White-matter markers for psychosis in a prospective ultra-high-risk cohort

Subjects at 'ultra high risk' (UHR) for developing psychosis have differences in white matter (WM) compared with healthy controls. WM integrity has not yet been investigated in UHR subjects in relation to the development of subsequent psychosis. Hence, we investigated a prospective cohort...

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Published in	Psychological medicine Vol. 40; no. 8; pp. 1297 - 1304
Main Authors	Bloemen, O. J. N., de Koning, M. B., Schmitz, N., Nieman, D. H., Becker, H. E., de Haan, L., Dingemans, P., Linszen, D. H., van Amelsvoort, T. A. M. J.
Format	Journal Article
Language	English
Published	Cambridge, UK Cambridge University Press 01.08.2010
Subjects	Adolescent Adult Adult and adolescent clinical studies Anisotropy Biological and medical sciences Brain Brain - pathology Chronic Disease Cohort Studies Diffusion Magnetic Resonance Imaging Disease Progression DT-MRI Female Frontal lobes Genetic Predisposition to Disease - genetics Genetic Predisposition to Disease - psychology High risk Humans Image Processing, Computer-Assisted Integrity Magnetic resonance imaging Male Medial temporal lobe Medical sciences Mental disorders Morality Nerve Fibers, Myelinated - pathology NMR Nuclear magnetic resonance Prospective Studies Psychiatric Status Rating Scales Psychology. Psychoanalysis. Psychiatry Psychopathology. Psychiatry Psychoses Psychosis Reference Values Research subjects Risk Factors Schizophrenia Schizophrenia - diagnosis Schizophrenia - genetics Schizophrenia - pathology Schizophrenic Psychology Schizotypal Personality Disorder - diagnosis Schizotypal Personality Disorder - genetics Schizotypal Personality Disorder - psychology Temporal lobes transition UHR Values white matter Young Adult white matter DT-MRI FA schizophrenia transition UHR Human High risk Central nervous system Biological marker Schizophrenia Nuclear magnetic resonance imaging White matter Encephalon Diffusion tensor imaging Psychosis Anisotropy Medical imagery
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ISSN	0033-2917 1469-8978 1469-8978
DOI	10.1017/S0033291709991711

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Abstract	Subjects at 'ultra high risk' (UHR) for developing psychosis have differences in white matter (WM) compared with healthy controls. WM integrity has not yet been investigated in UHR subjects in relation to the development of subsequent psychosis. Hence, we investigated a prospective cohort of UHR subjects comparing whole brain fractional anisotropy (FA) of those later developing psychosis (UHR-P) to those who did not (UHR-NP). We recruited 37 subjects fulfilling UHR criteria and 10 healthy controls. Baseline 3 Tesla magnetic resonance imaging (MRI) scans and Positive and Negative Syndrome Scale (PANSS) ratings were obtained. UHR subjects were assessed at 9, 18 and 24 months for development of frank psychosis. We compared baseline FA of UHR-P to controls and UHR-NP subjects. Furthermore, we related clinical data to MRI outcome in the patient population. Of the 37 UHR subjects, 10 had transition to psychosis. UHR-P subjects showed significantly lower FA values than control subjects in medial frontal lobes bilaterally. UHR-P subjects had lower FA values than UHR-NP subjects, lateral to the right putamen and in the left superior temporal lobe. UHR-P subjects showed higher FA values, compared with UHR-NP, in the left medial temporal lobe. In UHR-P, positive PANSS negatively correlated to FA in the left middle temporal lobe. In the total UHR group positive PANSS negatively correlated to FA in the right superior temporal lobe. UHR subjects who later develop psychosis have differences in WM integrity, compared with UHR subjects who do not develop psychosis and to healthy controls, in brain areas associated with schizophrenia.
AbstractList	Background: Subjects at 'ultra high risk' (UHR) for developing psychosis have differences in white matter (WM) compared with healthy controls. WM integrity has not yet been investigated in UHR subjects in relation to the development of subsequent psychosis. Hence, we investigated a prospective cohort of UHR subjects comparing whole brain fractional anisotropy (FA) of those later developing psychosis (UHR-P) to those who did not (UHR-NP). Method: We recruited 37 subjects fulfilling UHR criteria and 10 healthy controls. Baseline 3 Tesla magnetic resonance imaging (MRI) scans and Positive and Negative Syndrome Scale (PANSS) ratings were obtained. UHR subjects were assessed at 9, 18 and 24 months for development of frank psychosis. We compared baseline FA of UHR-P to controls and UHR-NP subjects. Furthermore, we related clinical data to MRI outcome in the patient population. Results: Of the 37 UHR subjects, 10 had transition to psychosis. UHR-P subjects showed significantly lower FA values than control subjects in medial frontal lobes bilaterally. UHR-P subjects had lower FA values than UHR-NP subjects, lateral to the right putamen and in the left superior temporal lobe. UHR-P subjects showed higher FA values, compared with UHR-NP, in the left medial temporal lobe. In UHR-P, positive PANSS negatively correlated to FA in the left middle temporal lobe. In the total UHR group positive PANSS negatively correlated to FA in the right superior temporal lobe. Conclusions: UHR subjects who later develop psychosis have differences in WM integrity, compared with UHR subjects who do not develop psychosis and to healthy controls, in brain areas associated with schizophrenia. [PUBLICATION ABSTRACT] Background. Subjects at 'ultra high risk' (UHR) for developing psychosis have differences in white matter (WM) compared with healthy controls. WM integrity has not yet been investigated in UHR subjects in relation to the development of subsequent psychosis. Hence, we investigated a prospective cohort of UHR subjects comparing whole brain fractional anisotropy (FA) of those later developing psychosis (UHR-P) to those who did not (UHR-NP). Method. We recruited 37 subjects fulfilling UHR criteria and 10 healthy controls. Baseline 3 Tesla magnetic resonance imaging (MRT) scans and Positive and Negative Syndrome Scale (PANSS) ratings were obtained. UHR subjects were assessed at 9, 18 and 24 months for development of frank psychosis. We compared baseline FA of UHR-P to controls and UHR-NP subjects. Furthermore, we related clinical data to MRI outcome in the patient population. Results. Of the 37 UHR subjects, 10 had transition to psychosis. UHR-P subjects showed significantly lower FA values than control subjects in medial frontal lobes bilaterally. UHR-P subjects had lower FA values than UHR-NP subjects, lateral to the right putamen and in the left superior temporal lobe. UHR-P subjects showed higher FA values, compared with UHR-NP, in the left medial temporal lobe. In UHR-P, positive PANSS negatively correlated to FA in the left middle temporal lobe. In the total UHR group positive PANSS negatively correlated to FA in the right superior temporal lobe. Conclusions. UHR subjects who later develop psychosis have differences in WM integrity, compared with UHR subjects who do not develop psychosis and to healthy controls, in brain areas associated with schizophrenia. Adapted from the source document. Subjects at 'ultra high risk' (UHR) for developing psychosis have differences in white matter (WM) compared with healthy controls. WM integrity has not yet been investigated in UHR subjects in relation to the development of subsequent psychosis. Hence, we investigated a prospective cohort of UHR subjects comparing whole brain fractional anisotropy (FA) of those later developing psychosis (UHR-P) to those who did not (UHR-NP).BACKGROUNDSubjects at 'ultra high risk' (UHR) for developing psychosis have differences in white matter (WM) compared with healthy controls. WM integrity has not yet been investigated in UHR subjects in relation to the development of subsequent psychosis. Hence, we investigated a prospective cohort of UHR subjects comparing whole brain fractional anisotropy (FA) of those later developing psychosis (UHR-P) to those who did not (UHR-NP).We recruited 37 subjects fulfilling UHR criteria and 10 healthy controls. Baseline 3 Tesla magnetic resonance imaging (MRI) scans and Positive and Negative Syndrome Scale (PANSS) ratings were obtained. UHR subjects were assessed at 9, 18 and 24 months for development of frank psychosis. We compared baseline FA of UHR-P to controls and UHR-NP subjects. Furthermore, we related clinical data to MRI outcome in the patient population.METHODWe recruited 37 subjects fulfilling UHR criteria and 10 healthy controls. Baseline 3 Tesla magnetic resonance imaging (MRI) scans and Positive and Negative Syndrome Scale (PANSS) ratings were obtained. UHR subjects were assessed at 9, 18 and 24 months for development of frank psychosis. We compared baseline FA of UHR-P to controls and UHR-NP subjects. Furthermore, we related clinical data to MRI outcome in the patient population.Of the 37 UHR subjects, 10 had transition to psychosis. UHR-P subjects showed significantly lower FA values than control subjects in medial frontal lobes bilaterally. UHR-P subjects had lower FA values than UHR-NP subjects, lateral to the right putamen and in the left superior temporal lobe. UHR-P subjects showed higher FA values, compared with UHR-NP, in the left medial temporal lobe. In UHR-P, positive PANSS negatively correlated to FA in the left middle temporal lobe. In the total UHR group positive PANSS negatively correlated to FA in the right superior temporal lobe.RESULTSOf the 37 UHR subjects, 10 had transition to psychosis. UHR-P subjects showed significantly lower FA values than control subjects in medial frontal lobes bilaterally. UHR-P subjects had lower FA values than UHR-NP subjects, lateral to the right putamen and in the left superior temporal lobe. UHR-P subjects showed higher FA values, compared with UHR-NP, in the left medial temporal lobe. In UHR-P, positive PANSS negatively correlated to FA in the left middle temporal lobe. In the total UHR group positive PANSS negatively correlated to FA in the right superior temporal lobe.UHR subjects who later develop psychosis have differences in WM integrity, compared with UHR subjects who do not develop psychosis and to healthy controls, in brain areas associated with schizophrenia.CONCLUSIONSUHR subjects who later develop psychosis have differences in WM integrity, compared with UHR subjects who do not develop psychosis and to healthy controls, in brain areas associated with schizophrenia. Subjects at 'ultra high risk' (UHR) for developing psychosis have differences in white matter (WM) compared with healthy controls. WM integrity has not yet been investigated in UHR subjects in relation to the development of subsequent psychosis. Hence, we investigated a prospective cohort of UHR subjects comparing whole brain fractional anisotropy (FA) of those later developing psychosis (UHR-P) to those who did not (UHR-NP). We recruited 37 subjects fulfilling UHR criteria and 10 healthy controls. Baseline 3 Tesla magnetic resonance imaging (MRI) scans and Positive and Negative Syndrome Scale (PANSS) ratings were obtained. UHR subjects were assessed at 9, 18 and 24 months for development of frank psychosis. We compared baseline FA of UHR-P to controls and UHR-NP subjects. Furthermore, we related clinical data to MRI outcome in the patient population. Of the 37 UHR subjects, 10 had transition to psychosis. UHR-P subjects showed significantly lower FA values than control subjects in medial frontal lobes bilaterally. UHR-P subjects had lower FA values than UHR-NP subjects, lateral to the right putamen and in the left superior temporal lobe. UHR-P subjects showed higher FA values, compared with UHR-NP, in the left medial temporal lobe. In UHR-P, positive PANSS negatively correlated to FA in the left middle temporal lobe. In the total UHR group positive PANSS negatively correlated to FA in the right superior temporal lobe. UHR subjects who later develop psychosis have differences in WM integrity, compared with UHR subjects who do not develop psychosis and to healthy controls, in brain areas associated with schizophrenia. Subjects at 'ultra high risk' (UHR) for developing psychosis have differences in white matter (WM) compared with healthy controls. WM integrity has not yet been investigated in UHR subjects in relation to the development of subsequent psychosis. Hence, we investigated a prospective cohort of UHR subjects comparing whole brain fractional anisotropy (FA) of those later developing psychosis (UHR-P) to those who did not (UHR-NP). We recruited 37 subjects fulfilling UHR criteria and 10 healthy controls. Baseline 3 Tesla magnetic resonance imaging (MRI) scans and Positive and Negative Syndrome Scale (PANSS) ratings were obtained. UHR subjects were assessed at 9, 18 and 24 months for development of frank psychosis. We compared baseline FA of UHR-P to controls and UHR-NP subjects. Furthermore, we related clinical data to MRI outcome in the patient population. Of the 37 UHR subjects, 10 had transition to psychosis. UHR-P subjects showed significantly lower FA values than control subjects in medial frontal lobes bilaterally. UHR-P subjects had lower FA values than UHR-NP subjects, lateral to the right putamen and in the left superior temporal lobe. UHR-P subjects showed higher FA values, compared with UHR-NP, in the left medial temporal lobe. In UHR-P, positive PANSS negatively correlated to FA in the left middle temporal lobe. In the total UHR group positive PANSS negatively correlated to FA in the right superior temporal lobe. UHR subjects who later develop psychosis have differences in WM integrity, compared with UHR subjects who do not develop psychosis and to healthy controls, in brain areas associated with schizophrenia.
Author	Nieman, D. H. de Koning, M. B. Dingemans, P. Becker, H. E. Schmitz, N. Bloemen, O. J. N. de Haan, L. van Amelsvoort, T. A. M. J. Linszen, D. H.
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DocumentTitleAlternate	White matter in prodromal patients O. J. N. Bloemen et al.
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Keywords	white matter DT-MRI FA schizophrenia transition UHR Human High risk Central nervous system Biological marker Schizophrenia Nuclear magnetic resonance imaging White matter Encephalon Diffusion tensor imaging Psychosis Anisotropy Medical imagery
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References	S0033291709991711_ref020 S0033291709991711_ref002 S0033291709991711_ref024 S0033291709991711_ref023 S0033291709991711_ref001 S0033291709991711_ref022 S0033291709991711_ref021 (S0033291709991711_ref033) 1993 S0033291709991711_ref006 S0033291709991711_ref005 S0033291709991711_ref027 S0033291709991711_ref026 S0033291709991711_ref004 S0033291709991711_ref003 S0033291709991711_ref009 S0033291709991711_ref008 S0033291709991711_ref029 S0033291709991711_ref007 S0033291709991711_ref031 S0033291709991711_ref030 S0033291709991711_ref013 S0033291709991711_ref035 S0033291709991711_ref012 S0033291709991711_ref034 S0033291709991711_ref011 S0033291709991711_ref032 S0033291709991711_ref010 Schmand (S0033291709991711_ref025) 1991; 22 S0033291709991711_ref017 S0033291709991711_ref016 S0033291709991711_ref015 Talairach (S0033291709991711_ref028) 1988 S0033291709991711_ref036 S0033291709991711_ref014 Mori (S0033291709991711_ref019) 2005 S0033291709991711_ref018
References_xml	– ident: S0033291709991711_ref021 doi: 10.1111/j.1600-0447.2005.00697.x – volume-title: Composite International Diagnostic Interview – Version 1.1 year: 1993 ident: S0033291709991711_ref033 – ident: S0033291709991711_ref029 doi: 10.1176/appi.ajp.162.12.2315 – ident: S0033291709991711_ref007 doi: 10.1097/00001756-199802160-00013 – ident: S0033291709991711_ref001 doi: 10.1016/j.schres.2003.12.002 – ident: S0033291709991711_ref023 doi: 10.1016/j.schres.2009.03.018 – ident: S0033291709991711_ref003 doi: 10.1006/nimg.2001.0961 – ident: S0033291709991711_ref031 doi: 10.1016/j.schres.2008.04.042 – ident: S0033291709991711_ref008 doi: 10.1111/j.1600-0447.2009.01372.x – ident: S0033291709991711_ref011 doi: 10.1016/j.schres.2008.07.023 – ident: S0033291709991711_ref024 doi: 10.1002/mrm.1910360612 – ident: S0033291709991711_ref026 doi: 10.1016/S0920-9964(01)00163-3 – ident: S0033291709991711_ref035 doi: 10.4088/JCP.v64n0607 – ident: S0033291709991711_ref013 doi: 10.1016/j.neuroimage.2005.02.013 – ident: S0033291709991711_ref006 doi: 10.1002/nbm.782 – ident: S0033291709991711_ref002 doi: 10.1006/nimg.2000.0582 – ident: S0033291709991711_ref012 doi: 10.1001/archgenpsychiatry.2008.514 – volume-title: Co-planar Stereotaxic Atlas of the Human Brain year: 1988 ident: S0033291709991711_ref028 – ident: S0033291709991711_ref030 doi: 10.1192/bjp.bp.107.043463 – volume-title: MRI Atlas of Human White Matter year: 2005 ident: S0033291709991711_ref019 – ident: S0033291709991711_ref020 doi: 10.1016/j.schres.2008.09.016 – volume: 22 start-page: 15 year: 1991 ident: S0033291709991711_ref025 article-title: [The Dutch Reading Test for Adults: a measure of premorbid intelligence level] publication-title: Tijdschrift voor Gerontologie en Geriatrie – ident: S0033291709991711_ref016 doi: 10.1093/schbul/sbm034 – ident: S0033291709991711_ref017 doi: 10.1192/bjp.191.51.s123 – ident: S0033291709991711_ref022 doi: 10.1159/000154476 – ident: S0033291709991711_ref036 doi: 10.1016/S0920-9964(02)00167-6 – ident: S0033291709991711_ref015 doi: 10.1001/archpsyc.58.8.769 – ident: S0033291709991711_ref032 doi: 10.1186/1471-244X-7-61 – ident: S0033291709991711_ref010 doi: 10.1176/appi.ajp.2008.07101640 – ident: S0033291709991711_ref009 doi: 10.1016/j.schres.2008.11.021 – ident: S0033291709991711_ref027 doi: 10.1001/archpsyc.1992.01820080032005 – ident: S0033291709991711_ref005 doi: 10.1016/S0006-3495(94)80775-1 – ident: S0033291709991711_ref004 doi: 10.1002/nbm.1940080707 – ident: S0033291709991711_ref014 doi: 10.1093/schbul/13.2.261 – ident: S0033291709991711_ref034 doi: 10.1016/j.schres.2008.03.022 – ident: S0033291709991711_ref018 doi: 10.1093/oxfordjournals.schbul.a007040
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Snippet	Subjects at 'ultra high risk' (UHR) for developing psychosis have differences in white matter (WM) compared with healthy controls. WM integrity has not yet... Background: Subjects at 'ultra high risk' (UHR) for developing psychosis have differences in white matter (WM) compared with healthy controls. WM integrity has... Background. Subjects at 'ultra high risk' (UHR) for developing psychosis have differences in white matter (WM) compared with healthy controls. WM integrity has...
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SubjectTerms	Adolescent Adult Adult and adolescent clinical studies Anisotropy Biological and medical sciences Brain Brain - pathology Chronic Disease Cohort Studies Diffusion Magnetic Resonance Imaging Disease Progression DT-MRI Female Frontal lobes Genetic Predisposition to Disease - genetics Genetic Predisposition to Disease - psychology High risk Humans Image Processing, Computer-Assisted Integrity Magnetic resonance imaging Male Medial temporal lobe Medical sciences Mental disorders Morality Nerve Fibers, Myelinated - pathology NMR Nuclear magnetic resonance Prospective Studies Psychiatric Status Rating Scales Psychology. Psychoanalysis. Psychiatry Psychopathology. Psychiatry Psychoses Psychosis Reference Values Research subjects Risk Factors Schizophrenia Schizophrenia - diagnosis Schizophrenia - genetics Schizophrenia - pathology Schizophrenic Psychology Schizotypal Personality Disorder - diagnosis Schizotypal Personality Disorder - genetics Schizotypal Personality Disorder - psychology Temporal lobes transition UHR Values white matter Young Adult
Title	White-matter markers for psychosis in a prospective ultra-high-risk cohort
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