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Advanced paternal age is a risk factor for schizophrenia in Iranians

机译:父辈高龄是伊朗人精神分裂症的危险因素

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Background Since 1958 many, but not all studies have demonstrated that paternal age is a risk factor for schizophrenia. There may be many different explanations for differences between studies, including study design, sample size, collection criteria, heterogeneity and the confounding effects of environmental factors that can for example perturb epigenetic programming and lead to an increase in disease risk. The small number of children in Western families makes risk comparisons between siblings born at different paternal ages difficult. In contrast, more Eastern families have children both at early and later periods of life. In the present study, a cross-sectional population study in an Iranian population was performed to compare frequency of schizophrenia in younger offspring (that is, older paternal age) versus older offspring. Methods A total of 220 patients with the diagnosis of schizophrenia (cases) from both psychiatric hospitals and private clinics and 220 individuals from other hospital wards (controls), matched for sex and age were recruited for this study. Patients with neurological problem, substance abuse, mental retardation and mood disorder were excluded from both groups. Results Birth rank comparisons revealed that 35% vs 24% of the cases vs the controls were in the third or upper birth rank ( P = 0.01). Also, the mean age of fathers at birth in case group (30 ± 6.26 years) was significantly more than the control group (26.45 ± 5.64 years; P = 0.0001). The age of 76 fathers at birth in case group was over 32 versus 33 fathers in control group. Individuals whose fathers' age was more than 32 (at birth) were at higher risk (2.77 times) for schizophrenia versus others ( P P = 0.02). Logistic regression analysis suggests that maternal age is less likely to be involved in the higher risk of schizophrenia than advanced parental age. Discussion This study demonstrates a relationship between paternal age and schizophrenia in large families of an Iranian population. Arguments have been put forth that DNA bases changes or epigenetic changes in sperm account for the increased risk associated with older fathers. However, it would not be surprising that both de novo germline mutations and epigenetic changes contribute to disease occurrence because DNA replication and DNA methylation are closely linked at both the macromolecular level (that is, methylation closely follows replication), and at the metabolic level (both processes require folate), and susceptible to modulation by the environment. Further research on samples such as those collected here are needed to sort out the contributions of de novo mutations versus epigenetic changes to schizophrenia.
机译:背景自1958年以来,许多(但不是全部)研究表明,父亲年龄是精神分裂症的危险因素。对于研究之间的差异可能有许多不同的解释,包括研究设计,样本量,收集标准,异质性和环境因素的混杂影响,这些因素可能会干扰表观遗传程序,例如导致疾病风险增加。西方家庭中的儿童数量很少,因此很难比较不同父亲年龄的兄弟姐妹之间的风险。相反,更多的东方家庭在生命的早期和晚期都有孩子。在本研究中,对伊朗人口进行了横断面人口研究,以比较年轻后代(即父辈年龄较大)与较大后代的精神分裂症发生频率。方法招募来自精神科医院和私人诊所的精神分裂症的220例患者(病例)和其他医院病房(对照)的220例性别和年龄相匹配的患者。两组均排除了神经系统问题,药物滥用,智力低下和情绪障碍的患者。结果出生等级比较显示,与对照组相比,35%vs 24%的病例处于第三或更高的出生等级(P = 0.01)。此外,病例组(30±6.26岁)的父亲平均出生年龄显着高于对照组(26.45±5.64岁; P = 0.0001)。病例组出生时76名父亲的年龄超过32岁,而对照组则为33名父亲。父亲的年龄超过32岁(出生时)的人与其他人相比,精神分裂症的风险更高(2.77倍)(P P = 0.02)。 Logistic回归分析表明,与高龄父母年龄相比,母亲年龄患精神分裂症的风险更高。讨论本研究证明了伊朗人口大家庭中父亲年龄与精神分裂症之间的关系。有人提出,精子中的DNA碱基改变或表观遗传改变导致与年长父亲有关的风险增加。但是,从头生殖系突变和表观遗传变化都有助于疾病的发生,这并不奇怪,因为DNA复制和DNA甲基化在大分子水平(即,甲基化紧随复制)和代谢水平(这两个过程都需要叶酸),并且容易受到环境的调节。需要对样本(如此处收集的样本)进行进一步研究,以弄清从头突变与精神分裂症的表观遗传变化之间的关系。

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