Cancer Risk Score Prediction Based on a Single-Nucleotide Polymorphism Network

被引:2
|
作者
Mahesworo, Bharuno [1 ,2 ,5 ]
Budiarto, Arif [2 ,3 ]
Hidayat, Alam Ahmad [2 ]
Pardamean, Bens [2 ,4 ]
机构
[1] Bina Nusantara Univ, Sch Comp Sci, Dept Stat, Jakarta, Indonesia
[2] Bina Nusantara Univ, Bioinformat & Data Sci Res Ctr, Jakarta, Indonesia
[3] Bina Nusantara Univ, Sch Comp Sci, Dept Comp Sci, Jakarta, Indonesia
[4] Bina Nusantara Univ, BINUS Grad Program, Master Comp Sci Program, Dept Comp Sci, Jakarta, Indonesia
[5] Bina Nusantara Univ, Sch Comp Sci, Dept Stat, Jakarta 11480, Indonesia
关键词
Data Analysis; Genetics; Risk Factors; Colorectal Neoplasms; Multifactorial Inheritance; ASSOCIATION; PREVENTION; GENES;
D O I
10.4258/hir.2022.28.3.247
中图分类号
R-058 [];
学科分类号
摘要
Objectives: Genome-wide association studies (GWAS) are performed to study the associations between genetic variants with respect to certain phenotypic traits such as cancer. However, the method that is commonly used in GWAS assumes that cer-tain traits are solely affected by a single mutation. We propose a network analysis method, in which we generate association networks of single-nucleotide polymorphisms (SNPs) that can differentiate case and control groups. We hypothesize that certain phenotypic traits are attributable to mutations in groups of associated SNPs. Methods: We propose a method based on a network analysis framework to study SNP-SNP interactions related to cancer incidence. We employed logistic regression to measure the significance of all SNP pairs from GWAS for the incidence of colorectal cancer and computed a cancer risk score based on the generated SNP networks. Results: We demonstrated our method in a dataset from a case-control study of colorectal cancer in the South Sulawesi population. From the GWAS results, 20,094 pairs of 200 SNPs were created. We obtained one cluster containing four pairs of five SNPs that passed the filtering threshold based on their p-values. A locus on chromosome 12 (12:54410007) was found to be strongly connected to the four variants on chromosome 1. A polygenic risk score was computed from the five SNPs, and a significant difference in colorectal cancer risk was obtained between the case and control groups. Conclusions: Our results demonstrate the applicability of our method to understand SNP-SNP interac-tions and compute risk scores for various types of cancer.
引用
收藏
页码:247 / 255
页数:9
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