Childhood developmental disorders: an academic and clinical convergence point for psychiatry, neurology, psychology and pediatrics

doi:10.1111/j.1469-7610.2008.02046.x

Review

. 2009 Jan;50(1-2):87-98.

doi: 10.1111/j.1469-7610.2008.02046.x.

Childhood developmental disorders: an academic and clinical convergence point for psychiatry, neurology, psychology and pediatrics

Allan L Reiss¹

Affiliations

PMID: 19220592
PMCID: PMC5756732
DOI: 10.1111/j.1469-7610.2008.02046.x

Review

Childhood developmental disorders: an academic and clinical convergence point for psychiatry, neurology, psychology and pediatrics

Allan L Reiss. J Child Psychol Psychiatry. 2009 Jan.

. 2009 Jan;50(1-2):87-98.

doi: 10.1111/j.1469-7610.2008.02046.x.

Author

Allan L Reiss¹

Affiliation

¹ Center for Interdisciplinary Brain Sciences Research, Stanford University School of Medicine, 401 Quarry Road, Stanford, CA 94305, USA. reiss@stanford.edu

PMID: 19220592
PMCID: PMC5756732
DOI: 10.1111/j.1469-7610.2008.02046.x

Abstract

Background: Significant advances in understanding brain development and behavior have not been accompanied by revisions of traditional academic structure. Disciplinary isolation and a lack of meaningful interdisciplinary opportunities are persistent barriers in academic medicine. To enhance clinical practice, research, and training for the next generation, academic centers will need to take bold steps that challenge traditional departmental boundaries. Such change is not only desirable but, in fact, necessary to bring about a truly innovative and more effective approach to treating disorders of the developing brain.

Methods: I focus on developmental disorders as a convergence point for transcending traditional academic boundaries. First, the current taxonomy of developmental disorders is described with emphasis on how current diagnostic systems inadvertently hinder research progress. Second, I describe the clinical features of autism, a phenomenologically defined condition, and Rett and fragile X syndromes, neurogenetic diseases that are risk factors for autism. Finally, I describe how the fields of psychiatry, psychology, neurology, and pediatrics now have an unprecedented opportunity to promote an interdisciplinary approach to training, research, and clinical practice and, thus, advance a deeper understanding of developmental disorders.

Results: Research focused on autism is increasingly demonstrating the heterogeneity of individuals diagnosed by DSM criteria. This heterogeneity hinders the ability of investigators to replicate research results as well as progress towards more effective, etiology-specific interventions. In contrast, fragile X and Rett syndromes are 'real' diseases for which advances in research are rapidly accelerating towards more disease-specific human treatment trials.

Conclusions: A major paradigm shift is required to improve our ability to diagnose and treat individuals with developmental disorders. This paradigm shift must take place at all levels - training, research and clinical activity. As clinicians and scientists who are currently constrained by disciplinary-specific history and training, we must move towards redefining ourselves as clinical neuroscientists with shared interests and expertise that permit a more cohesive and effective approach to improving the lives of patients.

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Conflict of interest statement

Conflict of interest statement: No conflicts declared.

Figures

**Figure 1**
A conceptualization of the current state of phenomenologically defined (e.g., DSM or ICD) disorders. In the center is a DSM-IV defined diagnosis, here shown with autism as the example. Multiple biological and environmental factors (shown around the periphery) modify risk for the development of aberrant ‘neural pathways’ during brain development. Some of these risk factors are of moderate or greater influence (e.g., MeCP2 mutations that lead to Rett syndrome shown here), and thus are able to increase the likelihood of brain dysfunction with relatively less influence from other genetic or environmental factors. Other factors, such as *FMR1* mutations associated with fragile X syndrome (also shown in the figure), may contribute moderately increased risk for autistic behavior. However, this risk can be moderated by measurable environmental factors related to the home and school (Hessl et al., 2001). ‘Neural pathways’ leading to manifestations of DSM defined disorders (shown as the intermediate step between risk factors and diagnosis) also would be expected to vary for a given DSM diagnosis, even though they might result in a (somewhat) similar phenotype. Examples of neural pathways influenced by *FMR1* mutations are shown in the figure (mGluR-metabotropic glutamate receptor, Ach-Acetylcholine system, GABA-gamma-aminobutyic acid). Given the lack of scientific precision of such phenomenologically based diagnostic taxonomies, alternatives to the DSM should be strongly considered for future research studies focused on elucidating the pathogenesis of (currently) idiopathic developmental disorders

**Figure 2**
The genetic basis for the fragile X full mutation. *FMR1* gene from X chromosome shown on left under typical conditions. Modal trinucleotide (CGG) repeat length is 29–30. Significantly expanded CGG repeats in the *FMR1* full mutation (right) lead to hypermethylation (CH₃), transcriptional repression and reduced levels of FMRP. Reduced levels of FMRP lead to neurobiological dysfunction and the cognitive-behavioral phenotype (also see Figure 3)

**Figure 3**
A hierarchical model for planning treatment strategies in fragile X syndrome. The left-hand side of the diagram shows the genetic and neurobiological mechanisms leading to brain dysfunction in this condition. Specifically, the *FMR1* mutation causes reduction in FMRP, leading to transcriptional dysregulation of FMRP mRNA targets (involved in synapse maturation and function). Other (non-*FMR1* related) genetic and environmental factors interact with this genetic-neurobiological pathway, ultimately culminating in the cognitive-behavioral phenotype associated with fragile X. The right-hand side of the diagram shows potential treatment approaches matched to the corresponding genetic and pathophysiological level on the left. Given that gene therapy approaches are not feasible at the present time, the most promising current approaches are at the level of pathways ‘downstream’ to reduced levels of FMRP (shown under the category of ‘FMRP-specific Biological Interventions). Abbreviations: FraX: fragile X syndrome; FMRP: fragile X mental retardation protein; mGlurR: metabotropic glutamate receptor; GABA: gammaaminobutyric acid. Asterisks (*) next to treatment approaches indicate ongoing trials in the Center for Interdisciplinary Brain Sciences Research at Stanford University

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References

1. APA. Diagnostic and statistical manual of mental disorders, fourth edition – text revision (DSMIV-TR) Arlington, VA: American Psychiatric Associaiton; 2000.
1. Bailey DB, Jr, Hatton DD, Skinner M. Early developmental trajectories of males with fragile X syndrome. American Journal of Mental Retardation. 1998;103:29–39. - PubMed
1. Barnea-Goraly N, Eliez S, Hedeus M, Menon V, White CD, Moseley M, et al. White matter tract alterations in fragile X syndrome: Preliminary evidence from diffusion tensor imaging. American Journal of Medical Genetics B: Neuropsychiatric Genetetics. 2003;118B:81–88. - PubMed
1. Berry-Kravis E, Abrams L, Coffey SM, Hall DA, Greco C, Gane LW, et al. Fragile X-associated tremor/ataxia syndrome: Clinical features, genetics, and testing guidelines. Movement Disorders. 2007;22:2018–2030. quiz 2140. - PubMed
1. Berry-Kravis E, Krause SE, Block SS, Guter S, Wuu J, Leurgans S, et al. Effect of CX516, an AMPA-modulating compound, on cognition and behavior in fragile X syndrome: A controlled trial. Journal of Child and Adolescent Psychopharmacology. 2006;16:525–540. - PubMed

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[1] APA. Diagnostic and statistical manual of mental disorders, fourth edition – text revision (DSMIV-TR) Arlington, VA: American Psychiatric Associaiton; 2000.

[2] APA. Diagnostic and statistical manual of mental disorders, fourth edition – text revision (DSMIV-TR) Arlington, VA: American Psychiatric Associaiton; 2000.

[3] Bailey DB, Jr, Hatton DD, Skinner M. Early developmental trajectories of males with fragile X syndrome. American Journal of Mental Retardation. 1998;103:29–39. - PubMed

[4] Bailey DB, Jr, Hatton DD, Skinner M. Early developmental trajectories of males with fragile X syndrome. American Journal of Mental Retardation. 1998;103:29–39. - PubMed

[5] Barnea-Goraly N, Eliez S, Hedeus M, Menon V, White CD, Moseley M, et al. White matter tract alterations in fragile X syndrome: Preliminary evidence from diffusion tensor imaging. American Journal of Medical Genetics B: Neuropsychiatric Genetetics. 2003;118B:81–88. - PubMed

[6] Barnea-Goraly N, Eliez S, Hedeus M, Menon V, White CD, Moseley M, et al. White matter tract alterations in fragile X syndrome: Preliminary evidence from diffusion tensor imaging. American Journal of Medical Genetics B: Neuropsychiatric Genetetics. 2003;118B:81–88. - PubMed

[7] Berry-Kravis E, Abrams L, Coffey SM, Hall DA, Greco C, Gane LW, et al. Fragile X-associated tremor/ataxia syndrome: Clinical features, genetics, and testing guidelines. Movement Disorders. 2007;22:2018–2030. quiz 2140. - PubMed

[8] Berry-Kravis E, Abrams L, Coffey SM, Hall DA, Greco C, Gane LW, et al. Fragile X-associated tremor/ataxia syndrome: Clinical features, genetics, and testing guidelines. Movement Disorders. 2007;22:2018–2030. quiz 2140. - PubMed

[9] Berry-Kravis E, Krause SE, Block SS, Guter S, Wuu J, Leurgans S, et al. Effect of CX516, an AMPA-modulating compound, on cognition and behavior in fragile X syndrome: A controlled trial. Journal of Child and Adolescent Psychopharmacology. 2006;16:525–540. - PubMed

[10] Berry-Kravis E, Krause SE, Block SS, Guter S, Wuu J, Leurgans S, et al. Effect of CX516, an AMPA-modulating compound, on cognition and behavior in fragile X syndrome: A controlled trial. Journal of Child and Adolescent Psychopharmacology. 2006;16:525–540. - PubMed

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Childhood developmental disorders: an academic and clinical convergence point for psychiatry, neurology, psychology and pediatrics

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Childhood developmental disorders: an academic and clinical convergence point for psychiatry, neurology, psychology and pediatrics

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