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在唐氏综合征小鼠模型中,三体的传递随母龄下降,这与人类唐氏综合征母亲中的现象相似。

Transmission of trisomy decreases with maternal age in mouse models of Down syndrome, mirroring a phenomenon in human Down syndrome mothers.

作者信息

Stern Shani, Biron David, Moses Elisha

机构信息

Laboratory of Genetics, Salk Institute for Biological Studies, 10010 N. Torrey Pines Rd., La Jolla, CA, 92037, USA.

Department of Physics, James Franck Institute and the Institute for Biophysical Dynamics, University of Chicago, 929 E. 57th St GCIS E139F, Chicago, IL, 60637, USA.

出版信息

BMC Genet. 2016 Jul 11;17(1):105. doi: 10.1186/s12863-016-0412-3.

Abstract

BACKGROUND

Down syndrome incidence in humans increases dramatically with maternal age. This is mainly the result of increased meiotic errors, but factors such as differences in abortion rate may play a role as well. Since the meiotic error rate increases almost exponentially after a certain age, its contribution to the overall incidence aneuploidy may mask the contribution of other processes.

RESULTS

To focus on such selection mechanisms we investigated transmission in trisomic females, using data from mouse models and from Down syndrome humans. In trisomic females the a-priori probability for trisomy is independent of meiotic errors and thus approximately constant in the early embryo. Despite this, the rate of transmission of the extra chromosome decreases with age in females of the Ts65Dn and, as we show, for the Tc1 mouse models for Down syndrome. Evaluating progeny of 73 Tc1 births and 112 Ts65Dn births from females aged 130 days to 250 days old showed that both models exhibit a 3-fold reduction of the probability to transmit the trisomy with increased maternal ageing. This is concurrent with a 2-fold reduction of litter size with maternal ageing. Furthermore, analysis of previously reported 30 births in Down syndrome women shows a similar tendency with an almost three fold reduction in the probability to have a Down syndrome child between a 20 and 30 years old Down syndrome woman.

CONCLUSIONS

In the two types of mice models for Down syndrome that were used for this study, and in human Down syndrome, older females have significantly lower probability to transmit the trisomy to the offspring. Our findings, taken together with previous reports of decreased supportive environment of the older uterus, add support to the notion that an older uterus negatively selects the less fit trisomic embryos.

摘要

背景

人类唐氏综合征的发病率随母亲年龄的增长而急剧上升。这主要是减数分裂错误增加的结果,但诸如流产率差异等因素也可能起作用。由于减数分裂错误率在一定年龄后几乎呈指数增长,其对非整倍体总体发病率的贡献可能掩盖了其他过程的贡献。

结果

为了关注此类选择机制,我们利用来自小鼠模型和唐氏综合征患者的数据,研究了三体雌性的遗传传递情况。在三体雌性中,三体的先验概率与减数分裂错误无关,因此在早期胚胎中大致恒定。尽管如此,在Ts65Dn雌性以及我们所展示的唐氏综合征Tc1小鼠模型中,额外染色体的传递率会随着年龄的增长而降低。对73例Tc1出生和112例Ts65Dn出生的后代进行评估,这些后代的母亲年龄在130天至250天之间,结果表明两个模型都显示出随着母亲年龄的增加,三体传递概率降低了3倍。这与随着母亲年龄增加产仔数减少2倍是同时发生的。此外,对先前报道的30例唐氏综合征女性分娩情况的分析显示出类似的趋势,20至30岁的唐氏综合征女性生育唐氏综合征患儿的概率几乎降低了3倍。

结论

在本研究中使用的两种唐氏综合征小鼠模型以及人类唐氏综合征中,年龄较大的雌性将三体传递给后代的概率显著更低。我们的研究结果,连同先前关于老年子宫支持环境下降的报道,进一步支持了老年子宫对不太健康的三体胚胎进行负面选择的观点。

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