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父亲年龄较大时所生子女有患遗传疾病的风险吗?

Are children of older fathers at risk for genetic disorders?

作者信息

Jung A, Schuppe H-C, Schill W-B

机构信息

Centre of Dermatology and Andrology, Justus Liebig University, Giessen, Germany.

出版信息

Andrologia. 2003 Aug;35(4):191-9. doi: 10.1046/j.1439-0272.2003.00579.x.

Abstract

Genetic risks related to paternal age should be of interest to clinical andrologists counselling older men who wish to father a child. Theoretically, the number of (pre-meiotic) mitotic cell divisions during spermatogenesis and their remarkable increase with ageing compared with oogenesis would be in favour of genetic risks for the offspring of older men. But for numerical and structural chromosomal anomalies, such an influence of paternal age has not been found. However, in several autosomal dominant disorders affecting three specific genes (fibroblast growth factor receptor 2 and 3, RET proto-oncogene) the risk for a child to be affected increases with paternal age at time of birth. For other autosomal dominant -X chromosomal dominant or recessive disorders, the available data are sufficient to support the concept of a positive relationship between paternal age and de novo gene mutations. Studies analysing gene sequences of affected children and their parents would allow further evaluation of this topic. The impact of paternal age on disorders with a complex genetic background, however, is a matter of debate. A significant effect of paternal age could not be shown for nonfamilial Alzheimer's disease, congenital heart defects, nonfamilial schizophrenia, acute lymphoblastic leukaemia or prostate cancer.

摘要

与父亲年龄相关的遗传风险应引起临床男科学专家的关注,他们会为希望生育孩子的老年男性提供咨询。从理论上讲,精子发生过程中(减数分裂前)有丝分裂细胞分裂的次数,以及与卵子发生相比其随年龄增长的显著增加,都表明老年男性的后代存在遗传风险。但对于染色体数目和结构异常,尚未发现父亲年龄有此类影响。然而,在几种影响三个特定基因(成纤维细胞生长因子受体2和3、RET原癌基因)的常染色体显性疾病中,孩子受影响的风险会随着父亲出生时的年龄增加而升高。对于其他常染色体显性、X染色体显性或隐性疾病,现有数据足以支持父亲年龄与新生基因突变之间存在正相关关系的概念。分析患病儿童及其父母的基因序列的研究将有助于进一步评估这一话题。然而,父亲年龄对具有复杂遗传背景的疾病的影响仍存在争议。对于散发性阿尔茨海默病、先天性心脏病、散发性精神分裂症、急性淋巴细胞白血病或前列腺癌,尚未显示出父亲年龄有显著影响。

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