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Personne :
Paccalet, Thomas

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Paccalet

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Thomas

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Université Laval

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ncf10904873

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  • PublicationRestreint
    Cognitive structure from childhood to adulthood in kindreds densely affected by schizophrenia and bipolar disorder
    (Elsevier Ltd., 2015-07-23) Mérette, Chantal; Jomphe, Valérie; Moreau, Isabel; Gilbert, Elsa; Paccalet, Thomas; Roy, Marc-André; Rouleau, Nancie; Cellard, Caroline; Maziade, Michel
    The developmental aspects of cognitive structures from childhood until adulthood and across different levels of risk for psychopathology have been little studied. The aim of the current study was to explore the cognitive factorial structure in subsamples from highly familial and densely affected kindreds of schizophrenia and bipolar disorder – i.e. affected adult members, non-affected adult members and high-risk youth. The same neuropsychological battery was administered in a sample of 480 participants: schizophrenia and bipolar patients (n=51), young high-risk offspring (n=61), non-affected adult relatives of patients (n=96), and controls (n=272). Exploratory Factorial Analysis was performed in the control sample and yielded a 5-factor solution: verbal comprehension, processing speed/working memory, visual learning and memory, verbal learning and memory, reasoning and problem solving. Confirmatory factor analysis indicated that the hierarchical 5-factor solution was well suited for the young high-risk offspring, the non-affected adult relatives of patient and the patients. A hierarchical model with a “g” factor was a good fit for all subsamples. These results suggest that cognitive impairments may aggregate in highly familial individuals.
  • PublicationAccès libre
    Polygenic risk scores distinguish patients from non-affected adult relatives and from normal controls in Schizophrenia and Bipolar Disorder multi-affected kindreds
    (Wiley, 2017-11-28) Mérette, Chantal; Boies, Sébastien; Paccalet, Thomas; Bureau, Alexandre; Maziade, Michel
    Recent studies have used results on SNP association with schizophrenia (SZ) and bipolar disorder (BD) to create polygenic risk scores (PRS) discriminating non‐familial unrelated patients from controls. Little is known about the role of PRS in densely affected multigenerational families. We tested PRS differences between affected SZ and BD family members from their non‐affected adult relatives (NAARs) in Eastern Quebec Kindreds and from controls. We examined 1227 subjects: from 17 SZ and BD kindreds, we studied 153 patients (57 SZ, 13 schizoaffective, and 83 BD) and 180 NAARs, and 894 unrelated controls from the Eastern Quebec population. PRS were derived from published case‐control association studies of SZ and BD. We also constructed a combined SZ and BD PRS by using SNPs from both SZ and BD PRS. SZ patients had higher SZ PRS than controls (p = 0.0039, R2 = 0.027) and BD patients had higher BD PRS than controls (p = 0.013, R2 = 0.027). Differences between affected subjects and NAARs and controls were significant with both SZ and BD PRS. Moreover, a combined SZ‐BD PRS was also significantly associated with SZ and BD when compared to NAARs (p = 0.0019, R2 = 0.010) and controls (p = 0.0025, R2 = 0.028), revealing a SZ‐BD commonality effect in PRS at the diagnosis level. The SZ and the BD PRS, however, showed a degree of specificity regarding thought disorder symptoms. Overall, our report would confirm the usefulness of PRS in capturing the contribution of common genetic variants to the risk of SZ and BD in densely affected families.