A meta-analysis of biotechnology genome-wide association data – Pubrica

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BIPOLAR AND MAJOR DEPRESSIVE DISORDER: A META-ANALYSIS OF BIOTECHNOLOGY GENOMEWIDE ASSOCIATION DATA An Academic presentation by Dr. Nancy Agnes, Head, Technical Operations, Pubrica Group: www.pubrica.com Email: sales@pubrica.com


TODAYS DISCUSSION In brief Introduction Evidence Support Continuity Between Major Depressive Disorder and Bipolar Disorders Factors of hypomania in major depressive disorder Conclusion About Pubrica


IN BRIEF

The Significant indirect evidence demonstrates that bipolar disorder (BIP) and major depressive disorder (MDD) are related (MDD). BIP and MDD have major depressive episodes in common; however, BIP is characterised by manic (bipolar 1) or hypomanic episodes in BIP (bipolar 2). Meta-Analysis

Writing

Services

Considering

overlap between genetic risk variables for both illnesses, genetic epidemiological and genomewide linkage studies are also consistent to discover common genetic risk factors.


To find common genetic risk factors, researchers conducted a survey. This blog reviews a meta-analysis combining data from genome-wide association studies by Liu and Youfang and coordinating with Blackwood (2009) for ascertainment and diagnostic assessment genotyping quality control and analysis.



INTRODUCTION Recent research has challenged conventional diagnosis approaches that divide mood disorders into two distinct categories: bipolar and depressive disorders. The present taxonomy of mood disorders opposes Kraepelin's concept of manic-depressive insanity as a single entity (illness). Recent study findings imply a relationship between bipolar disorders

(particularly

bipolar

II

disorder)

and

major

depressive disorder. The following features currently point to a link between bipolar II disease and major depressive disorder:


Mixed depressive states (mixed depression) and dysphoric (mixed) hypomania (opposite polarity symptoms in the same episode do not support mood disorder splitting); Family history (major depressive disorder is the most common mood disorder in relatives of bipolar probands); Lack of points of equivalence between the depressive syndromes of bipolar II disorder and major depressive disorder; Bipolar major depressive illness with depression mixed states, early-onset age, atypical characteristics, bipolar family history, irritability, racing thoughts, and psychomotor agitation;


A high proportion of major depressive disorders shift to bipolar disorders during longterm follow-up; A large proportion of people with serious depression have a history of manic or hypomanic symptoms; Factors of hypomania present in major depressive disorder episodes; The recurrent course of major depressive disorder; and Depressive symptoms are much more common than manic and hypomanic symptoms in the study of bipolar disorders.


EVIDENCE SUPPORT CONTINUITY BETWEEN MAJOR DEPRESSIVE DISORDER AND BIPOLAR DISORDERS Bipolar disorder bipolar II is the most similar to major depressive disorder. As

a

result,

Meta-Analysis

Experts

pursuing

consistency focused on the connections between these two illnesses. There are some similarities between bipolar II illness and major depressive disorder.


The procedures for determining, diagnosing, genotyping, quality control, and analysis are described elsewhere. Both investigations were carried out with the necessary ethical permissions, and all participants gave written informed consent. The majority of cases (81%) fulfilled DSM-IV (Diagnostic and Statistical Manual of Mental Disorders-IV) bipolar 1 criteria, with a lesser proportion (16%) fulfilling criteria for bipolar 2 (16%), schizoaffective disorder/manic type (2%), or bipolar NOS (not otherwise specified) criteria (1% ).


Single nucleotide polymorphisms (SNPs) were evaluated after quality control (18.7% were genotyped directly, and the rest were imputed). Cases satisfying DSM-IV (Diagnostic and Statistical Manual of Mental DisordersIV) criteria for MDD were found in clinical and community sources, while controls with low MDD risk were chosen from a population sample. Excessive missingness, uncommon genome-wide heterozygosity, and first- or second-generation mutations were all reasons for subjects being excluded.


Depressive mixed states were seen in around 30% of individuals with major depressive illness. Apart from the raised mood factor, the

FACTORS OF HYPOMANIA IN MAJOR DEPRESSIVE DISORDER

factor structure of hypomania (outside depression) was comparable to that of depressed mixed states.


In depressive diverse states (of major depressive disorder and bipolar II disorder), two hypomanic factors were found: the most common was a mental activation factor, which included racing and crowded thoughts and irritability, and the other was a motor activation factor, which included psychomotor agitation and more talkativeness. The occurrence of hypomania aspects inside the depression of major depressive disorder suggests that bipolar II disorder and major depressive disorder are associated. It was found that depression and depressive symptoms were much more common than mania, hypomania, and manic and hypomanic symptoms in bipolar disorders (especially bipolar II disorder). This finding supports a link between bipolar disorders and major depressive disorder


CONCLUSION CACNA1C risk polymorphisms may have a role in bipolar and unipolar major mood disorders, according to these Clinical MetaAnalysis Experts. According

to

certain

theories,

genetic

variation in CACNA1C might be a frequent, modest, and pleomorphic risk factor for mental disorders.


Alternatively, the overlap might be due to misclassification—for example, if some MDD patients were actually "bipolar-like" but were misclassified owing to diagnostic or nosological mistakes (despite using conventional and meticulous techniques), or if some BIP patients were similarly misclassified. The bipolar risk locus ANK3, on the other hand, received no support in this metaanalysis, indicating that its effect may be limited to BIP or that the power to detect an effect was low.


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