Abstract

Immune-defective mice and a perinatal surgical rodent model developed in our laboratories, both of which exhibit abnormal learning behaviors, show developmental brain anomalies that are similar to those seen in dyslexics. In the first period of the Program Project, we documented brain, behavioral and immunological abnormalities in an animal model. We carried out preliminary research that suggested a special role of the uterine environment for some immunological and behavioral characteristics. During the second period, we characterized further cellular, connectional, behavioral (including early life experience), and developmental characteristics of the anomalies, as well as genetic influences on their origin and effects of pharmacological manipulations. We also demonstrated the lack of substantial interaction among malformations, immunological parameters, and intrauterine environment. Related research in humans and animals demonstrated that the distinction between defects in low-level sensory processing and those in higher-level cognition is pivotal in determining the pathogenesis of dyslexia. The purpose of the continuation of this program project is to pursue lines of evidence that have been productive and convergent between our line of research and that of our colleagues. Four research projects and 4 core functions will comprise the Program Project. Two anatomy projects will look at the developmental anatomical consequences of minor cortical malformations, either spontaneous or induced, on connectionally related cortical and subcortical regions, in an attempt to explain functional abnormalities at both high and low levels of processing. Amelioration of anatomic effects will be attempted through environmental enrichment. A neurophysiology project will examine the synaptic characteristics of these connections, which are likely to be part of the mechanism by which cross-level developmental influences act. A neurobehavioral project will investigate behaviors at multiple levels of processing and the effects of early environmental manipulation. The 2 anatomical cores will support these projects and an especially designed neuroimaging core will be instituted to allow for longitudinal research in living animals and to optimize methods for best demonstrating minor cortical malformations in vivo . A data processing Core will serve all projects.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Research Program Projects (P01)
Project #
5P01HD020806-12
Application #
2673518
Study Section
Pediatrics Subcommittee (CHHD)
Project Start
1986-09-01
Project End
2002-03-31
Budget Start
1998-04-01
Budget End
1999-03-31
Support Year
12
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
Beth Israel Deaconess Medical Center
Department
Type
DUNS #
076593722
City
Boston
State
MA
Country
United States
Zip Code
02215

  Publications

Chen, Fuyi; Becker, Albert; LoTurco, Joseph (2016) Overview of Transgenic Glioblastoma and Oligoastrocytoma CNS Models and Their Utility in Drug Discovery. Curr Protoc Pharmacol 72:14.37.1-12
Truong, Dongnhu T; Rendall, Amanda R; Rosen, Glenn D et al. (2015) Morphometric changes in subcortical structures of the central auditory pathway in mice with bilateral nodular heterotopia. Behav Brain Res 282:61-9
Che, Alicia; Girgenti, Matthew J; LoTurco, Joseph (2014) The dyslexia-associated gene DCDC2 is required for spike-timing precision in mouse neocortex. Biol Psychiatry 76:387-96
Siddiqi, Faez; Chen, Fuyi; Aron, Abraham W et al. (2014) Fate mapping by piggyBac transposase reveals that neocortical GLAST+ progenitors generate more astrocytes than Nestin+ progenitors in rat neocortex. Cereb Cortex 24:508-20
Fitch, R Holy; Alexander, Michelle L; Threlkeld, Steven W (2013) Early neural disruption and auditory processing outcomes in rodent models: implications for developmental language disability. Front Syst Neurosci 7:58
Truong, Dongnhu T; Bonet, Ashley; Rendall, Amanda R et al. (2013) A behavioral evaluation of sex differences in a mouse model of severe neuronal migration disorder. PLoS One 8:e73144
Tarkar, Aarti; Loges, Niki T; Slagle, Christopher E et al. (2013) DYX1C1 is required for axonemal dynein assembly and ciliary motility. Nat Genet 45:995-1003
Chen, Fuyi; LoTurco, Joseph (2012) A method for stable transgenesis of radial glia lineage in rat neocortex by piggyBac mediated transposition. J Neurosci Methods 207:172-80
Maher, Brady J; LoTurco, Joseph J (2012) Disrupted-in-schizophrenia (DISC1) functions presynaptically at glutamatergic synapses. PLoS One 7:e34053
Threlkeld, Steven W; Hill, Courtney A; Szalkowski, Caitlin E et al. (2012) Effects of test experience and neocortical microgyria on spatial and non-spatial learning in rats. Behav Brain Res 235:130-5

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