Accepted for/Published in: JMIR Research Protocols
Date Submitted: Feb 27, 2019
Open Peer Review Period: Mar 5, 2019 - Mar 19, 2019
Date Accepted: Jul 19, 2019
(closed for review but you can still tweet)
Utilizing Pharmacogenomic Testing in Primary Care: A Pilot Randomized Control Study
ABSTRACT
Background:
Antidepressants are used by primary care providers to treat a variety of conditions including (but not limited to) depression and anxiety. A trial-and-error approach is typically used to identify effective therapy, as treatment efficacy and safety can vary based on the response, which is affected by certain gene types. Pharmacokinetic pharmacogenomic (PGx) testing provides phenotypic classification of individuals as poor, intermediate, extensive, and ultra-rapid cytochrome P450 metabolizers, providing information for optimal drug selection.
Objective:
The objective of this pilot study is to examine the feasibility, acceptability, and preliminary effectiveness of PGx testing when used after starting a new antidepressant medication.
Methods:
We are conducting a pilot study with physicians from six Department of Family Medicine (DFM) clinics at the University of Michigan (UM) who are willing to utilize PGx test results to manage antidepressant medication use. From enrolled physicians, patients were recruited to participate in a 6-month randomized, wait-list controlled trial in which patient participants newly prescribed an antidepressant had PGx testing, and were randomized equally to have the results released to their primary care physician as soon as results were available, or after 3 months. Patients were excluded if they had been taking the antidepressant for more than 4 weeks or if they had undergone PGx testing in the past. Physician participants completed a baseline survey to assess demographics, as well as knowledge, feasibility, and acceptability of PGx testing for this population. At the conclusion of the study, physician participants will complete a survey to assess knowledge, satisfaction, feasibility, acceptability, perceived effectiveness, and barriers to widespread adoption of PGx testing. Patient participants will complete a baseline, 3-, and 6-month assessment; control patient participants will have an additional 9-month assessment. Data collected will include the reason for antidepressant use, self-reported medication adherence, side effects, patient health questionnaire-8 item depression scale, generalized anxiety disorder-7 item scale, 12-Item Short Form Health Survey, work status/changes, and physician and emergency department visits. PGx knowledge and perceptions (including acceptability and feasibility), as well as demographic information will also be obtained.
Results:
We recruited 23 physician participants between November 2017 and January 2019, and 52 patient participants between January 2018 and April 2019. Currently, all physician and patient participants have been recruited and we expect data collection to conclude in January 2020.
Conclusions:
This study will examine the preliminary effectiveness of PGx testing after treatment initiation, as well as determine the feasibility and acceptability of PGx testing for use in primary care. Through this study, we expect to demonstrate the benefit of PGx testing, and lay the foundation for translating this approach into use within primary care. Clinical Trial: NCT03270891
Citation
Per the author's request the PDF is not available.
Copyright
© The authors. All rights reserved. This is a privileged document currently under peer-review/community review (or an accepted/rejected manuscript). Authors have provided JMIR Publications with an exclusive license to publish this preprint on it's website for review and ahead-of-print citation purposes only. While the final peer-reviewed paper may be licensed under a cc-by license on publication, at this stage authors and publisher expressively prohibit redistribution of this draft paper other than for review purposes.