通过个人基因组分析鉴定出的与日本克罗恩病易感性相关的低频白细胞介素23受体编码变异体
Low-Frequency IL23R Coding Variant Associated with Crohn's Disease Susceptibility in Japanese Subjects Identified by Personal Genomics Analysis.
作者信息
Onodera Kei, Arimura Yoshiaki, Isshiki Hiroyuki, Kawakami Kentaro, Nagaishi Kanna, Yamashita Kentaro, Yamamoto Eiichiro, Niinuma Takeshi, Naishiro Yasuyoshi, Suzuki Hiromu, Imai Kohzoh, Shinomura Yasuhisa
机构信息
Department of Gastroenterology, Rheumatology, and Clinical Immunology, Sapporo Medical University, Sapporo, Japan.
Department of Anatomy, Sapporo Medical University, Sapporo, Japan.
出版信息
PLoS One. 2015 Sep 16;10(9):e0137801. doi: 10.1371/journal.pone.0137801. eCollection 2015.
BACKGROUND
The common disease-common variant hypothesis is insufficient to explain the complexities of Crohn's disease (CD) genetics; therefore, rare variants are expected to be important in the disease. We explored rare variants associated with susceptibility to CD in Japanese individuals by personal genomic analysis.
METHODS
Two-step analyses were performed. The first step was a trio analysis with whole-exome sequence (WES) analysis and the second was a follow-up case-control association study. The WES analysis pipeline comprised Burrows-Wheeler Aligner, Picard, Genome Analysis Toolkit, and SAMTOOLS. Single nucleotide variants (SNVs)/indels were annotated and filtered by using programs implemented in ANNOVAR in combination with identity-by-descent (IBD), subsequently were subjected to the linkage based, and de novo based strategies. Finally, we conducted an association study that included 176 unrelated subjects with CD and 358 healthy control subjects.
RESULTS
In family members, 234,067-297,523 SNVs/indels were detected and they were educed to 106-146 by annotation based filtering. Fifty-four CD variants common to both individuals of the affected sib pair were identified. The linkage based strategy detected five candidate variants whereas the de novo based strategy identified no variants. Consequently, five candidates were analyzed in the case-control association study. CD showed a significant association with one variant in exon 4 of IL23R, G149R [rs76418789, P = 3.9E-5, odds ratio (OR) 0.21, 95% confidence interval (CI) 0.09-0.47 for the dominant model (AA + AG versus GG), and P = 7.3E-5, OR 0.21, 95% CI 0.10-0.48 for AG versus GG, and P = 7.2E-5, OR 0.23, 95% CI 0.10-0.50 for the allele model].
CONCLUSIONS
The present study, using personal genomics analysis of a small CD pedigree, is the first to show that the low-frequency non-synonymous variant of IL23R, rs76418789, protects against CD development in Japanese subjects.
背景
常见疾病-常见变异假说不足以解释克罗恩病(CD)遗传学的复杂性;因此,罕见变异预计在该疾病中起重要作用。我们通过个人基因组分析探索了日本人群中与CD易感性相关的罕见变异。
方法
进行了两步分析。第一步是采用全外显子组测序(WES)分析的三人组分析,第二步是后续的病例对照关联研究。WES分析流程包括Burrows-Wheeler比对器、Picard、基因组分析工具包和SAMTOOLS。单核苷酸变异(SNV)/插入缺失通过使用ANNOVAR中实现的程序结合同源性(IBD)进行注释和过滤,随后采用基于连锁和基于新生突变的策略。最后,我们进行了一项关联研究,纳入了176名无亲缘关系的CD患者和358名健康对照者。
结果
在家庭成员中,检测到234,067 - 297,523个SNV/插入缺失,通过基于注释的过滤将其减少到106 - 146个。在患病同胞对的两个个体中鉴定出54个共同的CD变异。基于连锁的策略检测到5个候选变异,而基于新生突变的策略未鉴定出变异。因此,在病例对照关联研究中对5个候选变异进行了分析。CD与IL23R外显子4中的一个变异G149R [rs76418789] 显示出显著关联,显性模型(AA + AG对GG)下P = 3.9E - 5,优势比(OR)0.21,95%置信区间(CI)0.09 - 0.47;AG对GG时P = 7.3E - 5,OR 0.21,95% CI 0.10 - 0.48;等位基因模型下P = 7.2E - 5,OR 0.23,95% CI 0.10 - 0.50。
结论
本研究通过对一个小的CD家系进行个人基因组分析,首次表明IL23R的低频非同义变异rs76418789可预防日本人群中CD的发生。
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