A comparative study on psychiatric disorders: Identification of shared pathways and common agents
Abstract
Distinct but closely related diseases generally
present shared symptoms, which address possible overlaps
among their pathogenic mechanisms. Identification of
significantly impacted shared pathways and other common
agents are expected to elucidate etiology of these disorders and
to help design better intervention strategies. In this research
effort, we studied six psychiatric disorders including
schizophrenia (SCZ), anorexia (AN), bipolar disorder (BD),
depressive disorder (DD), autism (AU) and attention deficit
hyperactivity disorder (ADHD). Our methodology can be
classified into the following two parts: In Part I, common
susceptibility genes; and in Part II, genome-wide association
studies (GWAS) data were used to find enriched pathways of
psychiatric disorders. 59 KEGG pathways were commonly
identified in both parts. 31 of these pathways are disease
pathways. Pathways related to cancer and infectious diseases
were predominant compared to others. Most of the acquired
pathways were in accordance with previous studies in literature.
A combination of susceptibility genes and GWAS data is an
effective approach to identify significantly impacted pathways
in multifactorial diseases. In this respect, shared modules were
determined after applying hierarchical clustering of the
enriched pathways. These identified modules may tell us the
association of psychiatric disorders with the enriched pathways.
Taken all together, common pathways and shared modules are
expected to highlight the causative factors and important
mechanisms behind complex psychiatric diseases, leading to
effective drug discovery.