Abstract
Current prescribing practices for major depressive disorder (MDD) produce limited treatment success. Although pharmacogenomics may improve outcomes by identifying genetically inappropriate medications, studies to date were limited in scope. Outpatients (N = 1167) diagnosed with MDD and with a patient- or clinician-reported inadequate response to at least one antidepressant were enrolled in the Genomics Used to Improve DEpression Decisions (GUIDED) trial – a rater- and patient-blind randomized controlled trial. Patients were randomized to treatment as usual (TAU) or a pharmacogenomics-guided intervention arm in which clinicians had access to a pharmacogenomic test report to inform medication selections (guided-care). Medications were considered congruent (‘use as directed’ or ‘use with caution’ test categories) or incongruent (‘use with increased caution and with more frequent monitoring’ test category) with test results. Unblinding occurred after week 8. Primary outcome was symptom improvement [change in 17-item Hamilton Depression Rating Scale (HAM-D17)] at week 8; secondary outcomes were response (≥50% decrease in HAM-D17) and remission (HAM-D17 ≤ 7) at week 8. At week 8, symptom improvement for guided-care was not significantly different than TAU (27.2% versus 24.4%, p = 0.107); however, improvements in response (26.0% versus 19.9%, p = 0.013) and remission (15.3% versus 10.1%, p = 0.007) were statistically significant. Patients taking incongruent medications prior to baseline who switched to congruent medications by week 8 experienced greater symptom improvement (33.5% versus 21.1%, p = 0.002), response (28.5% versus 16.7%, p = 0.036), and remission (21.5% versus 8.5%, p = 0.007) compared to those remaining incongruent. Pharmacogenomic testing did not significantly improve mean symptoms but did significantly improve response and remission rates for difficult-to-treat depression patients over standard of care (ClinicalTrials.gov NCT02109939).
| Original language | English |
|---|---|
| Pages (from-to) | 59-67 |
| Number of pages | 9 |
| Journal | Journal of Psychiatric Research |
| Volume | 111 |
| DOIs | |
| State | Published - Apr 2019 |
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Impact of pharmacogenomics on clinical outcomes in major depressive disorder in the GUIDED trial : A large, patient- and rater-blinded, randomized, controlled study. / Greden, John F.; Parikh, Sagar V.; Rothschild, Anthony J.; Thase, Michael E.; Dunlop, Boadie W.; DeBattista, Charles; Conway, Charles R.; Forester, Brent P.; Mondimore, Francis M.; Shelton, Richard C.; Macaluso, Matthew; Li, James; Brown, Krystal; Gilbert, Alexa; Burns, Lindsey; Jablonski, Michael R.; Dechairo, Bryan.
In: Journal of Psychiatric Research, Vol. 111, 04.2019, p. 59-67.Research output: Contribution to journal › Article › peer-review
TY - JOUR
T1 - Impact of pharmacogenomics on clinical outcomes in major depressive disorder in the GUIDED trial
T2 - A large, patient- and rater-blinded, randomized, controlled study
AU - Greden, John F.
AU - Parikh, Sagar V.
AU - Rothschild, Anthony J.
AU - Thase, Michael E.
AU - Dunlop, Boadie W.
AU - DeBattista, Charles
AU - Conway, Charles R.
AU - Forester, Brent P.
AU - Mondimore, Francis M.
AU - Shelton, Richard C.
AU - Macaluso, Matthew
AU - Li, James
AU - Brown, Krystal
AU - Gilbert, Alexa
AU - Burns, Lindsey
AU - Jablonski, Michael R.
AU - Dechairo, Bryan
N1 - Funding Information: JF Greden has been a Scientific Advisor for Janssen Pharmaceutical, Naurex (Allergan) Pharmaceutical, Cerecor Pharmaceutical, NeuralStem, Sage Therapeutics and Genomind; he received reimbursement as a speaker for Assurex Health in 2014. All work done as an unpaid consultant to Assurex and Myriad; he has never been employed by either. S Parikh has received research funding from the Ontario Brain Institute , the Canadian Institutes of Health Research , the James and Ethel Flinn Foundation , and is a paid consultant for Assurex Health; honoraria from Mensante Corporation, Takeda, and the Canadian Network for Mood and Anxiety Treatments (CANMAT); and has equity in Mensante. AJ Rothschild has received research support from Allergan , AssureRx , Janssen , the National Institute of Mental Health , Takeda , Eli-Lilly , and Pfizer , is a consultant to Alkermes, Eli Lilly and Company, GlaxoSmithKline, Myriad Genetics, Pfizer, Sage Therapeutics, and Sanofi-Aventis, and has received royalties for the Rothschild Scale for Antidepressant Tachyphylaxis (RSAT) ® ; Clinical Manual for the Diagnosis and Treatment of Psychotic Depression, American Psychiatric Press, 2009; The Evidence-Based Guide to Antipsychotic Medications, American Psychiatric Press, 2010; The Evidence-Based Guide to Antidepressant Medications, American Psychiatric Press, 2012, and UpToDate ® . M Thase received research funding from Assurex Health , Acadia , Agency for Healthcare Research and Quality , Alkermes , Avanir , Forest , Intracellular , Janssen , National Institute of Mental Health , Otsuka , Patient-Centered Outcomes Research Institute , Takeda , has served as a consultant for Acadia, Akilii, Alkermes, Allergan (Forest, Naurex), AstraZeneca, Cerecor, Eli Lilly, Fabre-Kramer, Gerson Lehrman Group, Guidepoint Global, Johnson & Johnson (Janssen, Ortho-McNeil), Lundbeck, MedAvante, Merck, Moksha8, Nestlé (PamLab), Novartis, Otsuka, Pfizer, Shire, Sunovion, Takeda, and has received royalties from American Psychiatric Press, Guilford Publications, Herald House, W.W. Norton & Company, Inc. BW Dunlop has received research support from Acadia , Assurex Health , Axsome , Janssen , and Takeda . C DeBattista has received research support from Assurex Health and Brain Resources . CR Conway has received research support from LivaNova and Bristol-Myers Squibb , the Stanley Medical Research Institute , the National Institute of Mental Health , NeoSync Inc , The Taylor Family Institute for Innovative Psychiatric Research, The August Busch IV Foundation, and the Barnes-Jewish Hospital Foundation; received speaking fees from Bristol-Myers Squibb and Otsuka Pharmaceuticals; serves as a research design consultant to LivaNova; and is a part time employee of the John Cochran Veterans Administration Hospital in St. Louis. BP Forester has received research funding from the National Institutes of Health , Rogers Family Foundation , Assurex Health , Eli Lilly , Biogen , and Roche and has served as a consultant for Eli Lilly and INSYS Therapeutics. F Mondimore received research funding from Assurex Health . R Shelton has served as a consultant for Acadia Pharmaceuticals, Allergan Inc., Cerecor, Inc., Janssen Pharmaceutica, Lundbeck A/S, Takeda Pharmaceuticals and received grant funding from Acadia Pharmaceuticals , Alkermes, Inc ., Allergan ., Assurex Health , Avanir Pharmaceuticals , Cerecor, Inc ., Genomind , Intracellular Therapies , Janssen Pharmaceutica , Otsuka Pharmaceuticals , and Takeda Pharmaceuticals . M Macalusco has conducted clinical trials research as principal investigator for Acadia, Alkermes, Allergan, Assurex Health, Eisai, Lundbeck, Janssen, Naurex/Aptinyx, and Neurim; all study contracts and payments were made to Kansas University Medical Cancer Research Institute. J Li, A Gilbert, L Burns, M Jablonski, and B Dechairo were employed by Assurex Health, Inc. at the time of this study. Funding Information: JF Greden has been a Scientific Advisor for Janssen Pharmaceutical, Naurex (Allergan) Pharmaceutical, Cerecor Pharmaceutical, NeuralStem, Sage Therapeutics and Genomind; he received reimbursement as a speaker for Assurex Health in 2014. All work done as an unpaid consultant to Assurex and Myriad; he has never been employed by either. S Parikh has received research funding from the Ontario Brain Institute, the Canadian Institutes of Health Research, the James and Ethel Flinn Foundation, and is a paid consultant for Assurex Health; honoraria from Mensante Corporation, Takeda, and the Canadian Network for Mood and Anxiety Treatments (CANMAT); and has equity in Mensante. AJ Rothschild has received research support from Allergan, AssureRx, Janssen, the National Institute of Mental Health, Takeda, Eli-Lilly, and Pfizer, is a consultant to Alkermes, Eli Lilly and Company, GlaxoSmithKline, Myriad Genetics, Pfizer, Sage Therapeutics, and Sanofi-Aventis, and has received royalties for the Rothschild Scale for Antidepressant Tachyphylaxis (RSAT)®; Clinical Manual for the Diagnosis and Treatment of Psychotic Depression, American Psychiatric Press, 2009; The Evidence-Based Guide to Antipsychotic Medications, American Psychiatric Press, 2010; The Evidence-Based Guide to Antidepressant Medications, American Psychiatric Press, 2012, and UpToDate®. M Thase received research funding from Assurex Health, Acadia, Agency for Healthcare Research and Quality, Alkermes, Avanir, Forest, Intracellular, Janssen, National Institute of Mental Health, Otsuka, Patient-Centered Outcomes Research Institute, Takeda, has served as a consultant for Acadia, Akilii, Alkermes, Allergan (Forest, Naurex), AstraZeneca, Cerecor, Eli Lilly, Fabre-Kramer, Gerson Lehrman Group, Guidepoint Global, Johnson & Johnson (Janssen, Ortho-McNeil), Lundbeck, MedAvante, Merck, Moksha8, Nestlé (PamLab), Novartis, Otsuka, Pfizer, Shire, Sunovion, Takeda, and has received royalties from American Psychiatric Press, Guilford Publications, Herald House, W.W. Norton & Company, Inc. BW Dunlop has received research support from Acadia, Assurex Health, Axsome, Janssen, and Takeda. C DeBattista has received research support from Assurex Health and Brain Resources. CR Conway has received research support from LivaNova and Bristol-Myers Squibb, the Stanley Medical Research Institute, the National Institute of Mental Health, NeoSync Inc, The Taylor Family Institute for Innovative Psychiatric Research, The August Busch IV Foundation, and the Barnes-Jewish Hospital Foundation; received speaking fees from Bristol-Myers Squibb and Otsuka Pharmaceuticals; serves as a research design consultant to LivaNova; and is a part time employee of the John Cochran Veterans Administration Hospital in St. Louis. BP Forester has received research funding from the National Institutes of Health, Rogers Family Foundation, Assurex Health, Eli Lilly, Biogen, and Roche and has served as a consultant for Eli Lilly and INSYS Therapeutics. F Mondimore received research funding from Assurex Health. R Shelton has served as a consultant for Acadia Pharmaceuticals, Allergan Inc., Cerecor, Inc., Janssen Pharmaceutica, Lundbeck A/S, Takeda Pharmaceuticals and received grant funding from Acadia Pharmaceuticals, Alkermes, Inc., Allergan., Assurex Health, Avanir Pharmaceuticals, Cerecor, Inc., Genomind, Intracellular Therapies, Janssen Pharmaceutica, Otsuka Pharmaceuticals, and Takeda Pharmaceuticals. M Macalusco has conducted clinical trials research as principal investigator for Acadia, Alkermes, Allergan, Assurex Health, Eisai, Lundbeck, Janssen, Naurex/Aptinyx, and Neurim; all study contracts and payments were made to Kansas University Medical Cancer Research Institute. J Li, A Gilbert, L Burns, M Jablonski, and B Dechairo were employed by Assurex Health, Inc. at the time of this study. Publisher Copyright: © 2019
PY - 2019/4
Y1 - 2019/4
N2 - Current prescribing practices for major depressive disorder (MDD) produce limited treatment success. Although pharmacogenomics may improve outcomes by identifying genetically inappropriate medications, studies to date were limited in scope. Outpatients (N = 1167) diagnosed with MDD and with a patient- or clinician-reported inadequate response to at least one antidepressant were enrolled in the Genomics Used to Improve DEpression Decisions (GUIDED) trial – a rater- and patient-blind randomized controlled trial. Patients were randomized to treatment as usual (TAU) or a pharmacogenomics-guided intervention arm in which clinicians had access to a pharmacogenomic test report to inform medication selections (guided-care). Medications were considered congruent (‘use as directed’ or ‘use with caution’ test categories) or incongruent (‘use with increased caution and with more frequent monitoring’ test category) with test results. Unblinding occurred after week 8. Primary outcome was symptom improvement [change in 17-item Hamilton Depression Rating Scale (HAM-D17)] at week 8; secondary outcomes were response (≥50% decrease in HAM-D17) and remission (HAM-D17 ≤ 7) at week 8. At week 8, symptom improvement for guided-care was not significantly different than TAU (27.2% versus 24.4%, p = 0.107); however, improvements in response (26.0% versus 19.9%, p = 0.013) and remission (15.3% versus 10.1%, p = 0.007) were statistically significant. Patients taking incongruent medications prior to baseline who switched to congruent medications by week 8 experienced greater symptom improvement (33.5% versus 21.1%, p = 0.002), response (28.5% versus 16.7%, p = 0.036), and remission (21.5% versus 8.5%, p = 0.007) compared to those remaining incongruent. Pharmacogenomic testing did not significantly improve mean symptoms but did significantly improve response and remission rates for difficult-to-treat depression patients over standard of care (ClinicalTrials.gov NCT02109939).
AB - Current prescribing practices for major depressive disorder (MDD) produce limited treatment success. Although pharmacogenomics may improve outcomes by identifying genetically inappropriate medications, studies to date were limited in scope. Outpatients (N = 1167) diagnosed with MDD and with a patient- or clinician-reported inadequate response to at least one antidepressant were enrolled in the Genomics Used to Improve DEpression Decisions (GUIDED) trial – a rater- and patient-blind randomized controlled trial. Patients were randomized to treatment as usual (TAU) or a pharmacogenomics-guided intervention arm in which clinicians had access to a pharmacogenomic test report to inform medication selections (guided-care). Medications were considered congruent (‘use as directed’ or ‘use with caution’ test categories) or incongruent (‘use with increased caution and with more frequent monitoring’ test category) with test results. Unblinding occurred after week 8. Primary outcome was symptom improvement [change in 17-item Hamilton Depression Rating Scale (HAM-D17)] at week 8; secondary outcomes were response (≥50% decrease in HAM-D17) and remission (HAM-D17 ≤ 7) at week 8. At week 8, symptom improvement for guided-care was not significantly different than TAU (27.2% versus 24.4%, p = 0.107); however, improvements in response (26.0% versus 19.9%, p = 0.013) and remission (15.3% versus 10.1%, p = 0.007) were statistically significant. Patients taking incongruent medications prior to baseline who switched to congruent medications by week 8 experienced greater symptom improvement (33.5% versus 21.1%, p = 0.002), response (28.5% versus 16.7%, p = 0.036), and remission (21.5% versus 8.5%, p = 0.007) compared to those remaining incongruent. Pharmacogenomic testing did not significantly improve mean symptoms but did significantly improve response and remission rates for difficult-to-treat depression patients over standard of care (ClinicalTrials.gov NCT02109939).
UR - http://www.scopus.com/inward/record.url?scp=85060922730&partnerID=8YFLogxK
U2 - 10.1016/j.jpsychires.2019.01.003
DO - 10.1016/j.jpsychires.2019.01.003
M3 - Article
C2 - 30677646
AN - SCOPUS:85060922730
VL - 111
SP - 59
EP - 67
JO - Journal of Psychiatric Research
JF - Journal of Psychiatric Research
SN - 0022-3956
ER -