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Game changer in the diagnosis of bipolar disorder using RNA editing-based blood biomarkers

Published online by Cambridge University Press:  13 August 2021

J.-D. Abraham*
Affiliation:
Neurology, ALCEDIAG/SYS2DIAG, MONTPELLIER, France
N. Salvetat
Affiliation:
Neurology, ALCEDIAG/SYS2DIAG, MONTPELLIER, France
F. Checa-Robles
Affiliation:
Neurology, ALCEDIAG/SYS2DIAG, MONTPELLIER, France
V. Patel
Affiliation:
Neurology, ALCEDIAG/SYS2DIAG, MONTPELLIER, France
C. Cayzac
Affiliation:
Neurology, ALCEDIAG/SYS2DIAG, MONTPELLIER, France
B. Dubuc
Affiliation:
Neurology, ALCEDIAG/SYS2DIAG, MONTPELLIER, France
D. Vetter
Affiliation:
Neurology, ALCEDIAG/SYS2DIAG, MONTPELLIER, France
J.-P. Lang
Affiliation:
Center For Psychiatry And Psychotherapy, Les Toises, Lausanne, Switzerland
P. Courtet
Affiliation:
Emergency Psychiatry And Acute Care, CHU Montpellier / INSERM, Montpellier, France
D. Kupfer
Affiliation:
Department Of Psychiatry, University of Pittsburgh School of Medicine, Pittsburgh, United States of America
D. Weissmann
Affiliation:
Neurology, ALCEDIAG/SYS2DIAG, MONTPELLIER, France
*
*Corresponding author.

Abstract

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Introduction

In clinical practice, differentiating Bipolar Disorder (BD) from unipolar depression is challenging due to the depressive symptoms, which are the core presentations of both disorders. Patients with BD are often misdiagnosed during depressive episodes resulting in a delay in proper treatment and a poor management of their condition.

Objectives

The aim of the present study is to discriminate between unipolar depression and BD using a panel of RNA edited blood biomarkers.

Methods

Depressed patients were classified according to clinical scores in MADRS and IDSC-30 depression scales. After blood collection and RNA extraction, we used whole-transcriptome sequencing to identify differential A-to-I editing events, and Targeted Next Generation Sequencing to validate those biomarkers.

Results

We discovered 646 variants differentially edited between depressed patients and control in a discovery cohort of 57 participants. After using stringent criteria and biological pathway analysis, 6 biomarker candidates were singled out and tested in a validation cohort of 160 patients suffering from unipolar depression and 95 BD patients in a depressive episode, which allowed a differential diagnosis of BD with an AUC of 0.935 and high specificity (Sp=84.6%) and sensitivity (Se=90.9%).

Conclusions

We have shown that a combination of 6 blood RNA editing-related biomarkers allows to discriminate unipolar and bipolar depression This 6 BMKs panel may be crucial to improve BD diagnosis and orientate the treatment therefore addressing the needs of millions of patients suffering from misdiagnosis and incorrect treatment for their diseases. This will change the game for the management of patients.

Disclosure

No significant relationships.

Type
Abstract
Creative Commons
Creative Common License - CCCreative Common License - BY
This is an Open Access article, distributed under the terms of the Creative Commons Attribution licence (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted re-use, distribution, and reproduction in any medium, provided the original work is properly cited.
Copyright
© The Author(s), 2021. Published by Cambridge University Press on behalf of the European Psychiatric Association
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