Sneller Marius H, de Boer Nini, Everaars Sophie, Schuurmans Max, Guloksuz Sinan, Cahn Wiepke, Luykx Jurjen J
Faculty of Biomedical Sciences, Utrecht University, Utrecht, Netherlands.
Department of Psychiatry, University Medical Center Utrecht Brain Center, University Medical Center Utrecht, Utrecht University, Utrecht, Netherlands.
Front Psychiatry. 2021 Mar 29;12:625935. doi: 10.3389/fpsyt.2021.625935. eCollection 2021.
Individuals with severe mental illness experience increased morbidity and mortality compared to the general population. Adverse effects of antipsychotics, including weight gain, may contribute to the development of metabolic syndrome (MetS), which is associated with increased risks of all-cause and cardiovascular disease mortality. We aim to provide a comprehensive overview of clinical, biochemical and genetic factors associated with MetS among patients with schizophrenia spectrum disorders using second-generation antipsychotics (SGA). A literature search was performed in Pubmed and Embase to identify all cohort studies, cross-sectional studies and clinical trials investigating associations with MetS in patients with schizophrenia spectrum disorders using SGAs. We extracted and enumerated clinical, biochemical and genetic factors reported to be associated with MetS. We defined factors associated with MetS as factors being reported as associated with MetS in two or more studies. 58 studies were included in this review ( = 12,123). In total, 62 factors were found to be associated with increased risk of MetS. Thirty one out of 58 studies investigated factors that were reported as associated with MetS in two or more studies. With regard to clinical factors, we found gender, higher age, concomitant use of mood stabilizers, higher baseline and current BMI, earlier SGA exposure, higher dose, longer duration of treatment, psychosis and tobacco smoking to be significantly associated with MetS. Furthermore, the biochemical factors hypo-adiponectinemia, elevated levels of C-reactive protein (CRP) and higher white blood cell (WBC) count were identified as factors associated with MetS. Among pharmacogenetic factors, the rs1414334 C-allele of the HTR2C-gene was associated with MetS in patients using SGA. In this systematic review investigating clinical, biochemical and genetic factors associated with MetS in patients using SGAs we found that higher age, higher baseline BMI, higher current BMI and male as well as female gender were positively associated with MetS across all antipsychotics. This study may set the stage for the application of clinical, biochemical and genetic factors to predict the risk of developing MetS in patients using SGAs. Future research is needed to determine which patients using SGAs are at risk to develop MetS in clinical practice.
与普通人群相比,患有严重精神疾病的个体发病率和死亡率更高。抗精神病药物的不良反应,包括体重增加,可能会导致代谢综合征(MetS)的发生,而代谢综合征与全因死亡和心血管疾病死亡风险的增加有关。我们旨在全面概述使用第二代抗精神病药物(SGA)的精神分裂症谱系障碍患者中与代谢综合征相关的临床、生化和遗传因素。在PubMed和Embase上进行了文献检索,以确定所有调查使用SGA的精神分裂症谱系障碍患者与代谢综合征相关性的队列研究、横断面研究和临床试验。我们提取并列举了据报道与代谢综合征相关的临床、生化和遗传因素。我们将与代谢综合征相关的因素定义为在两项或更多研究中被报道与代谢综合征相关的因素。本综述纳入了58项研究(n = 12,123)。总共发现62个因素与代谢综合征风险增加相关。58项研究中有31项调查了在两项或更多研究中被报道与代谢综合征相关的因素。关于临床因素,我们发现性别、年龄较大、同时使用心境稳定剂、基线和当前较高的体重指数(BMI)、更早接触SGA、更高剂量、更长治疗持续时间、精神病和吸烟与代谢综合征显著相关。此外,低脂联素血症、C反应蛋白(CRP)水平升高和白细胞(WBC)计数较高等生化因素被确定为与代谢综合征相关的因素。在药物遗传学因素中,HTR2C基因的rs1414334 C等位基因与使用SGA的患者的代谢综合征相关。在这项调查使用SGA的患者中与代谢综合征相关的临床、生化和遗传因素的系统综述中,我们发现年龄较大、基线BMI较高、当前BMI较高以及男性和女性性别在所有抗精神病药物中均与代谢综合征呈正相关。本研究可能为应用临床、生化和遗传因素预测使用SGA的患者发生代谢综合征的风险奠定基础。未来需要进行研究以确定在临床实践中哪些使用SGA的患者有发生代谢综合征的风险。
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