Meta-analyses of epigenetic age acceleration and GrimAge components of schizophrenia or first-episode psychosis.

IF 3 Q2 PSYCHIATRY
Toshiyuki Shirai, Satoshi Okazaki, Takaki Tanifuji, Shusuke Numata, Tomohiko Nakayama, Tomohiro Yoshida, Kentaro Mouri, Ikuo Otsuka, Noboru Hiroi, Akitoyo Hishimoto
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Abstract

Schizophrenia is a common chronic psychiatric disorder that causes age-related dysfunction. The life expectancy in patients with schizophrenia is ≥10 years shorter than that in the general population because of the higher risk of other diseases, such as cardiovascular diseases. Aging studies based on DNA methylation status have received considerable attention. Several epigenetic age accelerations and predicted values of aging-related proteins (GrimAge and GrimAge2 components) have been analyzed in multiple diseases. However, no studies have investigated up to GrimAge and GrimAge2 components between patients with schizophrenia and controls. Therefore, we aimed to conduct multiple regression analyses to investigate the association between schizophrenia and epigenetic age accelerations and GrimAge and GrimAge2 components in seven cohorts. Furthermore, we included patients with first-episode psychosis whose illness duration was often shorter than schizophrenia in our analysis. We integrated these results with meta-analyses, noting the acceleration of GrimAge, GrimAge2, and DunedinPACE, and increase in adrenomedullin, beta-2 microglobulin, cystatin C, and plasminogen activation inhibitor-1 levels, in patients with schizophrenia or first-episode psychosis. These results corroborated the finding that patients with schizophrenia had an increased risk of diabetes, cardiovascular disease, and cognitive dysfunction from a biological perspective. Patients with schizophrenia and first-episode psychosis showed differences in the results when compared with controls. Such analyses may lead to the development of novel therapeutic targets to patients with schizophrenia or relevant diseases from the perspective of aging in the future.

精神分裂症或首发精神病的表观遗传年龄加速和 GrimAge 成分的元分析。
精神分裂症是一种常见的慢性精神疾病,会导致与年龄相关的功能障碍。由于患心血管疾病等其他疾病的风险较高,精神分裂症患者的预期寿命比普通人群短≥10年。基于 DNA 甲基化状态的衰老研究受到了广泛关注。已经分析了多种疾病的几种表观遗传年龄加速度和衰老相关蛋白(GrimAge 和 GrimAge2 成分)的预测值。然而,还没有研究调查过精神分裂症患者和对照组之间的 GrimAge 和 GrimAge2 成分。因此,我们旨在进行多元回归分析,研究精神分裂症与表观遗传年龄加速以及七个队列中的 GrimAge 和 GrimAge2 成分之间的关联。此外,我们还将病程通常短于精神分裂症的首发精神病患者纳入分析范围。我们将这些结果与荟萃分析相结合,注意到精神分裂症或首发精神病患者的 GrimAge、GrimAge2 和 DunedinPACE 加速,肾上腺髓质素、β-2 微球蛋白、胱抑素 C 和纤溶酶原激活抑制剂-1 水平升高。这些结果从生物学角度证实了精神分裂症患者罹患糖尿病、心血管疾病和认知功能障碍的风险增加这一发现。与对照组相比,精神分裂症患者和首发精神病患者的结果存在差异。这些分析可能会为精神分裂症患者或未来从老龄化角度治疗相关疾病开发新的治疗靶点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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