Abstract

The proposed study is designed to identify biobehavioral """"""""markers"""""""" or """"""""indicators"""""""" of a genetic vulnerability to schizophrenia that, in weighted combination, will serve to predict future illness in the unaffected relatives of schizophrenic individuals. The project is divided into two research components. Phase I, for which funds are being requested, will serve to recruit the full sample, collect all of the biobehavioral data and complete baseline clinical assessments. Phase II is the clinical follow-up component, and will serve to establish clinical outcome and validate the data collected in Phase I. In Phase I, 100 adolescents with AXIS I schizophrenia spectrum disorders, 125 of their at-risk siblings, 100 normal controls matched to the patient probands and 125 siblings of the normal control probands will participate. Candidate markers will include measures of attention, smooth pursuit eye-movements, frontal lobe (executive) functions and temporal lobe (verbal memory) processing- all of which have been implicated in the pathophysiology of schizophrenia. The innovative aspect of this design is that, by selecting young patients as probands, a new at-risk population can be studied. The sibling risk rate for schizophrenia spectrum disorders is similar to that of the offspring of a schizophrenic parent. Nevertheless, at-risk siblings are virtually an untapped research population, since siblings of adult schizophrenic patients (more typically studied) are too old to constitute a viable high-risk sample. Moreover, the probands are themselves a group of considerable interest. Young patients in the early stages of psychosis, even though considered likely to have a severe form of schizophrenia, have rarely ben studied. In Phase I, a weighted composite of biobehavioral deficits will be derived (the Diathesis Index) that will differentiate the siblings of schizophrenic probands from the siblings of normal controls. It is assumed that this index reflects a biological vulnerability for schizophrenia. In Phase II, based on clinical outcome, a comparable composite of biobehavioral indicators (the Predictor Index) will be calculated to differentiate between the high-risk siblings who do and do not become ill. The Predictor Index will enable individuals with a true vulnerability for expressing schizophrenia to be identified, many years prior to onset of the illness. Comparisons between the Phase I Diathesis Index and the Phase II Predictor Index will indicate the extent to which deficits identifying individuals as being vulnerable relative to normal controls overlap with the deficits that lead to the actual expression os schizophrenia. In the long run, the Predictor Index is expected to provide a means of carrying out cost- effective population screening a currently unavailablE first step toward establishing effective intervention programs.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Mental Health (NIMH)
Type
Research Project (R01)
Project #
5R01MH050203-04
Application #
2675085
Study Section
Special Emphasis Panel (SRCM (01))
Project Start
1995-07-01
Project End
2001-06-30
Budget Start
1998-07-01
Budget End
2001-06-30
Support Year
4
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
Long Island Jewish Medical Center
Department
Type
DUNS #
City
New Hyde Park
State
NY
Country
United States
Zip Code
11040

  Publications

Olvet, Doreen M; CarriĆ³n, Ricardo E; Auther, Andrea M et al. (2015) Self-awareness of functional impairment in individuals at clinical high-risk for psychosis. Early Interv Psychiatry 9:100-7
Smith, Christopher W; Park, Sohee; Cornblatt, Barbara (2006) Spatial working memory deficits in adolescents at clinical high risk for schizophrenia. Schizophr Res 81:211-5
Seidman, Larry J; Giuliano, Anthony J; Smith, Christopher W et al. (2006) Neuropsychological functioning in adolescents and young adults at genetic risk for schizophrenia and affective psychoses: results from the Harvard and Hillside Adolescent High Risk Studies. Schizophr Bull 32:507-24
Lencz, Todd; Smith, Christopher W; McLaughlin, Danielle et al. (2006) Generalized and specific neurocognitive deficits in prodromal schizophrenia. Biol Psychiatry 59:863-71
Lencz, Todd; Smith, Christopher W; Auther, Andrea et al. (2004) Nonspecific and attenuated negative symptoms in patients at clinical high-risk for schizophrenia. Schizophr Res 68:37-48
Lencz, Todd; Smith, Christopher W; Auther, Andrea M et al. (2003) The assessment of ""prodromal schizophrenia"": unresolved issues and future directions. Schizophr Bull 29:717-28
Cornblatt, Barbara A; Lencz, Todd; Smith, Christopher W et al. (2003) The schizophrenia prodrome revisited: a neurodevelopmental perspective. Schizophr Bull 29:633-51
Cornblatt, Barbara A (2002) The New York high risk project to the Hillside recognition and prevention (RAP) program. Am J Med Genet 114:956-66
Lencz, T; Cornblatt, B; Bilder, R M (2001) Neurodevelopmental models of schizophrenia: pathophysiologic synthesis and directions for intervention research. Psychopharmacol Bull 35:95-125
Cornblatt, B A; Malhotra, A K (2001) Impaired attention as an endophenotype for molecular genetic studies of schizophrenia. Am J Med Genet 105:11-5

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