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父方接触哌甲酯会导致囊胚质量不佳及表观遗传变化。

Paternal Exposure to Methylphenidate Induces Poor-Quality Blastocyst and Epigenetic Changes.

作者信息

Gomes Ana Clara da Costa Nunes, Pagliari Laura Eduarda S C, Stumpp Taiza, Vendramini Vanessa

机构信息

Department of Morphology and Genetics, Laboratory of Reproductive and Developmental Biology (LaBReD), Paulista School of Medicine, Federal University of Sao Paulo - EPM/UNIFESP, São Paulo, Brazil.

出版信息

Mol Reprod Dev. 2025 May;92(5):e70026. doi: 10.1002/mrd.70026.

Abstract

Epigenetic changes caused by methylphenidate hydrochloride on paternal inheritance have been suggested in fish, yet a subject to be determined in mammals. In rats, we showed increased sperm DNA fragmentation and reduced embryonic viability. In the present report, male Wistar rats (n = 21) were divided into two groups: control and methylphenidate. The control group received 1 mL/kg of distilled water, while the methylphenidate group received 5 mg/kg by gavage from 38 to 68 days of age on a single daily dose. After this period, there was an interval before exposed rats started a mating schedule with untreated/normally cycling females. Morphological quality and key epigenetic marks in the blastocysts were assessed. Immunocytochemistry was performed in fresh blastocysts to quantify the trimethylated histones H3K4, H3K9, and H4K20. Treatment with methylphenidate reduced the mean quality of blastocysts by 43.57% (p = 0.02), as well as increased those classified as "poor" by more than 150% (p < 0.001). Epigenetic marks were also altered, with an increase in the intensity of H3K9me3 (p = 0.01), a reduction of H4K20me3 (p = 0.05) and a nonsignificant increase of H3K4me3 (p = 0.34). The results suggest that the decline in blastocyst quality is highly associated with subchronic use of this psychostimulant by adolescent males. This is the first report showing the risks posed by methylphenidate to the epigenetic signature of a mammalian blastocyst following paternal exposure.

摘要

已有研究表明,盐酸哌甲酯会引起鱼类父系遗传中的表观遗传变化,但在哺乳动物中这仍是一个有待确定的问题。在大鼠实验中,我们发现精子DNA碎片化增加,胚胎存活率降低。在本报告中,将21只雄性Wistar大鼠分为两组:对照组和哌甲酯组。对照组大鼠接受1毫升/千克的蒸馏水,而哌甲酯组大鼠从38日龄至68日龄每天经口灌胃给予5毫克/千克的剂量。在此期间过后,让接受处理的大鼠与未处理/正常发情的雌性大鼠开始交配前有一段间隔期。评估了囊胚的形态质量和关键表观遗传标记。对新鲜囊胚进行免疫细胞化学分析,以量化三甲基化组蛋白H3K4、H3K9和H4K20。哌甲酯处理使囊胚的平均质量降低了43.57%(p = 0.02),同时使被归类为“质量差”的囊胚数量增加了150%以上(p < 0.001)。表观遗传标记也发生了改变,H3K9me3强度增加(p = 0.01),H4K20me3减少(p = 0.05),H3K4me3有不显著增加(p = 0.34)。结果表明,囊胚质量下降与青春期雄性大鼠亚慢性使用这种精神兴奋剂密切相关。这是第一份报告显示父系接触哌甲酯对哺乳动物囊胚表观遗传特征构成的风险。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e07c/12100459/2f3d54e48aa8/MRD-92-e70026-g002.jpg

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