Abstract

This is a proposed Phase III of our Neurodevelopmental Study of Schizophrenia, in which we intend to assess the consequences of genetic and/or pre- and perinatal complications (PPCs) using high resolution structured magnetic resonance imaging (MRI). Studies of schizophrenia have implicated gray and white matter abnormalities in limbic-diencephalic, paralimbic, and prefrontal brain regions. These brain abnormalities result from genetic and/or environmental (i.e., obstetric) factors. Further, some nonpsychotic relatives of patients with schizophrenia suffer from similar, milder, (""""""""subsyndromal"""""""") dysfunctions. We are proposing a 5-year study to continue a 40-year prospective high risk study to directly test the consequences of genetic vulnerability (assessed by psychosis in the parent) and specific PPCs (i.e., chronic fetal hypoxia and infections in the second trimester), on cortical and subcortical brain volumes in adult offspring of parents with schizophrenia or affective psychoses. We have a unique opportunity to re-evaluate subjects that we have carefully studied by clinical and neuropsychological evaluations in Phase II of the study. The sample was originally ascertained from a community cohort of pregnancies drawn from the Providence and Boston cohorts of the National Collaborative Perinatal Project. At these sites, 17,741 pregnancies were followed prospectively and systematically recorded, and the offspring's mental and physical development were assessed at 4 and 8 months, and 1,4, and 7 years of age. We have systematically located, recruited, and diagnosed 200 parents with psychotic disorders, and 200 normal comparison parents, individually-matched on specific parent and offspring characteristics. 403 of their adult offspring, ages 31-37, have been identified in Phase II. We estimate that we will ascertain 85 percent of these 403 offspring for MRI. This study is unique in that we can specify developmental predictors of structural brain abnormalities and their functional consequences due to risk and obstetric status, for offspring who become psychotic, or exhibit subsyndromal expressions of the genetic diathesis. Further, we will identify the contribution of PPCs and/or genetic vulnerability to neural circuit abnormalities and demonstrate the specificity for schizophrenia versus affective psychosis. We will use a high resolution MRI and highly detailed, reliable image analysis techniques programs to link etiological predisposition to adult brain volumes (i.e., in limbic-diencephalic, paralimbic and cortical regions, and white matter tracts). This study has important implications for understand2ing the etiology and development of schizophrenia.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Mental Health (NIMH)
Type
Research Project (R01)
Project #
2R01MH050647-07
Application #
2851847
Study Section
Clinical Psychopathology Review Committee (CPP)
Program Officer
Heinssen, Robert K
Project Start
1993-05-01
Project End
2004-04-30
Budget Start
1999-06-15
Budget End
2000-04-30
Support Year
7
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
Harvard University
Department
Psychiatry
Type
Schools of Medicine
DUNS #
082359691
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

Gamma, Franziska; Goldstein, Jill M; Seidman, Larry J et al. (2014) Early intermodal integration in offspring of parents with psychosis. Schizophr Bull 40:992-1000
Buka, Stephen L; Seidman, Larry J; Tsuang, Ming T et al. (2013) The New England Family Study High-risk Project: neurological impairments among offspring of parents with schizophrenia and other psychoses. Am J Med Genet B Neuropsychiatr Genet 162B:653-60
Goldstein, Jill M; Cherkerzian, Sara; Tsuang, Ming T et al. (2013) Sex differences in the genetic risk for schizophrenia: history of the evidence for sex-specific and sex-dependent effects. Am J Med Genet B Neuropsychiatr Genet 162B:698-710
Seidman, L J; Cherkerzian, S; Goldstein, J M et al. (2013) Neuropsychological performance and family history in children at age 7 who develop adult schizophrenia or bipolar psychosis in the New England Family Studies. Psychol Med 43:119-31
Milanovic, Snezana M; Thermenos, Heidi W; Goldstein, Jill M et al. (2011) Medial prefrontal cortical activation during working memory differentiates schizophrenia and bipolar psychotic patients: a pilot FMRI study. Schizophr Res 129:208-10
Goldstein, Jill M; Cherkerzian, Sara; Seidman, Larry J et al. (2011) Sex-specific rates of transmission of psychosis in the New England high-risk family study. Schizophr Res 128:150-5
Thermenos, Heidi W; Goldstein, Jill M; Milanovic, Snezana M et al. (2010) An fMRI study of working memory in persons with bipolar disorder or at genetic risk for bipolar disorder. Am J Med Genet B Neuropsychiatr Genet 153B:120-31
Donatelli, Jo-Ann L; Seidman, Larry J; Goldstein, Jill M et al. (2010) Children of parents with affective and nonaffective psychoses: a longitudinal study of behavior problems. Am J Psychiatry 167:1331-8
Goldstein, Jill M; Buka, Stephen L; Seidman, Larry J et al. (2010) Specificity of familial transmission of schizophrenia psychosis spectrum and affective psychoses in the New England family study's high-risk design. Arch Gen Psychiatry 67:458-67
Seidman, Larry J; Buka, Stephen L; Goldstein, Jill M et al. (2006) Intellectual decline in schizophrenia: evidence from a prospective birth cohort 28 year follow-up study. J Clin Exp Neuropsychol 28:225-42

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