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通过辅助生殖出生的家鼠单核苷酸突变率增加。

Increased rate of single nucleotide mutation in house mice born through assisted reproduction.

作者信息

Blanco-Berdugo Laura, Garretson Alexis, Dumont Beth L

出版信息

bioRxiv. 2025 Jun 30:2025.06.27.662069. doi: 10.1101/2025.06.27.662069.

DOI:10.1101/2025.06.27.662069
PMID:40631205
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC12236792/
Abstract

UNLABELLED

Approximately 2.6% of live births in the United States are conceived using assisted reproductive technologies (ARTs). While some ART procedures, including in vitro fertilization (IVF) and intracytoplasmic sperm injection, are known to alter the epigenetic landscape of early embryonic development, their impact on DNA sequence stability is unclear. Here, we leverage the strengths of the laboratory mouse model system to investigate whether a standard ART regimen-ovarian hyperstimulation, gamete isolation, IVF, embryo culture, and embryo transfer-affects genome stability. Age-matched cohorts of ART-derived and naturally conceived C57BL/6J inbred mice were reared in a controlled setting and whole genome sequenced to ∼50x coverage. Using a rigorous pipeline for single nucleotide variant (dnSNV) discovery, we observe a ∼30% increase in the dnSNV rate in ART-compared to naturally-conceived mice. Analysis of the dnSNV mutation spectrum identified signature contributions related to germline DNA repair activity, affirming expectations and evidencing the quality of our dnSNV calls. We observed no enrichment of dnSNVs in specific genomic contexts, suggesting that the observed rate increase in ART-derived mice is a general genome-wide phenomenon. Similarly, we show that the developmental timing of dnSNVs is similar in ART- and natural-born cohorts. Together, our findings show that ART is moderately mutagenic in house mice and motivate future work to define the precise procedure(s) associated with this increased mutational vulnerability. While we caution that our findings cannot be immediately translated to humans, they nonetheless emphasize a pressing need for investigations on the potential mutagenicity of ART in our species.

SIGNIFICANCE STATEMENT

This study investigates whether assisted reproductive technologies (ARTs) increase the risk of inherited genetic mutations in offspring. Using a well-controlled mouse model system, we compared the de novo mutation burden in genomes of mice conceived through ART to a naturally conceived cohort. We find a ∼30% increase in new DNA mutations in ART-conceived mice, suggesting that ART procedures have a genome destabilizing effect. This increase in mutation rate appears to be uniform across the genome, rather than attributable to specific genomic contexts. While we caution against the direct translation of our findings to humans, our work nonetheless highlights the need for further research into the genetic safety of ART in people.

摘要

未标注

在美国,约2.6%的活产婴儿是通过辅助生殖技术(ART)受孕的。虽然一些ART程序,包括体外受精(IVF)和卵胞浆内单精子注射,已知会改变早期胚胎发育的表观遗传格局,但其对DNA序列稳定性的影响尚不清楚。在此,我们利用实验室小鼠模型系统的优势,研究标准ART方案——卵巢过度刺激、配子分离、IVF、胚胎培养和胚胎移植——是否会影响基因组稳定性。将年龄匹配的ART衍生和自然受孕的C57BL/6J近交小鼠群体在可控环境中饲养,并对全基因组进行测序,覆盖深度约为50倍。使用严格的单核苷酸变异(dnSNV)发现流程,我们观察到与自然受孕小鼠相比,ART小鼠的dnSNV率增加了约30%。对dnSNV突变谱的分析确定了与种系DNA修复活性相关的特征性贡献,证实了预期并证明了我们dnSNV检测的质量。我们在特定基因组背景下未观察到dnSNV的富集,这表明在ART衍生小鼠中观察到的率增加是全基因组范围内的普遍现象。同样,我们表明dnSNV的发育时间在ART和自然出生的群体中相似。总之,我们的研究结果表明,ART在家养小鼠中具有中度致突变性,并促使未来开展工作来确定与这种增加的突变易感性相关的精确程序。虽然我们提醒不能立即将我们的研究结果应用于人类,但它们仍然强调迫切需要研究ART在我们物种中的潜在致突变性。

意义声明

本研究调查辅助生殖技术(ART)是否会增加后代遗传基因突变的风险。使用一个严格控制的小鼠模型系统,我们将通过ART受孕的小鼠基因组中的新生突变负担与自然受孕群体进行了比较。我们发现ART受孕小鼠的新DNA突变增加了约30%,这表明ART程序具有基因组不稳定效应。这种突变率的增加似乎在整个基因组中是均匀的,而不是归因于特定的基因组背景。虽然我们提醒不要将我们的研究结果直接应用于人类,但我们的工作仍然强调需要进一步研究ART在人类中的遗传安全性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f0bd/12236792/26cac5951690/nihpp-2025.06.27.662069v1-f0003.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f0bd/12236792/18b297e08029/nihpp-2025.06.27.662069v1-f0001.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f0bd/12236792/1d6f1689367b/nihpp-2025.06.27.662069v1-f0002.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f0bd/12236792/26cac5951690/nihpp-2025.06.27.662069v1-f0003.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f0bd/12236792/18b297e08029/nihpp-2025.06.27.662069v1-f0001.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f0bd/12236792/1d6f1689367b/nihpp-2025.06.27.662069v1-f0002.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f0bd/12236792/26cac5951690/nihpp-2025.06.27.662069v1-f0003.jpg

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本文引用的文献

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