unused study
medications from their home. The envelope will be signed by the patient on shipping and
signed by the study coordinator or pharmacy on receiving. The patient will also have the
option of bringing their unused study medications to their scheduled MSH Fracture Clinic
appointment, if applicable, where the RA will meet them to reconcile the study medications.
Patients will be contacted via telephone by a RA to complete follow-up assessments 72 hours
following the initial ED visit. To assess the compliance of patients with discharge
instructions, they will be asked to complete a Medication Diary that consists of questions,
taking less than 1 minute to complete daily. If telephone contact is not successful on the
first day of scheduled follow-up, participants will be left a message to remind them of the
scheduled telephone interview. If telephone follow-up is not successful on the first day of
scheduled follow-up, attempts will be made on the 2nd and 3rd days. If contact is not made
within a 3 day timeframe, patients will be considered lost to follow-up, and their data will
be excluded from further analysis.
Outcome Measures The primary outcome of this study will be differences in pain severity 3
days following ED discharge as measured by the Brief Pain Inventory (BPI). BPI is the best
way to measure differences in pain severity in clinical trials. It measures pain severity
using the mean score of 4 questions (worst pain, least pain, average pain and current pain)
on a numeric rating scale (0-10).
Secondary outcomes will include differences in functional outcomes, analgesic use, side
effects, and adverse events. Participants' functional outcomes will be assessed using the BPI
- interference questions. Analgesic use will be quantified in pill counts collected from both
telephone follow-up surveys as well as on the Medication Diaries. Side effects will be
measured using a modified version of The Numerical Opioid Side Effect (NOSE) Assessment Tool
during the telephone follow-up, and adverse events are defined as falls, unplanned visits to
a healthcare provider (return ED visits, family physician, walk-in clinic), allergic
reaction, overdose, and death.
Data Analyses Data will be entered directly into a study specific Microsoft Excel database
(Microsoft Corporation, Redmond, Washington). Descriptive statistics will be summarized using
means with standard deviations (SD), medians with interquartile ranges (IQR) or frequencies
with 95% confidence intervals (CIs) where appropriate. The study design assumes three arms
(codeine, oxycodone and hydromorphone), therefore the 2-tailed alpha will be set to 0.025 to
adjust for the increased risk of type-I error with 3 pairwise comparisons. An
intention-to-treat analysis will be performed. To test for pairwise equality between groups,
a 1-way ANOVA will be employed. Proportional differences will be assessed using Pearson
chi-square statistic. Missing data points will be excluded from the analysis.
Assuming a mean (SD) change in pain scores between groups of 2.2 (3.0), a minimum clinically
important difference on the Brief Pain Inventory of 2.0 , a 2-tailed alpha of 0.025 to adjust
for 3 pairwise comparisons and a beta of 0.20, the investigators estimate that 47 patients
per group (N=141) will be required. To account for potential loss to follow-up, the
investigators will increase sample size by 25% per group, resulting in a final sample size of
177 patients (59 per group).
;
Status | Clinical Trial | Phase | |
---|---|---|---|
Completed |
NCT04484610 -
Appropriate Opioid Quantities for Acute Pain - Pharmacist Study
|
Phase 4 | |
Recruiting |
NCT05054179 -
Pecto-Intercostal Fascial Plane Block Catheter Trial for Reduction of Sternal Pain
|
Phase 2/Phase 3 | |
Completed |
NCT04548635 -
VR for Burn Dressing Changes at Home
|
Phase 2/Phase 3 | |
Recruiting |
NCT05370404 -
Prescribing vs. Recommending Over-The-Counter (PROTECT) Analgesics for Patients With Postoperative Pain:
|
N/A | |
Completed |
NCT06054945 -
Clinical Impact of IPACK Block Addition to Suprainguinal Fascia Iliaca Block
|
||
Completed |
NCT03825549 -
A Randomized Trial of Behavioral Economic Approaches to Reduce Unnecessary Opioid Prescribing
|
N/A | |
Completed |
NCT05995912 -
Efficacy and Safety of Etoricoxib-tramadol Tablet in Acute Postoperative Pain
|
Phase 2 | |
Recruiting |
NCT05589246 -
Regional Analgesia in Combination With Cryoanalgesia to Prevent Acute Pain Following Nuss Procedure
|
N/A | |
Recruiting |
NCT05572190 -
Evaluate the Safety and Pharmacokinetic Profile of ETR028 and ETR029 in Healthy Adult Subjects
|
Phase 1 | |
Terminated |
NCT04716413 -
Evaluating the Use of Sublingual Sufentanil in Patients With Suboxone Treatment
|
Phase 4 | |
Active, not recruiting |
NCT03537573 -
Provider-Targeted Behavioral Interventions to Prevent Unsafe Opioid Prescribing for Acute Pain in Primary Care
|
N/A | |
Not yet recruiting |
NCT06317844 -
Examination of Psychological and Physiological Pathways Linking Gratitude and Pain
|
N/A | |
Withdrawn |
NCT02957097 -
Gabapentin as a Pre-emptive Analgesic in Oral and Maxillofacial Surgical Procedures
|
Phase 4 | |
Completed |
NCT02565342 -
Interscalene Brachial Plexus Block to Treat Pain After Clavicular Surgery
|
Phase 4 | |
Terminated |
NCT02599870 -
Clinical Study to Evaluate Clinical Impact of PGx-Guided Treatment for Patients Undergoing Elective Spinal Surgical Procedures
|
N/A | |
Completed |
NCT02380989 -
Integrative Ayurveda Healing Relieves Minor Sports Injury Pain
|
Phase 2 | |
Completed |
NCT02984098 -
40% Orally Administered Dextrose Gel is More Effective Than 25% Dextrose
|
Phase 4 | |
Completed |
NCT02489630 -
Low Dose Ketamine as an Adjunct to Opiates for Acute Pain in the Emergency Department
|
Phase 4 | |
Completed |
NCT03107338 -
Preventive Treatment of Pain After Dental Implant Surgery
|
Phase 4 | |
Completed |
NCT02817477 -
Intranasal Ketamine for Acute Traumatic Pain
|
Phase 4 |