Abnormal G protein αs- and αi2-subunit mRNA expression in bipolar affective disorder

Spleiss, Olivia; Calker, Dietrich van; Schärer, LO; Adamovic, K; Berger, Thomas; Gebicke-Haerter, P.J.

doi:10.1038/sj.mp.4000393

Cited by 39 publications

(28 citation statements)

References 38 publications

(50 reference statements)

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“…On the contrary, a possible trait marker was proposed when increased levels of G s were found without a correlation with the pharmacological treatment of the patient [129]. Similar results have been reported in granulocytes for the mRNA levels codifying for G s [171].…”

Section: Studies In Peripheral Tissue Of Depressive Patientssupporting

confidence: 69%

“…The densities of 45 kDa G s have been reported to be increased in prefrontal cortex of suicide victims with major depression [36,149]. A significant decrease in both [171] PTX, pertussis toxin mRNA and protein levels of G i2 and G o , and a significant increase in levels of 45 kDa G s have been observed in prefrontal cortex of suicide subjects. These alterations were reported to be independent of the retrospective psychiatric diagnosis [49].…”

Section: Studies In Postmortem Human Brain Of Depressed Subjectsmentioning

confidence: 85%

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Heterotrimeric G Proteins: Insights into the Neurobiology of Mood Disorders

González-Maeso

Meana²

2006

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Mood disorders such as major depression and bipolar disorder are common, severe, chronic and often lifethreatening illnesses. Suicide is estimated to be the cause of death in up to approximately 10-15% of individuals with mood disorders. Alterations in the signal transduction through G protein-coupled receptor (GPCR) pathways have been reported in the etiopathology of mood disorders and the suicidal behavior. In this regard, the implication of certain GPCR subtypes such as 2A -adrenoceptor has been repeatedly described using different approaches. However, several discrepancies have been recently reported in density and functional status of the heterotrimeric G proteins both in major depression and bipolar disorder. A compilation of the most relevant research topics about the implication of heterotrimeric G proteins in the etiology of mood disorders (i.e., animal models of mood disorders, studies in peripheral tissue of depressive patients, and studies in postmortem human brain of suicide victims with mood disorders) will provide a broad perspective of this potential therapeutic target field. Proposed causes of the discrepancies reported at the level of G proteins in postmortem human brain of suicide victims will be discussed.

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Section: Studies In Peripheral Tissue Of Depressive Patientssupporting

confidence: 69%

Section: Studies In Postmortem Human Brain Of Depressed Subjectsmentioning

confidence: 85%

Heterotrimeric G Proteins: Insights into the Neurobiology of Mood Disorders

González-Maeso

Meana²

2006

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“…Table 3 shows the results of experimental studies on the effects of ADs and lithium on signaling cascades in the rat brain, and [31][32][33][34][35][36][37][38] At variance with these data, a region-selective impairment of phosphoinositide hydrolysis was reported in the occipital cortex. 29 The reduction of cAMP binding 26 due to a decrease in the R subunits of cAMP-dependent protein kinase may actually increase kinase activity and protein phosphorylation at subsaturating cAMP concentrations.…”

Section: The Signal Transduction Cascadesmentioning

confidence: 60%

Affective disorders, antidepressant drugs and brain metabolism

2003

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There is increasing evidence that affective disorders are associated with dysfunction of neurotransmitter postsynaptic transduction pathways and that chronic treatment with clinically active drugs results in adaptive modification of these pathways. Despite the close dependence of signal transduction on adenosine triphosphate (ATP) availability, the changes in energy metabolism in affective disorders are largely unknown. This question has been indirectly dealt with through functional imaging studies (PET, SPECT, MRS). Despite some inconsistencies, PET and SPECT studies suggest low activity in cortical (especially frontal) regions in depressed patients, both unipolar and bipolar, and normal or increased activity in the manic pole. Preliminary MRS studies indicate some alterations in brain metabolism, with reduced creatine phosphate and ATP levels in the brain of patients with affective disorders. However, the involvement of the energy metabolism in affective disorders is still debated. We propose direct neurochemical investigations on mitochondrial functional parameters of energy transduction, such as the activities of (a) the enzymatic systems of oxidative metabolic cycle (Kreb's cycle); (b) the electron transfer chain; (c) oxidative phosphorylation, and (d) the enzyme activities of ATP-requiring ATPases. These processes should be studied in affective disorders and in animals treated with antidepressant drugs or lithium.

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“…30 Selecting candidates based on expression data also led to the detection of associations of Gprotein-coupled receptor kinase3 (GRK3) 31 and other promising gene 32 with bipolar disorder. Altered expression level of G protein AS and AI2 subunits (GNAS, GNAI2) in the post-mortem brains from bipolar or lithium receiving subjects has also been reported, 33 although variants in the former gene are not apparently associated with bipolar disorder. 34 Recent animal studies demonstrated that chronic administration of antidepressants induces elevation of cAMP-responsive element binding protein gene (CREB1) expression- 35 and cAMP-responsive element modulator (CREM)-deficient mice showed emotional and behavioral changes.…”

Section: Neurotransmission Systemsmentioning

confidence: 99%

Genetic tests of biologic systems in affective disorders

et al. 2005

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To liberate candidate gene analyses from criticisms of inexhaustiveness of examination of specific candidate genes, or incompleteness in the choice of candidate genes to study for specific neurobiological pathways, study of sizeable sets of genes pertinent to each putative pathophysiological pathway is required. For many years, genes have been tested in a 'one by one' manner for association with major affective disorders, primarily bipolar illness. However, it is conceivable that not individual genes but abnormalities in several genes within a system or in several neuronal, neural, or hormonal systems are implicated in the functional hypotheses for etiology of affective disorders. Compilation of candidate genes for entire pathways is a challenge, but can reasonably be carried out for the major affective disorders as discussed here. We present here five groupings of genes implicated by neuropharmacological and other evidence, which suggest 252 candidate genes worth examining. Inexhaustiveness of gene interrogation would apply to many studies in which only one polymorphism per gene is analyzed. In contrast to whole-genome association studies, a study of a limited number of candidate genes can readily exploit information on genomic sequence variations obtained from databases and/or resequencing, and has an advantage of not having the complication of an extremely stringent statistical criterion for association. Molecular Psychiatry (2005) 10, 719-740.

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Abnormal G protein αs- and αi2-subunit mRNA expression in bipolar affective disorder

Cited by 39 publications

References 38 publications

Heterotrimeric G Proteins: Insights into the Neurobiology of Mood Disorders

Heterotrimeric G Proteins: Insights into the Neurobiology of Mood Disorders

Affective disorders, antidepressant drugs and brain metabolism

Genetic tests of biologic systems in affective disorders

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