Theoretical cross-comparative analysis on dynamics of small intestine and colon crypts during cancer initiation

被引:1
|
作者
Roznovat, Irina A. [1 ]
Ruskin, Heather J. [1 ]
机构
[1] Dublin City Univ, Ctr Sci Comp & Complex Syst Modelling SCI SYM, Sch Comp, Dublin 9, Ireland
关键词
cancer; tumours; biological organs; medical disorders; genetics; DNA; molecular biophysics; biochemistry; genomics; medical computing; cellular biophysics; theoretical cross-comparative analysis; small intestine; colon crypts; cancer initiation; inherited genome regulation; biological research; medical research; human diseases; autoimmune disorders; neuropsychiatric disorders; personalised medicine; targeted treatments; intraindividual epigenetic variation; disease predisposition; epigenome-wide association studies; computational model; human intestinal crypts; malignant systems; aberrant DNA methylation level; agent-based model; AgentCrypt model; potential methylation inhibitors; methylation modifications; time; 90; d; EPIGENOME-WIDE ASSOCIATION; DNA METHYLATION; MONTE-CARLO; STEM-CELL; MECHANISMS; MODEL; EPIGENETICS; SIMULATION; MUTATION; GENES;
D O I
10.1049/iet-syb.2015.0048
中图分类号
Q2 [细胞生物学];
学科分类号
071009 ; 090102 ;
摘要
Epigenetics is emerging as a fundamentally important area of biological and medical research that has implications for our understanding of human diseases including cancer, autoimmune and neuropsychiatric disorders. In the context of recent efforts on personalised medicine, a novel research direction is concerned with identification of intra-individual epigenetic variation linked to disease predisposition and development, i.e. epigenome-wide association studies. A computational model has been developed to describe the dynamics and structure of human intestinal crypts and to perform a comparative analysis on aberrant DNA methylation level induced in these during cancer initiation. The crypt framework, AgentCrypt, is an agent-based model of crypt dynamics, which handles intra- and inter-dependencies. In addition, the AgentCrypt model is used to investigate the effect of a set of potential inhibitors with respect to methylation modification in intestinal tissue during initiation of disease. Methylation level decrease over a relatively short period of 90 days is marked for the colon compared to the small intestine, although similar alterations are induced in both tissues. In addition, inhibitor effect is notable for abnormal crypt groups, with largest average methylation differences observed approximate to 0.75% lower in the colon and approximate to 0.79% lower in the small intestine with inhibitor present.
引用
收藏
页码:259 / 267
页数:9
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