Your search keyword '"Aitchison KJ"' showing total 177 results

1. Identifying the Common Genetic Basis of Antidepressant Response.

Author

Pain, O, Hodgson, K, Trubetskoy, V, Ripke, S, Marshe, VS, Adams, MJ, Byrne, EM, Campos, AI, Carrillo-Roa, T, Cattaneo, A, Als, TD, Souery, D, Dernovsek, MZ, Fabbri, C, Hayward, C, Henigsberg, N, Hauser, J, Kennedy, JL, Lenze, EJ, Lewis, G, Müller, DJ, Martin, NG, Mulsant, BH, Mors, O, Perroud, N, Porteous, DJ, Rentería, ME, Reynolds, CF, Rietschel, M, Uher, R, Wigmore, EM, Maier, W, Wray, NR, Aitchison, KJ, Arolt, V, Baune, BT, Biernacka, JM, Bondolfi, G, Domschke, K, Kato, M, Li, QS, Liu, Y-L, Serretti, A, Tsai, S-J, Turecki, G, Weinshilboum, R, GSRD Consortium, Major Depressive Disorder Working Group of the Psychiatric Genomics Consortium, McIntosh, AM, Lewis, CM, Pain, O, Hodgson, K, Trubetskoy, V, Ripke, S, Marshe, VS, Adams, MJ, Byrne, EM, Campos, AI, Carrillo-Roa, T, Cattaneo, A, Als, TD, Souery, D, Dernovsek, MZ, Fabbri, C, Hayward, C, Henigsberg, N, Hauser, J, Kennedy, JL, Lenze, EJ, Lewis, G, Müller, DJ, Martin, NG, Mulsant, BH, Mors, O, Perroud, N, Porteous, DJ, Rentería, ME, Reynolds, CF, Rietschel, M, Uher, R, Wigmore, EM, Maier, W, Wray, NR, Aitchison, KJ, Arolt, V, Baune, BT, Biernacka, JM, Bondolfi, G, Domschke, K, Kato, M, Li, QS, Liu, Y-L, Serretti, A, Tsai, S-J, Turecki, G, Weinshilboum, R, GSRD Consortium, Major Depressive Disorder Working Group of the Psychiatric Genomics Consortium, McIntosh, AM, and Lewis, CM

Abstract

BACKGROUND: Antidepressants are a first-line treatment for depression. However, only a third of individuals experience remission after the first treatment. Common genetic variation, in part, likely regulates antidepressant response, yet the success of previous genome-wide association studies has been limited by sample size. This study performs the largest genetic analysis of prospectively assessed antidepressant response in major depressive disorder to gain insight into the underlying biology and enable out-of-sample prediction. METHODS: Genome-wide analysis of remission (n remit = 1852, n nonremit = 3299) and percentage improvement (n = 5218) was performed. Single nucleotide polymorphism-based heritability was estimated using genome-wide complex trait analysis. Genetic covariance with eight mental health phenotypes was estimated using polygenic scores/AVENGEME. Out-of-sample prediction of antidepressant response polygenic scores was assessed. Gene-level association analysis was performed using MAGMA and transcriptome-wide association study. Tissue, pathway, and drug binding enrichment were estimated using MAGMA. RESULTS: Neither genome-wide association study identified genome-wide significant associations. Single nucleotide polymorphism-based heritability was significantly different from zero for remission (h 2 = 0.132, SE = 0.056) but not for percentage improvement (h 2 = -0.018, SE = 0.032). Better antidepressant response was negatively associated with genetic risk for schizophrenia and positively associated with genetic propensity for educational attainment. Leave-one-out validation of antidepressant response polygenic scores demonstrated significant evidence of out-of-sample prediction, though results varied in external cohorts. Gene-based analyses identified ETV4 and DHX8 as significantly associated with antidepressant response. CONCLUSIONS: This study demonstrates that antidepressant response is influenced by common genetic variation, has a genetic overlap sc

Published

2022

2. Sequence2Script: A Web-Based Tool for Translation of Pharmacogenetic Data Into Evidence-Based Prescribing Recommendations

Author

Bousman, CA, Wu, P, Aitchison, KJ, Cheng, T, Bousman, CA, Wu, P, Aitchison, KJ, and Cheng, T

Abstract

Pharmacogenomic (PGx) testing has emerged as an effective strategy for informing drug selection and dosing. This has led to an increase in the use of PGx testing in the clinic and has catalyzed the emergence of a burgeoning commercial PGx testing industry. However, not all PGx tests are equivalent in their approach to translating testing results into prescribing recommendations, due to an absence of regulatory standards. As such, those generating and using PGx data require tools for ensuring the prescribing recommendations they are provided align with current peer-reviewed PGx-based prescribing guidelines developed by expert groups or approved product labels. Herein, we present Sequence2Script (sequence2script.com), a simple, free, and transparent web-based tool to assist in the efficient translation of PGx testing results into evidence-based prescribing recommendations. The tool was designed with a wide-range of user groups (e.g., healthcare providers, laboratory staff, researchers) in mind. The tool supports 97 gene-drug pairs with evidence-based prescribing guidelines, allows users to adjust recommendations for concomitant inhibitors and inducers, and generates a clinical report summarizing the patient's genotype, inferred phenotype, phenoconverted phenotype (if applicable), and corresponding prescribing recommendations. In this paper, we describe each of the tool's features, provide use case examples, and discuss limitations of and future development plans for the tool. Although we recognize that Sequecnce2Script may not meet the needs of every user, the hope is that this novel tool will facilitate more standardized use of PGx testing results and reduce barriers to implementing these results into practice.

Published

2021

3. Interrater reliability of the Antipsychotic Non-Neurological Side-Effects Rating Scale measured in patients treated with clozapine

Author

Ohlsen, RI, Williamson, R., Yusufi, B., Mullan, J., Irving, D., Mukherjee, S., Page, E., Aitchison, KJ, and Barnes, TRE

Subjects

Drugs -- Adverse and side effects, Antipsychotic drugs -- Dosage and administration -- Complications and side effects -- Research, Pharmaceuticals and cosmetics industries, Psychology and mental health, Diagnosis, Complications and side effects, Research, Risk factors, Dosage and administration

Abstract

Byline: RI Ohlsen (MRC SGDP Centre and Division of Psychological Medicine and Psychiatry, Institute of Psychiatry, King's College London, London, UK, r.ohlsen@iop.kcl.ac.uk); R. Williamson (MRC SGDP Centre and Division of [...]

Published

2008

4. Antidepressant drug-specific prediction of depression treatment outcomes from genetic and clinical variables

Author

Iniesta R, Hodgson K, Stahl D, Malki K, Maier W, Rietschel M, Mors O, Hauser J, Henigsberg N, Dernovsek MZ, Souery D, Dobson R, Aitchison KJ, Farmer A, McGuffin P, Lewis CM, and Uher R

Abstract

Individuals with depression differ substantially in their response to treatment with antidepressants. Specific predictors explain only a small proportion of these differences. To meaningfully predict who will respond to which antidepressant, it may be necessary to combine multiple biomarkers and clinical variables. Using statistical learning on common genetic variants and clinical information in a training sample of 280 individuals randomly allocated to 12-week treatment with antidepressants escitalopram or nortriptyline, we derived models to predict remission with each antidepressant drug. We tested the reproducibility of each prediction in a validation set of 150 participants not used in model derivation. An elastic net logistic model based on eleven genetic and six clinical variables predicted remission with escitalopram in the validation dataset with area under the curve 0.77 (95%CI; 0.66-0.88; p = 0.004), explaining approximately 30% of variance in who achieves remission. A model derived from 20 genetic variables predicted remission with nortriptyline in the validation dataset with an area under the curve 0.77 (95%CI; 0.65-0.90; p 0.001), explaining approximately 36% of variance in who achieves remission. The predictive models were antidepressant drug-specific. Validated drug-specific predictions suggest that a relatively small number of genetic and clinical variables can help select treatment between escitalopram and nortriptyline.

Published

2018

5. Housekeeping gene expression is affected by antidepressant treatment in a mouse fibroblast cell line

Author

Sugden, K., Pariante, CM, McGuffin, P., Aitchison, KJ, and D'Souza, UM

Subjects

Antidepressants -- Health aspects, Fibroblasts -- Research, Gene expression -- Analysis, Genetically modified mice -- Physiological aspects, Polymerase chain reaction -- Usage, Pharmaceuticals and cosmetics industries, Psychology and mental health

Published

2010

6. Interplay between Schizophrenia Polygenic Risk Score and Childhood Adversity in First-Presentation Psychotic Disorder:A Pilot Study

Author

Trotta, Antonella, Iyegbe, Conrad Osamede, Di Forti, Marta, Sham, Pak, Campbell, Desmond, Cherny, Stacey, Mondelli, Valeria, Aitchison, KJ, Murray, Robin MacGregor, Vassos, Evangelos, and Fisher, Helen

Abstract

A history of childhood adversity is associated with psychotic disorder, with an increase in risk according to number or severity of exposures. However, it is not known why only some exposed individuals go on to develop psychosis. One possibility is pre-existing genetic vulnerability. Research on gene-environment interaction in psychosis has primarily focused on candidate genes, although the genetic effects are now known to be polygenic. This pilot study investigated whether the effect of childhood adversity on psychosis is moderated by the polygenic risk score for schizophrenia (PRS). Data were utilised from the Genes and Psychosis (GAP) study set in South London, UK. The GAP sample comprises 285 first-presentation psychosis cases and 256 unaffected controls with information on childhood adversity. We studied only white subjects (80 cases and 110 controls) with PRS data, as the PRS has limited predictive ability in patients of African ancestry. The occurrence of childhood adversity was assessed with the Childhood Experience of Care and Abuse Questionnaire (CECA.Q) and the PRS was based on genome-wide meta-analysis results for schizophrenia from the Psychiatric Genomics Consortium. Higher schizophrenia PRS and childhood adversities each predicted psychosis status. Nevertheless, no evidence was found for interaction as departure from additivity, indicating that the effect of polygenic risk scores on psychosis was not increased in the presence of a history of childhood adversity. These findings are compatible with a multifactorial threshold model in which both genetic liability and exposure to environmental risk contribute independently to the etiology of psychosis.

Published

2016

7. Familiality and SNP heritability of age at onset and episodicity in major depressive disorder

Author

Ferentinos, P, Koukounari, A, Power, R, Rivera, M, Uher, R, Craddock, N, Owen, MJ, Korszun, A, Jones, L, Jones, I, Gill, M, Rice, JP, Ising, M, Maier, W, Mors, O, Rietschel, M, Preisig, M, Binder, EB, Aitchison, KJ, Mendlewicz, J, Souery, D, Hauser, J, Henigsberg, N, Breen, G, Craig, IW, Farmer, AE, Müller-Myhsok, B, McGuffin, P, and Lewis, CM

Subjects

Adult, Male, Adolescent, Genotype, heritability, Interviews as Topic, Age at onset, episodicity, familiality, GCTA, heritability, major depression, Young Adult, Germany, Humans, familiality, Genetic Predisposition to Disease, ddc:610, Age of Onset, Aged, Aged, 80 and over, GCTA, Depressive Disorder, Major, Polymorphism, Genetic, Siblings, Age at onset, genetics [Depressive Disorder, Major], Original Articles, Middle Aged, United Kingdom, Phenotype, Linear Models, episodicity, Female, major depression

Abstract

BACKGROUND: Strategies to dissect phenotypic and genetic heterogeneity of major depressive disorder (MDD) have mainly relied on subphenotypes, such as age at onset (AAO) and recurrence/episodicity. Yet, evidence on whether these subphenotypes are familial or heritable is scarce. The aims of this study are to investigate the familiality of AAO and episode frequency in MDD and to assess the proportion of their variance explained by common single nucleotide polymorphisms (SNP heritability).METHOD: For investigating familiality, we used 691 families with 2-5 full siblings with recurrent MDD from the DeNt study. We fitted (square root) AAO and episode count in a linear and a negative binomial mixed model, respectively, with family as random effect and adjusting for sex, age and center. The strength of familiality was assessed with intraclass correlation coefficients (ICC). For estimating SNP heritabilities, we used 3468 unrelated MDD cases from the RADIANT and GSK Munich studies. After similarly adjusting for covariates, derived residuals were used with the GREML method in GCTA (genome-wide complex trait analysis) software.RESULTS: Significant familial clustering was found for both AAO (ICC = 0.28) and episodicity (ICC = 0.07). We calculated from respective ICC estimates the maximal additive heritability of AAO (0.56) and episodicity (0.15). SNP heritability of AAO was 0.17 (p = 0.04); analysis was underpowered for calculating SNP heritability of episodicity.CONCLUSIONS: AAO and episodicity aggregate in families to a moderate and small degree, respectively. AAO is under stronger additive genetic control than episodicity. Larger samples are needed to calculate the SNP heritability of episodicity. The described statistical framework could be useful in future analyses.

Published

2015

8. Interplay between Schizophrenia Polygenic Risk Score and Childhood Adversity in First-Presentation Psychotic Disorder: A Pilot Study.

Author

Walss-Bass, C, Trotta, A, Iyegbe, C, Di Forti, M, Sham, PC, Campbell, DD, Cherny, SS, Mondelli, V, Aitchison, KJ, Murray, RM, Vassos, E, Fisher, HL, Walss-Bass, C, Trotta, A, Iyegbe, C, Di Forti, M, Sham, PC, Campbell, DD, Cherny, SS, Mondelli, V, Aitchison, KJ, Murray, RM, Vassos, E, and Fisher, HL

Abstract

A history of childhood adversity is associated with psychotic disorder, with an increase in risk according to number or severity of exposures. However, it is not known why only some exposed individuals go on to develop psychosis. One possibility is pre-existing genetic vulnerability. Research on gene-environment interaction in psychosis has primarily focused on candidate genes, although the genetic effects are now known to be polygenic. This pilot study investigated whether the effect of childhood adversity on psychosis is moderated by the polygenic risk score for schizophrenia (PRS). Data were utilised from the Genes and Psychosis (GAP) study set in South London, UK. The GAP sample comprises 285 first-presentation psychosis cases and 256 unaffected controls with information on childhood adversity. We studied only white subjects (80 cases and 110 controls) with PRS data, as the PRS has limited predictive ability in patients of African ancestry. The occurrence of childhood adversity was assessed with the Childhood Experience of Care and Abuse Questionnaire (CECA.Q) and the PRS was based on genome-wide meta-analysis results for schizophrenia from the Psychiatric Genomics Consortium. Higher schizophrenia PRS and childhood adversities each predicted psychosis status. Nevertheless, no evidence was found for interaction as departure from additivity, indicating that the effect of polygenic risk scores on psychosis was not increased in the presence of a history of childhood adversity. These findings are compatible with a multifactorial threshold model in which both genetic liability and exposure to environmental risk contribute independently to the etiology of psychosis.

Published

2016

9. Is cerebral asymmetry associated with serotonin transporter in psychosis?

Author

Papili, P, Aitchison, KJ, Morgan, K, Fearon, P, Morgan, C, Lappin, J, Di Forti, M, Aas, M, Butt, A, Eyeson, J, La Cascia, C, Miorelli, A, Mondelli, V, Navari, S, Pariante, CM, Curtis, L, David, C, Murray, RM, Dazzan, P, Papili, P, Aitchison, KJ, Morgan, K, Fearon, P, Morgan, C, Lappin, J, Di Forti, M, Aas, M, Butt, A, Eyeson, J, La Cascia, C, Miorelli, A, Mondelli, V, Navari, S, Pariante, CM, Curtis, L, David, C, Murray, RM, and Dazzan, P

Subjects

CEREBRAL ASYMMETRY, psychosis, serotonin

Published

2006

10. Genome-wide association study of increasing suicidal ideation during antidepressant treatment in the GENDEP project

Author

Perroud, N, Uher, R, Ng, My, Guipponi, M, Hauser, J, Henigsberg, N, Maier, W, Mors, O, Gennarelli, Massimo, Rietschel, M, Souery, D, Dernovsek, Mz, Stamp, As, Lathrop, M, Farmer, A, Breen, G, Aitchison, Kj, Lewis, Cm, Craig, Iw, and Mcguffin, P.

Published

2012

11. GENDEP: Recent Pharmacogenetic and Personalized Therapy

Author

Aitchison, KJ, Keers, R, Uher, R, Perroud, N, Smith, R, Malki, K, Paya-Cano, J, Rietschel, M, Mors, Ole, Henigsberg, N, Maier, W, Hauser, J, Kozel, D, Souery, D, Schalkwyk, L, Lewis, C, Craig, W, and McGuffin, P

Published

2011

12. DOES STRESS CONTRIBUTE TO INFLAMMATORY AND METABOLIC ABNORMALITIES IN FIRST EPISODE PSYCHOSIS? RID G-8781-2011 RID E-6837-2010 RID B-1297-2011

Author

Mondelli, V, Aas, M, Belvederi Murri, M, Di Forti, M, Fisher, H, Handley, R, Hepgul, N, Marques, Tr, Morgan, C, Taylor, H, Aitchison, Kj, Dazzan, P, Murray, Rm, and Pariante, Cm

Subjects

NO

Published

2010

13. The Effect of Childhood Trauma and Antipsychotic Treatment on Inflammatory and Metabolic Markers in First-Episode Psychosis RID G-8781-2011 RID E-6837-2010 RID B-1297-2011

Author

Mondelli, V, Aas, M, Belvederi Murri, M, Di Forti, M, Fisher, H, Handley, R, Hepgul, N, Marques, Tr, Morgan, C, Taylor, H, Aitchison, Kj, Dazzan, P, Murray, Rm, and Pariante, Cm

Subjects

NO

Published

2010

14. Genetic predictors of response to serotonergic and noradrenergic antidepressants in major depressive disorder: a genome-wide analysis of individual-level data and a meta-analysis.

Author

Hay, PJ, Tansey, KE, Guipponi, M, Perroud, N, Bondolfi, G, Domenici, E, Evans, D, Hall, SK, Hauser, J, Henigsberg, N, Hu, X, Jerman, B, Maier, W, Mors, O, O'Donovan, M, Peters, TJ, Placentino, A, Rietschel, M, Souery, D, Aitchison, KJ, Craig, I, Farmer, A, Wendland, JR, Malafosse, A, Holmans, P, Lewis, G, Lewis, CM, Stensbøl, TB, Kapur, S, McGuffin, P, Uher, R, Hay, PJ, Tansey, KE, Guipponi, M, Perroud, N, Bondolfi, G, Domenici, E, Evans, D, Hall, SK, Hauser, J, Henigsberg, N, Hu, X, Jerman, B, Maier, W, Mors, O, O'Donovan, M, Peters, TJ, Placentino, A, Rietschel, M, Souery, D, Aitchison, KJ, Craig, I, Farmer, A, Wendland, JR, Malafosse, A, Holmans, P, Lewis, G, Lewis, CM, Stensbøl, TB, Kapur, S, McGuffin, P, and Uher, R

Abstract

BACKGROUND: It has been suggested that outcomes of antidepressant treatment for major depressive disorder could be significantly improved if treatment choice is informed by genetic data. This study aims to test the hypothesis that common genetic variants can predict response to antidepressants in a clinically meaningful way. METHODS AND FINDINGS: The NEWMEDS consortium, an academia-industry partnership, assembled a database of over 2,000 European-ancestry individuals with major depressive disorder, prospectively measured treatment outcomes with serotonin reuptake inhibiting or noradrenaline reuptake inhibiting antidepressants and available genetic samples from five studies (three randomized controlled trials, one part-randomized controlled trial, and one treatment cohort study). After quality control, a dataset of 1,790 individuals with high-quality genome-wide genotyping provided adequate power to test the hypotheses that antidepressant response or a clinically significant differential response to the two classes of antidepressants could be predicted from a single common genetic polymorphism. None of the more than half million genetic markers significantly predicted response to antidepressants overall, serotonin reuptake inhibitors, or noradrenaline reuptake inhibitors, or differential response to the two types of antidepressants (genome-wide significance p<5×10(-8)). No biological pathways were significantly overrepresented in the results. No significant associations (genome-wide significance p<5×10(-8)) were detected in a meta-analysis of NEWMEDS and another large sample (STAR*D), with 2,897 individuals in total. Polygenic scoring found no convergence among multiple associations in NEWMEDS and STAR*D. CONCLUSIONS: No single common genetic variant was associated with antidepressant response at a clinically relevant level in a European-ancestry cohort. Effects specific to particular antidepressant drugs could not be investigated in the current study. Please see lat

Published

2012

15. History of suicide attempts among patients with depression in the GENDEP project

Author

Perroud, N, Uher, R, Hauser, J, Rietschel, M, Henigsberg, N, Placentino, A, Kozel, D, Maier, W, Mors, O, Souery, D, Dmitrzak Weglarz, M, Jorgensen, L, Kovacic, Z, Giovannini, C, Mendlewicz, J, Zobel, A, Strohmaier, J, Mcguffin, P, Aitchison, K, Farmer, A, GIOVANNINI, CATERINA, McGuffin, P, Aitchison, KJ, Farmer, A., Perroud, N, Uher, R, Hauser, J, Rietschel, M, Henigsberg, N, Placentino, A, Kozel, D, Maier, W, Mors, O, Souery, D, Dmitrzak Weglarz, M, Jorgensen, L, Kovacic, Z, Giovannini, C, Mendlewicz, J, Zobel, A, Strohmaier, J, Mcguffin, P, Aitchison, K, Farmer, A, GIOVANNINI, CATERINA, McGuffin, P, Aitchison, KJ, and Farmer, A.

Abstract

Background: It has been proposed that a history of suicide attempts could be a correlate of severe depressive disorder and that suicide attempters (SA) could represent a particular subtype of subjects suffering from major depressive disorder. We investigated clinical and demographic characteristics associated with SA and tested the hypothesis that a history of suicide attempts predicts poor response to antidepressants. Methods: One-hundred-and-forty-one SA and 670 non-SA subjects with major depressive disorder (MDD) were treated for twelve weeks with escitalopram or nortriptyline in GENDEP, a part-randomized multi-center clinical and pharmacogenetic study. Baseline characteristics were compared using linear and logistic regression. Linear mixed models were used to analyse continuous outcomes during the twelve weeks of follow-up. Results: At baseline, SA subjects suffered from more severe depression (mean Montgomery-Asberg Depression Rating Scale: 30.29 (7.61) vs 28.43 (6.54), p = 0.0002), reported higher level of suicidal ideation (1.21 (0.82) vs 0.73 (0.48), p < 0.0001), had a younger age of onset and experienced more depressive episodes, had higher harm avoidance scores and poorer socio-demographic environment than non-SA individuals. However, during the twelve weeks of treatment and after adjustment for baseline severity of depression there was no difference in treatment response between SA and non-SA. Limitations: Due to its retrospective design, it is possible that more severely depressed subjects might report more suicide attempts than less depressed individuals. Conclusions: While SA differed from non-SA in several clinical and demographic characteristics, the antidepressants were similarly effective in SA as in comparably severely depressed subjects without a history of suicide attempts. © 2009 Elsevier B.V. All rights reserved.

Published

2010

16. Suicidal ideation during treatment of depression with escitalopram and nortriptyline in Genome-Based Therapeutic Drugs for Depression (GENDEP): A clinical trial

Author

Perroud, N, Uher, R, Marusic, A, Rietschel, M, Mors, O, Henigsberg, N, Hauser, J, Maier, W, Souery, D, Placentino, A, Szczepankiewicz, A, Jorgensen, L, Strohmaier, J, Zobel, A, Giovannini, C, Elkin, A, Gunasinghe, C, Gray, J, Campbell, D, Gupta, B, Farmer, A, Mcguffin, P, Aitchison, K, Farmer, AE, McGuffin, P, Aitchison, KJ, GIOVANNINI, CATERINA, Perroud, N, Uher, R, Marusic, A, Rietschel, M, Mors, O, Henigsberg, N, Hauser, J, Maier, W, Souery, D, Placentino, A, Szczepankiewicz, A, Jorgensen, L, Strohmaier, J, Zobel, A, Giovannini, C, Elkin, A, Gunasinghe, C, Gray, J, Campbell, D, Gupta, B, Farmer, A, Mcguffin, P, Aitchison, K, Farmer, AE, McGuffin, P, Aitchison, KJ, and GIOVANNINI, CATERINA

Abstract

BACKGROUND: Suicidal thoughts and behaviours during antidepressant treatment, especially during the first weeks of treatment, have prompted warnings by regulatory bodies. The aim of the present study is to investigate the course and predictors of emergence and worsening of suicidal ideation during tricyclic antidepressant and serotonin reuptake inhibitor treatment. METHODS: In a multicentre part-randomised open-label study, 811 adult patients with moderate to severe unipolar depression were allocated to flexible dosage of escitalopram or nortriptyline for 12 weeks. The suicidality items of three standard measures were integrated in a suicidal ideation score. Increases in this score were classified as treatment emergent suicidal ideation (TESI) or treatment worsening suicidal ideation (TWOSI) according to the absence or presence of suicidal ideation at baseline. RESULTS: Suicidal ideation decreased during antidepressant treatment. Rates of TESI and TWOSI peaked in the fifth week. Severity of depression predicted TESI and TWOSI. In men, nortriptyline was associated with a 9.8-fold and 2.4-fold increase in TESI and TWOSI compared to escitalopram, respectively. Retirement and history of suicide attempts predicted TWOSI. CONCLUSION: Increases in suicidal ideation were associated with depression severity and decreased during antidepressant treatment. In men, treatment with escitalopram is associated with lower risk of suicidal ideation compared to nortriptyline. Clinicians should remain alert to suicidal ideation beyond the initial weeks of antidepressant treatment.

Published

2009

17. Differential efficacy of escitalopram and nortriptyline on dimensional measures of depression

Author

Uher, R, Maier, W, Hauser, J, Marusic, A, Schmael, C, Mors, O, Henigsberg, N, Souery, D, Placentino, A, Rietschel, M, Zobel, A, Dmitrzak Weglarz, M, Petrovic, A, Jorgensen, L, Kalember, P, Giovannini, C, Barreto, M, Elkin, A, Landau, S, Farmer, A, Aitchison, K, Mcguffin, P, Aitchison, KJ, McGuffin, P., GIOVANNINI, CATERINA, Uher, R, Maier, W, Hauser, J, Marusic, A, Schmael, C, Mors, O, Henigsberg, N, Souery, D, Placentino, A, Rietschel, M, Zobel, A, Dmitrzak Weglarz, M, Petrovic, A, Jorgensen, L, Kalember, P, Giovannini, C, Barreto, M, Elkin, A, Landau, S, Farmer, A, Aitchison, K, Mcguffin, P, Aitchison, KJ, McGuffin, P., and GIOVANNINI, CATERINA

Abstract

BACKGROUND: Tricyclic antidepressants and serotonin reuptake inhibitors are considered to be equally effective, but differences may have been obscured by internally inconsistent measurement scales and inefficient statistical analyses. AIMS: To test the hypothesis that escitalopram and nortriptyline differ in their effects on observed mood, cognitive and neurovegetative symptoms of depression. METHOD: In a multicentre part-randomised open-label design (the Genome Based Therapeutic Drugs for Depression (GENDEP) study) 811 adults with moderate to severe unipolar depression were allocated to flexible dosage escitalopram or nortriptyline for 12 weeks. The weekly Montgomery-Asberg Depression Rating Scale, Hamilton Rating Scale for Depression, and Beck Depression Inventory were scored both conventionally and in a more novel way according to dimensions of observed mood, cognitive symptoms and neurovegetative symptoms. RESULTS: Mixed-effect linear regression showed no difference between escitalopram and nortriptyline on the three original scales, but symptom dimensions revealed drug-specific advantages. Observed mood and cognitive symptoms improved more with escitalopram than with nortriptyline. Neurovegetative symptoms improved more with nortriptyline than with escitalopram. CONCLUSIONS: The three symptom dimensions provided sensitive descriptors of differential antidepressant response and enabled identification of drug-specific effects.

Published

2009

18. Genetic predictors of response to antidepressants in the GENDEP project

Author

Uher, R, Huezo Diaz, P, Perroud, N, Smith, R, Rietschel, M, Mors, O, Hauser, J, Maier, W, Kozel, D, Henigsberg, N, Barreto, M, Placentino, A, Dernovsek, M, Schulze, T, Kalember, P, Zobel, A, Czerski, P, Larsen, E, Souery, D, Giovannini, C, Gray, J, Lewis, C, Farmer, A, Aitchison, K, Mcguffin, P, Craig, I, Dernovsek, MZ, Schulze, TG, Czerski, PM, Larsen, ER, Gray, JM, Lewis, CM, Aitchison, KJ, McGuffin, P, Craig, I., GIOVANNINI, CATERINA, Uher, R, Huezo Diaz, P, Perroud, N, Smith, R, Rietschel, M, Mors, O, Hauser, J, Maier, W, Kozel, D, Henigsberg, N, Barreto, M, Placentino, A, Dernovsek, M, Schulze, T, Kalember, P, Zobel, A, Czerski, P, Larsen, E, Souery, D, Giovannini, C, Gray, J, Lewis, C, Farmer, A, Aitchison, K, Mcguffin, P, Craig, I, Dernovsek, MZ, Schulze, TG, Czerski, PM, Larsen, ER, Gray, JM, Lewis, CM, Aitchison, KJ, McGuffin, P, Craig, I., and GIOVANNINI, CATERINA

Abstract

The objective of the Genome-based Therapeutic Drugs for Depression study is to investigate the function of variations in genes encoding key proteins in serotonin, norepinephrine, neurotrophic and glucocorticoid signaling in determining the response to serotonin-reuptake-inhibiting and norepinephrine-reuptake-inhibiting antidepressants. A total of 116 single nucleotide polymorphisms in 10 candidate genes were genotyped in 760 adult patients with moderate-to-severe depression, treated with escitalopram (a serotonin reuptake inhibitor) or nortriptyline (a norepinephrine reuptake inhibitor) for 12 weeks in an open-label part-randomized multicenter study. The effect of genetic variants on change in depressive symptoms was evaluated using mixed linear models. Several variants in a serotonin receptor gene (HTR2A) predicted response to escitalopram with one marker (rs9316233) explaining 1.1% of variance (P=0.0016). Variants in the norepinephrine transporter gene (SLC6A2) predicted response to nortriptyline, and variants in the glucocorticoid receptor gene (NR3C1) predicted response to both antidepressants. Two HTR2A markers remained significant after hypothesis-wide correction for multiple testing. A false discovery rate of 0.106 for the three strongest associations indicated that the multiple findings are unlikely to be false positives. The pattern of associations indicated a degree of specificity with variants in genes encoding proteins in serotonin signaling influencing response to the serotonin-reuptake-inhibiting escitalopram, genes encoding proteins in norepinephrine signaling influencing response to the norepinephrine-reuptake-inhibiting nortriptyline and a common pathway gene influencing response to both antidepressants. The single marker associations explained only a small proportion of variance in response to antidepressants, indicating a need for a multivariate approach to prediction.

Published

2009

19. Adverse reactions to antidepressants

Author

Uher, R, Farmer, A, Henigsberg, N, Rietschel, M, Mors, O, Maier, W, Kozel, D, Hauser, J, Souery, D, Placentino, A, Strohmaier, J, Perroud, N, Zobel, A, Rajewska Rager, A, Dernovsek, M, Larsen, E, Kalember, P, Giovannini, C, Barreto, M, Mcguffin, P, Aitchison, K, Dernovsek, MZ, Larsen, ER, McGuffin, P, Aitchison, KJ, GIOVANNINI, CATERINA, Uher, R, Farmer, A, Henigsberg, N, Rietschel, M, Mors, O, Maier, W, Kozel, D, Hauser, J, Souery, D, Placentino, A, Strohmaier, J, Perroud, N, Zobel, A, Rajewska Rager, A, Dernovsek, M, Larsen, E, Kalember, P, Giovannini, C, Barreto, M, Mcguffin, P, Aitchison, K, Dernovsek, MZ, Larsen, ER, McGuffin, P, Aitchison, KJ, and GIOVANNINI, CATERINA

Abstract

BACKGROUND: Adverse drug reactions are important determinants of non-adherence to antidepressant treatment, but their assessment is complicated by overlap with depressive symptoms and lack of reliable self-report measures. AIMS: To evaluate a simple self-report measure and describe adverse reactions to antidepressants in a large sample. METHOD: The newly developed self-report Antidepressant Side-Effect Checklist and the psychiatrist-rated UKU Side Effect Rating Scale were repeatedly administered to 811 adult participants with depression in a part-randomised multicentre open-label study comparing escitalopram and nortriptyline. RESULTS: There was good agreement between self-report and psychiatrists' ratings. Most complaints listed as adverse reactions in people with depression were more common when they were medication-free rather than during their treatment with antidepressants. Dry mouth (74%), constipation (33%) and weight gain (15%) were associated with nortriptyline treatment. Diarrhoea (9%), insomnia (36%) and yawning (16%) were more common during treatment with escitalopram. Problems with urination and drowsiness predicted discontinuation of nortriptyline. Diarrhoea and decreased appetite predicted discontinuation of escitalopram. CONCLUSIONS: Adverse reactions to antidepressants can be reliably assessed by self-report. Attention to specific adverse reactions may improve adherence to antidepressant treatment.

Published

2009

20. Reply to ‘MDMA can increase cortical levels by 800% in dance clubbers’ Parrott et al.

Author

Wolff, K, primary and Aitchison, KJ, additional

Published

2012

21. Housekeeping gene expression is affected by antidepressant treatment in a mouse fibroblast cell line

Author

Sugden, K., primary, Pariante, CM, additional, McGuffin, P., additional, Aitchison, KJ, additional, and D'Souza, UM, additional

Published

2008

22. A UK consensus on the administration of aripiprazole for the treatment of mania

Author

Aitchison, KJ, primary, Bienroth, M, additional, Cookson, J, additional, Gray, R, additional, Haddad, PM, additional, Moore, B, additional, Ratna, L, additional, Sullivan, G, additional, Taylor, D, additional, Taylor, M, additional, and Goodwin, GM, additional

Published

2008

23. Ecstasy (MDMA)-induced hyponatraemia is associated with genetic variants in CYP2D6 and COMT.

Author

Aitchison KJ, Tsapakis EM, Huezo-Diaz P, Kerwin RW, Forsling ML, and Wolff K

Published

2012

24. Reply to ‘MDMA can increase cortical levels by 800% in dance clubbers’ Parrott et al.

Author

Wolff, K and Aitchison, KJ

Subjects

*LETTERS to the editor, *ECSTASY (Drug), *HYDROCORTISONE

Abstract

A letter to the editor is presented in response to the article "MDMA can increase cortisol levels by 800% in dance clubbers," by A. C. Parrott and colleagues in the 2012 issue.

Published

2013

25. Genetic predictors of response to serotonergic and noradrenergic antidepressants in major depressive disorder: a genome-wide analysis of individual-level data and a meta-analysis.

Author

Tansey KE, Guipponi M, Perroud N, Bondolfi G, Domenici E, Evans D, Hall SK, Hauser J, Henigsberg N, Hu X, Jerman B, Maier W, Mors O, O'Donovan M, Peters TJ, Placentino A, Rietschel M, Souery D, Aitchison KJ, and Craig I

Abstract

Background: It has been suggested that outcomes of antidepressant treatment for major depressive disorder could be significantly improved if treatment choice is informed by genetic data. This study aims to test the hypothesis that common genetic variants can predict response to antidepressants in a clinically meaningful way.Methods and Findings: The NEWMEDS consortium, an academia-industry partnership, assembled a database of over 2,000 European-ancestry individuals with major depressive disorder, prospectively measured treatment outcomes with serotonin reuptake inhibiting or noradrenaline reuptake inhibiting antidepressants and available genetic samples from five studies (three randomized controlled trials, one part-randomized controlled trial, and one treatment cohort study). After quality control, a dataset of 1,790 individuals with high-quality genome-wide genotyping provided adequate power to test the hypotheses that antidepressant response or a clinically significant differential response to the two classes of antidepressants could be predicted from a single common genetic polymorphism. None of the more than half million genetic markers significantly predicted response to antidepressants overall, serotonin reuptake inhibitors, or noradrenaline reuptake inhibitors, or differential response to the two types of antidepressants (genome-wide significance p<5×10(-8)). No biological pathways were significantly overrepresented in the results. No significant associations (genome-wide significance p<5×10(-8)) were detected in a meta-analysis of NEWMEDS and another large sample (STAR*D), with 2,897 individuals in total. Polygenic scoring found no convergence among multiple associations in NEWMEDS and STAR*D.Conclusions: No single common genetic variant was associated with antidepressant response at a clinically relevant level in a European-ancestry cohort. Effects specific to particular antidepressant drugs could not be investigated in the current study. Please see later in the article for the Editors' Summary. [ABSTRACT FROM AUTHOR]

Published

2012

26. Special issue on Pharmacogenetics.

Author

Aitchison KJ and Reynolds GP

Published

2012

27. Optimizing the Prediction of Depression Remission: A Longitudinal Machine Learning Approach.

Author

Carr E, Rietschel M, Mors O, Henigsberg N, Aitchison KJ, Maier W, Uher R, Farmer A, McGuffin P, and Iniesta R

Abstract

Decisions about when to change antidepressant treatment are complex and benefit from accurate prediction of treatment outcome. Prognostic accuracy can be enhanced by incorporating repeated assessments of symptom severity collected during treatment. Participants (n = 714) from the Genome-Based Therapeutic Drugs for Depression study received escitalopram or nortriptyline over 12 weeks. Remission was defined as scoring ≤ 7 on the Hamilton Rating Scale. Predictors included demographic, clinical, and genetic variables (at 0 weeks) and measures of symptom severity (at 0, 2, 4, and 6 weeks). Longitudinal descriptors extracted with growth curves and topological data analysis were used to inform prediction of remission. Repeated assessments produced gradual and drug-specific improvements in predictive performance. By Week 4, models' discrimination in all samples reached levels that might usefully inform treatment decisions (area under the receiver operating curve (AUC) = 0.777 for nortriptyline; AUC = 0.807 for escitalopram; AUC = 0.794 for combined sample). Decisions around switching or modifying treatments for depression can be informed by repeated symptom assessments collected during treatment, but not until 4 weeks after the start of treatment., (© 2024 The Author(s). American Journal of Medical Genetics Part B: Neuropsychiatric Genetics published by Wiley Periodicals LLC.)

Published

2024

28. Features of immunometabolic depression as predictors of antidepressant treatment outcomes: pooled analysis of four clinical trials.

Author

Vreijling SR, Chin Fatt CR, Williams LM, Schatzberg AF, Usherwood T, Nemeroff CB, Rush AJ, Uher R, Aitchison KJ, Köhler-Forsberg O, Rietschel M, Trivedi MH, Jha MK, Penninx BWJH, Beekman ATF, Jansen R, and Lamers F

Subjects

Humans, Selective Serotonin Reuptake Inhibitors pharmacology, Selective Serotonin Reuptake Inhibitors therapeutic use, Treatment Outcome, Depression drug therapy, Antidepressive Agents therapeutic use

Abstract

Background: Profiling patients on a proposed 'immunometabolic depression' (IMD) dimension, described as a cluster of atypical depressive symptoms related to energy regulation and immunometabolic dysregulations, may optimise personalised treatment., Aims: To test the hypothesis that baseline IMD features predict poorer treatment outcomes with antidepressants., Method: Data on 2551 individuals with depression across the iSPOT-D ( n = 967), CO-MED ( n = 665), GENDEP ( n = 773) and EMBARC ( n = 146) clinical trials were used. Predictors included baseline severity of atypical energy-related symptoms (AES), body mass index (BMI) and C-reactive protein levels (CRP, three trials only) separately and aggregated into an IMD index. Mixed models on the primary outcome (change in depressive symptom severity) and logistic regressions on secondary outcomes (response and remission) were conducted for the individual trial data-sets and pooled using random-effects meta-analyses., Results: Although AES severity and BMI did not predict changes in depressive symptom severity, higher baseline CRP predicted smaller reductions in depressive symptoms ( n = 376, β pooled = 0.06, P = 0.049, 95% CI 0.0001-0.12, I 2 = 3.61%); this was also found for an IMD index combining these features ( n = 372, β pooled = 0.12, s.e. = 0.12, P = 0.031, 95% CI 0.01-0.22, I 2 = 23.91%), with a higher - but still small - effect size compared with CRP. Confining analyses to selective serotonin reuptake inhibitor users indicated larger effects of CRP (β pooled = 0.16) and the IMD index (β pooled = 0.20). Baseline IMD features, both separately and combined, did not predict response or remission., Conclusions: Depressive symptoms of people with more IMD features improved less when treated with antidepressants. However, clinical relevance is limited owing to small effect sizes in inconsistent associations. Whether these patients would benefit more from treatments targeting immunometabolic pathways remains to be investigated.

Published

2024

29. Haplotype phasing of CYP2D6: an allelic ratio method using Agena MassARRAY data.

Author

Thamilselvan M, Mather C, Wang Y, Foo JC, and Aitchison KJ

Subjects

Humans, Haplotypes, Genotype, Genetic Testing, Cytochrome P-450 CYP2D6 genetics, DNA Copy Number Variations

Abstract

Pharmacogenomics aims to use the genetic information of an individual to personalize drug prescribing. There is evidence that pharmacogenomic testing before prescription may prevent adverse drug reactions, increase efficacy, and reduce cost of treatment. CYP2D6 is a key pharmacogene of relevance to multiple therapeutic areas. Indeed, there are prescribing guidelines available for medications based on CYP2D6 enzyme activity as deduced from CYP2D6 genetic data. The Agena MassARRAY system is a cost-effective method of detecting genetic variation that has been clinically applied to other genes. However, its clinical application to CYP2D6 has to date been limited by weaknesses such as the inability to determine which haplotype was present in more than one copy for individuals with more than two copies of the CYP2D6 gene. We report application of a new protocol for CYP2D6 haplotype phasing of data generated from the Agena MassARRAY system. For samples with more than two copies of the CYP2D6 gene for which the prior consensus data specified which one was present in more than one copy, our protocol was able to conduct CYP2D6 haplotype phasing resulting in 100% concordance with the prior data. In addition, for three reference samples known to have more than two copies of CYP2D6 but for which the exact number of CYP2D6 genes was unknown, our protocol was able to resolve the number for two out of the three of these, and estimate the likely number for the third. Finally, we demonstrate that our method is applicable to CYP2D6 hybrid tandem configurations., (© 2024. The Author(s).)

Published

2024

30. Dimensions of temperament and character as predictors of antidepressant discontinuation, response and adverse reactions during treatment with nortriptyline and escitalopram.

Author

Köhler-Forsberg O, Keers R, Uher R, Hauser J, Maier W, Rietschel M, McGuffin P, Farmer AE, Aitchison KJ, and Mors O

Subjects

Humans, Escitalopram, Nortriptyline adverse effects, Character, Antidepressive Agents adverse effects, Personality Inventory, Temperament, Depressive Disorder, Major drug therapy

Abstract

Background: Personality traits may predict antidepressant discontinuation and response. However, previous studies were rather small, only explored a few personality traits and did not include adverse drug effects nor the interdependency between antidepressant discontinuation patterns and response., Methods: GENDEP included 589 patients with unipolar moderate-severe depression treated with escitalopram or nortriptyline for 12 weeks. Seven personality dimensions were measured using the self-reported 240-item Temperament and Character Inventory-Revised (TCI-R). We applied Cox proportional models to study discontinuation patterns, logistic and linear regression to investigate response and remission after 8 and 12 weeks, and mixed-effects linear models regarding time-varying treatment response and adverse drug reactions., Results: Low harm avoidance, low cooperativeness, high self-transcendence and high novelty seeking were associated with higher risks for antidepressant discontinuation, independent of depressed mood, adverse drug reactions, drug, sex and age. Regression analyses showed that higher novelty seeking and cooperativeness scores were associated with a greater likelihood of response and remission after 8 and 12 weeks, respectively, but we found no correlations with response in the mixed-effects models. Only high harm avoidance was associated with more self-reported adverse effects., Conclusions: This study, representing the largest investigation between several personality traits and response to two different antidepressants, suggests that correlations between personality traits and antidepressant treatment response may be confounded by differential rates of discontinuation. Future trials on personality in the treatment of depression need to consider this interdependency and study whether interventions aiming at improving compliance for some personality types may improve response to antidepressants.

Published

2023

31. Editorial: Precision psychiatry from a pharmacogenetics perspective.

Author

Brown LC, Allen JD, Eyre HA, Baune BT, Aitchison KJ, and Bousman CA

Abstract

Competing Interests: LB was previously employed by and/or owned stock in Myriad Genetics and Tempus Labs. LB has served as a consultant for the following organizations: IQ Genetix, InnovativeGX, Tempus Labs, Headlamp Health. She is a member of the Clinical Pharmacogenetics Implementation Consortium (CPIC), the Pharmacogene Variation Consortium (PharmVar), the Pharmacogenetics Research Network (PGRN), and the International Society of Psychiatric Genetics (ISPG). JA has served as a consultant for the following organizations: Mobility Health, Nurture Genomics, Precision Genetics, Tempus Labs. HE was previously employed by CNSdose Pty Ltd. BB received speaker honoraria from AstraZeneca, Bristol-Myers Squibb, Janssen, LivaNova, Lundbeck, Novartis, Otsuka, Pfizer, Servier, Wyeth, Biogen, Angelini, and Sumitomo Pharma. KA has received a research grant from Janssen Inc., Canada (fellowship for a trainee), and in-kind research support from Thermo Fisher Scientific, Luminex, Pacific Biosciences of California, and Agena Bioscience. She is a member of the Clinical Pharmacogenetics Implementation Consortium (CPIC), the Pharmacogene Variation Consortium (PharmVar), and the Genetic Testing Committee of the International Society of Psychiatric Genetics (ISPG). CB is founder and CEO of Sequence2Script Inc. LB was employed by Great Scott! Consulting. JA was employed by Medigenics Consulting.

Published

2023

32. Logistic Regression With Machine Learning Sheds Light on the Problematic Sexual Behavior Phenotype.

Author

Jiang S, Wallace K, Yang E, Roper L, Aryal G, Lee D, Lodhi RJ, Arnau R, Isenberg R, Green B, Wishart D, and Aitchison KJ

Subjects

Male, Humans, Logistic Models, Canada, Phenotype, Sexual Behavior, Machine Learning

Abstract

Objectives: There has been a longstanding debate about whether the mechanisms involved in problematic sexual behavior (PSB) are similar to those observed in addictive disorders, or related to impulse control or to compulsivity. The aim of this report was to contribute to this debate by investigating the association between PSB, addictive disorders (internet addiction, compulsive buying), measures associated with the construct known as reward deficiency (RDS), and obsessive-compulsive disorder (OCD)., Methods: A Canadian university Office of the Registrar invited 68,846 eligible students and postdoctoral fellows. Of 4710 expressing interest in participating, 3359 completed online questionnaires, and 1801 completed the Mini-International Neuropsychiatric Interview. PSB was measured by combining those screening positive (score at least 6) on the Sexual Addiction Screening Test-Revised Core with those self-reporting PSB. Current mental health condition(s) and childhood trauma were measured by self-report. OCD was assessed by a combination of self-report and Mini-International Neuropsychiatric Interview data., Results: Of 3341 participants, 407 (12.18%) screened positive on the Sexual Addiction Screening Test-Revised Core. On logistic regression, OCD, attention deficit, internet addiction, a family history of PSB, childhood trauma, compulsive buying, and male gender were associated with PSB. On multiple correspondence analysis, OCD appeared to cluster separately from the other measures, and the pattern of data differed by gender., Conclusions: In our sample, factors that have previously been associated with RDS and OCD are both associated with increased odds of PSB. The factors associated with RDS appear to contribute to a separate data cluster from OCD and to lie closer to PSB., (Copyright © 2022 The Author(s). Published by Wolters Kluwer Health, Inc. on behalf of the American Society of Addiction Medicine.)

Published

2023

33. Corrigendum: Validation of single nucleotide variant assays for human leukocyte antigen haplotypes HLA-B*15:02 and HLA-A*31:01 across diverse ancestral backgrounds.

Author

Buchner A, Hu X, and Aitchison KJ

Abstract

[This corrects the article DOI: 10.3389/fphar.2021.713178.]., (Copyright © 2022 Buchner, Hu and Aitchison.)

Published

2022

34. Identifying the Common Genetic Basis of Antidepressant Response.

Author

Pain O, Hodgson K, Trubetskoy V, Ripke S, Marshe VS, Adams MJ, Byrne EM, Campos AI, Carrillo-Roa T, Cattaneo A, Als TD, Souery D, Dernovsek MZ, Fabbri C, Hayward C, Henigsberg N, Hauser J, Kennedy JL, Lenze EJ, Lewis G, Müller DJ, Martin NG, Mulsant BH, Mors O, Perroud N, Porteous DJ, Rentería ME, Reynolds CF 3rd, Rietschel M, Uher R, Wigmore EM, Maier W, Wray NR, Aitchison KJ, Arolt V, Baune BT, Biernacka JM, Bondolfi G, Domschke K, Kato M, Li QS, Liu YL, Serretti A, Tsai SJ, Turecki G, Weinshilboum R, McIntosh AM, and Lewis CM

Abstract

Background: Antidepressants are a first-line treatment for depression. However, only a third of individuals experience remission after the first treatment. Common genetic variation, in part, likely regulates antidepressant response, yet the success of previous genome-wide association studies has been limited by sample size. This study performs the largest genetic analysis of prospectively assessed antidepressant response in major depressive disorder to gain insight into the underlying biology and enable out-of-sample prediction., Methods: Genome-wide analysis of remission ( n remit  = 1852, n nonremit  = 3299) and percentage improvement ( n  = 5218) was performed. Single nucleotide polymorphism-based heritability was estimated using genome-wide complex trait analysis. Genetic covariance with eight mental health phenotypes was estimated using polygenic scores/AVENGEME. Out-of-sample prediction of antidepressant response polygenic scores was assessed. Gene-level association analysis was performed using MAGMA and transcriptome-wide association study. Tissue, pathway, and drug binding enrichment were estimated using MAGMA., Results: Neither genome-wide association study identified genome-wide significant associations. Single nucleotide polymorphism-based heritability was significantly different from zero for remission ( h 2  = 0.132, SE = 0.056) but not for percentage improvement ( h 2  = -0.018, SE = 0.032). Better antidepressant response was negatively associated with genetic risk for schizophrenia and positively associated with genetic propensity for educational attainment. Leave-one-out validation of antidepressant response polygenic scores demonstrated significant evidence of out-of-sample prediction, though results varied in external cohorts. Gene-based analyses identified ETV4 and DHX8 as significantly associated with antidepressant response., Conclusions: This study demonstrates that antidepressant response is influenced by common genetic variation, has a genetic overlap schizophrenia and educational attainment, and provides a useful resource for future research. Larger sample sizes are required to attain the potential of genetics for understanding and predicting antidepressant response., (© 2021 The Authors.)

Published

2022

35. Correction: Methodology for clinical genotyping of CYP2D6 and CYP2C19.

Author

Henriques BC, Buchner A, Hu X, Wang Y, Yavorskyy V, Wallace K, Dong R, Martens K, Carr MS, Asl BB, Hague J, Sivapalan S, Maier W, Dernovsek MZ, Henigsberg N, Hauser J, Souery D, Cattaneo A, Mors O, Rietschel M, Pfeffer G, Hume S, and Aitchison KJ

Published

2022

36. The feasibility and acceptability of mobile application-based assessment of suicidality using self-report components of a novel tool, the Suicide Ideation and Behavior Assessment Tool (SIBAT).

Author

Chan EC, Wallace K, Yang EH, Roper L, Aryal G, Lodhi RJ, Isenberg R, Carnes P, Baskys A, Green B, and Aitchison KJ

Subjects

Feasibility Studies, Humans, Self Report, Suicidal Ideation, Surveys and Questionnaires, Mobile Applications, Suicide

Abstract

The aim of this study was to assess the validity of a mobile application-based self-report questionnaire in the assessment of suicidality. We developed a program for the administration of self-report components of the Suicide Ideation and Behavior Assessment Tool (SIBAT). We invited university students and trainees enrolled in a study of addictions to complete this component of the SIBAT using the program on their mobile devices or personal computer. 196 participants completed all required modules of the SIBAT, with 97 using their mobile device and 99 using their personal computer. Rates of completed questionnaires between the two groups were compared, as were the responses to the items and the total scores. There was a significant difference between proportions of scale completion in both groups, with a greater number of participants who used a personal computer to complete the scale not responding to all questions compared to participants who used a mobile device to complete the scale. Data collected via mobile device showed good concurrent validity with data collected via personal computer. A trend toward greater disclosure of suicidality was observed in the mobile device group however, replication of these findings using larger sample sizes is needed., (Copyright © 2021. Published by Elsevier B.V.)

Published

2022

37. Decreased Medial Prefrontal Cortex Glutamate Levels in Perimenopausal Women.

Author

Yap S, Luki J, Hanstock CC, Seres P, Shandro T, Hanstock SEC, Lirette A, Zhao HH, Aitchison KJ, and Le Melledo JM

Abstract

Objective: There is an increased risk of experiencing depression during perimenopause (PM), a period of rapidly changing female hormone concentrations. Women at particular risk of developing major depression (MD) during PM are those with history of mood sensitivity to female hormone fluctuations i.e., women with a history of premenstrual dysphoric disorder (PMDD) and/or post-partum depression (PPD). Depressive symptomology has been associated with fluctuations of glutamate (Glu) levels in the medial prefrontal cortex (MPFC) in MD patients as well as PMDD and PPD patients. The objective of the study was to compare MPFC Glu levels in healthy perimenopausal and reproductive-aged (RD) women. Methods: Medial prefrontal cortex Glu levels in healthy perimenopausal ( n = 15) and healthy RD women ( n = 16) were compared via Magnetic Resonance Spectroscopy (MRS) scan using a 3 Tesla (T) magnet. Absence of depressive symptomology and psychiatric comorbidity was confirmed via semi-structured interview. Participants were scanned during the early follicular phase (FP) of the menstrual cycle (MC). Results: Mean MPFC Glu concentrations were decreased in the PM group compared to RD group (PM mean = 0.57 ± 0.03, RD mean = 0.63 ± 0.06, t = -3.84, df = 23.97, p = 0.001). Conclusion: Perimenopause is associated with decreases in MPFC Glu levels. This decrease may be contributing to the increased risk of experiencing depression during PM. Further research should assess MPFC Glu levels in perimenopausal women suffering from MD., Competing Interests: KA declares receipt of two fellowship grants from Janssen Inc., Canada. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2021 Yap, Luki, Hanstock, Seres, Shandro, Hanstock, Lirette, Zhao, Aitchison and Le Melledo.)

Published

2021

38. Methodology for clinical genotyping of CYP2D6 and CYP2C19.

Author

Carvalho Henriques B, Buchner A, Hu X, Wang Y, Yavorskyy V, Wallace K, Dong R, Martens K, Carr MS, Behroozi Asl B, Hague J, Sivapalan S, Maier W, Dernovsek MZ, Henigsberg N, Hauser J, Souery D, Cattaneo A, Mors O, Rietschel M, Pfeffer G, Hume S, and Aitchison KJ

Subjects

Cytochrome P-450 CYP2C19 genetics, Genotype, Genotyping Techniques, Cytochrome P-450 CYP2D6 genetics, Cytochrome P-450 Enzyme System genetics

Abstract

Many antidepressants, atomoxetine, and several antipsychotics are metabolized by the cytochrome P450 enzymes CYP2D6 and CYP2C19, and guidelines for prescribers based on genetic variants exist. Although some laboratories offer such testing, there is no consensus regarding validated methodology for clinical genotyping of CYP2D6 and CYP2C19. The aim of this paper was to cross-validate multiple technologies for genotyping CYP2D6 and CYP2C19 against each other, and to contribute to feasibility for clinical implementation by providing an enhanced range of assay options, customizable automated translation of data into haplotypes, and a workflow algorithm. AmpliChip CYP450 and some TaqMan single nucleotide variant (SNV) and copy number variant (CNV) data in the Genome-based therapeutic drugs for depression (GENDEP) study were used to select 95 samples (out of 853) to represent as broad a range of CYP2D6 and CYP2C19 genotypes as possible. These 95 included a larger range of CYP2D6 hybrid configurations than have previously been reported using inter-technology data. Genotyping techniques employed were: further TaqMan CNV and SNV assays, xTAGv3 Luminex CYP2D6 and CYP2C19, PharmacoScan, the Ion AmpliSeq Pharmacogenomics Panel, and, for samples with CYP2D6 hybrid configurations, long-range polymerase chain reactions (L-PCRs) with Sanger sequencing and Luminex. Agena MassARRAY was also used for CYP2C19. This study has led to the development of a broader range of TaqMan SNV assays, haplotype phasing methodology with TaqMan adaptable for other technologies, a multiplex genotyping method for efficient identification of some hybrid haplotypes, a customizable automated translation of SNV and CNV data into haplotypes, and a clinical workflow algorithm., (© 2021. The Author(s).)

Published

2021

39. Internal consistency and concurrent validity of self-report components of a new instrument for the assessment of suicidality, the Suicide Ideation and Behavior Assessment Tool (SIBAT).

Author

Chan EC, Wallace K, Yang EH, Roper L, Aryal G, Lodhi RJ, Baskys A, Isenberg R, Carnes P, Green B, and Aitchison KJ

Subjects

Humans, Psychiatric Status Rating Scales, Psychometrics, Reproducibility of Results, Self Report, Suicidal Ideation, Suicide, Suicide, Attempted

Abstract

This study aimed to assess the internal consistency of self-report components of the Suicide Ideation and Behavior Assessment Tool (SIBAT) and validate it with relevant elements of the Mini International Neuropsychiatric Interview (MINI). The SIBAT is a newly developed instrument for the evaluation of suicidality. In this study, we invited university students and trainees participating in a study of addictions to complete the self-report component of the SIBAT as an add-on study. We evaluated the internal consistency of the self-report component of the SIBAT and validated it against the suicidality component of the MINI. Data were analysed using both complete case analysis and multiple imputation. SIBAT data were collected for 394 participants, 314 of whom had also completed the MINI. The internal consistency of modules 2, 3, and 5 of the SIBAT was high. Each item from module 5 had a statistically significant association with the corresponding item from the MINI. The sum of scores from modules 2 and 3 had a moderate correlation with the assessment of suicide risk determined by the MINI, and a strong correlation with the total score of SIBAT module 5. The completion median time of modules 2, 3 and 5 was 14.3 min., (Copyright © 2021. Published by Elsevier B.V.)

Published

2021

40. Potential therapeutic benefits of cannabinoid products in adult psychiatric disorders: A systematic review and meta-analysis of randomised controlled trials.

Author

McKee KA, Hmidan A, Crocker CE, Lam RW, Meyer JH, Crockford D, Trépanier A, Aitchison KJ, and Tibbo PG

Subjects

Adult, Anxiety Disorders, Humans, Randomized Controlled Trials as Topic, Attention Deficit Disorder with Hyperactivity, Cannabinoids, Stress Disorders, Post-Traumatic, Tourette Syndrome

Abstract

The utility of cannabinoids and cannabinoid-based products (CBPs) as a pharmacological aid to treat psychiatric disorders in adulthood is still poorly understood despite a number of comprehensive general reviews discussing the topic. With a focus on randomized controlled trial (RCT) data, this review and meta-analysis aimed to aggregate and evaluate all current high-quality (Level-1) research that specifically assessed the effectiveness of a CBP on a diagnosed adult psychiatric disorder. The following databases, from their inception to September 2020, were included in the search: Academic Search Premier, PubMed, Ovid MEDLINE®, Web of Science™, PsycARTICLES, PsycINFO, CINAHL (Nursing and Allied Health), and Scopus. Risk of bias for each study was individually assessed using the revised Cochrane tool. Of the 2397 papers identified, thirty-one RCTs met criteria for inclusion: ten trials focused on treating cannabis use disorder, six on schizophrenia, five on opioid/tobacco use disorder, three on anxiety disorders, two on Tourette's disorder, two on anorexia nervosa, and one trial each for attention-deficit/hyperactivity disorder, posttraumatic stress disorder, and obsessive compulsive disorder. This review finds limited evidence for the effectiveness of CBPs to acutely treat a narrow range of psychiatric symptoms. We report no evidence supporting the mid- to long-range effectiveness of any currently available CBP. In general, quality of the evidence was assessed as low- to moderate. Importantly, none of the studies discussed in this review presently endorse the use of cannabis flower as a method of treatment for any recognized psychiatric disorder. Larger, hypothesis driven RCTs are required prior to making further therapeutic recommendations., (Crown Copyright © 2021. Published by Elsevier Ltd. All rights reserved.)

Published

2021

41. Validation of Single Nucleotide Variant Assays for Human Leukocyte Antigen Haplotypes HLA-B*15:02 and HLA-A*31:01 Across Diverse Ancestral Backgrounds.

Author

Buchner A, Hu X, and Aitchison KJ

Abstract

The human leukocyte antigen haplotypes HLA-B*15:02 and HLA-A*31:01 have been linked to life-threatening adverse drug reactions to the anticonvulsants carbamazepine and oxcarbazepine. Identification of these haplotypes via pharmacogenetic techniques facilitates implementation of precision medicine to prevent such reactions. Using reference samples from diverse ancestral origins, we investigated the test analytical validity (i.e., ability to detect whether or not the haplotypes were present or absent) of TaqMan assays for single nucleotide variants previously identified as potentially being able to "tag" these haplotypes. A TaqMan custom assay for rs10484555 and an inventoried assay for rs17179220 and were able to identify with 100% sensitivity and 100% specificity HLA-B*15:02 and HLA-A*31:01 respectively. A custom assay for rs144012689 that takes into account a neighboring single nucleotide variant with manual calling was also able to identify HLA-B*15:02 with 100% sensitivity and 100% specificity. A custom assay for rs106235 identified HLA-A*31:01 with 100% sensitivity and 95% specificity. The slight reduction in specificity for the latter was owing to another haplotype ( HLA-A*33:03 ) also being detected. While any positive call using the rs106235 assay could therefore be further investigated, as the presence of the HLA-A*31:01 haplotype confers adverse drug reaction risk, the absence of false negatives (indexed by sensitivity) is more important than false positives. In summary, we present validated TaqMan assay methodology for efficient detection of HLA haplotypes HLA-B*15:02 and HLA-A*31:01 . Our data are relevant for other genotyping technologies that identify, or have the potential to identify, these haplotypes using single nucleotide variants., Competing Interests: KA is a member of the Pharmacogene Variation Consortium (PharmVar), a member of the Genetic Testing Committee of the International Society of Psychiatric Genetics, and of the Clinical Pharmacogenetics Implementation Consortium. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2021 Buchner, Hu and Aitchison.)

Published

2021

42. Sequence2Script: A Web-Based Tool for Translation of Pharmacogenetic Data Into Evidence-Based Prescribing Recommendations.

Author

Bousman CA, Wu P, Aitchison KJ, and Cheng T

Abstract

Pharmacogenomic (PGx) testing has emerged as an effective strategy for informing drug selection and dosing. This has led to an increase in the use of PGx testing in the clinic and has catalyzed the emergence of a burgeoning commercial PGx testing industry. However, not all PGx tests are equivalent in their approach to translating testing results into prescribing recommendations, due to an absence of regulatory standards. As such, those generating and using PGx data require tools for ensuring the prescribing recommendations they are provided align with current peer-reviewed PGx-based prescribing guidelines developed by expert groups or approved product labels. Herein, we present Sequence2Script (sequence2script.com), a simple, free, and transparent web-based tool to assist in the efficient translation of PGx testing results into evidence-based prescribing recommendations. The tool was designed with a wide-range of user groups (e.g., healthcare providers, laboratory staff, researchers) in mind. The tool supports 97 gene-drug pairs with evidence-based prescribing guidelines, allows users to adjust recommendations for concomitant inhibitors and inducers, and generates a clinical report summarizing the patient's genotype, inferred phenotype, phenoconverted phenotype (if applicable), and corresponding prescribing recommendations. In this paper, we describe each of the tool's features, provide use case examples, and discuss limitations of and future development plans for the tool. Although we recognize that Sequecnce2Script may not meet the needs of every user, the hope is that this novel tool will facilitate more standardized use of PGx testing results and reduce barriers to implementing these results into practice., Competing Interests: CB reports a grant from Alberta Innovates Strategic Research Project G2018000868, during the conduct of the study; and he has received in-kind testing kits from Myriad Neuroscience, CNSDose, Genomind, and AB-Biotics for research purposes but has not received payments or received any equity, stocks, or options in these companies or any other pharmacogenetic companies. He is a member of the Clinical Pharmacogenetics Implementation Consortium (CPIC) and Pharmacogene Variation Consortium (PharmVar). PW is a freelance/independent life science marketing consultant. KA reports a grant from Alberta Innovates Strategic Research Project G2018000868 during the conduct of the study; un-paid consultancy for HLS Therapeutics, fellowship grants for trainees from Janssen Inc., Canada outside the submitted work; and Member of CPIC and PharmVar; Coauthor, Haplotype Translators for CYP2D6 and CYP2C19. TC was employed by the company Ushiosoft Corporation. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2021 Bousman, Wu, Aitchison and Cheng.)

Published

2021

43. CYP2D6 and Antipsychotic Treatment Outcomes in Children and Youth: A Systematic Review.

Author

Maruf AA, Stein K, Arnold PD, Aitchison KJ, Müller DJ, and Bousman C

Subjects

Adolescent, Child, Humans, Treatment Outcome, Antipsychotic Agents therapeutic use, Cytochrome P-450 CYP2D6 genetics, Drug-Related Side Effects and Adverse Reactions, Pharmacogenetics, Risperidone pharmacokinetics, Risperidone therapeutic use

Abstract

Objective: To systematically review the impact of CYP2D6 genetic variation on antipsychotic pharmacokinetics, efficacy, and adverse drug reactions among children and youth. Method: The published literature was systematically searched in accordance with the Preferred Reporting Items for Systematic Reviews and Meta-Analyses recommendations and critically evaluated using standardized tools and consensus criteria. Results: A total of 20 eligible studies comprising 1078 children and youth were evaluated. The included studies were of fair to moderate quality and included mostly males, individuals of European ancestry, and those treated with risperidone. CYP2D6 poor metabolizers (PMs) were consistently shown to have increased concentrations of risperidone relative to normal metabolizers (NMs). PMs were also consistently shown to have a greater propensity to experience antipsychotic (primarily risperidone) associated adverse drug reactions relative to NMs. However, robust evidence for an association between CYP2D6 and efficacy was less apparent. Conclusion and Clinical Significance: The current knowledge base suggests that CYP2D6 genetic variation has an appreciable impact on antipsychotic pharmacokinetics and the propensity for adverse drug reactions, particularly among children receiving risperidone treatment. However, several limitations with the current literature (e.g., sample sizes, study design, sample heterogeneity) should be addressed in future studies. Assuming that future studies support the link between CYP2D6 genetic variation and antipsychotic outcomes, we would anticipate an increase in the implementation of CYP2D6 -guided antipsychotic drug selection and dose optimization in child and adolescent psychiatric services.

Published

2021

44. Identification of high-impact gene-drug pairs for pharmacogenetic testing in Alberta, Canada.

Author

Fan M, Yarema MC, Box A, Hume S, Aitchison KJ, and Bousman CA

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Alberta, Child, Child, Preschool, Clinical Decision-Making, Drug-Related Side Effects and Adverse Reactions epidemiology, Female, Genotype, Humans, Infant, Infant, Newborn, Male, Middle Aged, Pharmaceutical Preparations, Precision Medicine, Young Adult, Cytochrome P-450 CYP2C19 genetics, Cytochrome P-450 CYP2D6 genetics, Drug-Related Side Effects and Adverse Reactions genetics, Pharmacogenomic Testing

Abstract

Objectives: To facilitate decision-making and priority-setting related to Alberta's Pharmacogenomics (PGx) testing implementation strategy by identifying gene-drug pairs with the highest potential impact on prescribing practices in Alberta., Patients and Methods: Annual drug dispensing data for Alberta from 2012 to 2016 for 57 medications with PGx-based prescribing guidelines were obtained, along with population estimates and demographics (age and ethnicity). Frequencies of actionable PGx genotypes by ethnicity were obtained from the Pharmacogenomics Knowledgebase (PharmGKB). Annual dispensing activity for each of the 57 medications was calculated for the full population (all ages) and children/youth (0-19 years). Alberta ethnicity data were cross-referenced with genetic frequency data for each of the main ethnic groups from PharmGKB to estimate the proportion of individuals with actionable genotypes. Actionable genotype proportions and drug dispensing frequencies were collectively used to identify high impact gene-drug pairs., Results: We found (a) half of the drugs with PGx-based prescribing guidelines, namely, analgesics, proton pump inhibitors, psychotropics, and cardiovascular drugs, were dispensed at high frequencies (>1% of the entire population), (b) the dispensing rate for about one-third of these drugs increased over the 5-year study period, (c) between 1.1 and 45% of recipients of these drugs carried actionable genotypes, and (d) the gene-drug pairs with greatest impact in Alberta predominatly included CYP2C19 or CYP2D6., Conclusions: We uncovered specific patterns in drug dispensing and identified important gene-drug pairs that will inform the planning and development of an evidenced-based PGx testing service in Alberta, Canada. Adaptation of our approach may facilitate the process of evidence-based PGx testing implementation in other jurisdictions., (Copyright © 2021 Wolters Kluwer Health, Inc. All rights reserved.)

Published

2021

45. Are There Therapeutic Benefits of Cannabinoid Products in Adult Mental Illness?

Author

Tibbo PG, McKee KA, Meyer JH, Crocker CE, Aitchison KJ, Lam RW, and Crockford DN

Subjects

Adult, Canada, Humans, Societies, Medical, Cannabinoids, Mental Disorders drug therapy, Psychiatry

Abstract

A position statement developed by the Canadian Psychiatric Association's (CPA) Research Committee and approved by the CPA's Board of Directors on May 13, 2020.

Published

2021

46. Mobile App-Based Self-Report Questionnaires for the Assessment and Monitoring of Bipolar Disorder: Systematic Review.

Author

Chan EC, Sun Y, Aitchison KJ, and Sivapalan S

Abstract

Background: Bipolar disorder is a chronic, progressive illness characterized by recurrent episodes of mania and depression. Self-report scales have historically played a significant role in the monitoring of bipolar symptoms. However, these tools rely on episodic memory, which can be unreliable and do not allow the clinician to monitor brief episodic symptoms or the course of symptoms over shorter periods of time. Mobile app-based questionnaires have been suggested as a tool to improve monitoring of patients with bipolar disorder., Objective: This paper aims to determine the feasibility and validity of mobile app-based self-report questionnaires., Methods: We performed a systematic review of the literature according to the PRISMA (Preferred Reporting Items for Systematic Reviews and Meta-Analyses) guidelines. The PubMed, PsycInfo, Web of Science, Ovid MEDLINE, and EMBASE databases were searched for papers published in English that assessed adherence to and the validity of mobile app-based self-report questionnaires. Relevant studies published from database creation to May 22, 2020, were identified, and results examining the validity of and rates of adherence to app-based self-report questionnaires are reported., Results: A total of 13 records were identified for inclusion in this review. Of these studies, 4 assessed the concurrent validity of mobile app-based self-report tools, with the majority of findings indicating significant associations between data collected using these tools and the Young Mania Rating Scale, Hamilton Depression Rating Scale-17, or Montgomery-Åsberg Depression Rating Scale (P<.001 to P=.24). Three studies comparing the variability or range of symptoms between patients with bipolar disorder and healthy controls suggested that these data are capable of differentiating between known groups. Two studies demonstrated statistically significant associations between data collected via mobile app-based self-report tools and instruments assessing other clinically important factors. Adherence rates varied across the studies examined. However, good adherence rates (>70%) were observed in all but 1 study using a once-daily assessment. There was a wide range of adherence rates observed in studies using twice-daily assessments (42%-95%)., Conclusions: These findings suggest that mobile app-based self-report tools are valid in the assessment of symptoms of mania and depression in euthymic patients with bipolar disorder. Data collected using these tools appear to differ between patients with bipolar disorder and healthy controls and are significantly associated with other clinically important measures. It is unclear at this time whether these tools can be used to detect acute episodes of mania or depression in patients with bipolar disorder. Adherence data indicate that patients with bipolar disorder show good adherence to self-report assessments administered daily for the duration of the study periods evaluated., (©Eric C Chan, Yuting Sun, Katherine J Aitchison, Sudhakar Sivapalan. Originally published in JMIR Formative Research (http://formative.jmir.org), 08.01.2021.)

Published

2021

47. Review and Consensus on Pharmacogenomic Testing in Psychiatry.

Author

Bousman CA, Bengesser SA, Aitchison KJ, Amare AT, Aschauer H, Baune BT, Asl BB, Bishop JR, Burmeister M, Chaumette B, Chen LS, Cordner ZA, Deckert J, Degenhardt F, DeLisi LE, Folkersen L, Kennedy JL, Klein TE, McClay JL, McMahon FJ, Musil R, Saccone NL, Sangkuhl K, Stowe RM, Tan EC, Tiwari AK, Zai CC, Zai G, Zhang J, Gaedigk A, and Müller DJ

Subjects

Anticonvulsants therapeutic use, Cytochrome P-450 CYP2C19 genetics, Cytochrome P-450 CYP2D6 genetics, Dose-Response Relationship, Drug, HLA Antigens genetics, Humans, Pharmacogenomic Testing standards, Practice Guidelines as Topic, Psychiatry standards, Urea Cycle Disorders, Inborn drug therapy, Urea Cycle Disorders, Inborn genetics, Antidepressive Agents therapeutic use, Antipsychotic Agents therapeutic use, Pharmacogenomic Testing methods, Psychiatry methods

Abstract

The implementation of pharmacogenomic (PGx) testing in psychiatry remains modest, in part due to divergent perceptions of the quality and completeness of the evidence base and diverse perspectives on the clinical utility of PGx testing among psychiatrists and other healthcare providers. Recognizing the current lack of consensus within the field, the International Society of Psychiatric Genetics assembled a group of experts to conduct a narrative synthesis of the PGx literature, prescribing guidelines, and product labels related to psychotropic medications as well as the key considerations and limitations related to the use of PGx testing in psychiatry. The group concluded that to inform medication selection and dosing of several commonly-used antidepressant and antipsychotic medications, current published evidence, prescribing guidelines, and product labels support the use of PGx testing for 2 cytochrome P450 genes ( CYP2D6, CYP2C19 ). In addition, the evidence supports testing for human leukocyte antigen genes when using the mood stabilizers carbamazepine ( HLA-A and HLA-B ), oxcarbazepine ( HLA-B ), and phenytoin (CYP2C9, HLA-B). For valproate, screening for variants in certain genes ( POLG, OTC, CSP1 ) is recommended when a mitochondrial disorder or a urea cycle disorder is suspected. Although barriers to implementing PGx testing remain to be fully resolved, the current trajectory of discovery and innovation in the field suggests these barriers will be overcome and testing will become an important tool in psychiatry., Competing Interests: Dr. Bousman reports a grant from Alberta Innovates Strategic Research Project G2018000868, during the conduct of the study; and he has received in-kind testing kits from Myriad Neuroscience, CNSDose, Genomind, and AB-Biotics for research purposes but has not received payments or received any equity, stocks, or options in these companies or any other pharmacogenetic companies. Dr. Bengesser has nothing to disclose. Dr. Aitchison reports grants from Alberta Innovates Strategic Research Project G2018000868, other from Neuroscience and Mental Health Institute, other from Department of Psychiatry, during the conduct of the study; non-financial support from HLS Therapeutics, grants from Janssen Inc., Canada, outside the submitted work; and Member, Pharmacogene Variation Consortium (PharmVar); Coauthor, Haplotype Translators for CYP2D6 and CYP2C19; Member, Alberta Cannabis Research and Innovation Network; Member, Schizophrenia Society of Alberta; Board Member, Canadian Consortium for Early Intervention in Psychosis. Dr. Amare has nothing to disclose. Dr. Aschauer has nothing to disclose. Dr. Baune has nothing to disclose. Ms. Behroozi Asl reports grants from Alberta Innovates, during the conduct of the study. Dr. Bishop reports personal fees from OptumRx, outside the submitted work; and he is a member of the Clinical Pharmacogenetics Implementation Consortium. Dr. Burmeister reports personal fees from Chinese University of Hong Kong (Shen Zhen), personal fees from Research Grants Council (RGC) of Hong Kong, personal fees from Alexander von Humboldt Foundation, outside the submitted work. Dr. Chaumette reports personal fees from Janssen-Cilag, grants from Fondation Bettencourt-Schueller, outside the submitted work. Dr. Chen has nothing to disclose. Dr. Cordner has nothing to disclose. Dr. Deckert reports grants from DFG, grants from BMBF, grants from Vogel-Foundation, grants from EU, grants from Bavarian Secretary of Commerce, outside the submitted work. Dr. Degenhardt has nothing to disclose. Dr. DeLisi has nothing to disclose. Dr. Folkersen has nothing to disclose. Dr. Kennedy has a patent 'PGx of Antipsychotic Response'; and 'PGx of Wt Gain' both pending. No licensees. Dr. Kennedy's affiliated hospital, (which is not his employer) the Centre for Addiction and Mental Health, is a part owner of the Canadian subsidiary of Myriad Neuroscience, USA. Dr. Klein reports grants from NIH/NHGRI, during the conduct of the study. Dr. McClay has nothing to disclose. Dr. McMahon has nothing to disclose. Dr. Musil reports personal fees from Otsuka/Lundbeck, outside the submitted work. Dr. Saccone reports that her spouse is listed as an inventor on Issued U.S. Patent 8,080,371, “Markers for Addiction” covering the use of certain single nucleotide polymorphisms in determining the diagnosis, prognosis, and treatment of addiction. Dr. Sangkuhl reports grants from NIH/NHGRI, during the conduct of the study. Dr. Stowe has nothing to disclose. Dr. Tan has nothing to disclose. Dr. Tiwari reports that he is a co-investigator on two pharmacogenetic studies where genetic test kits were provided as in-kind contribution by Assurex Health (Myriad Neuroscience) but he did not receive any payments or any equity, stocks, or options from this company or any other pharmacogenetic companies. Dr. Tiwari is also a co-inventor on a patent assessing risk for antipsychotic-induced weight gain. Dr. C. Zai has a patent for suicide markers issued, and a patent for antipsychotic-induced weight gain markers pending. Dr. G. Zai has nothing to disclose. Dr. Zhang has nothing to disclose. Dr. Gaedigk has nothing to disclose. Dr. Müller reports to be a co-investigator on two pharmacogenetic studies where genetic test kits were provided as in-kind contribution by Myriad Neuroscience. He did not receive any payments or any equity, stocks, or options from any pharmacogenetic companies. Dr. Müller is also a co-inventor on two patent assessing risk for antipsychotic-induced weight gain (pending)., (Thieme. All rights reserved.)

Published

2021

48. How Can Drug Metabolism and Transporter Genetics Inform Psychotropic Prescribing?

Author

Carvalho Henriques B, Yang EH, Lapetina D, Carr MS, Yavorskyy V, Hague J, and Aitchison KJ

Abstract

Many genetic variants in drug metabolizing enzymes and transporters have been shown to be relevant for treating psychiatric disorders. Associations are strong enough to feature on drug labels and for prescribing guidelines based on such data. A range of commercial tests are available; however, there is variability in included genetic variants, methodology, and interpretation. We herein provide relevant background for understanding clinical associations with specific variants, other factors that are relevant to consider when interpreting such data (such as age, gender, drug-drug interactions), and summarize the data relevant to clinical utility of pharmacogenetic testing in psychiatry and the available prescribing guidelines. We also highlight areas for future research focus in this field., Competing Interests: KA is a member of the Pharmacogene Variation Consortium, Clinical Pharmacogenetics Implementation Consortium, has received two research grants in the last two years from Janssen Inc., Canada (fellowship grants for trainees) and provided consultancy services (unpaid) for HLS Therapeutics. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2020 Carvalho Henriques, Yang, Lapetina, Carr, Yavorskyy, Hague and Aitchison.)

Published

2020

49. Pharmacogenetic Testing Options Relevant to Psychiatry in Canada: Options de tests pharmacogénétiques pertinents en psychiatrie au Canada.

Author

Maruf AA, Fan M, Arnold PD, Müller DJ, Aitchison KJ, and Bousman CA

Subjects

Canada, Genotype, Humans, Mental Disorders genetics, Pharmacogenetics, Antidepressive Agents therapeutic use, Mental Disorders drug therapy, Pharmacogenomic Testing, Psychiatry

Abstract

Objective: To identify and assess pharmacogenetic testing options relevant to psychiatry in Canada., Method: Searches of published literature, websites, and Standard Council of Canada's Laboratory Directory were conducted to identify pharmacogenetic tests available in Canada. Identified tests were assessed on 8 key questions related to analytical validity, accessibility, test ordering, delivery of test results, turnaround time, cost, clinical trial evidence, and gene/allele content., Results: A total of 13 pharmacogenetic tests relevant to psychiatry in Canada were identified. All tests were highly accessible, and most were conducted in accredited laboratories. Both direct-to-consumer and clinician-gated testing were identified, with turnaround times and cost ranging from 2 to 40 days and CAD$199 to CAD$2310, respectively. Two tests were supported by randomized controlled trials. All tests met minimum gene and allele panel recommendations for psychiatry, but no 2 panels were identical. No test was unequivocally superior to all other tests., Conclusions: Pharmacogenetic testing in Canada is readily available but highly variable in terms of ordering procedures, delivery of results, turnaround times, cost, and gene/allele content. As such, it is important for psychiatrists and other health-care providers to understand the differences between the available tests to ensure appropriate selection and implementation within their practice.

Published

2020

50. A functional variant in the serotonin receptor 7 gene (HTR7), rs7905446, is associated with good response to SSRIs in bipolar and unipolar depression.

Author

Wei YB, McCarthy M, Ren H, Carrillo-Roa T, Shekhtman T, DeModena A, Liu JJ, Leckband SG, Mors O, Rietschel M, Henigsberg N, Cattaneo A, Binder EB, Aitchison KJ, and Kelsoe JR

Subjects

Adult, Aged, Aged, 80 and over, Animals, Citalopram therapeutic use, Female, Fluoxetine therapeutic use, Humans, Male, Middle Aged, Paroxetine therapeutic use, Retrospective Studies, Selective Serotonin Reuptake Inhibitors pharmacology, Sertraline therapeutic use, Young Adult, Depressive Disorder, Major drug therapy, Depressive Disorder, Major genetics, Receptors, Serotonin genetics, Selective Serotonin Reuptake Inhibitors therapeutic use

Abstract

Predicting antidepressant response has been a clinical challenge for mood disorder. Although several genome-wide association studies have suggested a number of genetic variants to be associated with antidepressant response, the sample sizes are small and the results are difficult to replicate. Previous animal studies have shown that knockout of the serotonin receptor 7 gene (HTR7) resulted in an antidepressant-like phenotype, suggesting it was important to antidepressant action. In this report, in the first stage, we used a cost-effective pooled-sequencing strategy to sequence the entire HTR7 gene and its regulatory regions to investigate the association of common variants in HTR7 and clinical response to four selective serotonin reuptake inhibitors (SSRIs: citalopram, paroxetine, fluoxetine and sertraline) in a retrospective cohort mainly consisting of subjects with bipolar disorder (n = 359). We found 80 single-nucleotide polymorphisms (SNPs) with false discovery rate < 0.05 associated with response to paroxetine. Among the significant SNPs, rs7905446 (T/G), which is located at the promoter region, also showed nominal significance (P < 0.05) in fluoxetine group. GG/TG genotypes for rs7905446 and female gender were associated with better response to two SSRIs (paroxetine and fluoxetine). In the second stage, we replicated this association in two independent prospective samples of SSRI-treated patients with major depressive disorder: the MARS (n = 253, P = 0.0169) and GENDEP studies (n = 432, P = 0.008). The GG/TG genotypes were consistently associated with response in all three samples. Functional study of rs7905446 showed greater activity of the G allele in regulating expression of HTR7. The G allele displayed higher luciferase activity in two neuronal-related cell lines, and estrogen treatment decreased the activity of only the G allele. Electrophoretic mobility shift assay suggested that the G allele interacted with CCAAT/enhancer-binding protein beta transcription factor (TF), while the T allele did not show any interaction with any TFs. Our results provided novel pharmacogenomic evidence to support the role of HTR7 in association with antidepressant response.

Published

2020