期刊界 All Journals 搜尽天下杂志传播学术成果专业期刊搜索期刊信息化学术搜索

MHCII类分子提呈经过加工的抗原给CD4 T淋巴细胞 ,在诱发免疫反应中起重要作用。MHCII类分子不正常表达会引起严重的免疫缺陷疾病 ,如裸淋巴细胞综合征 (BLS)等。目前已识别出四种不同的MHCII调控基因。这些基因分别编码RFXANK、RFX5、RFXAP和CIITA。其中 ,前三个是RFX复合物的亚基 ,RFX是一种结合于所有MHCII类基因启动子上的泛式表达的因子。CIITA是MHCII类分子表达的主要调控因子 ,其严密调控的表达模式决定了MHCII类分子表达的细胞特异性 ,及能否被诱导且在何种水平上表达。本文着重介绍近年来国内外对MHCII类分子表达及其调控研究的新进展相似文献

6.

Mutation in the class II trans-activator leading to a mild immunodeficiency 总被引：1，自引：0，他引：1

Wiszniewski W Fondaneche MC Le Deist F Kanariou M Selz F Brousse N Steimle V Barbieri G Alcaide-Loridan C Charron D Fischer A Lisowska-Grospierre B 《Journal of immunology (Baltimore, Md. : 1950)》2001,167(3):1787-1794

相似文献

7.

CIITA leucine-rich repeats control nuclear localization, in vivo recruitment to the major histocompatibility complex (MHC) class II enhanceosome, and MHC class II gene transactivation

下载免费PDF全文

Hake SB Masternak K Kammerbauer C Janzen C Reith W Steimle V 《Molecular and cellular biology》2000,20(20):7716-7725

相似文献

8.

The RFX family interacts at the collagen (COL1A2) start site and represses transcription 总被引：4，自引：0，他引：4

Sengupta PK Fargo J Smith BD 《The Journal of biological chemistry》2002,277(28):24926-24937

相似文献

9.

Histone deacetylase 1/mSin3A disrupts gamma interferon-induced CIITA function and major histocompatibility complex class II enhanceosome formation

下载免费PDF全文

Zika E Greer SF Zhu XS Ting JP 《Molecular and cellular biology》2003,23(9):3091-3102

相似文献

10.

Identification of class II transcriptional activator-induced genes by representational difference analysis: discoordinate regulation of the DN alpha/DO beta heterodimer

Taxman DJ Cressman DE Ting JP 《Journal of immunology (Baltimore, Md. : 1950)》2000,165(3):1410-1416

相似文献

11.

Analysis of the defect in IFN-gamma induction of MHC class II genes in G1B cells: identification of a novel and functionally critical leucine-rich motif (62-LYLYLQL-68) in the regulatory factor X 5 transcription factor

Brickey WJ Wright KL Zhu XS Ting JP 《Journal of immunology (Baltimore, Md. : 1950)》1999,163(12):6622-6630

相似文献

12.

Peroxisome proliferator-activated receptor gamma interacts with CIITA x RFX5 complex to repress type I collagen gene expression

Xu Y Farmer SR Smith BD 《The Journal of biological chemistry》2007,282(36):26046-26056

相似文献

13.

Genomic mapping of the MHC transactivator CIITA using an integrated ChIP-seq and genetical genomics approach

Daniel Wong Wanseon Lee Peter Humburg Seiko Makino Evelyn Lau Vivek Naranbhai Benjamin P Fairfax Kenneth Chan Katharine Plant Julian C Knight 《Genome biology》2014,15(10)

Background

The master transactivator CIITA is essential to the regulation of Major Histocompatibility Complex (MHC) class II genes and an effective immune response. CIITA is known to modulate a small number of non-MHC genes involved in antigen presentation such as CD74 and B2M but its broader genome-wide function and relationship with underlying genetic diversity has not been resolved.

Results

We report the first genome-wide ChIP-seq map for CIITA and complement this by mapping inter-individual variation in CIITA expression as a quantitative trait. We analyse CIITA recruitment for pathophysiologically relevant primary human B cells and monocytes, resting and treated with interferon-gamma, in the context of the epigenomic regulatory landscape and DNA-binding proteins associated with the CIITA enhanceosome including RFX, CREB1/ATF1 and NFY. We confirm recruitment to proximal promoter sequences in MHC class II genes and more distally involving the canonical CIITA enhanceosome. Overall, we map 843 CIITA binding intervals involving 442 genes and find 95% of intervals are located outside the MHC and 60% not associated with RFX5 binding. Binding intervals are enriched for genes involved in immune function and infectious disease with novel loci including major histone gene clusters. We resolve differentially expressed genes associated in trans with a CIITA intronic sequence variant, integrate with CIITA recruitment and show how this is mediated by allele-specific recruitment of NF-kB.

Conclusions

Our results indicate a broader role for CIITA beyond the MHC involving immune-related genes. We provide new insights into allele-specific regulation of CIITA informative for understanding gene function and disease.