Xueping Zhou’s research while affiliated with National Institutes of Health and other places

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Publications (6)


Table 1 Hippocampal subfield volume in childhood-onset schizophrenia versus siblings and controls.
7 T MRI reveals hippocampal structural abnormalities associated with memory intrusions in childhood-onset schizophrenia
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July 2018

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52 Reads

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2 Citations

Schizophrenia Research

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Xueping Zhou

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The hippocampus exhibits striking volume reductions in schizophrenia (van Erp et al., 2016), with regionally specific changes in subfields cornu ammonis 1 to 4 (CA1-4), dentate gyrus, and subiculum (Mathew et al., 2014). Models of hippocampal function suggest an association with memory deficits in schizophrenia patients; for example, impairment of the pattern separation component of declarative memory in schizophrenia suggests dentate gyrus dysfunction (Das et al., 2014). As yet, however, there is incomplete understanding of how subfield structure contributes to these impairments. Relatedly, intrusions—a memory error where individuals mistakenly recall words from an incorrect list or never presented in any list—are associated with genetic risk for schizophrenia (Cannon et al., 2000), but hypothesized hippocampal pathophysiology remains unexplored. Childhood-onset schizophrenia, defined as onset before age 13, is a rare, possibly more homogenous, and severe form of the adult-onset disorder (Gochman et al., 2011). [...]

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Fig. 1. Decreased connectedness in both childhood-and adult-onset schizophrenia patients compared to their respective controls. T-values shown in blue indicate that both COS (A) and AOS (B) patients showed significantly decreased connectedness (i.e., lower average correlation of each voxel's time series with all other brain voxels) in a broad set of brain regions compared to their controls. 21% of AOS regions with reduced connectedness were spatially overlapped with COS (in red outline). Results were corrected for multiple comparisons, with degrees of freedom of 56 (A) and 46 (B). Talairach coordinates of these regions are listed in Table S3 for COS and Table S4 for AOS, with shared regions starred. No regions with increased connectedness were found in either COS or AOS patients compared to controls. (For interpretation of the references to color in this figure legend, the reader is referred to the web version of this article.) 
Fig. 3. Clusters of regions with reduced functional connectivity in childhood-and adult-onset schizophrenia patients compared to their controls. Voxels are colored by membership in the two major clusters defined in Fig. S4: a 'red' cluster including different components of the default-mode network in AOS and COS, and additional language and attention related areas only in COS (Cluster 1), and a 'green' cluster including somatosensory, motor and auditory regions in both AOS and COS (Cluster 2). Results were corrected for multiple comparisons (see Methods for details). Talairach coordinates of each region are shown in Tables S3 (COS) and S4 (AOS). (For interpretation of the references to color in this figure legend, the reader is referred to the web version of this article.) 
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Attenuated resting-state functional connectivity in patients with childhood- and adult-onset schizophrenia

January 2018

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206 Reads

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26 Citations

Schizophrenia Research

Background: Childhood-onset schizophrenia (COS) is a rare, severe form of the adult-onset disorder (AOS). Our previous resting-state fMRI study identified attenuated functional connectivity in COS compared with controls. Here, we ask whether COS and AOS patients and their siblings exhibit similar abnormalities of functional connectivity. Methods: A whole-brain, data-driven approach was used to assess resting-state functional connectivity differences in COS (patients/siblings/controls, n: 26/28/33) and AOS (n: 19/28/30). There were no significant differences in age, sex, or head motion across groups in each dataset and as designed, the COS dataset has a significantly lower age than the AOS. Results: Both COS and AOS patients showed decreased functional connectivity relative to controls among a wide set of brain regions (P<0.05, corrected), but their siblings did not. Decreased connectivity in COS and AOS patients showed no amplitude differences and was not modulated by age-at-onset or medication doses. Cluster analysis revealed that these regions fell into two large-scale networks: one sensorimotor network and one centered on default-mode network regions, but including higher-order cognitive areas only in COS. Decreased connectivity between these two networks was notable (P<0.05, corrected) for both patient groups. Conclusions: A shared pattern of attenuated functional connectivity was found in COS and AOS, supporting the continuity of childhood-onset and adult-onset schizophrenia. Connections were altered between sensorimotor areas and default-mode areas in both COS and AOS, suggesting potential abnormalities in processes of self-monitoring and sensory prediction. The absence of substantial dysconnectivity in siblings indicates that attenuation is state-related.


Reduced Functional Brain Activation and Connectivity During a Working Memory Task in Childhood-Onset Schizophrenia

December 2017

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72 Reads

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19 Citations

Journal of the American Academy of Child & Adolescent Psychiatry

Objective: Working memory (WM) deficits are consistently reported in schizophrenia and are related to poor functional outcomes. Functional magnetic resonance imaging studies of adult-onset schizophrenia have reported decreased functional activations and connectivity in the WM network, but no prior functional magnetic resonance imaging study has examined WM in childhood-onset schizophrenia (COS). The aim of this study was to examine the neural correlates of WM in COS. Method: Adult patients with COS (n = 32, 21.3 ± 1.1 years), nonpsychotic siblings of patients with COS (n = 30, 19.4 ± 0.8 years), and healthy controls (n = 39, 20.0 ± 0.7 years) completed 1- and 2-back WM tasks during 3-T functional magnetic resonance imaging. Functional activation and connectivity analyses were conducted. A separate group of 23 younger patients with COS (17.9 ± 7.4 years) could not perform the tasks after twice completing a standard training and are not included in this report. Results: Patients with COS who were included scored significantly lower than controls on all tasks (p < .001). Patients with COS showed significantly lower activations in the dorsolateral prefrontal cortices, posterior parietal cortices, cerebellum, and caudate and decreased frontoparietal and corticostriatal functional connectivity compared with controls (p < .05, corrected). Siblings had functional activations and connectivity intermediate between those of patients and controls in a similar set of regions (p < .05, corrected). In patients, functional connectivity strength in the left frontoparietal network correlated positively with accuracy scores during the 1-back task (p = .0023, corrected). Conclusion: Decreased functional activation and connectivity in the WM network in COS supports pathophysiologic continuity with adult-onset schizophrenia. The low participation rate and accuracy of the patients highlights the disease severity of COS. Hypo-activations and hypo-connectivity were shared by siblings of patients with COS, suggesting COS as a potential endophenotype. Clinical trial registration information: Evaluating Genetic Risk Factors for Childhood-Onset Schizophrenia; http://ClinicalTrials.gov;NCT00001198.


Symptom dimensions and subgroups in childhood-onset schizophrenia

November 2017

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172 Reads

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21 Citations

Schizophrenia Research

Objective: This study investigated symptom dimensions and subgroups in the National Institute of Mental Health (NIMH) childhood-onset schizophrenia (COS) cohort and their similarities to adult-onset schizophrenia (AOS) literature. Method: Scores from the Scales for the Assessment of Positive and Negative Symptoms (SAPS & SANS) from 125 COS patients were assessed for fit with previously established symptom dimensions from AOS literature using confirmatory factor analysis (CFA). K-means cluster analysis of each individual's scores on the best fitting set of dimensions was used to form patient clusters, which were then compared using demographic and clinical data. Results: CFA showed the SAPS & SANS data was well suited to a 2-dimension solution, including positive and negative dimensions, out of five well established models. Cluster analysis identified three patient groups characterized by different dimension scores: (1) low scores on both dimensions, (2) high negative, low positive scores, and (3) high scores on both dimensions. These groups had different Full scale IQ, Children's Global Assessment Scale (CGAS) scores, ages of onset, and prevalence of some co-morbid behavior disorders (all p<3.57E-03). Conclusion: Our analysis found distinct symptom-based subgroups within the NIMH COS cohort using an established AOS symptom structure. These findings confirm the heterogeneity of COS and were generally consistent with AOS literature.



Figure 1. Age of onset of childhood-onset schizophrenia 
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Lack of Gender-Related Differences in Childhood-Onset Schizophrenia

July 2016

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157 Reads

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24 Citations

Journal of the American Academy of Child & Adolescent Psychiatry

Objective Gender differences, including younger age of onset and greater premorbid deficits in men, have been reported in adult-onset schizophrenia. This study comprehensively evaluated gender differences in childhood-onset schizophrenia (COS), a rare variant of the disorder. Method Demographic, premorbid, clinical, familial, and cognitive characteristics, presence of chromosomal abnormalities, and brain magnetic resonance imaging cortical volumes were evaluated in 133 patients with COS. Cortical analyses included age- and gender-matched healthy volunteers (n = 124). Results Males with COS (n = 72) had a slightly but significantly younger age of onset than females with COS (mean age 9.51 ± 2.28 versus 10.29 ± 1.63 years, t131 = 2.21, p = .03), higher verbal IQ scores (83.00 ± 15.97 versus 75.58 ± 15.10, t89 = 2.24, p = .03), and higher rates of comorbid pervasive developmental disorder (28.17% versus 6.90%, χ²1 = 9.54, p < .01) and attention-deficit/hyperactivity disorder (43.86% versus 21.43%, χ²1 = 5.40, p = .02). There were no significant gender differences across other demographic, IQ, or clinical measurements, frequency of chromosomal abnormalities, family clinical measurements, premorbid functioning, or in gender-by-disorder interactions for magnetic resonance imaging brain measurements. Conclusion The present comprehensive examination found few remarkable gender differences in COS. Although less striking than that seen in adult-onset schizophrenia, males with COS had a younger age of onset. Attention-deficit/hyperactivity disorder and pervasive developmental disorder rates were high in COS overall, suggesting greater neurodevelopmental vulnerability in COS. However, the gender ratios of these comorbidities in COS mirror those of the general populations, indicating that these gender differences might be unrelated to COS.

Citations (5)


... Iwabuchi et al. (42) compared machine learning classification of gray matter and white matter intensity images acquired at 3T and 7T, showing improved accuracy, sensitivity, and specificity of patient classification at 7T. Reduced hippocampus and hippocampal subfield volumes are a robust finding at lower field strengths in schizophrenia-spectrum disorders (43,44). These findings have been replicated at 7T in first-episode psychosis (41) and childhood-onset schizophrenia (45), with the latter reporting multiscale associations with cognitive impairment. In an innovative study highlighting the qualitative improvements of UHF-sMRI, Kirov et al. (46) visualized the granule cell layer of the hippocampal dentate gyrus at 232 × 232 × 1,500 µm in 16 schizophrenia patients and 15 healthy controls. ...

Reference:

Ultra-high field neuroimaging in psychosis: A narrative review
7 T MRI reveals hippocampal structural abnormalities associated with memory intrusions in childhood-onset schizophrenia

Schizophrenia Research

... However, while accumulating evidence suggests that the core network changes in cortical-striatal circuits mainly involve prefrontal, temporal and subcortical regions [7][8][9], it remains unclear how these changes are related to psychotic symptoms (also known as positive manifestations, which are the key features of schizophrenia), such as hallucinations and delusions. For example, functional connectivity (FC) studies have reported altered connectivity in the default mode network (DMN) and sensorimotor network (SMN) in AOS patients [10,11], but these changes were not related to psychotic symptoms. It has also been reported that the disorganization of brain function in this disorder progressed from a local region to more distributed networks. ...

Attenuated resting-state functional connectivity in patients with childhood- and adult-onset schizophrenia

Schizophrenia Research

... Most areas recognized for their role in WM exhibited load-dependent activity and connectivity when performing WM tasks in SZ [35]; our results are in concordance with this literature. Impaired functional activation and connectivity in FPN during WM tasks have been demonstrated in SZ [37,38]. Our previous work [39] reported that compared to HCs, SZ had increased temporal variability of degree centrality in the inferior parietal lobe under the "2-back" load, which was the critical node of FPN in our results. ...

Reduced Functional Brain Activation and Connectivity During a Working Memory Task in Childhood-Onset Schizophrenia
  • Citing Article
  • December 2017

Journal of the American Academy of Child & Adolescent Psychiatry

... [9][10][11] COS (onset <13 years) is rare in occurrence, and symptom dimensions include both positive and negative symptoms, with disorganisation being less common. 12 Developmental deviance, especially in the speech and language domains, and poor premorbid adjustment before illness onset have been reported in COS. 13,14 The diagnosis of psychotic symptoms in children is often complex because of the symptomatic overlap with other emotional, behavioural and neurodevelopmental disorders. ...

Symptom dimensions and subgroups in childhood-onset schizophrenia
  • Citing Article
  • November 2017

Schizophrenia Research

... Several biopsychosocial approaches, including genetic, susceptibility, and neurodevelopmental differences, have been proposed to explain the sex differences [17]. Additionally, earlier research demonstrated sex differences in adolescent patients with SCZ pathogenesis and prognosis, with outcomes quite comparable to those of adult patients [18,19]. For example, males were shown to adhere to treatment better among adolescents with patients with SCZ, although females did better regarding social cognition [20]. ...

Lack of Gender-Related Differences in Childhood-Onset Schizophrenia

Journal of the American Academy of Child & Adolescent Psychiatry