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HLA-E是唯一逃避CpG甲基化且在滋养层来源的人细胞系JAR中具有转录活性的I类基因。

HLA-E is the only class I gene that escapes CpG methylation and is transcriptionally active in the trophoblast-derived human cell line JAR.

作者信息

Boucraut J, Guillaudeux T, Alizadeh M, Boretto J, Chimini G, Malecaze F, Semana G, Fauchet R, Pontarotti P, Le Bouteiller P

机构信息

Laboratoire d'Immunologie, Faculté de Médecine de la Timone, Marseille, France.

出版信息

Immunogenetics. 1993;38(2):117-30. doi: 10.1007/BF00190899.

Abstract

Polymorphic as well as HLA-F and -G genes are repressed in the human cell line JAR, derived from a tumor of trophoblast origin. By contrast, the HLA-E gene as well as the non-HLA novel coding-sequence, R1, located 5' to HLA-E, both remain transcriptionally active. We first demonstrated the role of DNA methylation in the repression of class I genes (except HLA-E) in JAR by the use of the 5-Azacytidine demethylating agent. Following treatment, JAR clones reexpressed polymorphic class I transcripts and cell surface alpha chains. Using methylation-sensitive rare cutter enzymes on JAR genomic DNA, followed by classical or pulse field gel electrophoresis and hybridization with HLA locus-specific probes, we found methylated CpG islands in the 5' region of all class I genes, except for HLA-E. These results, establishing an inverse relationship between states of methylation and transcriptional activity within the MHC class I chromosomal region in JAR, and the observations that the HLA-E and R1 genes were ubiquitously expressed, suggest that the HLA-E chromosomal domain might have functional importance including the presence of housekeeping genes.

摘要

多态性基因以及HLA - F和 - G基因在源自滋养层细胞瘤的人细胞系JAR中受到抑制。相比之下,HLA - E基因以及位于HLA - E 5'端的非HLA新编码序列R1均保持转录活性。我们首先通过使用5 - 氮杂胞苷去甲基化剂证明了DNA甲基化在JAR中I类基因(HLA - E除外)抑制中的作用。处理后,JAR克隆重新表达多态性I类转录本和细胞表面α链。在JAR基因组DNA上使用甲基化敏感的稀有切割酶,然后进行经典或脉冲场凝胶电泳,并与HLA位点特异性探针杂交,我们在所有I类基因的5'区域发现了甲基化的CpG岛,但HLA - E除外。这些结果在JAR的MHC I类染色体区域内建立了甲基化状态与转录活性之间的反比关系,并且观察到HLA - E和R1基因普遍表达,这表明HLA - E染色体结构域可能具有功能重要性,包括存在管家基因。

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