Using a pharmacogenetic clinical decision support system to improve psychopharmacotherapy dosing in patients with affective disorders

Michael Zastrozhin; Valentin Skryabin; Alexander Sorokin; Oleg Buzik; Inessa Bedina; Elena Grishina; Kristina Ryzhikova; Valery Shipitsyn; Evgeny Bryun; Dmitry Sychev

doi:10.1515/dmpt-2019-0033

Using a pharmacogenetic clinical decision support system to improve psychopharmacotherapy dosing in patients with affective disorders

Drug Metab Pers Ther. 2020 Sep 1;35(4). doi: 10.1515/dmpt-2019-0033.

Authors

Affiliations

¹ Department of Healthcare, Moscow Research and Practical Center on Addictions of the Moscow, Moscow, Russia.
² Russian Medical Academy of Continuous Professional Education of the Ministry of Health of the Russian Federation, Moscow, Russia.

PMID: 32870807
DOI: 10.1515/dmpt-2019-0033

Abstract

Objectives: Although pharmacogenetic tests provide the information on a genotype and the predicted phenotype, these tests do not themselves provide the interpretation of data for a physician. Currently, there are approximately two dozen pharmacogenomic clinical decision support systems (CDSSs) used in psychiatry. Implementation of the CDSSs forming the recommendations on drug and dose selection according to the results of pharmacogenetic testing is an urgent task. Fulfillment of this task will allow increasing the efficacy of therapy and decreasing the risk of undesirable side effects.

Methods: The study included 118 male patients (48 in the main group and 70 in the control group) with affective disorders and comorbid alcohol use disorder. To evaluate the efficacy and safety of therapy, several international psychometric scales and rating scales to measure side effects were used. Genotyping was performed using the real-time polymerase chain reaction with allele-specific hybridization. Pharmacogenetic testing results were interpreted using free software PGX2 (LLE Medicine, Russian Federation, Biomedical Cluster of Skolkovo, Moscow Innovative Cluster; www.pgx2.com).

Results: The statistically significant differences across the scores on psychometric scales were revealed. For instance, the total score on the Hamilton Rating Scale for Depression by day 9 was 9.0 [8.0; 10.0] for the main group and 11.0 [10.0; 12.0] (p<0.001) for the control group and by day 16 it was 4.0 [2.0; 6.0] for the main group and 14.0 [13.0; 14.0] (p<0.001) for the control group. The UKU Side-Effect Rating Scale (UKU) also revealed a statistically significant difference. The total score on the UKU scale by day 9 was 4.0 [4.0; 5.0] for the main group and 5.0 [5.0; 6.0] (p<0.001) for the control group and by day 16 this difference grew significantly: 3.0 [0.0; 4.2] for the main group and 9.0 [7.0; 11.0] (p<0.001) for the control group.

Conclusions: Pharmacogenetic-guided personalization of the drug dose in patients with affective disorders and comorbid alcohol use disorder can reduce the risk of undesirable side effects and pharmacoresistance. It allows recommending the use of pharmacogenetic CDSSs for optimizing drug dosage.

Keywords: clinical decision support system; fluvoxamine; personalized medicine; pharmacogenetics.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Decision Support Systems, Clinical*
Humans
Male
Mood Disorders / drug therapy
Mood Disorders / genetics
Pharmacogenetics* / methods
Pharmacogenomic Testing