Skip to main content
Schizophrenia is a uniquely human, enormously complex neurodevelopmental disorder (1, 2), characterized by a combination of genetic susceptibility factors and environmental insults that converge on a developmental timeline (3, 4). The recent emergence of high-throughput, unbiased genetic assessment methods such as genome-wide association studies (GWAS), combined with assessments of several thousand patients have provided us with a better understanding of the underlying genetics of schizophrenia (5). It appears that two often-interrelated genetic mechanisms are at work. The first mechanism encompasses rare, almost individually specific genome changes where small chromosomal regions are either deleted or duplicated (referred to as copy number variants [CNVs]) (6) and have strong disease-predisposing effects (7). The second mechanism is related to common variants in our genome that are found in both healthy individuals and those with disorders, but with slightly different frequencies. On their own, each of these common single-nucleotide polymorphisms (SNPs) are only small contributors to the emergence of the disease, but in large numbers and in the right combinations they can explain a significant proportion of the genetic underpinnings of the disease (5).
Many previously published study results suggest that genetic susceptibility, either from SNPs or CNVs, converge with environmental insults and jointly alter the gene expression (mRNA production) of the developing brain (3). This tips the balance of neurochemistry and alters the connectivity and information processing of the brain, ultimately resulting in complex behavioral changes, which we recognize as a diagnosis (8). This mechanism holds true not only for schizophrenia but for a host of other neurodevelopmental disabilities, including autism spectrum disorders (ASD).
Several years ago, a group of investigators led by Dr. Joel Kleinman created an interesting, and much underappreciated, data set, termed BrainCloud (9). This resource cataloged mRNA expression levels from 269 human postmortem dorsolateral prefrontal cortical samples ranging from fetal life up to 80 years of age, providing us with a glimpse into the molecular processes that shape the emergence of our cognitive abilities. The present study of Birnbaum et al. (10) in this issue of the Journal further builds on this data set, attempting to link brain development to neuropsychiatric diseases. The central premise of their study is simple, but often underappreciated: if we want to understand uniquely human neuropsychiatric and neurodevelopmental disorders, a significant set of clues will come from understanding human brain development itself (11).
Birnbaum et al. (10) first defined genes with “fetal effect,” and found that 25% of the more than 30,000 gene probes revealed transcript levels that were overexpressed or underexpressed in fetal life compared with the postnatal period. Then, they defined sets of risk genes that have been implicated as disease-predisposing for six neuropsychiatric disorders, including syndromic neurodevelopmental disorders, ASD, intellectual disability, schizophrenia, bipolar affective disorder, and neurodegenerative disorders. The authors then employed various statistical approaches as they explored the expression of these disease-predisposing gene sets in the BrainCloud data set. The outcome of this experiment was quite revealing: the authors observed increased fetal expression of disease-predisposing genes for syndromic neurodevelopmental disorders, intellectual disability, and ASD. In contrast, a statistically significant fetal underexpression of transcripts was reported for the gene set associated with neurodegenerative disorders. In a secondary analysis, the authors found that the ASD findings were a result of enrichment in transcripts originating from rare variants (CNVs) rather than the common variants (SNPs). Surprisingly, the group of schizophrenia or bipolar disease-predisposing genes (originating either from SNP, CNV, or exome sequencing studies) did not show enrichment in either direction. However, although the majority of schizophrenia susceptibility genes did not show fetal effects, these genes were still found to be important for neural development: gene ontology classification (12) revealed that they belonged to gene pathways related to “nervous system development” and “neuron differentiation.” Furthermore, within each CNV locus associated with schizophrenia, one or two genes were enriched in prenatal abundance, suggesting that they might be of particular relevance for disease-associated fetal pathogenesis.
Every excellent study raises a host of new questions and lays the foundation of new experiments, and the research endeavor of Birnbaum et al. is not different in this regard. First, this study can be considered a proof of principle endeavor, with limited resolution. The transcriptome of different brain cell types is unique, and we do not know if the observed correlations are limited to certain subpopulations of cells or if they are characteristic of multiple brain regions. Regional transcriptomes are complexly regulated, and combining the approach of the present study with high-quality spatio-temporal data sets and analyses (1315) will further increase the resolution and specificity of these findings.
Second, it is surprising that present findings do not support a fetal effect associated with schizophrenia-predisposing genes derived from GWAS, CNV analysis, or exome sequencing of rare variants. However, the lack of this association should not be interpreted as proof that schizophrenia is not a neurodevelopmental disorder: the findings may suggest technical limitations of including inappropriately large or not well-established chromosomal regions in the study. Furthermore, we cannot exclude the possibility that the fetal effect is present in other regions (e.g., other neocortical, hippocampal, or subcortical areas), or that the schizophrenia-associated neurodevelopmental processes may be transcriptome-independent. Differentiating between these possibilities should be a focus of further studies.
Third, the authors found a surprising signature for genes involved in neurodegeneration. This is a very intriguing finding, and it suggests a dichotomy between neurodevelopmental and neurodegenerative mechanisms from the early onset: disruption of genes with enriched fetal expression leads to diseases that manifest with symptoms in early postnatal life, while the low expression of the neurodegenerative genes during prenatal development “postpones” the pathophysiology of neurodevelopmental disorders to later postnatal time periods. Simply, one can argue that disruption of genes with high expression during fetal life affects “brain construction,” while genes expressed at low levels prenatally are responsible for “brain maintenance” later in life.
The study also highlights the urgent need for better bioinformatics tools. We are generating GWAS, DNA and RNA sequence, and gene expression data at an amazing speed and volume. While tools for data mining of specific data types are developing at a reasonable pace, the tools and standards of integrating data sets from different sources significantly lag behind (16). Without them we are not able to observe the meaningful relationships between data sets, and the generated data remains only moderately informative.
Does the present study uncover the essence of schizophrenia, autism, or other neuropsychiatric disorders? Of course not. Over the last decades we have learned that nothing is ever conclusive in schizophrenia or ASD research. There is no smoking gun. There are no simple interpretations. But every day we are gathering more pieces of this enormous jigsaw puzzle, and the studies by Birnbaum et al. might just represent one of the important corner pieces. Recently, when visiting Cold Spring Harbor Laboratories I asked Dr. James Watson if he was aware of the enormity of the DNA discovery at the time when it was made. After a short pause and a walk back down memory lane, he responded with a smile: “We were not thinking about that.” Perhaps we should learn from this example and focus on accumulating high-quality data, noticing the important relationships rather than trying to solve the disease. And over time, when we have enough puzzle pieces from the many various research domains, the picture of schizophrenia and other disorders will emerge. But I admit: it is so hard to wait!

References

1.
Lewis DA, Levitt P: Schizophrenia as a disorder of neurodevelopment. Annu Rev Neurosci 2002; 25:409–432
2.
Weinberger DR: Implications of normal brain development for the pathogenesis of schizophrenia. Arch Gen Psychiatry 1987; 44:660–669
3.
Horváth S, Mirnics K: Schizophrenia as a disorder of molecular pathways. Biol Psychiatry (Epub ahead of print, Jan 10, 2014)
4.
Horváth S, Mirnics K: Immune system disturbances in schizophrenia. Biol Psychiatry 2014; 75:316–323
5.
Ripke S, O’Dushlaine C, Chambert K, Moran JL, Kähler AK, Akterin S, Bergen SE, Collins AL, Crowley JJ, Fromer M, Kim Y, Lee SH, Magnusson PK, Sanchez N, Stahl EA, Williams S, Wray NR, Xia K, Bettella F, Borglum AD, Bulik-Sullivan BK, Cormican P, Craddock N, de Leeuw C, Durmishi N, Gill M, Golimbet V, Hamshere ML, Holmans P, Hougaard DM, Kendler KS, Lin K, Morris DW, Mors O, Mortensen PB, Neale BM, O’Neill FA, Owen MJ, Milovancevic MP, Posthuma D, Powell J, Richards AL, Riley BP, Ruderfer D, Rujescu D, Sigurdsson E, Silagadze T, Smit AB, Stefansson H, Steinberg S, Suvisaari J, Tosato S, Verhage M, Walters JT, Levinson DF, Gejman PV, Kendler KS, Laurent C, Mowry BJ, O’Donovan MC, Owen MJ, Pulver AE, Riley BP, Schwab SG, Wildenauer DB, Dudbridge F, Holmans P, Shi J, Albus M, Alexander M, Campion D, Cohen D, Dikeos D, Duan J, Eichhammer P, Godard S, Hansen M, Lerer FB, Liang KY, Maier W, Mallet J, Nertney DA, Nestadt G, Norton N, O’Neill FA, Papadimitriou GN, Ribble R, Sanders AR, Silverman JM, Walsh D, Williams NM, Wormley B, Arranz MJ, Bakker S, Bender S, Bramon E, Collier D, Crespo-Facorro B, Hall J, Iyegbe C, Jablensky A, Kahn RS, Kalaydjieva L, Lawrie S, Lewis CM, Lin K, Linszen DH, Mata I, McIntosh A, Murray RM, Ophoff RA, Powell J, Rujescu D, Van Os J, Walshe M, Weisbrod M, Wiersma D, Donnelly P, Barroso I, Blackwell JM, Bramon E, Brown MA, Casas JP, Corvin AP, Deloukas P, Duncanson A, Jankowski J, Markus HS, Mathew CG, Palmer CN, Plomin R, Rautanen A, Sawcer SJ, Trembath RC, Viswanathan AC, Wood NW, Spencer CC, Band G, Bellenguez C, Freeman C, Hellenthal G, Giannoulatou E, Pirinen M, Pearson RD, Strange A, Su Z, Vukcevic D, Donnelly P, Langford C, Hunt SE, Edkins S, Gwilliam R, Blackburn H, Bumpstead SJ, Dronov S, Gillman M, Gray E, Hammond N, Jayakumar A, McCann OT, Liddle J, Potter SC, Ravindrarajah R, Ricketts M, Tashakkori-Ghanbaria A, Waller MJ, Weston P, Widaa S, Whittaker P, Barroso I, Deloukas P, Mathew CG, Blackwell JM, Brown MA, Corvin AP, McCarthy MI, Spencer CC, Bramon E, Corvin AP, O’Donovan MC, Stefansson K, Scolnick E, Purcell S, McCarroll SA, Sklar P, Hultman CM, Sullivan PF; Multicenter Genetic Studies of Schizophrenia ConsortiumPsychosis Endophenotypes International ConsortiumWellcome Trust Case Control Consortium 2: Genome-wide association analysis identifies 13 new risk loci for schizophrenia. Nat Genet 2013; 45:1150–1159
6.
Malhotra D, Sebat J: CNVs: harbingers of a rare variant revolution in psychiatric genetics. Cell 2012; 148:1223–1241
7.
Purcell SM, Moran JL, Fromer M, Ruderfer D, Solovieff N, Roussos P, O’Dushlaine C, Chambert K, Bergen SE, Kähler A, Duncan L, Stahl E, Genovese G, Fernández E, Collins MO, Komiyama NH, Choudhary JS, Magnusson PK, Banks E, Shakir K, Garimella K, Fennell T, DePristo M, Grant SG, Haggarty SJ, Gabriel S, Scolnick EM, Lander ES, Hultman CM, Sullivan PF, McCarroll SA, Sklar P: A polygenic burden of rare disruptive mutations in schizophrenia. Nature 2014; 506:185–190
8.
Horváth S, Mirnics K: Breaking the gene barrier in schizophrenia. Nat Med 2009; 15:488–490
9.
Colantuoni C, Lipska BK, Ye T, Hyde TM, Tao R, Leek JT, Colantuoni EA, Elkahloun AG, Herman MM, Weinberger DR, Kleinman JE: Temporal dynamics and genetic control of transcription in the human prefrontal cortex. Nature 2011; 478:519–523
10.
Birnbaum R, Jaffe AE, Hyde TM, Kleinman JE, Weinberger DR: Prenatal expression patterns of genes associated with neuropsychiatric disorders. Am J Psychiatry 2014; 171:758–767
11.
Tebbenkamp AT, Willsey AJ, State MW, Sestan N: The developmental transcriptome of the human brain: implications for neurodevelopmental disorders. Curr Opin Neurol 2014; 27:149–156
12.
Ashburner M, Ball CA, Blake JA, Botstein D, Butler H, Cherry JM, Davis AP, Dolinski K, Dwight SS, Eppig JT, Harris MA, Hill DP, Issel-Tarver L, Kasarskis A, Lewis S, Matese JC, Richardson JE, Ringwald M, Rubin GM, Sherlock G; The Gene Ontology Consortium: Gene ontology: tool for the unification of biology. Nat Genet 2000; 25:25–29
13.
Kang HJ, Kawasawa YI, Cheng F, Zhu Y, Xu X, Li M, Sousa AM, Pletikos M, Meyer KA, Sedmak G, Guennel T, Shin Y, Johnson MB, Krsnik Z, Mayer S, Fertuzinhos S, Umlauf S, Lisgo SN, Vortmeyer A, Weinberger DR, Mane S, Hyde TM, Huttner A, Reimers M, Kleinman JE, Sestan N: Spatio-temporal transcriptome of the human brain. Nature 2011; 478:483–489
14.
Pletikos M, Sousa AM, Sedmak G, Meyer KA, Zhu Y, Cheng F, Li M, Kawasawa YI, Sestan N: Temporal specification and bilaterality of human neocortical topographic gene expression. Neuron 2014; 81:321–332
15.
Johnson MB, Kawasawa YI, Mason CE, Krsnik Z, Coppola G, Bogdanović D, Geschwind DH, Mane SM, State MW, Sestan N: Functional and evolutionary insights into human brain development through global transcriptome analysis. Neuron 2009; 62:494–509
16.
Liu L, Lei J, Sanders SJ, Willsey AJ, Kou Y, Cicek AE, Klei L, Lu C, He X, Li M, Muhle RA, Ma’ayan A, Noonan JP, Sestan N, McFadden KA, State MW, Buxbaum JD, Devlin B, Roeder K: DAWN: a framework to identify autism genes and subnetworks using gene expression and genetics. Mol Autism 2014; 5:22

Information & Authors

Information

Published In

Go to American Journal of Psychiatry
Go to American Journal of Psychiatry
American Journal of Psychiatry
Pages: 705 - 708
PubMed: 24980163

History

Accepted: April 2014
Published online: 1 July 2014
Published in print: July 2014

Authors

Details

Szatmár Horváth, M.D., Ph.D.
From the Department of Psychiatry and the Vanderbilt Kennedy Center for Research on Human Development, Vanderbilt University, Nashville, Tenn., and the Department of Psychiatry, University of Szeged, Hungary.
Károly Mirnics, M.D., Ph.D.
From the Department of Psychiatry and the Vanderbilt Kennedy Center for Research on Human Development, Vanderbilt University, Nashville, Tenn., and the Department of Psychiatry, University of Szeged, Hungary.

Notes

Address correspondence to Dr. Mirnics ([email protected]).

Funding Information

The authors report no financial relationships with commercial interests.Dr. Mirnics is supported by NIMH grants R01MH067234 and R01 MH079299.

Metrics & Citations

Metrics

Citations

Export Citations

If you have the appropriate software installed, you can download article citation data to the citation manager of your choice. Simply select your manager software from the list below and click Download.

For more information or tips please see 'Downloading to a citation manager' in the Help menu.

Format
Citation style
Style
Copy to clipboard

View Options

View options

PDF/EPUB

View PDF/EPUB

Get Access

Login options

Already a subscriber? Access your subscription through your login credentials or your institution for full access to this article.

Personal login Institutional Login Open Athens login
Purchase Options

Purchase this article to access the full text.

PPV Articles - American Journal of Psychiatry

PPV Articles - American Journal of Psychiatry

Not a subscriber?

Subscribe Now / Learn More

PsychiatryOnline subscription options offer access to the DSM-5-TR® library, books, journals, CME, and patient resources. This all-in-one virtual library provides psychiatrists and mental health professionals with key resources for diagnosis, treatment, research, and professional development.

Need more help? PsychiatryOnline Customer Service may be reached by emailing [email protected] or by calling 800-368-5777 (in the U.S.) or 703-907-7322 (outside the U.S.).

Media

Figures

Other

Tables

Share

Share

Share article link

Share