White Matter Microstructure in Individuals at Clinical High Risk of Psychosis: A Whole-Brain Diffusion Tensor Imaging Study

Hohenberg, Christian Clemm von; Pasternak, Ofer; Kubicki, Marek; Ballinger, Thomas; Vu, Mai-Anh; Swisher, Tali; Green, Katie; Giwerc, Michelle Y.; Dahlben, Brian; Goldstein, Jill M.; Woo, Tsung-Ung W.; Petryshen, Tracey L.; Mesholam-Gately, Raquelle I.; Woodberry, Kristen A.; Thermenos, Heidi W.; Mulert, Christoph; McCarley, Robert W.; Seidman, Larry J.; Shenton, Martha E.

doi:10.1093/schbul/sbt079

Cited by 98 publications

(76 citation statements)

References 40 publications

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“…The forceps major communicates somatosensory information be tween the parietal and occipital lobes via the splenium, a struc ture shown to be impaired in individuals at early and later stages of psychosis 1 as well as ultrahigh risk individuals. 53 A re port by Waltz and colleagues 54 demonstrated that individuals with schizophrenia showed a selective deficit in the ability to learn from positive outcomes but no deficits in learning from negative outcomes. This motivational deficit correlated with negative symptoms but not with neuropsychological measures of working memory, suggesting that the observation was not a neuropsychological deficit.…”

Section: Discussionmentioning

confidence: 99%

White matter tractography in early psychosis: clinical and neurocognitive associations

Hatton

Lagopoulos

Hermens

et al. 2014

jpn

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Section: Discussionmentioning

confidence: 99%

White matter tractography in early psychosis: clinical and neurocognitive associations

Hatton

Lagopoulos

Hermens

et al. 2014

jpn

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“…6 Both a neurodevelopmental model, 7,8 implying that WM alterations are present before disease onset and a postonset progression model, indicating that structural brain abnormalities progress over time after disease onset, have been proposed. 9,10 In support of the neurodevelopmental model, several cross-sectional DTI studies have revealed microstructural WM alterations in frontotemporal and -parietal connections in first-degree relatives without symptoms, 11,12 in clinical high-risk populations before onset, 13,14 and in patients with early onset psychosis. 15 Indeed, the lifetime trajectory of WM alterations in schizophrenia suggests higher percentages of WM loss in the first years of the illness, implicating altered neurodevelopment.…”

Section: Introductionmentioning

confidence: 91%

Differential Time Course of Microstructural White Matter in Patients With Psychotic Disorder and Individuals at Risk: A 3-Year Follow-up Study

Domen¹,

Peeters²,

Michielse³

et al. 2016

Schizophrenia Bulletin

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“…40 However, their method involved hypothesisfree whole brain white matter group comparisons, and, therefore, might not have been sufficiently sensitive to detect subtle changes in the thalamo-cortical white matter connections.…”

Section: Introductionmentioning

confidence: 99%

Altered Thalamo-Cortical White Matter Connectivity: Probabilistic Tractography Study in Clinical-High Risk for Psychosis and First-Episode Psychosis

Cho

Shenton

Kubicki

et al. 2015

SCHBUL

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Disrupted thalamo-cortical connectivity is regarded as a core psychopathology in patients diagnosed with schizophrenia. However, whether the thalamo-cortical white matter connectivity is disrupted before the onset of psychosis is still unknown. To determine this gap in knowledge, the strength of thalamo-cortical white matter anatomical connectivity in subjects at clinical-high risk for psychosis (CHR) was compared to that of first-episode psychosis (FEP) and healthy controls. A total of 37 CHR, 21 FEP, and 37 matched healthy controls underwent diffusion-weighted magnetic resonance imaging to examine the number of probabilistic tractography "counts" representing thalamo-cortical white matter connectivity. We also investigated the relationship with psychopathology. For FEP, the connectivity between the thalamus and parietal cortex was significantly increased (F = 5.65, P < .05) compared to that of healthy controls. However, the connectivity between thalamus and orbitofrontal cortex was significantly reduced compared to both healthy controls (F = 11.86, P < .005) and CHR (F = 6.63, P < .05). Interestingly, CHR exhibited a similar pattern as FEP, albeit with slightly reduced magnitude. Compared to healthy controls, there was a significant decrease (F = 4.16, P < .05) in CHR thalamo-orbitofrontal connectivity. Also, the strength of the thalamo-orbitofrontal connectivity was correlated with the Global Assessment of Functioning score in CHR (r = .35, P < .05). This observed pattern of white matter connectivity disruptions in FEP and in CHR suggests that this pattern of disconnectivity not only highlights the involvement of thalamus but also might be useful as an early biomarker for psychosis.

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White Matter Microstructure in Individuals at Clinical High Risk of Psychosis: A Whole-Brain Diffusion Tensor Imaging Study

Cited by 98 publications

References 40 publications

White matter tractography in early psychosis: clinical and neurocognitive associations

White matter tractography in early psychosis: clinical and neurocognitive associations

Differential Time Course of Microstructural White Matter in Patients With Psychotic Disorder and Individuals at Risk: A 3-Year Follow-up Study

Altered Thalamo-Cortical White Matter Connectivity: Probabilistic Tractography Study in Clinical-High Risk for Psychosis and First-Episode Psychosis

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