Use of multiple polygenic risk scores for distinguishing schizophrenia-spectrum disorder and affective psychosis categories in a first-episode sample; the EU-GEI study
- Rodriguez, V.
- Alameda, L.
- Quattrone, D.
- Tripoli, G.
- Gayer-Anderson, C.
- Spinazzola, E.
- Trotta, G.
- Jongsma, H.E.
- Stilo, S.
- La Cascia, C.
- Ferraro, L.
- La Barbera, D.
- Lasalvia, A.
- Tosato, S.
- Tarricone, I.
- Bonora, E.
- Jamain, S.
- Selten, J.P.
- Velthorst, E.
- de Haan, L.
- Llorca, P.M.
- Arrojo, M.
- Bobes, J.
- Bernardo, M.
- Arango, C.
- Kirkbride, J.
- Jones, P.B.
- Rutten, B.P.
- Richards, A.
- Sham, P.C.
- O'Donovan, M.
- Van Os, J.
- Morgan, C.
- Di Forti, M.
- Murray, R.M.
- Vassos, E.
DOIAbstract
Background Schizophrenia (SZ), bipolar disorder (BD) and depression (D) run in families. This susceptibility is partly due to hundreds or thousands of common genetic variants, each conferring a fractional risk. The cumulative effects of the associated variants can be summarised as a polygenic risk score (PRS). Using data from the EUropean Network of national schizophrenia networks studying Gene-Environment Interactions (EU-GEI) first episode case-control study, we aimed to test whether PRSs for three major psychiatric disorders (SZ, BD, D) and for intelligent quotient (IQ) as a neurodevelopmental proxy, can discriminate affective psychosis (AP) from schizophrenia-spectrum disorder (SSD). Methods Participants (842 cases, 1284 controls) from ...
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