Clinical and genetic differences between bipolar disorder type 1 and 2 in multiplex families

Guzmán-Parra, José; Streit, Fabian; Forstner, Andreas J.; Strohmaier, Jana; Gonzalez, Maria J.; Flores, Susana Gil; Fabeiro, Francisco J. Cabaleiro; Noriega, Francisco del Río; Pérez, Fermín; González, Jesus Haro; Díaz, Guillermo Orozco; Diego-Otero, Yolanda de; Moreno‐Küstner, Berta; Auburger, Georg; Degenhardt, Franziska; Heilmann‐Heimbach, Stefanie; Herms, Stefan; Hoffmann, Per; Frank, Josef; Foo, Jerome C.; Sirignano, Lea; Witt, Stephanie H.; Cichon, Sven; Rivas, Fabio; Mayoral, Fermín; Nöthen, Markus M.; Andlauer, Till F. M.; Rietschel, Marcella

doi:10.1038/s41398-020-01146-0

Cited by 25 publications

(18 citation statements)

References 58 publications

(82 reference statements)

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“…The bipolar spectrum includes 7 of the 37 patients with bipolar disorder had committed suicide, a number close to known prevalence of death by suicide in BD. Suicide mainly occurs during the depressive state of the disease and – occasionally-during a manic episode and could be connected to certain patterns of gene expression [61], biomarker differences [63] and vary during an acute or prolonged depressive or manic or mixed episode) [64], including the cerebellum. Finally, the genetic characteristics of post-mortem brain tissue sampling could be divergent from the same characteristics of the living brain, in health and disease; still they remain one of the cornerstones of research on the neurobiology of the CNS and its disorders [65], [66], [67] [68].…”

Section: Discussionmentioning

confidence: 99%

A characteristic cerebellar biosignature for bipolar disorder, identified with fully automatic machine learning

Thomaidis

Michos

Papadimitriou³

et al. 2022

Preprint

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Objective: Complex machine learning classification algorithms using transcriptome data from post-mortem cerebellar tissue of bipolar patients and unaffected controls, have been recently included in pipelines for patient control classification and identification of characteristic biomarkers. Transcriptomic profile differences between patients and controls, can provide useful information about the role of the cerebellum in the pathogenesis of bipolar disorder and mood deregulation and in normal mood regulation and physiology. User-friendly, fully automated machine learning algorithms, using data extracted from established repositories, could achieve extremely high classification scores and disease- related predictive biomarker identification, in very short time frames and scaled down to small datasets, thus facilitating research on mood disorders. Method: An application of a fully automated machine learning platform, based on the most suitable algorithm selection and relevant set of hyper- parameter values, for classification between patients and controls and the production of models for biosignature selection, is presented. Transcriptome data used for the analysis were downloaded from the BioDataome preprocessed datasets database. The Dataome dataset, derived from the parent Gene Expression Omnibus GSE35974 (2013) and GSE35978 datasets, which have been originally produced from the cerebellar and parietal lobe tissue of deceased bipolar patients and unaffected controls, (from the Stanley Medical Research Institute Neuropathology Consortium and Array collections), using Affymetrix Human Gene 1.0 ST Array. Patient and control groups were closely matched for age and sex . Results: Bipolar patients have been identified from controls based on the cerebellar transcriptomic profile with AUC 0.929 and Average Precision 0.955. Patients and Controls have been classified in two separated groups with no close to the boundary cases. Using 6 of the characteristic features discovered during the selection process, 99,6% classification accuracy was achieved. The three biomarkers contributing most to the predictive power of the model (92,7%), are also deregulated in temporal lobe epilepsy. Conclusion: The cerebellar transcriptome of bipolar patients has a discrete profile and can be used for further exploration of the role of this area in health and disease. 93% AUC and 96% Precision were achieved during classification between unaffected controls and patients with Bipolar Disorder.

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Section: Discussionmentioning

confidence: 99%

A characteristic cerebellar biosignature for bipolar disorder, identified with fully automatic machine learning

Thomaidis

Michos

Papadimitriou³

et al. 2022

Preprint

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“… 53 Second, a comparison of bipolar disorder types 1 and 2 showed that these two groups do not have a similar profile of polygenic risk, at least regarding the risk of depression. 54 Third, bipolar disorder PRS are associated not only with other psychiatric phenotypes, but also with several clinical features and potential biomarkers in different psychiatric conditions. 55 Finally, certain clinically relevant features in bipolar disorder, such as response to lithium treatment or age at onset, are not associated with bipolar disorder PRS but are associated with other psychiatric PRS.…”

Section: Polygenicity and Polygenic Scoresmentioning

confidence: 99%

Genomic and neuroimaging approaches to bipolar disorder

et al. 2022

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Background To date, besides genome-wide association studies, a variety of other genetic analyses (e.g. polygenic risk scores, whole-exome sequencing and whole-genome sequencing) have been conducted, and a large amount of data has been gathered for investigating the involvement of common, rare and very rare types of DNA sequence variants in bipolar disorder. Also, non-invasive neuroimaging methods can be used to quantify changes in brain structure and function in patients with bipolar disorder. Aims To provide a comprehensive assessment of genetic findings associated with bipolar disorder, based on the evaluation of different genomic approaches and neuroimaging studies. Method We conducted a PubMed search of all relevant literatures from the beginning to the present, by querying related search strings. Results ANK3, CACNA1C, SYNE1, ODZ4 and TRANK1 are five genes that have been replicated as key gene candidates in bipolar disorder pathophysiology, through the investigated studies. The percentage of phenotypic variance explained by the identified variants is small (approximately 4.7%). Bipolar disorder polygenic risk scores are associated with other psychiatric phenotypes. The ENIGMA-BD studies show a replicable pattern of lower cortical thickness, altered white matter integrity and smaller subcortical volumes in bipolar disorder. Conclusions The low amount of explained phenotypic variance highlights the need for further large-scale investigations, especially among non-European populations, to achieve a more complete understanding of the genetic architecture of bipolar disorder and the missing heritability. Combining neuroimaging data with genetic data in large-scale studies might help researchers acquire a better knowledge of the engaged brain regions in bipolar disorder.

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“…Many of the samples studied include individuals with a broad range of bipolar spectrum disorders, and analyses did not differentiate those with bipolar I from those with bipolar II or cyclothymic disorders. Given increasing evidence for genetic differentiation in the forms of disorder [ 81 ], examining effects within subtypes will be an important goal for future research. It is also the case that most studies were only statistically powered to examine change in the level of manic symptoms, and not the onset or recurrence of disorder.…”

Section: Limitations and Future Directionsmentioning

confidence: 99%

Social and environmental variables as predictors of mania: a review of longitudinal research findings

Johnson

Weinberg

2022

Discov Ment Health

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Considerable evidence suggests that psychosocial variables can shape the course of bipolar disorder. Here, though, we focus on the more specific idea that the social environment can predict the course of mania. We systematically review evidence from longitudinal studies concerning how social support, family interactions, traumatic life events, and recent life events relate to the age of onset, the frequency of episode recurrence, and the severity of manic symptoms. Although we find some evidence that the course of mania can be worsened by social environmental factors, the links are specific. Among social variables, some studies indicate that conflict and hostility are predictive, but more general social relationship qualities have not been found to predict mania. Some research indicates that childhood trauma, and recent life events involving goal attainment or sleep disruption can predict mania. Taken together, the profile of variables involving recent exposure that are most predictive include those that are activating, reward-related, or sleep-disrupting, which fits with general psychological hypotheses of behavioral activation and sleep disruption as important for mania. We discuss gaps in the literature, and we note future directions for research, including the need for more integrative, longitudinal research on a fuller range of social and biological risk variables.

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Clinical and genetic differences between bipolar disorder type 1 and 2 in multiplex families

Cited by 25 publications

References 58 publications

A characteristic cerebellar biosignature for bipolar disorder, identified with fully automatic machine learning

A characteristic cerebellar biosignature for bipolar disorder, identified with fully automatic machine learning

Genomic and neuroimaging approaches to bipolar disorder

Social and environmental variables as predictors of mania: a review of longitudinal research findings

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