ITPKC and CASP3 polymorphisms and risks for IVIG unresponsiveness and coronary artery lesion formation in Kawasaki disease

被引:0
|
作者
Y Onouchi
Y Suzuki
H Suzuki
M Terai
K Yasukawa
H Hamada
T Suenaga
T Honda
A Honda
H Kobayashi
T Takeuchi
N Yoshikawa
J Sato
S Shibuta
M Miyawaki
K Oishi
H Yamaga
N Aoyagi
S Iwahashi
R Miyashita
Y Murata
R Ebata
K Higashi
K Ozaki
K Sasago
T Tanaka
A Hata
机构
[1] Laboratory for Cardiovascular Diseases,Department of Public Health
[2] Center for Genomic Medicine RIKEN,Department of Pediatrics
[3] Chiba University Graduate School of Medicine,Department of Pediatrics
[4] Wakayama Medical University,Department of Pediatrics
[5] Tokyo Women's Medical University Yachiyo Medical Center,Department of Pediatrics
[6] Chiba University Graduate School of Medicine,Department of Pediatrics
[7] Asahi General Hospital,Department of Pediatrics
[8] Funabashi Municipal Medical Center,Department of Pediatrics
[9] Social Insurance Kinan Hospital,Department of Pediatrics
[10] Hashimoto Municipal Hospital,Department of Pediatrics
[11] Naga Hospital,Department of Pediatrics
[12] Wakayama Rosai Hospital,Department of Pediatrics
[13] Hidaka General Hospital,Department of Pediatrics
[14] Izumiotsu Municipal Hospital,undefined
[15] Sendai City Hospital,undefined
来源
The Pharmacogenomics Journal | 2013年 / 13卷
关键词
Kawasaki's disease; ITPKC; CASP3; SNP; IVIG resistance; coronary artery lesion;
D O I
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中图分类号
学科分类号
摘要
Functional single-nucleotide polymorphisms (SNPs) in inositol 1,4,5-trisphosphate 3-kinase C (ITPKC) (rs28493229) and caspase-3 (CASP3) (rs113420705; formerly rs72689236) are associated with susceptibility to Kawasaki's disease (KD). To evaluate the involvement of these 2 SNPs in the risk for intravenous immunoglobulin (IVIG) unresponsiveness, we investigated 204 Japanese KD patients who received a single IVIG dose of 2 g kg−1 (n=70) or 1 g kg−1 daily for 2 days (n=134). The susceptibility allele of both SNPs showed a trend of overrepresentation in IVIG non-responders and, in combined analysis of these SNPs, patients with at least 1 susceptible allele at both loci had a higher risk for IVIG unresponsiveness (P=0.0014). In 335 prospectively collected KD patients who were treated with IVIG (2 g kg−1), this 2-locus model showed a more significant association with resistance to initial and additional IVIG (P=0.011) compared with individual SNPs. We observed a significant association when all KD patients with coronary artery lesions were analyzed with the 2-locus model (P=0.0031). Our findings strongly suggest the existence of genetic factors affecting patients’ responses to treatment and the risk for cardiac complications, and provide clues toward understanding the pathophysiology of KD inflammation.
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页码:52 / 59
页数:7
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