Epigenetic influences in the aetiology of cancers arising from breast and prostate: a hypothesised transgenerational evolution in chromatin accessibility.
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引用次数: 0
Abstract
Epidemiological studies have consistently supported the notion that environmental and/or dietary factors play a central role in the aetiology of cancers of the breast and prostate. However, for more than five decades investigators have failed to identify a single cause-and-effect factor, which could be implicated; identification of a causative entity would allow the implementation of an intervention strategy in at-risk populations. This suggests a more complex pathoaetiology for these cancer sites, compared to others. When one examines the increases or decreases in incidence of specific cancers amongst migrant populations, it is notable that disease arising in colon or stomach requires one or at most two generations to exhibit a change in incidence to match that of high-incidence regions, whereas for breast or prostate cancer, at least three generations are required. This generational threshold could suggest a requirement for nonmutation-driven epigenetic alterations in the F0/F1 generations (parental/offspring adopting a more westernized lifestyle), which then predisposes the inherited genome of subsequent generations to mutagenic/genotoxic alterations leading to the development of sporadic cancer in these target sites. As such, individual susceptibility to carcinogen insult would not be based per se on polymorphisms in activating/detoxifying/repair enzymes, but on elevated accessibility of crucial target genes (e.g., oncogenes, tumour suppressor genes) or hotspots therein to mutation events. This could be termed a genomic susceptibility organizational structure (SOS). Several exposures including alcohol and heavy metals are epigens (i.e., modifiers of the epigenome), whereas others are mutagenic/genotoxic, for example, heterocyclic aromatic amines; humans are continuously and variously exposed to mixtures of these agents. Within such a transgenerational multistage model of cancer development, determining the interaction between epigenetic modification to generate a genomic SOS and genotoxic insult will facilitate a new level of understanding in the aetiology of cancer.
流行病学研究一直支持这样一种观点,即环境和/或饮食因素在乳腺癌和前列腺癌的病因中起着核心作用。然而,五十多年来,研究人员一直未能找到一个可以牵涉其中的单一因果因素;找到一个致病实体,就可以对高危人群实施干预策略。这表明,与其他癌症相比,这些癌症部位的病因更为复杂。在研究特定癌症在流动人口中发病率的增减时,值得注意的是,结肠癌或胃癌的发病率需要一代或最多两代人的努力才能达到高发地区的水平,而乳腺癌或前列腺癌的发病率至少需要三代人的努力。这一世代阈值可能表明,F0/F1 代(父母/后代采用更西化的生活方式)需要非突变驱动的表观遗传学改变,从而使后代的遗传基因组易受突变/遗传毒性改变的影响,导致这些目标部位发生散发性癌症。因此,个人对致癌物质的易感性本身并不是基于活化/解毒/修复酶的多态性,而是基于关键靶基因(如致癌基因、肿瘤抑制基因)或其中热点突变事件的易感性升高。这可以称为基因组易感性组织结构(SOS)。包括酒精和重金属在内的几种暴露是表观遗传因子(即表观基因组的修饰因子),而其他暴露则具有诱变/遗传毒性,例如杂环芳香胺;人类持续且不同程度地暴露于这些物质的混合物中。在这种癌症发展的跨代多阶段模型中,确定表观遗传修饰产生基因组 SOS 与基因毒性损伤之间的相互作用,将有助于对癌症病因的理解达到一个新的高度。
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