Abstract

The overall goals of the proposed research are to achieve a better understanding of both the genetics and the phenotype(s) of developmental dyslexia. Genetic heterogeneity appears to be very likely in dyslexia, but key features of the linguistic phenotype appear to be common across etiologies. Whether certain clinical correlates of dyslexia are part of the phenotype(s) is much less clear.
The specific aims of this project are (1) to test alternative models of genetic transmission of dyslexia and to obtain better information about both the transmissible phenotype and genetic parameters important of linkage analysis; (2) to more precisely map the dyslexia locus on chromosome 15 and to confirm or disconfirm a second possible locus on chromosome 6 near the HLA region; (3) to screen the genome for other regions which appear to contribute to the dyslexia phenotype(s); (4) to clarify the development of the underlying linguistic phenotype and components of the reading process; (5) to determine which phonological processing deficits are causal predictors of later familial dyslexia; and (6) to determine whether and how apparent clinical correlates of dyslexia are related to the dyslexia phenotype(s). The methodology that is proposed to meet these objectives consists of (1) segregation analyses using POINTER (Lalouel, et al., 1983) of three large samples of dyslexic families; (2) continued linkage studies of 25 large dyslexic families; (3) a sibling pair linkage study using 100 dyslexic DZ twins pairs; (4) a cross -sectional study of the linguistic phenotype in both family and clinic dyslexics; (5) a longitudinal study of the linguistic precursors of reading in preschool children of either high or low familial risk for dyslexia; and (6) longitudinal, cosegregation, and coheritability analyses of apparent clinical correlates of the dyslexia phenotype. Achieving these objectives will lead to a clearer, neuroscientific understanding of the effects of genes on a specific and culturally significant aspect of human cognition. Clinically, this research will contribute to a well-grounded approach to early identification and treatment of this common developmental disorder.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Mental Health (NIMH)
Type
Research Scientist Development Award - Research (K02)
Project #
2K02MH000419-07
Application #
3069781
Study Section
Research Scientist Development Review Committee (MHK)
Project Start
1988-01-01
Project End
1994-06-30
Budget Start
1989-08-01
Budget End
1990-06-30
Support Year
7
Fiscal Year
1989
Total Cost
Indirect Cost

  Institution

Name
University of Denver
Department
Type
Schools of Arts and Sciences
DUNS #
City
Denver
State
CO
Country
United States
Zip Code
80208

  Publications

Pennington, B F; Filipek, P A; Lefly, D et al. (2000) A twin MRI study of size variations in human brain. J Cogn Neurosci 12:223-32
Pennington, B F (1999) Toward an integrated understanding of dyslexia: genetic, neurological, and cognitive mechanisms. Dev Psychopathol 11:629-54
Pennington, B F; Filipek, P A; Lefly, D et al. (1999) Brain morphometry in reading-disabled twins. Neurology 53:723-9
Gilger, J W; Pennington, B F; Harbeck, R J et al. (1998) A twin and family study of the association between immune system dysfunction and dyslexia using blood serum immunoassay and survey data. Brain Cogn 36:310-33
Pennington, B F; Smith, S D (1997) Genetic analysis of dyslexia and other complex behavioral phenotypes. Curr Opin Pediatr 9:636-41
Pennington, B F; Ozonoff, S (1996) Executive functions and developmental psychopathology. J Child Psychol Psychiatry 37:51-87