Focused transcription from the human CR2/CD21 core promoter is regulated by synergistic activity of TATA and Initiator elements in mature B cells

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作者
Rhonda L Taylor
Mark N Cruickshank
Mahdad Karimi
Han Leng Ng
Elizabeth Quail
Kenneth M Kaufman
John B Harley
Lawrence J Abraham
Betty P Tsao
Susan A Boackle
Daniela Ulgiati
机构
[1] School of Pathology and Laboratory Medicine,Division of Rheumatology, Department of Medicine
[2] Centre for Genetic Origins of Health and Disease,Division of Rheumatology
[3] The University of Western Australia,undefined
[4] Biochemistry and Molecular Biology,undefined
[5] School of Chemistry and Biochemistry,undefined
[6] The University of Western Australia,undefined
[7] Telethon Kids Institute,undefined
[8] The University of Western Australia,undefined
[9] Cincinnati Children's Hospital Medical Center,undefined
[10] US Department of Veterans Affairs Medical Center,undefined
[11] University of California at Los Angeles,undefined
[12] University of Colorado School of Medicine,undefined
[13] Aurora,undefined
[14] CO,undefined
[15] USA,undefined
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关键词
B cells; core promoter; CR2/CD21; molecular biology; transcription factor;
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摘要
Complement receptor 2 (CR2/CD21) is predominantly expressed on the surface of mature B cells where it forms part of a coreceptor complex that functions, in part, to modulate B-cell receptor signal strength. CR2/CD21 expression is tightly regulated throughout B-cell development such that CR2/CD21 cannot be detected on pre-B or terminally differentiated plasma cells. CR2/CD21 expression is upregulated at B-cell maturation and can be induced by IL-4 and CD40 signaling pathways. We have previously characterized elements in the proximal promoter and first intron of CR2/CD21 that are involved in regulating basal and tissue-specific expression. We now extend these analyses to the CR2/CD21 core promoter. We show that in mature B cells, CR2/CD21 transcription proceeds from a focused TSS regulated by a non-consensus TATA box, an initiator element and a downstream promoter element. Furthermore, occupancy of the general transcriptional machinery in pre-B versus mature B-cell lines correlate with CR2/CD21 expression level and indicate that promoter accessibility must switch from inactive to active during the transitional B-cell window.
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页码:119 / 131
页数:12
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