AN ATF/CREB-BINDING SITE IS ESSENTIAL FOR CELL-SPECIFIC AND INDUCIBLE TRANSCRIPTION OF THE MURINE MIP-1-BETA CYTOKINE GENE

被引：31

作者：

PROFFITT, J

CRABTREE, G

GROVE, M

DAUBERSIES, P

BAILLEUL, B

WRIGHT, E

PLUMB, M

机构：

[1] MRC, RADIOBIOL UNIT, DIDCOT OX11 0RD, OXON, ENGLAND

[2] ST JAMES UNIV HOSP, IMPERIAL CANC RES FUND, CANC MED RES UNIT, LEEDS LS9 7TF, W YORKSHIRE, ENGLAND

[3] DUKE UNIV, MED CTR, DEPT PHARMACOL, DURHAM, NC 27710 USA

[4] INST RECH CANC LILLE, INSERM, U124, F-59045 LILLE, FRANCE

来源：

GENE | 1995年 / 152卷 / 02期

基金：

英国医学研究理事会;

关键词：

TRANSCRIPTIONAL REGULATION; PROMOTER; DNA-BINDING FACTOR; IMMEDIATE EARLY RESPONSE GENE;

D O I：

10.1016/0378-1119(94)00701-S

中图分类号：

Q3 [遗传学];

学科分类号：

071007 ; 090102 ;

摘要：

The murine macrophage inflammatory protein IP mRNA (MIP-IB) is rapidly and transiently induced in macrophages by lipopolysacharride (LPS), serum or cycloheximide. Functional studies of the MIP-1 beta proximal promoter indicate that it is cell-specific, and serum- and LPS-responsive in macrophages. A 76-bp proximal promoter sequence (-51 to - 127 bp) confers cell-specific and LPS-inducible activity when placed upstream from a heterologous promoter in both orientations. One essential cis-regulatory element within the enhancer-like sequence is an activating transcription factor/cAMP response element (CRE)-binding protein (ATF/CREB)-binding site, although the promoter is not cAMP responsive. Electrophoretic mobility shift assays and mutational analyses suggest that the promoter site is bound by nuclear protein complexes containing cAMP-independent members of the ATF/CREB family of proteins and c-Jun, and are functionally distinct from the AP1-related TPA-response element (TRE) binding activity.

引用

页码：173 / 179

页数：7

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