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首页> 外文期刊>Proceedings of the Nutrition Society >Session 2: Personalised nutrition Epigenomics: a basis for understanding individual differences?: Symposium on ‘The challenge of translating nutrition research into public health nutrition’
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Session 2: Personalised nutrition Epigenomics: a basis for understanding individual differences?: Symposium on ‘The challenge of translating nutrition research into public health nutrition’

机译:第2节:个性化营养表观基因组学:了解个体差异的基础?:关于“将营养研究转化为公共卫生营养的挑战”专题讨论会

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Epigenetics encompasses changes to marks on the genome that are copied from one cell generation to the next, which may alter gene expression but which do not involve changes in the primary DNA sequence. These marks include DNA methylation (methylation of cytosines within CpG dinucleotides) and post-translational modifications (acetylation, methylation, phosphorylation and ubiquitination) of the histone tails protruding from nucleosome cores. The sum of genome-wide epigenetic patterns is known as the epigenome. It is hypothesised that altered epigenetic marking is a means through which evidence of environmental exposures (including nutritional status and dietary exposure) is received and recorded by the genome. At least some of these epigenetic marks are remembered through multiple cell generations and their effects may be revealed in altered gene expression and cell function. Altered epigenetic marking allows plasticity of phenotype in a fixed genotype. Despite their identical genotypes, monozygotic twins show increasing epigenetic diversity with age and with divergent lifestyles. Differences in epigenetic markings may explain some inter-individual variation in disease risk and in response to nutritional interventions.
机译:表观遗传学包括从一个细胞世代复制到另一细胞世代的基因组上标记的变化,这可能会改变基因表达,但不涉及一级DNA序列的变化。这些标记包括从核小体核心突出的组蛋白尾巴的DNA甲基化(CpG二核苷酸内的胞嘧啶甲基化)和翻译后修饰(乙酰化,甲基化,磷酸化和泛素化)。全基因组表观遗传模式的总和称为表观基因组。假设表观遗传标记的改变是一种通过基因组接收并记录环境暴露证据(包括营养状况和饮食暴露)的手段。这些表观遗传标记中至少有一些是通过多代细胞记忆的,其作用可能在基因表达和细胞功能改变中得以揭示。改变的表观遗传标记允许固定基因型的表型可塑性。尽管它们的基因型相同,但单卵双胞胎显示出随着年龄的增长和生活方式的不同,表观遗传多样性也在增加。表观遗传标记的差异可能解释了疾病风险和对营养干预措施的个体差异。

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