The Life STORRIED study is a multicenter randomized clinical trial in the United States. Central ethical approval has been confirmed by The University of Pennsylvania institutional review board (reference approval no. 826673). Recruitment at other centers began once local ethical approval was obtained. The study began data collection on June 28, 2017.
Experimental Plan
Eligible patients presenting to participating sites (emergency departments and associated urgent care and observation units) from four geographically distinct health systems will be randomized to one of three study arms:
1) Control group (Arm 1): Patients receive a standardized, general risk information sheet (General Risk Comparator) only. This study arm represents a risk communication approach commonly employed in clinical practice (Fig 1a).
2) PRT Intervention group (Arm 2): standardized, general risk information sheet plus a probabilistic opioid risk tool (Fig 1b).
3) NERT Intervention group (Arm 3): standardized, general risk information sheet plus a narrative enhanced probabilistic opioid risk tool (Fig 1c).
Patients will be stratified by complaint (renal colic or back/neck pain) and hospital center (University of Pennsylvania, Northwell Health, Mayo Clinic, or University of Alabama at Birmingham). Electronic consent, randomization within strata and hospital center will occur automatically through Way to Health (WTH), a web-based data collection platform for behaviorally oriented randomized clinical trials, during the enrollment process [21] using computer generated random numbers. All outcomes data are collected through the WTH platform, a secure, electronic database accessible only to researchers.
Opioid Risk Tool (ORT): For participants randomized into either intervention arm, WTH will display one of three ORT images— “at risk,” “high risk,” or “highest risk” for opioid misuse— based on participant responses to the ORT survey (Fig 2). Using a standardized script, study staff will discuss and interpret the ORT image with patients and provide a hard copy for participant possession.
Video narratives: For participants randomized to the narrative enhanced probabilistic risk tool arm, WTH will also display eight video narratives (Fig 3). Each narrative is a one- to three- minute, first-person, interview-based vignette of a patient or caregiver sharing personal perspectives and experiences of acute pain and opioid use and misuse. Together, the eight narrative videos feature patients of diverse backgrounds and risk levels to offer a balanced, varied commentary. The narratives are displayed in a menu format on a table computer and participants can watch any story by touching the picture of the storyteller. Study staff will encourage the participant to watch as many videos as desired, provide disposable earphones, and exit the room for privacy until the patient has completed viewing the videos.
The videos were developed by the research team to maximize factors such as identification with characters, perceived realism, normative values, and reinforcement. They were also reviewed for clarity and salience and tested through an iterative process with a core group of patient investigators and community stakeholders.
Study overview and objective
The primary objective of this study is to determine whether risk-informed communication with or without a narrative-enhanced tool can improve functional outcomes and patient-centered outcomes in the domains of knowledge, opioid use, and patient/provider therapeutic alignment. Specifically, the study will measure the effectiveness of different risk communication strategies using the following outcomes (for a full list of primary and secondary measures, response type, collection points, and their relevance to patients and other stakeholders (see Table 1)):
1) Knowledge as measured by risk awareness and treatment preferences for fewer opioids, particularly among those at higher risk for addiction
2) Reduced use of opioids as measured by quantity of opioids taken, functional improvement, and repeat use of unscheduled visits for pain at 14 days
3) Patient/provider alignment as measured by concordance between patient preference and finalized prescription plan and the presence of shared decision making
We hypothesize that, compared to study patients receiving only a generalized risk information sheet or information sheet plus probabilistic risk communication tool, patients receiving narrative enhanced risk communication will:
1) Demonstrate greater knowledge as determined by awareness of risk for opioid dependency
2) a. Select a treatment plan with fewer opioids; b. Take fewer opioids for fewer days, while achieving the same degree of pain relief and improved functional status
3) a. Enjoy greater levels of concordance between the patient-preferred and provider-selected treatment plans; b. Engage in greater shared decision making with their provider.
Setting
Patients will be recruited from acute care settings (emergency department, urgent care or observation unit) in four United States hospital centers: the University of Pennsylvania in Philadelphia, Pennsylvania (east coast with an urban patient population), Northwell Health in Long Island, New York (east coast with a suburban patient population), the Mayo Clinic in Rochester, Minnesota (midwest with a rural patient population), and the University of Alabama in Birmingham, Alabama (southeast, with an urban patient population). These centers were selected to capture geographically and ethnically diverse patient populations and clinical practices.
Sample population and recruitment
Our sample population includes patients presenting to participating study sites with a chief complaint suggestive of acute renal colic or musculoskeletal neck or back pain. A trained project manager, research coordinator, or research associate will identify potentially eligible patients based on chart review and collaborate with the treating clinician to confirm patient eligibility for the study. Patients will be concurrently enrolled at all participating study sites five to seven days per week, whenever a trained enroller is available. Data audits, for completeness and accuracy are conducted monthly by the study team. Adverse events or other unintended effects of the trial will be reported immediately to the sponsor, the central IRB, and the office of human research at the home institution. Additionally, all important protocol modifications will be communicated to relevant parties, such as investigators, the IRB, participants and our funder PCORI.
Selection of Participants
The study inclusion criteria are as follows:
1) Patients 18-70 years of age presenting to an acute care setting AND
2) Chief complaint indicative of acute neck, back, and/or flank pain OR uncomplicated kidney stones AND
3) Capable of providing informed consent AND
4) English-speaking OR Spanish-speaking with English comprehension AND
5) Able to access a smartphone or email account regularly AND
6) The treating clinician anticipates discharge within 24 hours with a diagnosis of renal calculi or musculoskeletal back pain
Exclusion criteria include pregnancy, in police custody, under the influence of drugs or alcohol, mentally or cognitively unstable, suicidal, homicidal, or unable to take opioids or non-steroidal anti-inflammatories for any reason. Additionally, patients who display aberrant drug use behavior or have used opioid medications in the past 30 days— excluding opioids taken for the current condition within 48 hours of this acute care admission— are ineligible. Patients with a known history of chronic kidney disease (GFR<60) are also ineligible, because they may not be able to take NSAIDS.
Baseline enrollment (Day 0)
Enrollment takes approximately thirty minutes and will be conducted in the flow of patient care. Once an eligible patient is identified via chart review and clinician consultation, study staff will use a standardized script to greet the patient, introduce the study, obtain written informed consent, and conduct baseline enrollment activities.
After providing informed consent, participants will answer questions from a series of surveys, including: 1) an informational profile of demographic data (gender, race, ethnicity, education level) [22, 23, 24]; 2) the Revised American Pain Society Patient Outcome Questionnaire [25]; 3) the 20-Item Short Form Survey from the Medical Outcomes Study [26]; 4) a tobacco use survey [23]; 5) the Opioid Risk Tool [27]; 6) the Screener and Opioid Assessment for Patients with Pain- Revised [28]; and 7) a pain relief preference survey. Participant responses to survey questions will be recorded in real time on a secure, password-protected iPad or tablet owned by the study. Study staff will administer surveys 1) through 3) and 7), whereas participants will complete surveys 4) through 6) directly on the study tablet computer due to the sensitive nature of these questions.
All participants will be given a generalized, fact-based risk information sheet for renal colic or neck/back pain, based on chief complaint. During enrollment, patients will have three minutes to familiarize themselves with the risk information sheet and ask questions to study staff.
Participant follow-up (Days 1-7, Day 14, Day 90)
On days one through seven and fourteen after enrollment, WTH will send participants automated email or text messages containing links to secure, online follow-up surveys. These brief surveys collect information on patient satisfaction and outlook [25], pain management strategies and functional outcomes, behavioral and functional characteristics [26, 29], medication use behaviors [30], quality of life [26], health literacy [31], and health numeracy [32]. Patients randomized to the narrative enhanced probabilistic risk tool arm will also receive messages encouraging them to continue to view the eight video narratives through an individualized WTH portal.
Ninety days after enrollment, study staff will contact participants by text or phone to conduct a 20-minute follow-up survey of the above attributes, as well as recall of opioid risk level and/or viewing of video narratives for patients randomized to the corresponding intervention arms.
Patient and stakeholder engagement
Patients and other key stakeholders are and will be engaged in this study throughout the entire research process. Four patients are formally involved in this study as Patient Investigators, full members of the core research team who provide perspective on research questions, methodologies, and patient-related outcomes. As current and former patients presenting with acute and/or chronic pain, Patient Investigators have unique and extensive input including diverse experiences with opioids. Additionally, the UPHS Patient and Family Education Committee, a formal group of hospital staff, patient advocates and community members who meet regularly to help patient and their families navigate hospital care, will provide study input. These stakeholders will also be engaged in the interpretation and dissemination of study findings as the trial progresses.
Text and email reminders are used to promote continuous engagement and follow up among study participants. Small cash incentives are used to maximize retention and promote follow up. All subjects are eligible to receive up to $50 dollars for completing enrollment and follow up surveys. For the 90 day survey, if the subjects do not respond to the electronic reminders, research staff will call the participant to remind them to complete survey and, if necessary, to conduct the surveys by telephone.
All study staff will complete IRB certified training regarding human subjects’ protection and will be thoroughly trained and supervised in the conduct of the research protocol. A project manager, responsible for general study oversight, will ensure all study procedures are followed and that any issues are brought to the attention of the investigators and resolved in a timely manner. Enrollment staff including research coordinators and research associates will be trained to demonstrate sensitivity to the pain experiences of patients and to neutrally present the intervention tools. Scripts and role playing will be used when training enrollment staff about how to approach patients, present the study, and maintain a nonjudgmental, neutral approach to collecting information on the amount and type of pain medication taken, history of substance abuse, and other sensitive psychosocial risks.
Statistical Analysis: Data will be analyzed in an intention to treat fashion. Standard statistical tests (2 and ANOVA or Kruskal Wallis test) will be performed to determine outcome distributions and whether patients differ with regard to demographics in the 3 study groups. A data monitoring board was not needed for this study as due to the anticipated low risk of the communication-based interventions and was approved by the central IRB. The investigators will have final access to the trial dataset. There are no contractual limitations to the investigators’ access to these data. The following statistical techniques will be employed for each of our 3 goals of the study:
1. To demonstrate greater knowledge of risk for opioid dependency, concordance between individual risk as measured by the ORT, and follow-up at 2 weeks and three months about their recall of their risk category (measured by at risk, high risk, highest risk) and corresponding risk percentage (6/100, 28/100, or 91/100), a Cohen’s weighted kappa will be calculated for NERT & PRT treatment groups, and then compared using a 2-sample Z-test and/or confidence intervals for the difference. Additional analyses will include dichotomizing concordance (concordant/discordant) as the outcome and developing logistic regression models including treatment arm, demographics (age, gender, ethnicity), and risk category. This will allow for comparison of NERT & PRT treatment groups while adjusting for potential confounders.
2. To test the hypothesis that patients in the NERT group will take significantly less morphine equivalents than patients in PRT or control group, the primary analytic technique will be a Poisson (log-linear) regression or a Negative Binomial (ZINB) regression [33]. Models will be developed using SAS procedures GENMOD or COUNTREG using a log link and Poisson or a ZINB distribution. All models will be adjusted for baseline pain level, condition, and any complications, as well as possible modifiers/confounders such as age, gender, race, education, employment, insurance, income (SES), and marital/relationship status. To assess differences in number of days to no/minimal pain, number of days to cessation of opioid use, and time to return to functional status over the 3-month study period among the 3 treatment arms utilizing Kaplan-Meier curves and Cox proportional-hazard models. The log rank test will be used to assess differences in rate of cessation of opioid use and rate of return to functionality between the 3 treatment groups. Additionally, at the 3-month interview, functionality will be assessed with MOS-20 scales [25]. For this analysis, a 2-way ANOVA (group and condition as main effects) will be used.
3. To assess trust in the provider using the trust in physician scale (range of scores 11-55) [34] [35], and patient shared decision making using the CollaboRATE scale [36], a 2-way ANOVA at 3 months and at discharge, respectively will be used. To test the hypothesis that patients in the NERT group will have greater satisfaction with adequacy of pain management compared to PRT and control groups, 2 analytic techniques will be used. Satisfaction will be assessed using selected items from the American Pain Society Patient Outcome Questionnaire. To assess differences in the absolute score at 2 weeks and 3 months between the 3 treatment arms, an analysis of covariance will be performed with treatment group and condition as main effects, an interaction term crossing approach with condition, and covaried on baseline scores. In addition to this analysis, patient satisfaction will be dichotomized; 1-3 (not satisfied), 4-6 (satisfied) and a generalized linear model (SAS GLM procedure) with a log link, Gaussian or binomial error, and robust estimates of the standard errors of the model coefficients will be employed [37]. Finally, to assess agreement between Patient Preference and Provider Decision, a Cohen’s weighted kappa will be calculated for each treatment arm.
Sample Size and Power Calculation: To determine the number of patients needed in each group for sufficient sample size we considered one of the primary outcomes measured in 2 ways (# of morphine equivalents at 14 days, # of days to no opioids). The final sample size was based on the number of days (rate) to no opioid use as this was the largest sample size needed to detect a clinically meaningful effect between PRT and NERT. Using a 2-sided log-rank test with an overall starting sample size of 1100 subjects achieves 80% power at a 0.05 significance level to detect a hazard ratio of 0.46 when the proportion not taking opioids at 2 weeks in the PRT group is 0.70 (an effect size as small as 15%) and the loss to follow-up (LTF) is 20-25%. Using a conservative estimate of a final sample size, we will have more than sufficient power (>80%) to detect, a difference in number of morphine equivalents at 14 days as small as six, 5 mg doses of oxycodone.
For the control arm, at least 300 patients will be enrolled. Using an effect size of 10-15% difference in proportions, which we considered to be clinically meaningful and also obtainable based on our pilot data, and conservatively estimating a 20-25% loss to follow-up in this group, we will have sufficient power with sample size 225 to evaluate a 10% difference assuming that 95% and 85% will no longer be taking opioids at 2 weeks in the NERT vs control group, respectively.