Psychiatry - Research Publications

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Start date: 2010 × End date: 2019 × Author: Pantelis, Christos × Author: Bousman, Chad × Author: Sundram, Suresh ×

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    Peripheral Transcription of NRG-ErbB Pathway Genes Are Upregulated in Treatment-Resistant Schizophrenia
    Mostaid, MS ; Lee, TT ; Chana, G ; Sundram, S ; Weickert, CS ; Pantelis, C ; Everall, I ; Bousman, C (FRONTIERS MEDIA SA, 2017-11-06)
    Investigation of peripheral gene expression patterns of transcripts within the NRG-ErbB signaling pathway, other than neuregulin-1 (NRG1), among patients with schizophrenia and more specifically treatment-resistant schizophrenia (TRS) is limited. The present study built on our previous work demonstrating elevated levels of NRG1 EGFα, EGFβ, and type I(Ig2) containing transcripts in TRS by investigating 11 NRG-ErbB signaling pathway mRNA transcripts (NRG2, ErbB1, ErbB2, ErbB3, ErbB4, PIK3CD, PIK3R3, AKT1, mTOR, P70S6K, eIF4EBP1) in whole blood of TRS patients (N = 71) and healthy controls (N = 57). We also examined the effect of clozapine exposure on transcript levels using cultured peripheral blood mononuclear cells (PBMCs) from 15 healthy individuals. Five transcripts (ErbB3, PIK3CD, AKT1, P70S6K, eIF4EBP1) were significantly elevated in TRS patients compared to healthy controls but only expression of P70S6K (Pcorrected = 0.018), a protein kinase linked to protein synthesis, cell growth, and cell proliferation, survived correction for multiple testing using the Benjamini-Hochberg method. Investigation of clinical factors revealed that ErbB2, PIK3CD, PIK3R3, AKT1, mTOR, and P70S6K expression were negatively correlated with duration of illness. However, no transcript was associated with chlorpromazine equivalent dose or clozapine plasma levels, the latter supported by our in vitro PBMC clozapine exposure experiment. Taken together with previously published NRG1 results, our findings suggest an overall upregulation of transcripts within the NRG-ErbB signaling pathway among individuals with schizophrenia some of which attenuate over duration of illness. Follow-up studies are needed to determine if the observed peripheral upregulation of transcripts within the NRG-ErbB signaling pathway are specific to TRS or are a general blood-based marker of schizophrenia.
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    The impact of premorbid and current intellect in schizophrenia: cognitive, symptom, and functional outcomes
    Wells, R ; Swaminathan, V ; Sundram, S ; Weinberg, D ; Bruggemann, J ; Jacomb, I ; Cropley, V ; Lenroot, R ; Pereira, AM ; Zalesky, A ; Bousman, C ; Pantelis, C ; Weickert, CS ; Weickert, TW (SPRINGERNATURE, 2015)
    BACKGROUND: Cognitive heterogeneity among people with schizophrenia has been defined on the basis of premorbid and current intelligence quotient (IQ) estimates. In a relatively large, community cohort, we aimed to independently replicate and extend cognitive subtyping work by determining the extent of symptom severity and functional deficits in each group. METHODS: A total of 635 healthy controls and 534 patients with a diagnosis of schizophrenia or schizoaffective disorder were recruited through the Australian Schizophrenia Research Bank. Patients were classified into cognitive subgroups on the basis of the Wechsler Test of Adult Reading (a premorbid IQ estimate) and current overall cognitive abilities into preserved, deteriorated, and compromised groups using both clinical and empirical (k-means clustering) methods. Additional cognitive, functional, and symptom outcomes were compared among the resulting groups. RESULTS: A total of 157 patients (29%) classified as 'preserved' performed within one s.d. of control means in all cognitive domains. Patients classified as 'deteriorated' (n=239, 44%) performed more than one s.d. below control means in all cognitive domains except estimated premorbid IQ and current visuospatial abilities. A separate 138 patients (26%), classified as 'compromised,' performed more than one s.d. below control means in all cognitive domains and displayed greater impairment than other groups on symptom and functional measures. CONCLUSIONS: In the present study, we independently replicated our previous cognitive classifications of people with schizophrenia. In addition, we extended previous work by demonstrating worse functional outcomes and symptom severity in the compromised group.
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    Meta-analysis reveals associations between genetic variation in the 5′ and 3′regions of Neuregulin-1 and schizophrenia
    Mostaid, MS ; Mancuso, SG ; Liu, C ; Sundram, S ; Pantelis, C ; Everall, IP ; Bousman, CA (SPRINGERNATURE, 2017-01-17)
    Genetic, post-mortem and neuroimaging studies repeatedly implicate neuregulin-1 (NRG1) as a critical component in the pathophysiology of schizophrenia. Although a number of risk haplotypes along with several genetic polymorphisms in the 5' and 3' regions of NRG1 have been linked with schizophrenia, results have been mixed. To reconcile these conflicting findings, we conducted a meta-analysis examining 22 polymorphisms and two haplotypes in NRG1 among 16 720 cases, 20 449 controls and 2157 family trios. We found significant associations for three polymorphisms (rs62510682, rs35753505 and 478B14-848) at the 5'-end and two (rs2954041 and rs10503929) near the 3'-end of NRG1. Population stratification effects were found for the rs35753505 and 478B14-848(4) polymorphisms. There was evidence of heterogeneity for all significant markers and the findings were robust to publication bias. No significant haplotype associations were found. Our results suggest genetic variation at the 5' and 3' ends of NRG1 are associated with schizophrenia and provide renewed justification for further investigation of NRG1's role in the pathophysiology of schizophrenia.
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    Elevated peripheral expression of neuregulin-1 (NRG1) mRNA isoforms in clozapine-treated schizophrenia patients
    Mostaid, MS ; Lee, TT ; Chana, G ; Sundram, S ; Weickert, CS ; Pantelis, C ; Everall, I ; Bousman, C (NATURE PUBLISHING GROUP, 2017-12-11)
    Differential expression of neuregulin-1 (NRG1) mRNA isoforms and proteins has been reported in schizophrenia, primarily in post-mortem brain tissue. In this study, we examined 12 NRG1 SNPs, eight NRG1 mRNA isoforms (type I, type I(Ig2), type II, type III, type IV, EGFα, EGFβ, pan-NRG1) in whole blood, and NRG1-β1 protein in serum of clozapine-treated schizophrenia patients (N = 71) and healthy controls (N = 57). In addition, using cultured peripheral blood mononuclear cells (PBMC) from 15 healthy individuals, we examined the effect of clozapine on NRG1 mRNA isoform and protein expression. We found elevated levels of NRG1 mRNA, specifically the EGFα (P = 0.0175), EGFβ (P = 0.002) and type I(Ig2) (P = 0.023) containing transcripts, but lower NRG1-β1 serum protein levels (P = 0.019) in schizophrenia patients compared to healthy controls. However, adjusting for smoking status attenuated the difference in NRG1-β1 serum levels (P = 0.050). Examination of clinical factors showed NRG1 EGFα (P = 0.02) and EGFβ (P = 0.02) isoform expression was negatively correlated with age of onset. However, we found limited evidence that NRG1 mRNA isoform or protein expression was associated with current chlorpromazine equivalent dose or clozapine plasma levels, the latter corroborated by our PBMC clozapine exposure experiment. Our SNP analysis found no robust expression quantitative trait loci. Our results represent the first comprehensive investigation of NRG1 isoforms and protein expression in the blood of clozapine-treated schizophrenia patients and suggest levels of some NRG1 transcripts are upregulated in those with schizophrenia.
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    Widespread white matter microstructural differences in schizophrenia across 4322 individuals: results from the ENIGMA Schizophrenia DTI Working Group
    Kelly, S ; Jahanshad, N ; Zalesky, A ; Kochunov, P ; Agartz, I ; Alloza, C ; Andreassen, OA ; Arango, C ; Banaj, N ; Bouix, S ; Bousman, CA ; Brouwer, RM ; Bruggemann, J ; Bustillo, J ; Cahn, W ; Calhoun, V ; Cannon, D ; Carr, V ; Catts, S ; Chen, J ; Chen, J-X ; Chen, X ; Chiapponi, C ; Cho, KK ; Ciullo, V ; Corvin, AS ; Crespo-Facorro, B ; Cropley, V ; De Rossi, P ; Diaz-Caneja, CM ; Dickie, EW ; Ehrlich, S ; Fan, F-M ; Faskowitz, J ; Fatouros-Bergman, H ; Flyckt, L ; Ford, JM ; Fouche, J-P ; Fukunaga, M ; Gill, M ; Glahn, DC ; Gollub, R ; Goudzwaard, ED ; Guo, H ; Gur, RE ; Gur, RC ; Gurholt, TP ; Hashimoto, R ; Hatton, SN ; Henskens, FA ; Hibar, DP ; Hickie, IB ; Hong, LE ; Horacek, J ; Howells, FM ; Pol, HEH ; Hyde, CL ; Isaev, D ; Jablensky, A ; Jansen, PR ; Janssen, J ; Jonsson, EG ; Jung, LA ; Kahn, RS ; Kikinis, Z ; Liu, K ; Klauser, P ; Knoechel, C ; Kubicki, M ; Lagopoulos, J ; Langen, C ; Lawrie, S ; Lenroot, RK ; Lim, KO ; Lopez-Jaramillo, C ; Lyall, A ; Magnotta, V ; Mandl, RCW ; Mathalon, DH ; McCarley, RW ; McCarthy-Jones, S ; McDonald, C ; McEwen, S ; McIntosh, A ; Melicher, T ; Mesholam-Gately, R ; Michie, PT ; Mowry, B ; Mueller, BA ; Newell, DT ; O'Donnell, P ; Oertel-Knoechel, V ; Oestreich, L ; Paciga, SA ; Pantelis, C ; Pasternak, O ; Pearlson, G ; Pellicano, GR ; Pereira, A ; Zapata, JP ; Piras, F ; Potkin, SG ; Preda, A ; Rasser, PE ; Roalf, DR ; Roiz, R ; Roos, A ; Rotenberg, D ; Satterthwaite, TD ; Savadjiev, P ; Schall, U ; Scott, RJ ; Seal, ML ; Seidman, LJ ; Weickert, CS ; Whelan, CD ; Shenton, ME ; Kwon, JS ; Spalletta, G ; Spaniel, F ; Sprooten, E ; Stablein, M ; Stein, DJ ; Sundram, S ; Tan, Y ; Tan, S ; Tang, S ; Temmingh, HS ; Westlye, LT ; Tonnesen, S ; Tordesillas-Gutierrez, D ; Doan, NT ; Vaidya, J ; van Haren, NEM ; Vargas, CD ; Vecchio, D ; Velakoulis, D ; Voineskos, A ; Voyvodic, JQ ; Wang, Z ; Wan, P ; Wei, D ; Weickert, TW ; Whalley, H ; White, T ; Whitford, TJ ; Wojcik, JD ; Xiang, H ; Xie, Z ; Yamamori, H ; Yang, F ; Yao, N ; Zhang, G ; Zhao, J ; van Erp, TGM ; Turner, J ; Thompson, PM ; Donohoe, G (SPRINGERNATURE, 2018-05)
    The regional distribution of white matter (WM) abnormalities in schizophrenia remains poorly understood, and reported disease effects on the brain vary widely between studies. In an effort to identify commonalities across studies, we perform what we believe is the first ever large-scale coordinated study of WM microstructural differences in schizophrenia. Our analysis consisted of 2359 healthy controls and 1963 schizophrenia patients from 29 independent international studies; we harmonized the processing and statistical analyses of diffusion tensor imaging (DTI) data across sites and meta-analyzed effects across studies. Significant reductions in fractional anisotropy (FA) in schizophrenia patients were widespread, and detected in 20 of 25 regions of interest within a WM skeleton representing all major WM fasciculi. Effect sizes varied by region, peaking at (d=0.42) for the entire WM skeleton, driven more by peripheral areas as opposed to the core WM where regions of interest were defined. The anterior corona radiata (d=0.40) and corpus callosum (d=0.39), specifically its body (d=0.39) and genu (d=0.37), showed greatest effects. Significant decreases, to lesser degrees, were observed in almost all regions analyzed. Larger effect sizes were observed for FA than diffusivity measures; significantly higher mean and radial diffusivity was observed for schizophrenia patients compared with controls. No significant effects of age at onset of schizophrenia or medication dosage were detected. As the largest coordinated analysis of WM differences in a psychiatric disorder to date, the present study provides a robust profile of widespread WM abnormalities in schizophrenia patients worldwide. Interactive three-dimensional visualization of the results is available at www.enigma-viewer.org.
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    Exploring the moderating effects of dopaminergic polymorphisms and childhood adversity on brain morphology in schizophrenia-spectrum disorders
    Hoffmann, C ; Van Rheenen, TE ; Mancuso, SG ; Zalesky, A ; Bruggemann, J ; Lenroot, RK ; Sundram, S ; Weickert, CS ; Weickert, TW ; Pantelis, C ; Cropley, V ; Bousman, CA (ELSEVIER IRELAND LTD, 2018-11-30)
    Genetic and environmental etiologies may contribute to schizophrenia and its associated neurobiological profile. We examined the interaction between dopaminergic polymorphisms, childhood adversity and diagnosis (schizophrenia/schizoaffective disorder) on dopamine-related brain structures. Childhood adversity histories and structural MRI data were obtained from 249 (153 schizophrenia/schizoaffective, 96 controls) participants registered in the Australian Schizophrenia Research Bank. Polymorphisms in DRD2 and COMT were genotyped and a dopaminergic risk allelic load (RAL) was calculated. Regression analysis was used to test the main and interaction effects of RAL, childhood adversity and diagnosis on volumes of dopamine-related brain structures (caudate, putamen, nucleus accumbens, dorsolateral prefrontal cortex and hippocampus). A schizophrenia/schizoaffective diagnosis showed significant main effects on bilateral hippocampus, left dorsolateral prefrontal cortex and bilateral putamen volumes. RAL showed a significant main effect on left putamen volumes. Furthermore, across the whole sample, a significant two-way interaction between dopaminergic RAL and childhood adversity was found for left putamen volumes. No brain structure volumes were predicted by a three-way interaction that included diagnosis. Our finding suggests the left putamen may be particularly sensitive to dopaminergic gene-environment interactions regardless of diagnosis. However, larger studies are needed to assess whether these interactions are more or less pronounced in those with schizophrenia/schizoaffective disorders.
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    Widespread Volumetric Reductions in Schizophrenia and Schizoaffective Patients Displaying Compromised Cognitive Abilities
    Van Rheenen, TE ; Cropley, V ; Zalesky, A ; Bousman, C ; Wells, R ; Bruggemann, J ; Sundram, S ; Weinberg, D ; Lenroot, RK ; Pereira, A ; Weickert, CS ; Weickert, TW ; Pantelis, C (OXFORD UNIV PRESS, 2018-05)
    OBJECTIVE: Progress toward understanding brain mechanisms in psychosis is hampered by failures to account for within-group heterogeneity that exists across neuropsychological domains. We recently identified distinct cognitive subgroups that might assist in identifying more biologically meaningful subtypes of psychosis. In the present study, we examined whether underlying structural brain abnormalities differentiate these cognitively derived subgroups. METHOD: 1.5T T1 weighted structural scans were acquired for 168 healthy controls and 220 patients with schizophrenia/schizoaffective disorder. Based on previous work, 47 patients were categorized as being cognitively compromised (impaired premorbid and current IQ), 100 as cognitively deteriorated (normal premorbid IQ, impaired current IQ), and 73 as putatively cognitively preserved (premorbid and current IQ within 1 SD of controls). Global, subcortical and cortical volume, thickness, and surface area measures were compared among groups. RESULTS: Whole cortex, subcortical, and regional volume and thickness reductions were evident in all subgroups compared to controls, with the largest effect sizes in the compromised group. This subgroup also showed abnormalities in regions not seen in the other patient groups, including smaller left superior and middle frontal areas, left anterior and inferior temporal areas and right lateral medial and inferior frontal, occipital lobe and superior temporal areas. CONCLUSIONS: This pattern of more prominent brain structural abnormalities in the group with the most marked cognitive impairments-both currently and putatively prior to illness onset, is consistent with the concept of schizophrenia as a progressive neurodevelopmental disorder. In this group, neurodevelopmental and neurodegenerative factors may be important for cognitive function.