Will Brain Cells Derived From Induced Pluripotent Stem Cells or Directly Converted From Somatic Cells (iNs) Be Useful for Schizophrenia Research?

Filippich, Cheryl; Wolvetang, Ernst J.; Mowry, Bryan

doi:10.1093/schbul/sbt103

Cited by 2 publications

(1 citation statement)

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“…Finding loci and genes for schizophrenia is a triumph, but it is merely the start of a long process towards meaningful biological understanding, let alone better treatment, of the disorder. Genetics augments but does not replace the other key elements in drug development, and does not remove the many other hurdles ( Filippich et al, 2013 ; Hyman, 2014 ; Pratt et al, 2012 ; Winchester et al, 2014 ). But at least the genetic findings provide a strong rationale for, and firm foundations on which to build, the next generation of studies, as we sequence rather than sample the genome, integrate genomics with the other ‘omics’, develop new analytical and bioinformatic tools, discover how genes interact with each other and with the environment, and clarify how the genes and their variants actually drive the pathophysiology.…”

Section: Discussionmentioning

confidence: 99%

Recent genetic findings in schizophrenia and their therapeutic relevance

2014

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Over 100 loci are now associated with schizophrenia risk as identified by single nucleotide polymorphisms (SNPs) in genome-wide association studies. These findings mean that ‘genes for schizophrenia’ have unquestionably been found. However, many questions remain unanswered, including several which affect their therapeutic significance. The SNPs individually have minor effects, and even cumulatively explain only a modest fraction of the genetic predisposition. The remainder likely results from many more loci, from rare variants, and from gene–gene and gene–environment interactions. The risk SNPs are almost all non-coding, meaning that their biological significance is unclear; probably their effects are mediated via an influence on gene regulation, and emerging evidence suggests that some key molecular events occur during early brain development. The loci include novel genes of unknown function as well as genes and pathways previously implicated in the pathophysiology of schizophrenia, e.g. NMDA receptor signalling. Genes in the latter category have the clearer therapeutic potential, although even this will be a challenging process because of the many complexities concerning the genetic architecture and mediating mechanisms. This review summarises recent schizophrenia genetic findings and some key issues they raise, particularly with regard to their implications for identifying and validating novel drug targets.

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