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Review
. 2013 Dec:39 Suppl 3:S149-56.
doi: 10.1016/S0013-7006(13)70114-3.

[Mixed depressions: clinical and neurophysiological biomarkers]

[Article in French]
Affiliations
Review

[Mixed depressions: clinical and neurophysiological biomarkers]

[Article in French]
J-A Micoulaud Franchi et al. Encephale. 2013 Dec.

Abstract

Epidemiological studies of major depressive episodes (MDE) highlighted the frequent association of symptoms or signs of mania or hypomania with depressive syndrome. Beyond the strict definition of DSM-IV, epidemiological recognition of a subset of MDE characterized by the presence of symptoms or signs of the opposite polarity is clinically important because it is associated with pejorative prognosis and therapeutic response compared to the subgroup of "typical MDE". The development of DSM-5 took into account the epidemiological data. DSM-5 opted for a more dimensional perspective in implementing the concept of "mixed features" from an "episode" to a "specification" of mood disorder. As outlined in the DSM-5: "Mixed features associated with a major depressive episode have been found to be a significant risk factor for the development of bipolar I and II disorder. As a result, it is clinically useful to note the presence of this specifier for treatment planning and monitoring of response to therapeutic". However, the mixed features are sometimes difficult to identify, and neurophysiological biomarkers would be useful to make a more specific diagnosis. Two neurophysiological models make it possible to better understand MDE with mixed features : i) the emotional regulation model that highlights a tendency to hyper-reactive and unstable emotion response, and ii) the vigilance regulation model that highlights, through EEG recording, a tendency to unstable vigilance. Further research is required to better understand relationships between these two models. These models provide the opportunity of a neurophysiological framework to better understand the mixed features associated with MDE and to identify potential neurophysiological biomarkers to guide therapeutic strategies.

Keywords: Arousal; Bipolar disorders; Depression; Dépression; Electro-encephalography; Electro-encéphalographie; Emotional reactivity; Eveil; Réactivité émotionnelle; Régulation de la vigilance; Troubles bipolaires; Vigilance regulation.

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