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Chimeric oncogenic interferon regulatory factor-2 (IRF-2): Degradation products are biologically active
Chimeric oncogenic interferon regulatory factor-2 (IRF-2): Degradation products are biologically active
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摘要:
Interferon Regulatory Factor-2 (IRF-2) belongs to IRF family, was identified as a mammalian transcription factor involved in Interferon beta (IFNβ) gene regulation. Besides that IRF-2 is involved in immunomodulation, hematopoietic differentiation, cell cycle regulation and oncogenesis. We have done molecular sub-cloning and expression of recombinant murine IRF-2 as GST (Glutathione-S-Transferase)- IRF-2 fusion protein in E. coli/XL-1blue cells. Recombinant IRF-2 with GST moiety at N-terminus expressed as GST-IRF-2 (~66 kd) in E. coli along with different low molecular mass degradation products revealed approximately 30, 42, 60 and 62 kd by SDS-PAGE and Western blot, respectively. We further confirm that degradation takes place at C-terminus of the fusion protein not at N-terminus as anti-GST antibody was detecting all bands in the immunoblot. The recombinant IRF-2 was biologically active along with their degradation products in terms of their DNA binding activity as assessed by Electrophoretically Mobility Shift Assay (EMSA). We observed three different molecular mass DNA/protein complexes (1 - 3) with Virus Response Element (VRE) derived from human Interferon IFNβ gene and five different molecular mass complexes (1 - 5) with IRF-E motif (GAAAGT)4 in EMSA gel. GST only expressed from empty vector did not bind to these DNA elements. To confirm that the binding is specific, all complexes were competed out completely when challenged with 100-X fold molar excess of IRF-E oligo under cold competition. It means degradation products along with full-length protein are able to interact with VREβ as well as IRF-E motif. This means degradation products may regulate the target gene (s) activation/repression via interacting with VRE/IRF-E.
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| 篇名 | Chimeric oncogenic interferon regulatory factor-2 (IRF-2): Degradation products are biologically active | ||
| 来源期刊 | 美国分子生物学期刊(英文) | 学科 | 医学 |
| 关键词 | Recombinant INTERFERON REGULATORY Factor-2 (IRF-2) DNA Binding Domain (DBD) C-TERMINUS of IRF-2 EMSA | ||
| 年,卷(期) | 2012,(4) | 所属期刊栏目 | |
| 研究方向 | 页码范围 | 371-379 | |
| 页数 | 9页 | 分类号 | R73 |
| 字数 | 语种 | ||
| DOI | |||
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Recombinant
INTERFERON
REGULATORY
Factor-2
(IRF-2)
DNA
Binding
Domain
(DBD)
C-TERMINUS
of
IRF-2
EMSA
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研究去脉
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美国分子生物学期刊(英文)
主办单位:
美国科研出版社
出版周期:
季刊
ISSN:
2161-6620
CN:
开本:
出版地:
武汉市江夏区汤逊湖北路38号光谷总部空间
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191
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