Putative Transcriptomic Biomarkers in the Inflammatory Cytokine Pathway Differentiate Major Depressive Disorder Patients from Control Subjects and Bipolar Disorder Patients

Timothy Powell; Peter McGuffin; Ursula M. D'Souza; Sarah Cohen-Woods; Georgina M. Hosang; Charlotte Martin; Keith Matthews; Richard K. Day; Anne E. Farmer; Katherine E. Tansey; Leonard C. Schalkwyk

doi:10.1371/journal.pone.0091076

Putative Transcriptomic Biomarkers in the Inflammatory Cytokine Pathway Differentiate Major Depressive Disorder Patients from Control Subjects and Bipolar Disorder Patients

Timothy Powell, Peter McGuffin, Ursula M. D'Souza, Sarah Cohen-Woods, Georgina M. Hosang, Charlotte Martin, Keith Matthews, Richard K. Day, Anne E. Farmer, Katherine E. Tansey, Leonard C. Schalkwyk

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Abstract

Mood disorders consist of two etiologically related, but distinctly treated illnesses, major depressive disorder (MDD) and bipolar disorder (BPD). These disorders share similarities in their clinical presentation, and thus show high rates of misdiagnosis. Recent research has revealed significant transcriptional differences within the inflammatory cytokine pathway between MDD patients and controls, and between BPD patients and controls, suggesting this pathway may possess important biomarker properties. This exploratory study attempts to identify disorder-specific transcriptional biomarkers within the inflammatory cytokine pathway, which can distinguish between control subjects, MDD patients and BPD patients. This is achieved using RNA extracted from subject blood and applying synthesized complementary DNA to quantitative PCR arrays containing primers for 87 inflammation-related genes. Initially, we use ANOVA to test for transcriptional differences in a 'discovery cohort' (total n = 90) and then we use t-tests to assess the reliability of any identified transcriptional differences in a 'validation cohort' (total n = 35). The two most robust and reliable biomarkers identified across both the discovery and validation cohort were Chemokine (C-C motif) ligand 24 (CCL24) which was consistently transcribed higher amongst MDD patients relative to controls and BPD patients, and C-C chemokine receptor type 6 (CCR6) which was consistently more lowly transcribed amongst MDD patients relative to controls. Results detailed here provide preliminary evidence that transcriptional measures within inflammation-related genes might be useful in aiding clinical diagnostic decision-making processes. Future research should aim to replicate findings detailed in this exploratory study in a larger medication-free sample and examine whether identified biomarkers could be used prospectively to aid clinical diagnosis.

Original language	English
Article number	e91076
Number of pages	9
Journal	PL o S One
Volume	9
Issue number	3
DOIs	https://doi.org/10.1371/journal.pone.0091076
Publication status	Published - 11 Mar 2014

Keywords

TUMOR-NECROSIS-FACTOR
MOOD DISORDERS
FUNCTIONAL-CHARACTERIZATION
CONTEMPORARY CONFUSION
SEROTONIN TRANSPORTER
UNIPOLAR DEPRESSION
GENE
CLASSIFICATION
METAANALYSIS
RECEPTOR

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Putative Transcriptomic Biomarkers in the_POWELL Accepted 6Feb2014 GOLDFinal published version, 307 KBLicence: CC BY

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Powell, T., McGuffin, P., D'Souza, U. M., Cohen-Woods, S., Hosang, G. M., Martin, C., Matthews, K., Day, R. K., Farmer, A. E., Tansey, K. E., & Schalkwyk, L. C. (2014). Putative Transcriptomic Biomarkers in the Inflammatory Cytokine Pathway Differentiate Major Depressive Disorder Patients from Control Subjects and Bipolar Disorder Patients. PL o S One , 9(3), Article e91076. https://doi.org/10.1371/journal.pone.0091076

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title = "Putative Transcriptomic Biomarkers in the Inflammatory Cytokine Pathway Differentiate Major Depressive Disorder Patients from Control Subjects and Bipolar Disorder Patients",

abstract = "Mood disorders consist of two etiologically related, but distinctly treated illnesses, major depressive disorder (MDD) and bipolar disorder (BPD). These disorders share similarities in their clinical presentation, and thus show high rates of misdiagnosis. Recent research has revealed significant transcriptional differences within the inflammatory cytokine pathway between MDD patients and controls, and between BPD patients and controls, suggesting this pathway may possess important biomarker properties. This exploratory study attempts to identify disorder-specific transcriptional biomarkers within the inflammatory cytokine pathway, which can distinguish between control subjects, MDD patients and BPD patients. This is achieved using RNA extracted from subject blood and applying synthesized complementary DNA to quantitative PCR arrays containing primers for 87 inflammation-related genes. Initially, we use ANOVA to test for transcriptional differences in a 'discovery cohort' (total n = 90) and then we use t-tests to assess the reliability of any identified transcriptional differences in a 'validation cohort' (total n = 35). The two most robust and reliable biomarkers identified across both the discovery and validation cohort were Chemokine (C-C motif) ligand 24 (CCL24) which was consistently transcribed higher amongst MDD patients relative to controls and BPD patients, and C-C chemokine receptor type 6 (CCR6) which was consistently more lowly transcribed amongst MDD patients relative to controls. Results detailed here provide preliminary evidence that transcriptional measures within inflammation-related genes might be useful in aiding clinical diagnostic decision-making processes. Future research should aim to replicate findings detailed in this exploratory study in a larger medication-free sample and examine whether identified biomarkers could be used prospectively to aid clinical diagnosis.",

keywords = "TUMOR-NECROSIS-FACTOR, MOOD DISORDERS, FUNCTIONAL-CHARACTERIZATION, CONTEMPORARY CONFUSION, SEROTONIN TRANSPORTER, UNIPOLAR DEPRESSION, GENE, CLASSIFICATION, METAANALYSIS, RECEPTOR",

author = "Timothy Powell and Peter McGuffin and D'Souza, {Ursula M.} and Sarah Cohen-Woods and Hosang, {Georgina M.} and Charlotte Martin and Keith Matthews and Day, {Richard K.} and Farmer, {Anne E.} and Tansey, {Katherine E.} and Schalkwyk, {Leonard C.}",

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Powell, T, McGuffin, P, D'Souza, UM, Cohen-Woods, S, Hosang, GM, Martin, C, Matthews, K, Day, RK, Farmer, AE, Tansey, KE & Schalkwyk, LC 2014, 'Putative Transcriptomic Biomarkers in the Inflammatory Cytokine Pathway Differentiate Major Depressive Disorder Patients from Control Subjects and Bipolar Disorder Patients', PL o S One , vol. 9, no. 3, e91076. https://doi.org/10.1371/journal.pone.0091076

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AU - Powell, Timothy

AU - McGuffin, Peter

AU - D'Souza, Ursula M.

AU - Cohen-Woods, Sarah

AU - Hosang, Georgina M.

AU - Martin, Charlotte

AU - Matthews, Keith

AU - Day, Richard K.

AU - Farmer, Anne E.

AU - Tansey, Katherine E.

AU - Schalkwyk, Leonard C.

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N2 - Mood disorders consist of two etiologically related, but distinctly treated illnesses, major depressive disorder (MDD) and bipolar disorder (BPD). These disorders share similarities in their clinical presentation, and thus show high rates of misdiagnosis. Recent research has revealed significant transcriptional differences within the inflammatory cytokine pathway between MDD patients and controls, and between BPD patients and controls, suggesting this pathway may possess important biomarker properties. This exploratory study attempts to identify disorder-specific transcriptional biomarkers within the inflammatory cytokine pathway, which can distinguish between control subjects, MDD patients and BPD patients. This is achieved using RNA extracted from subject blood and applying synthesized complementary DNA to quantitative PCR arrays containing primers for 87 inflammation-related genes. Initially, we use ANOVA to test for transcriptional differences in a 'discovery cohort' (total n = 90) and then we use t-tests to assess the reliability of any identified transcriptional differences in a 'validation cohort' (total n = 35). The two most robust and reliable biomarkers identified across both the discovery and validation cohort were Chemokine (C-C motif) ligand 24 (CCL24) which was consistently transcribed higher amongst MDD patients relative to controls and BPD patients, and C-C chemokine receptor type 6 (CCR6) which was consistently more lowly transcribed amongst MDD patients relative to controls. Results detailed here provide preliminary evidence that transcriptional measures within inflammation-related genes might be useful in aiding clinical diagnostic decision-making processes. Future research should aim to replicate findings detailed in this exploratory study in a larger medication-free sample and examine whether identified biomarkers could be used prospectively to aid clinical diagnosis.

AB - Mood disorders consist of two etiologically related, but distinctly treated illnesses, major depressive disorder (MDD) and bipolar disorder (BPD). These disorders share similarities in their clinical presentation, and thus show high rates of misdiagnosis. Recent research has revealed significant transcriptional differences within the inflammatory cytokine pathway between MDD patients and controls, and between BPD patients and controls, suggesting this pathway may possess important biomarker properties. This exploratory study attempts to identify disorder-specific transcriptional biomarkers within the inflammatory cytokine pathway, which can distinguish between control subjects, MDD patients and BPD patients. This is achieved using RNA extracted from subject blood and applying synthesized complementary DNA to quantitative PCR arrays containing primers for 87 inflammation-related genes. Initially, we use ANOVA to test for transcriptional differences in a 'discovery cohort' (total n = 90) and then we use t-tests to assess the reliability of any identified transcriptional differences in a 'validation cohort' (total n = 35). The two most robust and reliable biomarkers identified across both the discovery and validation cohort were Chemokine (C-C motif) ligand 24 (CCL24) which was consistently transcribed higher amongst MDD patients relative to controls and BPD patients, and C-C chemokine receptor type 6 (CCR6) which was consistently more lowly transcribed amongst MDD patients relative to controls. Results detailed here provide preliminary evidence that transcriptional measures within inflammation-related genes might be useful in aiding clinical diagnostic decision-making processes. Future research should aim to replicate findings detailed in this exploratory study in a larger medication-free sample and examine whether identified biomarkers could be used prospectively to aid clinical diagnosis.

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KW - MOOD DISORDERS

KW - FUNCTIONAL-CHARACTERIZATION

KW - CONTEMPORARY CONFUSION

KW - SEROTONIN TRANSPORTER

KW - UNIPOLAR DEPRESSION

KW - GENE

KW - CLASSIFICATION

KW - METAANALYSIS

KW - RECEPTOR

U2 - 10.1371/journal.pone.0091076

DO - 10.1371/journal.pone.0091076

M3 - Article

SN - 1932-6203

VL - 9

JO - PL o S One

JF - PL o S One

IS - 3

M1 - e91076

ER -

Putative Transcriptomic Biomarkers in the Inflammatory Cytokine Pathway Differentiate Major Depressive Disorder Patients from Control Subjects and Bipolar Disorder Patients

Abstract

Keywords

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