The Common Pathophysiology of Monoaminergic Psychoses: a New Hypothesis

The purpose of this study was to examine whether biological variables, such as erythrocyte membrane transports and plasma levels of monoamine precursor amino acids (tyrosine, tryptophan and phenylalanine), exhibit a particular pattern relatively to DSM-III depressive subgroups (dysthymic disorders, major recurrent depression and biopolar depression), when they are treated synthetically by a stepwise discriminant analysis. We conducted two tests in 97 subjects (64 depressed patients vs. 33 controls): the first before any antidepressant treatment, and the second after pharmacotherapy and clinical improvement. Our results clearly indicate a satisfying homogeneity for the controls and bipolar depressed patients as opposed to dysthymic disorders and major recurrent depression in both tests. The most informative biological variables are the erythrocyte membrane transports before treatment, tryptophan parameters after clinical improvement. Evidence is provided that multivariate analysis constitutes an interesting approach in biological psychiatry.

Section: Discussionmentioning

confidence: 53%

Section: Discussionmentioning

confidence: 99%

A Multivariate Analysis of Red Blood Cell Membrane Transports and Plasma Levels of L-Tyrosine and L-Tryptophan in Depressed Patients before Treatment and after Clinical Improvement

Chiaroni

Azorin²,

Bovier

et al. 1990

“…Monoamines as well as their precursors, the amino acids ¿-tyrosine (TYR) and ¿-tryptophan (TRP), have been implicated in biological mechanisms of mood dis orders [Wurtman and Fernstrom, 1972;Tissot, 1975;Coppen and Wood, 1978;Möller et al, 1983], Prelimi nary studies have measured the arteriovenous differ ences of these two amino acid concentrations: the blood transport of TYR to the brain was reduced in depressed patients whereas transport of TRP was increased. More over a close relationship was observed between the blood-brain barrier and plasma red cell transport of TRP (r = 0.946, p < 0.01) [Tissot et al, 1978;Gaillard and Tissot, 1979;Tissot, 1984], This observation brought us to use the red cell membrane as a peripheral model to further investigate the transport mechanism of these two amino acids [Widmer et al, 1982], In a previous study we showed that in depressed bipo lar subjects (DSM III criteria: 296.5 x), erythrocyte mem brane transport (MT) of TYR was significantly lower than in normal subjects (p < 0.001), and MT TRP remained within the normal range.…”

Section: Introductionmentioning

confidence: 99%

Evolution of Red Blood Cell Membrane Transport and Plasma Level of L-Tyrosine and L-Tryptophan in Depressed Treated Patients According to Clinical Improvement

Bovier¹,

Widmer²,

Gaillard³

et al. 1988

The erythrocyte membrane transport (MT) of L-tyrosine (TYR) and L-tryptophan (TRP) and their plasma concentration showed abnormal mean values in 37 depressed patients compared to control subjects before treatment. The pattern of these abnormal values differed according to the clinical subgroup (DSM III criteria). In bipolar disorders the TYR values were all low and the TRP values showed little change, except a low level of plasma TRP. In major depressions, MT were abnormal (MT TYR low, MT TRP high) with a very low plasma TRP. In dysthymic disorders the TYR and TRP values were normal. The normalization of the above biochemical variables was significantly correlated with the clinical improvement; however, the plasma concentration of TRP remained abnormal in some patients who had recovered. In contrast, only plasma TYR and TRP were significantly increased in patients without recovery.

“…Rappelons que, pour la psychose maniaco-dépressive, quatre hypothèses concurrentes ou complémentaires ont cours: sérotoninergique (2); catécholaminergique (9,10); rapport sérotonine/ catécholamines augmenté (13) et ionique (3,4). Pour la schizophrénie, deux hypothèses complémentaires semblent solides: dopaminergique (12) et rapport dopamine/sérotonine augmenté (11,13). L'un de nous (13) a proposé la synthèse suivante: les perturbations des métabolismes rappelées ci-dessus pour raient être corrélées à des modifications de la capture par le cerveau du trypto phane et de la tyrosine circulants.…”

Section: Introductionunclassified

“…Si l'on admet que le 5-HTP et la ¿-dopa sont très probablement transportés par le même système que le tryptophane et la tyrosine (7) et que la production de 5-HT et de DA, à partir du ¿-5-HTP et de la /.-dopa, qui ont pénétré dans le cerveau, n'est pas limitée par l'étape de l'hydroxylation, on peut attendre qu'une perfusion de ¿-5-HTP ou de ¿-dopa, tant par compétition directe au niveau des mécanismes de transport que par régulation rétroactive de ces derniers sous l'effet de la production, dans le cerveau, de 5-HT et de DA, provoque des modifications importantes de la capture du tryptophane et de la tyrosine endogènes (13). Ce travail, mené conjointement par le Service de Psychiatrie de l'Institut national de Neurologie de Mexico et de la Clinique universitaire de Psychiatrie de Genève, constitue un premier essai de vérification de ce modèle.…”

Section: Introductionunclassified

Capture du tryptophane et de la tyrosine plasmatiques dans quelques cas de psychose maniaco-dépressive et de schizophrénie

Tissot¹,

Castellanos²,

Gaillard³

et al. 1978

Self Cite

The uptake of tryptophan and tyrosine by the brain has been studied in 6 manic-depressive patients and in 8 schizophrenics. In an attempt to saturate the blood-brain transport mechanisms, this uptake has been evaluated by measuring the arteriovenous differences (arterial plasma-internal jugular plasma) of these two amino acids before and after perfusion with Z,-dopa and L-5-HTP. Considering a positive difference as an uptake and a negative one as an outflow, results show (1) in melancholia an uptake of tryptophan and an outflow of tyrosine; (2) in mania an uptake of tyrosine and an outflow of tryptophan, and (3) in schizophrenia an outflow of tryptophan accompanied with either an uptake or an outflow of tyrosine. In addition, the kinetics of tryptophan binding to plasma proteins and the ratio of tryptophan/tyrosine uptake are different in manic-depressive illness and in schizophrenia. These results support the view that a disturbance in the blood-brain transport mechanisms of tryptophan and tyrosine could be involved in the physiopathology of manic-depressive illness and schizophrenia.