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Hippocampal volume change in depression: late- and early-onset illness compared

机译:抑郁症海马体积变化:较早和较早发病

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Background Evidence for structural hippocampal change in depression is limited despite reports of neuronal damage due to hypercortisolaemia and vascular pathology. Aims To compare hippocampal and white matter structural change in demographically matched controls and participants with early-onset and late-onset depression. Method High-resolution volumetric magnetic resonance imaging (MRI) and rating of MRI hyperintensities. Results Atotal of 51 people with depression and 39 control participants were included. Participants with late-onset depression had bilateral hippocampal atrophy compared with those with early-onset depression and controls. Hippocampal volumes did not differ between control participants and those with early-onset depression. Age of depression onset correlated (negatively) with hippocampal volume but lifetime duration of depression did not. Hyperintensity ratings did not differ between groups. Conclusions Results suggest that acquired biological factors are of greater importance in late-than in early-onset illness and that pathological processes other than exposure to hypercortisolaemia of depression underlie hippocampal atrophy in depression of late life.
机译:背景尽管有报道称由于过度皮质醇血症和血管病变导致神经元受损,但抑郁症海马结构发生变化的证据有限。目的比较人口统计学匹配的对照组和患有早发和晚发抑郁的参与者的海马和白质结构变化。方法高分辨率体磁共振成像(MRI)和MRI高强度评估。结果共纳入51名抑郁症患者和39名对照组参与者。与早发性抑郁症和对照组相比,迟发性抑郁症的参与者双侧海马萎缩。对照参与者和早发性抑郁症患者的海马体积没有差异。抑郁发作的年龄与海马体积(负)相关,但抑郁的终生持续时间与年龄无关。高强度等级在两组之间没有差异。结论结果表明,获得性生物学因素在迟发性疾病中比在早发性疾病中更重要,并且除了暴露于抑郁症的高皮质醇血症外,病理过程是晚期抑郁症海马萎缩的基础。

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