Nishiyama Chiharu, Akizawa Yushiro, Nishiyama Makoto, Tokura Tomoko, Kawada Hiroshi, Mitsuishi Kouichi, Hasegawa Masanari, Ito Tomonobu, Nakano Nobuhiro, Okamoto Atsushi, Takagi Atsushi, Yagita Hideo, Okumura Ko, Ogawa Hideoki
Atopy (Allergy) Research Center, Department of Dermatology, Juntendo University School of Medicine, 2-1-1 Hongo, Bunkyo-ku, Tokyo 113-8421, Japan.
J Immunol. 2004 Nov 15;173(10):6458-64. doi: 10.4049/jimmunol.173.10.6458.
The beta subunit of the high-affinity IgE receptor (FcepsilonRI) plays an important role in IgE-mediated allergic reactions as an amplifier for cell surface expression and signal transduction of FcepsilonRI. FcepsilonRIbeta is presumed to be one of the genes linked with atopic diseases. However, the validity of the associations previously found between single nucleotide polymorphisms (SNPs) in FcepsilonRIbeta and atopic diseases is questionable. In the present study, we found correlation between the SNP of FcepsilonRIbeta at +6960A/G, resulting in a Glu237Gly amino acid substitution, and the cell surface expression level of FcepsilonRI on blood basophils, although it has been shown that the Glu237Gly mutation itself does not affect the surface expression or function of FcepsilonRI. We additionally found four SNPs in the promoter region of FcepsilonRIbeta, among which -426T/C and -654C/T were tightly linked with +6960A/G. Reporter plasmids carrying the -426C and -654T promoter displayed higher transcriptional activity than those carrying the -426T and -654C promoter. We found that transcription factor YY1 preferentially bound and transactivated the -654T promoter. Furthermore, expression of FcepsilonRI beta-chain mRNA in basophils from individuals who have the minor heterozygous genotype was significantly higher than that of the major homozygous genotype. These results suggest that the SNPs in the FcepsilonRIbeta promoter are causally linked with atopy via regulation of FcepsilonRI expression.
高亲和力IgE受体(FcepsilonRI)的β亚基作为FcepsilonRI细胞表面表达和信号转导的放大器,在IgE介导的过敏反应中起重要作用。FcepsilonRIβ被认为是与特应性疾病相关的基因之一。然而,先前在FcepsilonRIβ单核苷酸多态性(SNP)与特应性疾病之间发现的关联的有效性值得怀疑。在本研究中,我们发现FcepsilonRIβ在+6960A/G处的SNP与血液嗜碱性粒细胞上FcepsilonRI的细胞表面表达水平相关,该SNP导致Glu237Gly氨基酸取代,尽管已表明Glu237Gly突变本身不影响FcepsilonRI的表面表达或功能。我们还在FcepsilonRIβ的启动子区域发现了四个SNP,其中-426T/C和-654C/T与+6960A/G紧密连锁。携带-426C和-654T启动子的报告质粒显示出比携带-426T和-654C启动子的报告质粒更高的转录活性。我们发现转录因子YY1优先结合并反式激活-654T启动子。此外,具有次要杂合基因型个体的嗜碱性粒细胞中FcepsilonRIβ链mRNA的表达明显高于主要纯合基因型个体。这些结果表明,FcepsilonRIβ启动子中的SNP通过调节FcepsilonRI表达与特应性存在因果关系。
