Introduction

The National Institute on Drug Abuse¹ defines medication misuse as “taking a medication in a manner or dose other than prescribed; taking someone else's prescription, even if for a legitimate medical complaint such as pain; or taking a medication to feel euphoria (ie, to get high).”^(p.2) The misuse of controlled medications is an evolving epidemic that has continued to persist in the last decade.² The misuse of opioids, benzodiazepines, and stimulants is widely recognized by both prescribers and patients as it is a leading cause of hospitalizations, emergency room visits, and deaths.³ Wide recognition of opioid misuse has resulted in increased provider awareness and subsequent decreased dispensing.⁴ In 2018, the Centers for Disease Control released data showing a decrease in prescription opioid–involved deaths by 13.5% from 2017.⁵ This reduction is thought to be due to increased awareness, changes in prescribing habits, and decreased stigmas associated with receiving treatment for OUD.⁶

A less widely recognized yet related topic is medication misuse involving noncontrolled prescription medications (NCPM). It is demonstrated that patients with co-occurring mental health disorders are 3 times more likely to misuse NCPM.⁷ It is also shown that individuals often misuse NCPM in combination with other prescriptions, non-prescriptions, or substances.⁸ Documented motivations for misusing a NCPM are not well-studied, but some motivations for misuse of NCPM include to self-medicate for existing physical or mental health disorders, to achieve the high feeling associated with misuse, and because of perceived safety of abusing NCPM instead of substances.⁷

Federally, gabapentin is an NCPM; however, it has a moderate amount of evidence surrounding its misuse potential.⁹ Due to this, several states have adjusted the scheduling of gabapentin making it a controlled substance. In the state of South Carolina, gabapentin remains classified as an NCPM. Historically, it was thought that gabapentin did not have misuse potential, and it was frequently prescribed for a variety of conditions, including seizure disorders, peripheral neuropathy, and insomnia.¹⁰ Within the past decade, a misuse signal has emerged.¹⁰ Gabapentin is thought to inhibit the release of excitatory neurotransmitters through its inhibition of voltage-gated calcium channels, resulting in central nervous system effects, including dizziness and fatigue.¹¹ Survey studies have been conducted looking at the rates of gabapentin misuse in the general population and found it to be as high as 1.1%.¹² Two studies looked at rates of gabapentin misuse in treatment facilities for substance use; rates of misuse were found to be 22% overall.¹² Patients with a history of OUD were found to be more likely to also misuse gabapentin.¹² The misuse of gabapentin is thought to be due in part to its ease of access, its affordability, and minimal adverse side effects associated with its use.¹⁰ Notably, pregabalin, a medication with structural similarities to gabapentin, is a federally controlled substance due to its misuse potential.¹³ Pregabalin and gabapentin differ in regard to some pharmacokinetic properties.¹⁴ For example, pregabalin does not depend on active transport for absorption, whereas gabapentin does.¹⁴ This property results in predictable, linear pharmacokinetics with pregabalin compared with gabapentin, exhibiting saturable, nonlinear pharmacokinetics.¹⁴ These properties theoretically make gabapentin less desirable for misuse.

Other agents, such as quetiapine, bupropion, trazodone, clonidine, and venlafaxine, are associated with reports of misuse.^15-23 These medications have varying pharmacodynamic properties that may underlie their potential misuse. Some medications are misused along with other medications or substances for greater effect, whereas others are used to recover from or mitigate the adverse effects of medications or substances.^18,23 As an example, clonidine is a centrally acting alpha agonist and is hypothesized to boost the effects of methadone and cocaine by minimizing withdrawal symptoms, enhancing sedation, and optimizing a patient's high.¹⁷ Whereas several studies review the theoretical explanations behind misusing these agents, few studies determine the clinical significance of this misuse.

An estimated 38% of patients admitted to a psychiatric hospital have co-occurring mental health and SUDs.²⁴ It is largely known that opioids and other controlled medications are being misused, but NCPM misuse is less consistently reported. Due to the gap in literature regarding the clinical significance or frequency of NCPM misuse, this study aims to identify prescriber perceptions of NCPM misuse and to evaluate patient reported patterns of misuse at this academic medical center.

Methods

Results

Characteristics of Patients

In total, 79 patients completed the survey between November 2020 and March 2021; 3 patient surveys were excluded due to missing data. Missing data is defined as patients not answering any questions regarding medication misuse but only baseline demographic information. As a result, 76 patient surveys were included in the final analysis. Demographics are included in Table 1. The median age of patients was 34.5 years (IQR 29-49), and patients were predominantly male (n = 40; 53.3%). Depression (n = 45; 59.2%) and anxiety (n = 45; 59.2%) were the most commonly reported admission reasons. To note, of the patient surveys included, not all surveys had all medication misuse questions fully answered, leading to differing sample sizes for each endpoint based on response rates of individual questions.

TABLE 1 Baseline demographics for included patients (N = 76) and prescribers (N = 46)

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Secondary Outcomes

Rates of NCPM Misuse Among Various Comorbid Conditions

As shown in Table 2, there was no difference in the rate of NCPM misuse in patients admitted secondary to SUD (n = 9; 31% vs n = 16; 34%; P = .786), anxiety (n = 14; 48.3% vs n = 31; 66%; P = .128), suicidal ideation (n = 18; 62.1% vs n = 21; 44.7%; P = .141), or depression (n = 17; 58.6% vs n = 28; 59.6%; P = .934). Opioid and cannabis use disorders were reported more frequently in patients who misuse NCPM vs those who do not (opioid: n = 7; 24.1% vs n = 2; 4.3%, P = .023; cannabis: n = 4; 13.8% vs n = 0; 0%; P = .019; Table 3). No differences in misuse rates were seen among patients with AUD, hallucinogen use disorder, or stimulant use disorder (P > .05). Additionally, there was no difference in the rate of NCPM misuse in patients with any of the comorbidities analyzed. Notably, this included ADHD, chronic pain, or hepatitis C virus (P > .99; Table 4).

TABLE 2 Demographics among respondents with noncontrolled prescription medication (NCPM) misuse (N = 29) versus without (N = 47)

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TABLE 3 SUDs among respondents with noncontrolled prescription medication (NCPM) misuse (N = 29) versus without (N = 47)

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TABLE 4 Comorbidities among respondents with (N = 29) versus without (N = 47) noncontrolled prescription medication (NCPM) misuse

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Patient-Specific Outcomes

Oral (n = 25; 86.2%) misuse of NCPM was most common, whereas the intranasal route was rare (n = 3; 10.3%). Misuse of NCPM to get high was the most commonly reported reason for misuse (n = 10; 38.5%). The most commonly reported definition of medication misuse was taking more medication than prescribed (n = 58; 85.3%).

Prescriber-Specific Outcomes

The most common definition of medication misuse was taking medication that is not prescribed solely for the purpose of getting high (n = 44; 95.7%). Prescribers reported utilizing different prescribing habits in patients with a history of substance use (n = 42; 91.3%), for those with multiple controlled substance prescriptions in the prescription drug monitoring database (n = 36; 78.3%), and in patients with a history of nonadherence (n = 28; 60.9%).

Discussion

To our knowledge, this is the first prospective study evaluating both patient patterns and prescriber perceptions of NCPM misuse. Our study was designed most similarly to a self-report questionnaire published by Wilens et al²² investigating the concomitant use of prescription medications among opioid- and/or alcohol-dependent patients seeking inpatient detoxification. In our study, 38.4% of patients surveyed reported NCPM misuse. This finding matches the findings from Wilens et al²² as 30% of their surveyed population reported prescription medication misuse. The findings in our study specifically emphasize the potential for increased rates of NCPM misuse within the past several years. The aforementioned study analyzes both noncontrolled and controlled medication misuse, whereas this study only reviews NCPM misuse but finds comparable rates of misuse. Additionally, all patients reporting misuse in the Wilens et al²² study were a part of the OUD subsample with none from the AUD subsample. The findings of our study align with the findings of Wilens et al²² because it was more common for patients with OUD to report NCPM misuse.

Additionally, results suggest that perceptions of NCPM misuse by prescribers do not necessarily align with patient-reported patterns of NCPM misuse. Despite previous literature signaling a potential for misuse, we were surprised to discover that trazodone was the most common patient-reported medication of misuse in our sample. Trazodone is generally considered a safe medication to prescribe as an adjunct to other medications for insomnia.^23,25 This is exemplified by trazodone being a frequently utilized medication at our institution and only 28.9% of prescribers identifying trazodone as a high-risk medication for misuse. The format of our survey and the small sample size did not allow us to delineate the pattern and intent behind its misuse. Published literature^23,25 determines trazodone to have low misuse potential, but given our results, more research is needed.

Similar to trazodone, quetiapine is frequently prescribed at this institution, even for off-label indications, such as delirium and insomnia despite 66.7% of prescribers identifying quetiapine as a high-risk medication. Both trazodone and quetiapine are theorized to have misuse potential due to having sedative and anxiolytic properties, but again, the exact mechanism is not fully elucidated.^16,25 These results highlight the need for enhanced education to prescribers. Additionally, all health care providers should keep these findings in mind when caring for patients. Everyone can play an active role in optimizing prescribing of these medications and minimizing polypharmacy.

The finding of OUD and cannabis use disorders being reported more frequently in patients who misuse NCPM is consistent with previously conducted literature.²² Additionally, the finding that other SUDs, including alcohol, hallucinogen, and stimulant use disorders, were not associated with NCPM misuse is important and reassuring. In a previously conducted study,²² no significantly higher rates of medication misuse are seen in patients misusing alcohol.

Several limitations exist in our study with most being directly related to the inherent limitations of the survey study design. Due to the data being a direct result of surveys, there is an inherent risk for reporting bias, and thus, results could be impacted. Overall, there were low participation rates for both patients and prescribers resulting in a smaller sample size than initially expected. This small sample size could impact the overall generalizability, so caution should be used when interpreting the results. Also, due to varying levels of education typically represented within this population, there may have been a lack of understanding for some of the survey questions within the patient survey that could influence the results. When analyzing the patient surveys, 3 surveys were not completed in their entirety and had to be excluded. More extensive education to patients and team members distributing surveys could provide a solution to this limitation. The utilization of paper surveys for patients resulted in issues with coordinating survey distribution and collection. This process required several individuals to work together as a team to ensure surveys were completed and returned for analysis. Last, this study was not designed to assess misuse pattern/intent based on individual medications. A much larger sample size would be needed to assess that endpoint.

After completion of this study, several steps can be taken to optimize clinical practice. To start, wide dissemination of the study findings to prescribers will be completed at our institution to raise awareness of NCPM misuse and promote safe prescribing. Also, education sessions will be provided to prescribers regularly to assess current prescribing patterns and ensure polypharmacy is avoided when possible.

Our study determined that NCPM misuse is prevalent and occurs frequently within our institution. Prescribers were generally aware of NCPM misuse as a whole; however, psychiatric prescribers were more familiar than general medicine prescribers. NCPM misuse is a prevalent and important topic that warrants more attention in the literature. Future studies should be aimed at determining the most likely mechanism of misuse for trazodone based on the findings of this study. Future studies aimed at analyzing the intent of NCPM misuse would help to fill a gap that still exists in the literature.