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精神分裂症超高危人群中强迫症的纵向研究。

A longitudinal study of obsessive-compulsive disorder in individuals at ultra-high risk for psychosis.

机构信息

Melbourne Neuropsychiatry Centre, University of Melbourne and Melbourne Health, Australia.

出版信息

J Psychiatr Res. 2011 Sep;45(9):1140-5. doi: 10.1016/j.jpsychires.2011.03.005. Epub 2011 Mar 26.

Abstract

BACKGROUND

We evaluated whether (1) a diagnosis of obsessive-compulsive disorder (OCD) at baseline, or (2) the persistence, remission or emergence of de novo OCD at follow-up, were associated with the development of different psychotic disorders in a cohort of individuals at ultra-high risk (UHR) for psychosis.

METHODS

Patients were assessed for OCD at baseline and after a mean of 7.4 years follow-up and classified into: (i) Non-OCD group - patients without OCD both at baseline and follow-up (n = 269; 86.2%), (ii) Incident OCD group - patients without OCD at baseline but with OCD at follow-up (n = 17; 5.4%), (iii) Remitting OCD group - patients with OCD at baseline but without OCD at follow-up (n = 20; 6.4%), (iv) Persistent OCD group - patients with OCD both at baseline and at follow-up (n = 6; 1.9%). Rates of different DSM-IV psychotic disorders at follow-up were compared across these groups.

RESULTS

Patients who displayed remitting OCD were not related to the development of any DSM-IV psychotic disorder. A diagnosis of incident OCD was associated with greater rates of psychotic disorders at follow-up, particularly mood disorders with psychotic features and psychotic disorders not otherwise specified (PDNOS), and greater baseline severity of general psychopathology, alogia, and avolition-apathy. Two of the six patients (40%) with persistent OCD developed schizophrenia, while only 12.5%, 5.0%, and 9.7% of incident, remitting, and non-OCD groups, respectively, exhibited the same condition at follow-up. Rates of antipsychotic use in the previous two years were not significantly different between the groups.

CONCLUSIONS

Our findings suggest that, in a cohort of individuals at UHR for psychosis, remission of OCD does not increase the risk of psychosis, while de novo OCD was associated with development of mood disorders with psychotic features and PDNOS.

摘要

背景

我们评估了在精神病超高风险(UHR)人群队列中,(1)基线时的强迫症(OCD)诊断,或(2)随访时新发 OCD 的持续、缓解或出现,是否与不同精神分裂症障碍的发展相关。

方法

在基线和平均 7.4 年随访后评估患者的 OCD,并将患者分为以下几类:(i)非 OCD 组 - 基线和随访时均无 OCD(n=269;86.2%),(ii)新发 OCD 组 - 基线时无 OCD,但随访时有 OCD(n=17;5.4%),(iii)缓解 OCD 组 - 基线时有 OCD,但随访时无 OCD(n=20;6.4%),(iv)持续 OCD 组 - 基线和随访时均有 OCD(n=6;1.9%)。比较这些组在随访时不同 DSM-IV 精神分裂症障碍的发生率。

结果

显示缓解 OCD 的患者与任何 DSM-IV 精神分裂症障碍的发展无关。新发 OCD 的诊断与随访时更高的精神分裂症障碍发生率相关,特别是心境障碍伴精神病性特征和未特定的精神病性障碍,以及更基线时的一般精神病理学、言语贫乏和意志缺失-冷漠的严重程度。六名持续 OCD 患者中的两名(40%)发展为精神分裂症,而只有 12.5%、5.0%和 9.7%的新发、缓解和非 OCD 组分别在随访时出现相同情况。在过去两年中,各组使用抗精神病药物的比率没有显著差异。

结论

我们的发现表明,在精神病 UHR 人群队列中,OCD 的缓解不会增加患精神分裂症的风险,而新发 OCD 与心境障碍伴精神病性特征和未特定的精神病性障碍的发展相关。

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