An electroencephalographic signature predicts antidepressant response in major depression

Wei Wu; Yu Zhang; Jing Jiang; Molly Lucas; Gregory A. Fonzo; Camarin E. Rolle; Crystal Cooper; Cherise Chin-Fatt; Noralie Krepel; Carena A. Cornelssen; Rachael Wright; Russell T. Toll; Hersh M. Trivedi; Karen Monuszko; Trevor L. Caudle; Kamron Sarhadi; Manish K. Jha; Joseph M. Trombello; Thilo Deckersbach; Phil Adams; Patrick J. McGrath; Myrna M. Weissman; Maurizio Fava; Diego A. Pizzagalli; Martijn Arns; Madhukar H. Trivedi; Amit Etkin

doi:10.1038/s41587-019-0397-3

An electroencephalographic signature predicts antidepressant response in major depression

Wei Wu, Yu Zhang, Jing Jiang, Molly Lucas, Gregory A. Fonzo, Camarin E. Rolle, Crystal Cooper, Cherise Chin-Fatt, Noralie Krepel, Carena A. Cornelssen, Rachael Wright, Russell T. Toll, Hersh M. Trivedi, Karen Monuszko, Trevor L. Caudle, Kamron Sarhadi, Manish K. Jha, Joseph M. Trombello, Thilo Deckersbach, Phil AdamsPatrick J. McGrath, Myrna M. Weissman, Maurizio Fava, Diego A. Pizzagalli, Martijn Arns, Madhukar H. Trivedi, Amit Etkin^*

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

Antidepressants are widely prescribed, but their efficacy relative to placebo is modest, in part because the clinical diagnosis of major depression encompasses biologically heterogeneous conditions. Here, we sought to identify a neurobiological signature of response to antidepressant treatment as compared to placebo. We designed a latent-space machine-learning algorithm tailored for resting-state electroencephalography (EEG) and applied it to data from the largest imaging-coupled, placebo-controlled antidepressant study (n = 309). Symptom improvement was robustly predicted in a manner both specific for the antidepressant sertraline (versus placebo) and generalizable across different study sites and EEG equipment. This sertraline-predictive EEG signature generalized to two depression samples, wherein it reflected general antidepressant medication responsivity and related differentially to a repetitive transcranial magnetic stimulation treatment outcome. Furthermore, we found that the sertraline resting-state EEG signature indexed prefrontal neural responsivity, as measured by concurrent transcranial magnetic stimulation and EEG. Our findings advance the neurobiological understanding of antidepressant treatment through an EEG-tailored computational model and provide a clinical avenue for personalized treatment of depression.

Original language	English
Pages (from-to)	439-447
Number of pages	15
Journal	Nature Biotechnology
Volume	38
Issue number	4
Early online date	10 Feb 2020
DOIs	https://doi.org/10.1038/s41587-019-0397-3
Publication status	Published - Apr 2020

Keywords

TRANSCRANIAL MAGNETIC STIMULATION
SINGLE-TRIAL EEG
BRAIN-FUNCTION
OSCILLATIONS
MECHANISMS
MODERATORS
BIOMARKERS
CONFLICT
NETWORKS
OUTCOMES

Access to Document

10.1038/s41587-019-0397-3

Cite this

Wu, W., Zhang, Y., Jiang, J., Lucas, M., Fonzo, G. A., Rolle, C. E., Cooper, C., Chin-Fatt, C., Krepel, N., Cornelssen, C. A., Wright, R., Toll, R. T., Trivedi, H. M., Monuszko, K., Caudle, T. L., Sarhadi, K., Jha, M. K., Trombello, J. M., Deckersbach, T., ... Etkin, A. (2020). An electroencephalographic signature predicts antidepressant response in major depression. Nature Biotechnology, 38(4), 439-447. https://doi.org/10.1038/s41587-019-0397-3

@article{81deb559b3de4f6fa490e68876320d6f,

title = "An electroencephalographic signature predicts antidepressant response in major depression",

abstract = "Antidepressants are widely prescribed, but their efficacy relative to placebo is modest, in part because the clinical diagnosis of major depression encompasses biologically heterogeneous conditions. Here, we sought to identify a neurobiological signature of response to antidepressant treatment as compared to placebo. We designed a latent-space machine-learning algorithm tailored for resting-state electroencephalography (EEG) and applied it to data from the largest imaging-coupled, placebo-controlled antidepressant study (n = 309). Symptom improvement was robustly predicted in a manner both specific for the antidepressant sertraline (versus placebo) and generalizable across different study sites and EEG equipment. This sertraline-predictive EEG signature generalized to two depression samples, wherein it reflected general antidepressant medication responsivity and related differentially to a repetitive transcranial magnetic stimulation treatment outcome. Furthermore, we found that the sertraline resting-state EEG signature indexed prefrontal neural responsivity, as measured by concurrent transcranial magnetic stimulation and EEG. Our findings advance the neurobiological understanding of antidepressant treatment through an EEG-tailored computational model and provide a clinical avenue for personalized treatment of depression.",

keywords = "TRANSCRANIAL MAGNETIC STIMULATION, SINGLE-TRIAL EEG, BRAIN-FUNCTION, OSCILLATIONS, MECHANISMS, MODERATORS, BIOMARKERS, CONFLICT, NETWORKS, OUTCOMES",

author = "Wei Wu and Yu Zhang and Jing Jiang and Molly Lucas and Fonzo, {Gregory A.} and Rolle, {Camarin E.} and Crystal Cooper and Cherise Chin-Fatt and Noralie Krepel and Cornelssen, {Carena A.} and Rachael Wright and Toll, {Russell T.} and Trivedi, {Hersh M.} and Karen Monuszko and Caudle, {Trevor L.} and Kamron Sarhadi and Jha, {Manish K.} and Trombello, {Joseph M.} and Thilo Deckersbach and Phil Adams and McGrath, {Patrick J.} and Weissman, {Myrna M.} and Maurizio Fava and Pizzagalli, {Diego A.} and Martijn Arns and Trivedi, {Madhukar H.} and Amit Etkin",

note = "Funding Information: A.E. (lifetime disclosure) has been receiving salary and equity from Alto Neuroscience since 1 November 2019, to which the pending patent for SELSER has been licensed from Stanford. He holds equity in Mindstrong Health, Akili Interactive and Sizung for unrelated work, has received research funding from the National Institute of Mental Health, Department of Veterans Affairs, Cohen Veterans Bioscience, Brain and Behavior Research Foundation, Dana Foundation, Brain Resource Inc. and the Stanford Neurosciences Institute and consulted for Cervel, Takaeda, Posit Science, Acadia, Otsuka, Lundbeck and Janssen. Over the past 3 years, D.A.P. has received consulting fees from Alkermes, BlackThorn Therapeutics, Boehreinger Ingelheim, Posit Science and Takeda Pharmaceuticals. He has received funding from NIMH, the Dana Foundation and Brain and Behavior Research Foundation. T.D.{\textquoteright}s research has been funded by NIH, NIMH, National Alliance for Research on Schizophrenia & Depression, TSA, IOCDF, Tufts University, DBDAT and Otsuka Pharmaceuticals. He has received honoraria, consultation fees and/or royalties from the MGH Psychiatry Academy, BrainCells Inc., Clintara, LLC, Inc., Systems Research and Applications Corporation, Boston University, the Catalan Agency for Health Technology Assessment and Research, the National Association of Social Workers Massachusetts, the Massachusetts Medical Society, Tufts University, National Institute of Drug Abuse, NIMH, Oxford University Press, Guilford Press and Rutledge. He has also participated in research funded by DARPA, NIH, NIA, Agency for Healthcare Research and Quality, PCORI, Janssen Pharmaceuticals, The Forest Research Institute, Shire Development Inc., Medtronic, Cyberonics, Northstar and Takeda. P.M. has received funding from the National Institute of Mental Health, New York State Department of Mental Hygiene, Research Foundation for Mental Hygiene (New York State), Forest Research Laboratories, Sunovion Pharmaceuticals and Naurex Pharmaceuticals (now Allergan). In the past 2 years, M.W. received funding from the NIMH, the National Institute on Drug Abuse, the National Alliance for Research on Schizophrenia and Depression, the Sackler Foundation, the Templeton Foundation; and receives royalties from the Oxford University Press, Perseus Press, the American Psychiatric Association Press and MultiHealth Systems. M.F. has received research support from Abbot Laboratories; Alkermes, Inc.; American Cyanamid; Aspect Medical Systems; AstraZeneca; Avanir Pharmaceuticals; BioResearch; BrainCells Inc.; Bristol-Myers Squibb; CeNeRx BioPharma; Cephalon; Clintara, LLC; Cerecor; Covance; Covidien; Eli Lilly and Company; EnVivo Pharmaceuticals, Inc.; Euthymics Bioscience, Inc.; Forest Pharmaceuticals, Inc.; Ganeden Biotech, Inc.; GlaxoSmithKline; Harvard Clinical Research Institute; Hoffman-LaRoche; Icon Clinical Research; i3 Innovus/ Ingenix; Janssen R&D, LLC; Jed Foundation; Johnson & Johnson Pharmaceutical Research & Development; Lichtwer Pharma GmbH; Lorex Pharmaceuticals; Lundbeck Inc.; MedAvante; Methylation Sciences Inc.; National Alliance for Research on Schizophrenia & Depression; National Center for Complementary and Alternative Medicine; National Institute of Drug Abuse; NIMH; Neuralstem, Inc.; Novartis AG; Organon Pharmaceuticals; PamLab, LLC.; Pfizer Inc.; Pharmacia-Upjohn; Pharmaceutical Research Associates., Inc.; Pharmavite LLC; PharmoRx Therapeutics; Photothera; Reckitt Benckiser; Roche Pharmaceuticals; RCT Logic, LLC (formerly Clinical Trials Solutions, LLC); Sanofi-Aventis US LLC; Shire; Solvay Pharmaceuticals, Inc.; Stanley Medical Research Institute; Synthelabo; Tal Medical; and Wyeth-Ayerst Laboratories. He has served as advisor or consultant to Abbott Laboratories; Acadia; Affectis Pharmaceuticals AG; Alkermes, Inc.; Amarin Pharma Inc.; Aspect Medical Systems; AstraZeneca; Auspex Pharmaceuticals; Avanir Pharmaceuticals; AXSOME Therapeutics; Bayer AG; Best Practice Project Management, Inc.; Biogen; BioMarin Pharmaceuticals, Inc.; Biovail Corporation; BrainCells Inc; Bristol-Myers Squibb; CeNeRx BioPharma; Cephalon, Inc.; Cerecor; CNS Response, Inc.; Compellis Pharmaceuticals; Cypress Pharmaceutical, Inc.; DiagnoSearch Life Sciences (P) Ltd.; Dinippon Sumitomo Pharma Co. Inc.; Dov Pharmaceuticals, Inc.; Edgemont Pharmaceuticals, Inc.; Eisai Inc.; Eli Lilly and Company; EnVivo Pharmaceuticals, Inc.; ePharmaSolutions; EPIX Pharmaceuticals, Inc.; Euthymics Bioscience, Inc.; Fabre-Kramer Pharmaceuticals, Inc.; Forest Pharmaceuticals, Inc.; Forum Pharmaceuticals; GenOmind, LLC; GlaxoSmithKline; Grunenthal GmbH; i3 Innovus/Ingenis; Intracellular; Janssen Pharmaceutica; Jazz Pharmaceuticals, Inc.; Johnson & Johnson Pharmaceutical Research & Development, LLC; Knoll Pharmaceuticals Corp.; Labopharm Inc.; Lorex Pharmaceuticals; Lundbeck Inc.; MedAvante, Inc.; Merck & Co., Inc.; MSI Methylation Sciences, Inc.; Naurex, Inc.; Nestle Health Sciences; Neuralstem, Inc.; Neuronetics, Inc.; NextWave Pharmaceuticals; Novartis AG; Nutrition 21; Orexigen Therapeutics, Inc.; Organon Pharmaceuticals; Osmotica; Otsuka Pharmaceuticals; Pamlab, LLC.; Pfizer Inc.; PharmaStar; Pharmavite LLC.; PharmoRx Therapeutics; Precision Human Biolaboratory; Prexa Pharmaceuticals, Inc.; Puretech Ventures; PsychoGenics; Psylin Neurosciences, Inc.; RCT Logic, LLC Formerly Clinical Trials Solutions, LLC; Rexahn Pharmaceuticals, Inc.; Ridge Diagnostics, Inc.; Roche; Sanofi-Aventis US LLC.; Sepracor Inc.; Servier Laboratories; Schering-Plough Corporation; Solvay Pharmaceuticals, Inc.; Somaxon Pharmaceuticals, Inc.; Somerset Pharmaceuticals, Inc.; Sunovion Pharmaceuticals; Supernus Pharmaceuticals, Inc.; Synthelabo; Taisho Pharmaceutical; Takeda Pharmaceutical Company Limited; Tal Medical, Inc.; Tetragenex Pharmaceuticals, Inc.; TransForm Pharmaceuticals, Inc.; Transcept Pharmaceuticals, Inc.; Vanda Pharmaceuticals, Inc.; and VistaGen. He has received speaking or publishing fees from Adamed, Co; Advanced Meeting Partners; American Psychiatric Association; American Society of Clinical Psychopharmacology; AstraZeneca; Belvoir Media Group; Boehringer Ingelheim GmbH; Bristol-Myers Squibb; Cephalon, Inc.; CME Institute/ Physicians Postgraduate Press, Inc.; Eli Lilly and Company; Forest Pharmaceuticals, Inc.; GlaxoSmithKline; Imedex, LLC; MGH Psychiatry Academy/Primedia; MGH Psychiatry Academy/Reed Elsevier; Novartis AG; Organon Pharmaceuticals; Pfizer Inc.; PharmaStar; United BioSource, Corp.; and Wyeth-Ayerst Laboratories. He has equity holdings in Compellis and PsyBrain, Inc.; he has a patent for Sequential Parallel Comparison Design, which is licensed by MGH to Pharmaceutical Product Development, LLC (PPD); and a patent application for a combination of Ketamine plus Scopolamine in Major Depressive Disorder, licensed by MGH to Biohaven; and he receives copyright royalties for the MGH Cognitive & Physical Functioning Questionnaire, Sexual Functioning Inventory, ATRQ, Discontinuation-Emergent Signs & Symptoms, Symptoms of Depression Questionnaire, and SAFER; Lippincott, Williams & Wilkins; Wolkers Kluwer; and World Scientific Publishing Co. Pte. Ltd. M.H.T. is or has been an advisor/consultant and received fees from (lifetime disclosure): Abbott Laboratories, Inc., Abdi Ibrahim, Akzo (Organon Pharmaceuticals Inc.), Alkermes, AstraZeneca, Axon Advisors, Bristol-Myers Squibb Company, Cephalon, Inc., Cerecor, CME Institute of Physicians, Concert Pharmaceuticals, Inc., Eli Lilly & Company, Evotec, Fabre-Kramer Pharmaceuticals, Inc., Forest Pharmaceuticals, GlaxoSmithKline, Janssen Global Services, LLC, Janssen Pharmaceutica Products, LP, Johnson & Johnson PRD, Libby, Lundbeck, Meade Johnson, MedAvante, Medtronic, Merck, Mitsubishi Tanabe Pharma Development America, Inc., Naurex, Neuronetics, Otsuka Pharmaceuticals, Pamlab, Parke-Davis Pharmaceuticals, Inc., Pfizer Inc., PgxHealth, Phoenix Marketing Solutions, Rexahn Pharmaceuticals, Ridge Diagnostics, Roche Products Ltd., Sepracor, SHIRE Development, Sierra, SK Life and Science, Sunovion, Takeda, Tal Medical/ Puretech Venture, Targacept, Transcept, VantagePoint, Vivus and Wyeth-Ayerst Laboratories. In addition, he has received grants/research support from: Agency for Healthcare Research and Quality, Cyberonics, Inc., National Alliance for Research in Schizophrenia and Depression, National Institute of Mental Health and the National Institute on Drug Abuse. J.M.T. currently owns stock in Merck and Gilead Sciences and within the past 36 months has previously owned stock in Johnson & Johnson. M.A. holds options from Brain Resource, is Director and Owner of Research Institute Brainclinics, has equity in neuroCare Group and is co-inventor on four patent applications (A61B5/0402; US2007/0299323, A1; WO2010/139361 A1) related to EEG, neuromodulation and psychophysiology, but does not own these nor receives any proceeds related to these patents; he receives Research Institute Brainclinics funding from Brain Resource and neuroCare Group and equipment support from Deymed, neuroConn and Magventure. All other authors report no competing interests. Funding Information: We thank C.J. Keller and S. Kim. The EMBARC study was supported by the National Institute of Mental Health of the National Institutes of Health (NIH) under award nos, U01MH092221 (M.H.T.) and U01MH092250 (P.J.M., R.V.P. and M.M.W.). Data from the second depressed cohort were acquired under R01MH103324 (A.E.) and Big Idea in Neuroscience research funds from the Stanford Neurosciences Institute (A.E.). This work was also funded in part by the Hersh Foundation (M.H.T.). A.E. and W.W. were additionally funded by NIH grant no. DP1 MH116506. W.W. was also funded by National Key Research and Development Plan of China (grant no. 2017YFB1002505) and the National Natural Science Foundation of China (grant nos. 61876063 and 61836003). Publisher Copyright: {\textcopyright} 2020, The Author(s), under exclusive licence to Springer Nature America, Inc.",

year = "2020",

month = apr,

doi = "10.1038/s41587-019-0397-3",

language = "English",

volume = "38",

pages = "439--447",

journal = "Nature Biotechnology",

issn = "1087-0156",

publisher = "Nature Publishing Group",

number = "4",

}

Wu, W, Zhang, Y, Jiang, J, Lucas, M, Fonzo, GA, Rolle, CE, Cooper, C, Chin-Fatt, C, Krepel, N, Cornelssen, CA, Wright, R, Toll, RT, Trivedi, HM, Monuszko, K, Caudle, TL, Sarhadi, K, Jha, MK, Trombello, JM, Deckersbach, T, Adams, P, McGrath, PJ, Weissman, MM, Fava, M, Pizzagalli, DA, Arns, M, Trivedi, MH & Etkin, A 2020, 'An electroencephalographic signature predicts antidepressant response in major depression', Nature Biotechnology, vol. 38, no. 4, pp. 439-447. https://doi.org/10.1038/s41587-019-0397-3

TY - JOUR

T1 - An electroencephalographic signature predicts antidepressant response in major depression

AU - Wu, Wei

AU - Zhang, Yu

AU - Jiang, Jing

AU - Lucas, Molly

AU - Fonzo, Gregory A.

AU - Rolle, Camarin E.

AU - Cooper, Crystal

AU - Chin-Fatt, Cherise

AU - Krepel, Noralie

AU - Cornelssen, Carena A.

AU - Wright, Rachael

AU - Toll, Russell T.

AU - Trivedi, Hersh M.

AU - Monuszko, Karen

AU - Caudle, Trevor L.

AU - Sarhadi, Kamron

AU - Jha, Manish K.

AU - Trombello, Joseph M.

AU - Deckersbach, Thilo

AU - Adams, Phil

AU - McGrath, Patrick J.

AU - Weissman, Myrna M.

AU - Fava, Maurizio

AU - Pizzagalli, Diego A.

AU - Arns, Martijn

AU - Trivedi, Madhukar H.

AU - Etkin, Amit

N1 - Funding Information: A.E. (lifetime disclosure) has been receiving salary and equity from Alto Neuroscience since 1 November 2019, to which the pending patent for SELSER has been licensed from Stanford. He holds equity in Mindstrong Health, Akili Interactive and Sizung for unrelated work, has received research funding from the National Institute of Mental Health, Department of Veterans Affairs, Cohen Veterans Bioscience, Brain and Behavior Research Foundation, Dana Foundation, Brain Resource Inc. and the Stanford Neurosciences Institute and consulted for Cervel, Takaeda, Posit Science, Acadia, Otsuka, Lundbeck and Janssen. Over the past 3 years, D.A.P. has received consulting fees from Alkermes, BlackThorn Therapeutics, Boehreinger Ingelheim, Posit Science and Takeda Pharmaceuticals. He has received funding from NIMH, the Dana Foundation and Brain and Behavior Research Foundation. T.D.’s research has been funded by NIH, NIMH, National Alliance for Research on Schizophrenia & Depression, TSA, IOCDF, Tufts University, DBDAT and Otsuka Pharmaceuticals. He has received honoraria, consultation fees and/or royalties from the MGH Psychiatry Academy, BrainCells Inc., Clintara, LLC, Inc., Systems Research and Applications Corporation, Boston University, the Catalan Agency for Health Technology Assessment and Research, the National Association of Social Workers Massachusetts, the Massachusetts Medical Society, Tufts University, National Institute of Drug Abuse, NIMH, Oxford University Press, Guilford Press and Rutledge. He has also participated in research funded by DARPA, NIH, NIA, Agency for Healthcare Research and Quality, PCORI, Janssen Pharmaceuticals, The Forest Research Institute, Shire Development Inc., Medtronic, Cyberonics, Northstar and Takeda. P.M. has received funding from the National Institute of Mental Health, New York State Department of Mental Hygiene, Research Foundation for Mental Hygiene (New York State), Forest Research Laboratories, Sunovion Pharmaceuticals and Naurex Pharmaceuticals (now Allergan). In the past 2 years, M.W. received funding from the NIMH, the National Institute on Drug Abuse, the National Alliance for Research on Schizophrenia and Depression, the Sackler Foundation, the Templeton Foundation; and receives royalties from the Oxford University Press, Perseus Press, the American Psychiatric Association Press and MultiHealth Systems. M.F. has received research support from Abbot Laboratories; Alkermes, Inc.; American Cyanamid; Aspect Medical Systems; AstraZeneca; Avanir Pharmaceuticals; BioResearch; BrainCells Inc.; Bristol-Myers Squibb; CeNeRx BioPharma; Cephalon; Clintara, LLC; Cerecor; Covance; Covidien; Eli Lilly and Company; EnVivo Pharmaceuticals, Inc.; Euthymics Bioscience, Inc.; Forest Pharmaceuticals, Inc.; Ganeden Biotech, Inc.; GlaxoSmithKline; Harvard Clinical Research Institute; Hoffman-LaRoche; Icon Clinical Research; i3 Innovus/ Ingenix; Janssen R&D, LLC; Jed Foundation; Johnson & Johnson Pharmaceutical Research & Development; Lichtwer Pharma GmbH; Lorex Pharmaceuticals; Lundbeck Inc.; MedAvante; Methylation Sciences Inc.; National Alliance for Research on Schizophrenia & Depression; National Center for Complementary and Alternative Medicine; National Institute of Drug Abuse; NIMH; Neuralstem, Inc.; Novartis AG; Organon Pharmaceuticals; PamLab, LLC.; Pfizer Inc.; Pharmacia-Upjohn; Pharmaceutical Research Associates., Inc.; Pharmavite LLC; PharmoRx Therapeutics; Photothera; Reckitt Benckiser; Roche Pharmaceuticals; RCT Logic, LLC (formerly Clinical Trials Solutions, LLC); Sanofi-Aventis US LLC; Shire; Solvay Pharmaceuticals, Inc.; Stanley Medical Research Institute; Synthelabo; Tal Medical; and Wyeth-Ayerst Laboratories. He has served as advisor or consultant to Abbott Laboratories; Acadia; Affectis Pharmaceuticals AG; Alkermes, Inc.; Amarin Pharma Inc.; Aspect Medical Systems; AstraZeneca; Auspex Pharmaceuticals; Avanir Pharmaceuticals; AXSOME Therapeutics; Bayer AG; Best Practice Project Management, Inc.; Biogen; BioMarin Pharmaceuticals, Inc.; Biovail Corporation; BrainCells Inc; Bristol-Myers Squibb; CeNeRx BioPharma; Cephalon, Inc.; Cerecor; CNS Response, Inc.; Compellis Pharmaceuticals; Cypress Pharmaceutical, Inc.; DiagnoSearch Life Sciences (P) Ltd.; Dinippon Sumitomo Pharma Co. Inc.; Dov Pharmaceuticals, Inc.; Edgemont Pharmaceuticals, Inc.; Eisai Inc.; Eli Lilly and Company; EnVivo Pharmaceuticals, Inc.; ePharmaSolutions; EPIX Pharmaceuticals, Inc.; Euthymics Bioscience, Inc.; Fabre-Kramer Pharmaceuticals, Inc.; Forest Pharmaceuticals, Inc.; Forum Pharmaceuticals; GenOmind, LLC; GlaxoSmithKline; Grunenthal GmbH; i3 Innovus/Ingenis; Intracellular; Janssen Pharmaceutica; Jazz Pharmaceuticals, Inc.; Johnson & Johnson Pharmaceutical Research & Development, LLC; Knoll Pharmaceuticals Corp.; Labopharm Inc.; Lorex Pharmaceuticals; Lundbeck Inc.; MedAvante, Inc.; Merck & Co., Inc.; MSI Methylation Sciences, Inc.; Naurex, Inc.; Nestle Health Sciences; Neuralstem, Inc.; Neuronetics, Inc.; NextWave Pharmaceuticals; Novartis AG; Nutrition 21; Orexigen Therapeutics, Inc.; Organon Pharmaceuticals; Osmotica; Otsuka Pharmaceuticals; Pamlab, LLC.; Pfizer Inc.; PharmaStar; Pharmavite LLC.; PharmoRx Therapeutics; Precision Human Biolaboratory; Prexa Pharmaceuticals, Inc.; Puretech Ventures; PsychoGenics; Psylin Neurosciences, Inc.; RCT Logic, LLC Formerly Clinical Trials Solutions, LLC; Rexahn Pharmaceuticals, Inc.; Ridge Diagnostics, Inc.; Roche; Sanofi-Aventis US LLC.; Sepracor Inc.; Servier Laboratories; Schering-Plough Corporation; Solvay Pharmaceuticals, Inc.; Somaxon Pharmaceuticals, Inc.; Somerset Pharmaceuticals, Inc.; Sunovion Pharmaceuticals; Supernus Pharmaceuticals, Inc.; Synthelabo; Taisho Pharmaceutical; Takeda Pharmaceutical Company Limited; Tal Medical, Inc.; Tetragenex Pharmaceuticals, Inc.; TransForm Pharmaceuticals, Inc.; Transcept Pharmaceuticals, Inc.; Vanda Pharmaceuticals, Inc.; and VistaGen. He has received speaking or publishing fees from Adamed, Co; Advanced Meeting Partners; American Psychiatric Association; American Society of Clinical Psychopharmacology; AstraZeneca; Belvoir Media Group; Boehringer Ingelheim GmbH; Bristol-Myers Squibb; Cephalon, Inc.; CME Institute/ Physicians Postgraduate Press, Inc.; Eli Lilly and Company; Forest Pharmaceuticals, Inc.; GlaxoSmithKline; Imedex, LLC; MGH Psychiatry Academy/Primedia; MGH Psychiatry Academy/Reed Elsevier; Novartis AG; Organon Pharmaceuticals; Pfizer Inc.; PharmaStar; United BioSource, Corp.; and Wyeth-Ayerst Laboratories. He has equity holdings in Compellis and PsyBrain, Inc.; he has a patent for Sequential Parallel Comparison Design, which is licensed by MGH to Pharmaceutical Product Development, LLC (PPD); and a patent application for a combination of Ketamine plus Scopolamine in Major Depressive Disorder, licensed by MGH to Biohaven; and he receives copyright royalties for the MGH Cognitive & Physical Functioning Questionnaire, Sexual Functioning Inventory, ATRQ, Discontinuation-Emergent Signs & Symptoms, Symptoms of Depression Questionnaire, and SAFER; Lippincott, Williams & Wilkins; Wolkers Kluwer; and World Scientific Publishing Co. Pte. Ltd. M.H.T. is or has been an advisor/consultant and received fees from (lifetime disclosure): Abbott Laboratories, Inc., Abdi Ibrahim, Akzo (Organon Pharmaceuticals Inc.), Alkermes, AstraZeneca, Axon Advisors, Bristol-Myers Squibb Company, Cephalon, Inc., Cerecor, CME Institute of Physicians, Concert Pharmaceuticals, Inc., Eli Lilly & Company, Evotec, Fabre-Kramer Pharmaceuticals, Inc., Forest Pharmaceuticals, GlaxoSmithKline, Janssen Global Services, LLC, Janssen Pharmaceutica Products, LP, Johnson & Johnson PRD, Libby, Lundbeck, Meade Johnson, MedAvante, Medtronic, Merck, Mitsubishi Tanabe Pharma Development America, Inc., Naurex, Neuronetics, Otsuka Pharmaceuticals, Pamlab, Parke-Davis Pharmaceuticals, Inc., Pfizer Inc., PgxHealth, Phoenix Marketing Solutions, Rexahn Pharmaceuticals, Ridge Diagnostics, Roche Products Ltd., Sepracor, SHIRE Development, Sierra, SK Life and Science, Sunovion, Takeda, Tal Medical/ Puretech Venture, Targacept, Transcept, VantagePoint, Vivus and Wyeth-Ayerst Laboratories. In addition, he has received grants/research support from: Agency for Healthcare Research and Quality, Cyberonics, Inc., National Alliance for Research in Schizophrenia and Depression, National Institute of Mental Health and the National Institute on Drug Abuse. J.M.T. currently owns stock in Merck and Gilead Sciences and within the past 36 months has previously owned stock in Johnson & Johnson. M.A. holds options from Brain Resource, is Director and Owner of Research Institute Brainclinics, has equity in neuroCare Group and is co-inventor on four patent applications (A61B5/0402; US2007/0299323, A1; WO2010/139361 A1) related to EEG, neuromodulation and psychophysiology, but does not own these nor receives any proceeds related to these patents; he receives Research Institute Brainclinics funding from Brain Resource and neuroCare Group and equipment support from Deymed, neuroConn and Magventure. All other authors report no competing interests. Funding Information: We thank C.J. Keller and S. Kim. The EMBARC study was supported by the National Institute of Mental Health of the National Institutes of Health (NIH) under award nos, U01MH092221 (M.H.T.) and U01MH092250 (P.J.M., R.V.P. and M.M.W.). Data from the second depressed cohort were acquired under R01MH103324 (A.E.) and Big Idea in Neuroscience research funds from the Stanford Neurosciences Institute (A.E.). This work was also funded in part by the Hersh Foundation (M.H.T.). A.E. and W.W. were additionally funded by NIH grant no. DP1 MH116506. W.W. was also funded by National Key Research and Development Plan of China (grant no. 2017YFB1002505) and the National Natural Science Foundation of China (grant nos. 61876063 and 61836003). Publisher Copyright: © 2020, The Author(s), under exclusive licence to Springer Nature America, Inc.

PY - 2020/4

Y1 - 2020/4

N2 - Antidepressants are widely prescribed, but their efficacy relative to placebo is modest, in part because the clinical diagnosis of major depression encompasses biologically heterogeneous conditions. Here, we sought to identify a neurobiological signature of response to antidepressant treatment as compared to placebo. We designed a latent-space machine-learning algorithm tailored for resting-state electroencephalography (EEG) and applied it to data from the largest imaging-coupled, placebo-controlled antidepressant study (n = 309). Symptom improvement was robustly predicted in a manner both specific for the antidepressant sertraline (versus placebo) and generalizable across different study sites and EEG equipment. This sertraline-predictive EEG signature generalized to two depression samples, wherein it reflected general antidepressant medication responsivity and related differentially to a repetitive transcranial magnetic stimulation treatment outcome. Furthermore, we found that the sertraline resting-state EEG signature indexed prefrontal neural responsivity, as measured by concurrent transcranial magnetic stimulation and EEG. Our findings advance the neurobiological understanding of antidepressant treatment through an EEG-tailored computational model and provide a clinical avenue for personalized treatment of depression.

AB - Antidepressants are widely prescribed, but their efficacy relative to placebo is modest, in part because the clinical diagnosis of major depression encompasses biologically heterogeneous conditions. Here, we sought to identify a neurobiological signature of response to antidepressant treatment as compared to placebo. We designed a latent-space machine-learning algorithm tailored for resting-state electroencephalography (EEG) and applied it to data from the largest imaging-coupled, placebo-controlled antidepressant study (n = 309). Symptom improvement was robustly predicted in a manner both specific for the antidepressant sertraline (versus placebo) and generalizable across different study sites and EEG equipment. This sertraline-predictive EEG signature generalized to two depression samples, wherein it reflected general antidepressant medication responsivity and related differentially to a repetitive transcranial magnetic stimulation treatment outcome. Furthermore, we found that the sertraline resting-state EEG signature indexed prefrontal neural responsivity, as measured by concurrent transcranial magnetic stimulation and EEG. Our findings advance the neurobiological understanding of antidepressant treatment through an EEG-tailored computational model and provide a clinical avenue for personalized treatment of depression.

KW - TRANSCRANIAL MAGNETIC STIMULATION

KW - SINGLE-TRIAL EEG

KW - BRAIN-FUNCTION

KW - OSCILLATIONS

KW - MECHANISMS

KW - MODERATORS

KW - BIOMARKERS

KW - CONFLICT

KW - NETWORKS

KW - OUTCOMES

U2 - 10.1038/s41587-019-0397-3

DO - 10.1038/s41587-019-0397-3

M3 - Article

C2 - 32042166

SN - 1087-0156

VL - 38

SP - 439

EP - 447

JO - Nature Biotechnology

JF - Nature Biotechnology

IS - 4

ER -