Influence de l'histoire dépressive sur les paramètres biologiques dans la dépression majeure - 17/02/08

Doi : ENC-02-2002-28-1-0013-7006-101019-ART6

R. VanWijnendaele^[1],
P. Hubain^[1],
M. Dramaix^[2],
J. Mendlewicz^[1],
P. Linkowski^[1]
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^[1] Hôpital Erasme, Service de Psychiatrie. Université Libre de Bruxelles, 808, route de Lennik, 1070 Bruxelles, Belgique.
^[2] École de Santé publique, Université Libre de Bruxelles, Belgique.

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De multiples études ont montré des anomalies du test de suppression à la dexaméthasone (DST) ainsi que du sommeil dans la dépression. Ces perturbations sont étroitement corrélées à l'âge des sujets ainsi qu'à la sévérité des symptômes dépressifs. Différents éléments plaident pour une aggravation progressive des dépressions et de leur composante biologique au fil des épisodes. Nous avons étudié les anomalies biologiques d'une cohorte de 130 patients atteints de dépression majeure et évalué de manière rétrospective leurs antécédents dépressifs, afin de vérifier cette hypothèse. Nous avons de surcroît étudié l'effet du stress, évalué par l'item 216 du SADS, sur ces variables biologiques. Les résultats ne sont pas en faveur d'une aggravation des anomalies biologiques avec les antécédents dépressifs. La seule corrélation qui a été retrouvée, après correction de l'effet confondant de l'âge, est entre l'âge de début de la pathologie dépressive et le DST. La mesure que nous avons utilisée du stress n'avait d'influence significative que sur le pourcentage d'éveil et nous avons observé une tendance à l'augmentation du stress au fil des épisodes, sans que ce soit significatif.

The effects of the history of the depressive illness on some biological anomalies of depression : DST and polysomnography

Background – Major depressive disorder is associated with several biological abnormalities. Amoung them, sleep disturbances and alterations of hypothalamic structures and cortisol system have been largely studied. Most studies have found a relationship between depression and alteration of sleep. Electroencephalic sleep profiles during depression demonstrate abnormalities of sleep continuity, reduction of slow waves sleep and REM pressure ^{[27KUPFER DJ. Sleep research in depressive illness : clinical implications. A testing menu. Biol Psychiat 1995 ; 38 : 391-403.

Cliquez ici pour aller à la section Références]}. The cortisol system, investigated by the Dexamethasone Suppression Test (DST), is abnormal in about an half of the depressed subjects. We confirm a cortisol escape from suppression by dexamethasone ^{[21HUBAIN PP, STANER L, DRAMAIX M et al . The dexamethasone suppression test and sleep electroencephalogram in nonbipolar major depressed inpatients : a multivariate analysis. Biol Psychiatry 1998 ; 43 : 220-9.

Cliquez ici pour aller à la section Références]}. A complex dysregulation of the Hypothalamic Pituitary Adrenal axis (HPA) is thought to explain this escape ^{[15GOLD WP, GOODWIN FK, CHROUSOS GP. Clinical and biochemical manifestations of depression, relation to the neurobiology of stress (second of two parts). N Engl J Med 1988 ; 319 (7) : 413-20

Cliquez ici pour aller à la section Références]}^{[33NEMEROFF CB. The corticotropin-releasing factor (CRF) hypothesis of depression : new findings and new directions. Molecul Psychiatry 1996 ; 1 : 336-42.

Cliquez ici pour aller à la section Références]}. The HPA has been first involved in the theory of stress. There are two ways to study this. First by looking at early adversities and genetic susceptibility to stress, and second by studying acute stressors and depressive reactions ^{[8CHECKLEY S. The neuroendocrinology of depression and chronic stress. Br Med Bull 1996 ; 52 (3) : 597-617.

Cliquez ici pour aller à la section Références]}. The sensitization model postulated that the acute abnormalities of depression may leave biological scares. Those scares could make people more vulnerable to latter depressive triggers ^{[34POST M. Transduction of psychosocial stress into the neurobiology of recurrent affective disorder. Am J Psychiatry 1992 ; 149 (8) : 999-1010.

Cliquez ici pour aller à la section Références]}. We could then suppose that biological correlates of depression become more severe during the course of the illness. The present study further examines relationships between DST, polysomnography and some clinical and epidemiological characteristics of the depressive illness. We tried to examine if there were increasing biological disturbances during the course of the illness. We also examined the effect of the history of illness on the psychosocial stressors, and the effects of those stressors on the biological correlates of depression. Methods – The DST and polysomnographic recordings were performed in a sample of 130 inpatients with primary major depressive disorder, unipolar form, as defined with the RDC ^{[41SPITZER RL, ENDICOTT J, ROBBINS E. Research Diagnostic Criteria : rational and reliability. Arch Gen Psychiatry 1978 ; 35 : 773-82.

Cliquez ici pour aller à la section Références]}. All of those patients have been consecutively admitted to the Sleep Laboratory of the Department of Psychiatry, Erasme Hospital, between 1981 and 1992. This population has been previously reported elsewhere ^{[19HUBAIN P, VAN VEEREN C, STANER L et al . Neuroendocrine and sleep variables in major depressed inpatients : role of severity. Psychiatr Res 1996 ; 63 : 83-92.

Cliquez ici pour aller à la section Références]}^{[20HUBAIN PP. Contribution à l'étude des aspects cliniques et biologiques de la dépression majeure. Thèse de la Faculté de Médecine de Mons-Hainaut, 1997.

Cliquez ici pour aller à la section Références]}^{[21HUBAIN PP, STANER L, DRAMAIX M et al . The dexamethasone suppression test and sleep electroencephalogram in nonbipolar major depressed inpatients : a multivariate analysis. Biol Psychiatry 1998 ; 43 : 220-9.

Cliquez ici pour aller à la section Références]}. The depressive symptom severity was assessed with the 24-items HRSD ^{[17HAMILTON M. A rating scale for depression. J Neurol Neurosurg Psychiatry 1960 ; 23 : 56-62.

Cliquez ici pour aller à la section Références]}. The Newcastle Endogenous Depression Diagnostic Index was used to assess the endogenous character of the depressive episode ^{[5CARNEY MWP, ROTH M, GARSIDE F. The diagnostic of depressive symptoms and the prediction of ECT response. Br J Psychiatry 1965 ; 111 : 659-74.

Cliquez ici pour aller à la section Références]}. The history of the illness and the impact of psychosocial stressors were assessed retrospectively using the interview associated with the RDC ^{[41SPITZER RL, ENDICOTT J, ROBBINS E. Research Diagnostic Criteria : rational and reliability. Arch Gen Psychiatry 1978 ; 35 : 773-82.

Cliquez ici pour aller à la section Références]}, the SADS ^{[7CHARLES G, ANSSEAU M. Guides pour le diagnostic des troubles affectifs et de la schizophrénie. Acta Psychiatr Belgica 1987 ; 87 : 361-516.

Cliquez ici pour aller à la section Références]}. Psychosocial stressor has been assessed using the item 216 of the SADS. We must remind that it is not a precise measurement of stress. Results – Table I shows clinical characteristics and biological variables in our 130 depressed patients. No correlation were found between number of depressive episodes and DST or EEG sleep records ( table II ). Age of onset was correlated with DST and all sleep EEG parameters (REM latency, REM density, awakening and slow wave sleep). But the age was a major confounding factor. When corrected the results for age, a significant correlation between age of onset and DST still remained, but no correlation between age of onset and EEG sleep results ( table III ). The psychosocial stressors were correlated only with awakening. A positive trend was found between an augmentation of psychosocial stressors and the number of episodes (p = 0.06). Conclusion – This study does not support the view that the biological correlates of depression are worsening with the course of the illness. We found only correlation between age of onset and DST, but a possible confounding effect of age cannot formerly be excluded. The impact of psychosocial stressors on the biological correlates of depression was minimal. The only significant correlation found was between awakening and psychosocial stressors. We found no correlation between psychosocial stressors and the course of depression. Those results do not support the view of a sensitization of the illness, but it should be remember that evaluation of psychosocial stressors by item 216 of the SADS was probably not a sufficient sensitive measure. We suggest thus that the impact of the history of depression on biological correlates of depression is not very strong. An alternative explanation of the lack of correlation found is that we used inaccurate measurement of the course of depression. For example, we had no evaluation of the quality of remission between different episodes of depression and of subsyndromic depression. Recent works show the importance of this ^{[6CASTELNAU C, OLIÉ JP, LÔO H. Troubles dépressifs «subliminaires»: description et intérêt pour la prévention secondaire en psychiatrie. Encephale 1998 ; 24 : 405-14.

Cliquez ici pour aller à la section Références]}^{[9CORNWALL PL, SCOTT J. Partial remission in depressive disorders. Acta Psychiatr Scand 1997 ; 95 : 265-71.

Cliquez ici pour aller à la section Références]}. The major limitations of this work were the retrospective character of the study and the low precision of the evaluation of psychosocial stressors used.