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Global burden of 369 diseases and injuries in 204 countries and territories, 1990-2019: a systematic analysis for the Global Burden of Disease Study 2019.204 个国家和地区 1990-2019 年 369 种疾病和伤害导致的全球负担:2019 年全球疾病负担研究的系统分析。
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Risk of Subjection to Violence and Perpetration of Violence in Persons With Psychiatric Disorders in Sweden.瑞典精神障碍患者遭受暴力和实施暴力的风险。
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精神共病与瑞典慢性呼吸系统疾病、心血管疾病和糖尿病患者过早死亡和自杀风险:一项涉及超过 100 万患者及其未受影响兄弟姐妹的全国匹配队列研究。

Psychiatric comorbidity and risk of premature mortality and suicide among those with chronic respiratory diseases, cardiovascular diseases, and diabetes in Sweden: A nationwide matched cohort study of over 1 million patients and their unaffected siblings.

机构信息

Department of Psychiatry, University of Oxford, Warneford Hospital, Oxford, United Kingdom.

Department of Medical Epidemiology and Biostatistics, Karolinska Institutet, Stockholm, Sweden.

出版信息

PLoS Med. 2022 Jan 27;19(1):e1003864. doi: 10.1371/journal.pmed.1003864. eCollection 2022 Jan.

DOI:10.1371/journal.pmed.1003864
PMID:35085232
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8794193/
Abstract

BACKGROUND

Persons with noncommunicable diseases have elevated rates of premature mortality. The contribution of psychiatric comorbidity to this is uncertain. We aimed to determine the risks of premature mortality and suicide in people with common noncommunicable diseases, with and without psychiatric disorder comorbidity.

METHODS AND FINDINGS

We used nationwide registries to study all individuals born in Sweden between 1932 and 1995 with inpatient and outpatient diagnoses of chronic respiratory diseases (n = 249,825), cardiovascular diseases (n = 568,818), and diabetes (n = 255,579) for risks of premature mortality (≤age 65 years) and suicide until 31 December 2013. Patients diagnosed with either chronic respiratory diseases, cardiovascular diseases, or diabetes were compared with age and sex-matched population controls (n = 10,345,758) and unaffected biological full siblings (n = 1,119,543). Comorbidity with any psychiatric disorder, and by major psychiatric categories, was examined using diagnoses from patient registers. Associations were quantified using stratified Cox regression models that accounted for time at risk, measured sociodemographic factors, and unmeasured familial confounders via sibling comparisons. Within 5 years of diagnosis, at least 7% (range 7.4% to 10.8%; P < 0.001) of patients with respiratory diseases, cardiovascular diseases, or diabetes (median age at diagnosis: 48 to 54 years) had died from any cause, and 0.3% (0.3% to 0.3%; P < 0.001) had died from suicide, 25% to 32% of people with these medical conditions had co-occurring lifetime diagnoses of any psychiatric disorder, most of which antedated the medical diagnosis. Comorbid psychiatric disorders were associated with higher all-cause mortality (15.4% to 21.1%) when compared to those without such conditions (5.5% to 9.1%). Suicide mortality was also elevated (1.2% to 1.6% in comorbid patients versus 0.1% to 0.1% without comorbidity). When we compared relative risks with siblings without noncommunicable diseases and psychiatric disorders, the comorbidity with any psychiatric disorder was associated with substantially increased mortality rates (adjusted HR range: aHRCR = 7.2 [95% CI: 6.8 to 7.7; P < 0.001] to aHRCV = 8.9 [95% CI: 8.5 to 9.4; P < 0.001]). Notably, comorbid substance use disorders were associated with a higher mortality rate (aHR range: aHRCR = 8.3 [95% CI: 7.6 to 9.1; P < 0.001] to aHRCV = 9.9 [95% CI: 9.3 to 10.6; P < 0.001]) than depression (aHR range: aHRCR = 5.3 [95% CI: 4.7 to 5.9; P < 0.001] to aHRCV = 7.4 [95% CI: 7.0 to 7.9; P < 0.001]), but risks of suicide were similar for these 2 psychiatric comorbidities. One limitation is that we relied on secondary care data to assess psychiatric comorbidities, which may have led to missing some patients with less severe comorbidities. Residual genetic confounding is another limitation, given that biological full siblings share an average of half of their cosegregating genes. However, the reported associations remained large even after adjustment for shared and unmeasured familial confounders.

CONCLUSIONS

In this longitudinal study of over 1 million patients with chronic health diseases, we observed increased risks of all-cause and suicide mortality in individuals with psychiatric comorbidities. Improving assessment, treatment, and follow-up of people with comorbid psychiatric disorders may reduce the risk of mortality in people with chronic noncommunicable diseases.

摘要

背景

患有非传染性疾病的人过早死亡的几率较高。精神共病对这一情况的影响尚不确定。我们旨在确定患有常见非传染性疾病且伴有或不伴有精神障碍共病的患者过早死亡和自杀的风险。

方法和发现

我们使用全国性登记处,研究了在瑞典出生于 1932 年至 1995 年之间的所有患有慢性呼吸系统疾病(n=249825)、心血管疾病(n=568818)和糖尿病(n=255579)的个体,评估他们在截至 2013 年 12 月 31 日之前的过早死亡(≤65 岁)和自杀的风险。将患有慢性呼吸系统疾病、心血管疾病或糖尿病的患者与年龄和性别匹配的人群对照组(n=10345758)和未受影响的生物学全同胞(n=1119543)进行比较。使用患者登记处的诊断来检查任何精神障碍的共病情况,以及主要精神障碍类别。使用分层 Cox 回归模型来量化关联,该模型考虑了风险时间、测量的社会人口学因素以及通过同胞比较来衡量未测量的家族混杂因素。在诊断后的 5 年内,至少有 7%(范围 7.4%至 10.8%;P<0.001)患有呼吸、心血管或糖尿病的患者(中位诊断年龄:48 至 54 岁)已死于任何原因,0.3%(0.3%至 0.3%;P<0.001)已死于自杀,患有这些疾病的人群中,25%至 32%同时患有任何精神障碍的终生诊断,其中大部分诊断先于医疗诊断。与没有这种情况的患者相比,共患精神障碍与全因死亡率较高(15.4%至 21.1%)相关。自杀死亡率也升高(共病患者中为 1.2%至 1.6%,无共病患者中为 0.1%至 0.1%)。当我们将相对风险与无传染性疾病和精神障碍的同胞进行比较时,任何精神障碍的共病与死亡率显著升高相关(调整后的 HR 范围:aHRCR=7.2 [95%CI:6.8 至 7.7;P<0.001]至 aHRCV=8.9 [95%CI:8.5 至 9.4;P<0.001])。值得注意的是,共患物质使用障碍与更高的死亡率相关(aHR 范围:aHRCR=8.3 [95%CI:7.6 至 9.1;P<0.001]至 aHRCV=9.9 [95%CI:9.3 至 10.6;P<0.001]),高于抑郁(aHR 范围:aHRCR=5.3 [95%CI:4.7 至 5.9;P<0.001]至 aHRCV=7.4 [95%CI:7.0 至 7.9;P<0.001]),但这两种精神共病的自杀风险相似。一个局限性是,我们依赖于二级护理数据来评估精神共病,这可能导致一些病情较轻的患者漏诊。另一个局限性是,由于生物学全同胞平均共享一半的共分离基因,因此仍然存在遗传混杂的问题。然而,即使在调整了共享和未测量的家族混杂因素后,所报告的关联仍然很大。

结论

在这项对 100 多万患有慢性健康疾病的患者进行的纵向研究中,我们观察到伴有精神障碍共病的患者全因和自杀死亡率增加。改善对伴有精神障碍共病患者的评估、治疗和随访可能会降低慢性非传染性疾病患者的死亡率。