雄性后代虽然没有遗传 eNOS 缺乏,但小鼠的父源性 eNOS 缺乏会影响葡萄糖稳态和肝脏糖原。
Paternal eNOS deficiency in mice affects glucose homeostasis and liver glycogen in male offspring without inheritance of eNOS deficiency itself.
机构信息
Fifth Department of Medicine (Nephrology/Endocrinology/Rheumatology), University Medical Centre Mannheim, University of Heidelberg, Heidelberg, Germany.
Key Laboratory of Study and Discovery of Small Targeted Molecules of Hunan Province, School of Medicine, Hunan Normal University, Changsha, China.
出版信息
Diabetologia. 2022 Jul;65(7):1222-1236. doi: 10.1007/s00125-022-05700-x. Epub 2022 Apr 30.
AIMS/HYPOTHESIS: It was shown that maternal endothelial nitric oxide synthase (eNOS) deficiency causes fatty liver disease and numerically lower fasting glucose in female wild-type offspring, suggesting that parental genetic variants may influence the offspring's phenotype via epigenetic modifications in the offspring despite the absence of a primary genetic defect. The aim of the current study was to analyse whether paternal eNOS deficiency may cause the same phenotype as seen with maternal eNOS deficiency.
METHODS
Heterozygous (+/-) male eNOS (Nos3) knockout mice or wild-type male mice were bred with female wild-type mice. The phenotype of wild-type offspring of heterozygous male eNOS knockout mice was compared with offspring from wild-type parents.
RESULTS
Global sperm DNA methylation decreased and sperm microRNA pattern altered substantially. Fasting glucose and liver glycogen storage were increased when analysing wild-type male and female offspring of +/- eNOS fathers. Wild-type male but not female offspring of +/- eNOS fathers had increased fasting insulin and increased insulin after glucose load. Analysing candidate genes for liver fat and carbohydrate metabolism revealed that the expression of genes encoding glucocorticoid receptor (Gr; also known as Nr3c1) and peroxisome proliferator-activated receptor gamma coactivator 1-alpha (Pgc1a; also known as Ppargc1a) was increased while DNA methylation of Gr exon 1A and Pgc1a promoter was decreased in the liver of male wild-type offspring of +/- eNOS fathers. The endocrine pancreas in wild-type offspring was not affected.
CONCLUSIONS/INTERPRETATION: Our study suggests that paternal genetic defects such as eNOS deficiency may alter the epigenome of the sperm without transmission of the paternal genetic defect itself. In later life wild-type male offspring of +/- eNOS fathers developed increased fasting insulin and increased insulin after glucose load. These effects are associated with increased Gr and Pgc1a gene expression due to altered methylation of these genes.
目的/假设:研究表明,母体内皮型一氧化氮合酶(eNOS)缺乏会导致脂肪肝疾病和空腹血糖数值降低,这表明尽管没有主要的遗传缺陷,父母的遗传变异可能通过后代的表观遗传修饰来影响后代的表型。本研究的目的是分析父源性 eNOS 缺乏是否会导致与母源性 eNOS 缺乏相同的表型。
方法
杂合子( +/- )雄性 eNOS(Nos3)基因敲除小鼠或野生型雄性小鼠与野生型雌性小鼠交配。杂合子雄性 eNOS 基因敲除小鼠的野生型后代的表型与野生型父母的后代进行比较。
结果
全精子 DNA 甲基化减少,精子 microRNA 模式发生显著改变。当分析 +/- eNOS 父亲的野生型雄性和雌性后代时,空腹血糖和肝糖原储存增加。 +/- eNOS 父亲的野生型雄性后代而非雌性后代,空腹胰岛素和葡萄糖负荷后胰岛素增加。分析肝脂肪和碳水化合物代谢的候选基因时发现,编码糖皮质激素受体(Gr;也称为 Nr3c1)和过氧化物酶体增殖物激活受体γ共激活因子 1-α(Pgc1a;也称为 Ppargc1a)的基因表达增加,而 Gr 外显子 1A 和 Pgc1a 启动子的 DNA 甲基化减少。野生型后代的内分泌胰腺未受影响。
结论/解释:我们的研究表明,父源性遗传缺陷,如 eNOS 缺乏,可能会改变精子的表观基因组,而不会传递父源性遗传缺陷本身。在以后的生活中, +/- eNOS 父亲的野生型雄性后代会出现空腹胰岛素增加和葡萄糖负荷后胰岛素增加。这些影响与 Gr 和 Pgc1a 基因表达增加有关,这是由于这些基因的甲基化改变所致。
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