首页> 美国卫生研究院文献>Schizophrenia Bulletin >Shared Neurocognitive Dysfunctions in Young Offspring at Extreme Risk for Schizophrenia or Bipolar Disorder in Eastern Quebec Multigenerational Families
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Shared Neurocognitive Dysfunctions in Young Offspring at Extreme Risk for Schizophrenia or Bipolar Disorder in Eastern Quebec Multigenerational Families

机译:魁北克东部多代家庭中处于精神分裂症或双相情感障碍极度危险的年轻后代中共有的神经认知功能障碍

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摘要

Background: Adult patients having schizophrenia (SZ) or bipolar disorder (BP) may have in common neurocognitive deficits. Former evidence suggests impairments in several neuropsychological functions in young offspring at genetic risk for SZ or BP. Moreover, a dose-response relation may exist between the degree of familial loading and cognitive impairments. This study examines the cognitive functioning of high-risk (HR) offspring of parents having schizophrenia (HRSZ) and high-risk offspring of parents having bipolar disorder (HRBP) descending from densely affected kindreds. Methods: The sample consisted of 45 young offspring (mean age of 17.3 years) born to a parent having SZ or BP descending from large multigenerational families of Eastern Québec that are densely affected by SZ or BP and followed up since 1989. The offspring were administered a lifetime best-estimate diagnostic procedure (Diagnostic and Statistical Manual of Mental Disorders, Fourth Edition [DSM-IV]) and an extensive standard neuropsychological battery. Raw scores were compared with age- and gender-matched controls. Results: The offspring displayed differences in memory and executive functions when compared with controls. Moderate to large effect sizes (Cohen d) ranging from 0.65 to 1.25 (for IQ and memory) were observed. Several of the cognitive dysfunctions were present in both HRSZ and HRBP, even when considering DSM-IV clinical status. Conclusions: HRSZ and HRBP shared several aspects of their cognitive impairment. Our data suggest that the extremely high genetic and familial loading of these HRs may have contributed to a quantitatively increased magnitude of the cognitive impairments in both HR subgroups, especially in memory. These offspring at heightened risk present difficulties in processing information that warrant preventive research.
机译:背景:患有精神分裂症(SZ)或双相情感障碍(BP)的成年患者可能具有常见的神经认知功能障碍。以前的证据表明,在患有SZ或BP遗传风险的年轻后代中,一些神经心理学功能受到了损害。此外,在家族负荷的程度和认知障碍之间可能存在剂量反应关系。这项研究检查了患有精神分裂症的父母的高危(HR)后代和患有重度患病的双相情感障碍的父母的高危后代(HRBP)的认知功能。方法:该样本由45名年轻后代组成,这些后代的父母是SZ或BP的父母,他们的父母来自魁北克东部大型多代家庭,这些家庭受SZ或BP的影响很大,自1989年以来一直接受随访。一生中最佳估计的诊断程序(《精神障碍诊断和统计手册》,第四版[DSM-IV])和广泛的标准神经心理学工具。将原始分数与年龄和性别匹配的对照进行比较。结果:与对照相比,后代显示出记忆力和执行功能的差异。观察到从0.65到1.25(对于IQ和记忆力)的中等到较大的效应大小(Cohen d)。即使考虑DSM-IV的临床状况,HRSZ和HRBP中都存在几种认知功能障碍。结论:HRSZ和HRBP共享其认知障碍的几个方面。我们的数据表明,这些HR的极高的遗传和家族负荷可能导致两个HR亚组的认知障碍的数量增加,尤其是在记忆方面。这些高风险的后代在处理需要进行预防性研究的信息方面存在困难。

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