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首页> 外文期刊>Cellular Oncology: Analytical Cellular Pathology >Genetic Predisposition to Sporadic Cancer: How to Handle Major Effects of Minor Genes?
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Genetic Predisposition to Sporadic Cancer: How to Handle Major Effects of Minor Genes?

机译:散发性癌症的遗传易感性:如何处理轻微基因的主要影响?

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摘要

Predisposition to non-familial, sporadic cancer is strongly influenced by multiple tumor susceptibility genes (TSGs), each with apparently minor effects on the cancer phenotype. Sequence analysis of the human genome has yielded numerous single nucleotide polymorphisms (SNPs), raising the expectation that new low-penetrance TSGs will be identified that can be used to estimate an individuals cancer risk. However, mouse models for human cancer showed that the effects of many low-penetrance TSGs are highly variable due to their involvement in epistatic interactions. Together, these interacting TSGs form large molecular networks, which represent cancer-associated biological modules that influence the tumorigenic process. As a consequence, although allelic variation in one TSG on a permissive genetic Background can have major effects on tumor development, the net effect of allelic variation in multiple interacting TSGs remains hard to predict. Therefore, the predictive value of SNP-analysis to estimate an individuals cancer risk will be restricted to those TSGs that exhibit single-gene effects. New strategies need to be developed to evaluate cancer risk associated with biological modules that are influenced by TSG-networks.
机译:对非家族性的倾向于多种肿瘤敏感基因(TSG)的强烈影响,每个肿瘤易感基因(TSG)都对癌症表型显然较小的影响。人类基因组的序列分析已经产生了许多单一核苷酸多态性(SNP),提高了预期,即将识别新的低渗Tsgs可用于估计个体癌症风险。然而,人类癌症的小鼠模型表明,由于它们的认识相互作用,许多低渗Tsgs的效果是高度变化的。这些相互作用的TSG在一起形成大分子网络,其代表影响致瘤过程的癌症相关的生物模块。结果,尽管一个TSG对允许遗传背景上的等位基因变异可能对肿瘤发育具有重大影响,但多个相互作用TSG的等位基因变异的净效应仍然难以预测。因此,SNP分析估计个体癌症风险的预测值将仅限于表现出单基因效应的TSG。需要制定新的策略以评估与受TSG网络影响的生物模块相关的癌症风险。

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