Different members of the Sp1 multigene family exert opposite transcritional regulation of the long terminal repeat of HIV-1

Majello, Barbara; Luca, Pasquale De; Hagen, Gustav; Suske, Guntram; Lania, Luigi

doi:10.1093/nar/22.23.4914

Cited by 237 publications

(263 citation statements)

References 31 publications

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“…A three zinc finger domain is highly conserved in members of this family, resulting in similar binding affinities to GC, GT and GA boxes. Sp1, Sp2 and Sp4 activate gene transcription, whereas Sp3 may function either as an activator or a repressor (49)(50)(51)(52)(53)(54)(55).…”

Section: Discussionmentioning

confidence: 99%

Overlapping Sp1 and AP2 binding sites in a promoter element of the lens-specific MIP gene

Ohtaka-Maruyama

Wang

et al. 1998

Nucleic Acids Research

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The MIP gene, the founder of the MIP family of channel proteins, is specifically expressed in fiber cells of the ocular lens and expression is regulated temporally and spatially during development. We previously found that a DNA fragment containing 253 bp of 5′-flanking sequence and 42 bp of exon 1 of the human MIP gene contains regulatory elements responsible for lensspecific expression of the MIP gene. In this report we have analyzed the function of overlapping Sp1 and AP2 binding sites present in the MIP promoter. Using DNase I footprinting analysis we found that purified Sp1 and AP2 transcription factors interact with several domains of the human MIP promoter sequence -253/+42. Furthermore, addition of purified Sp1 to Drosophila nuclear extracts activates in vitro transcription from the MIP promoter -253/+42. This promoter activity is competed by oligonucleotides containing domains footprinted with Sp1. Using promoter-reporter gene (CAT) constructs we found that the sequence -39/-70 contains a cis regulatory element essential for promoter activity in transient assays in lens cells. EMSA analysis showed that lens nuclear extracts contain factors that bind to the MIP 5′-flanking sequence containing overlapping Sp1 and AP2 binding domains at positions -37/-65. Supershift experiments with lens nuclear extracts indicated that Sp3 is also able to interact with this regulatory element, suggesting that Sp1 and Sp3 may be involved in regulation of transcription of the MIP gene in the lens.

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Section: Discussionmentioning

confidence: 99%

Overlapping Sp1 and AP2 binding sites in a promoter element of the lens-specific MIP gene

Ohtaka-Maruyama

Wang

et al. 1998

Nucleic Acids Research

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“…Sp3 has been reported to repress Sp1-mediated transcriptional activation, suggesting that it may be an inhibitory member of the Sp family of regulators (Majello et al, 1994;Hagen et al, 1995). However, the recent ®nding that Sp1 and Sp3 encode multiple proteins that di er in their capacity to stimulate or repress transcription, suggests that transcriptional control by the Sp family members is much more complex (Persengiev et al, 1995;Kennett et al, 1997;Dennig et al, 1997).…”

Section: Cooperation Of P300 and Sp1 In Cell Cycle Arrest During DI Ementioning

confidence: 99%

“…Two Sp3-related proteins of 78 kDa and 80 kDa, arising via internal translational initiation within Sp3 mRNA, have been described (Kennett et al, 1997). These two isoforms inhibit Spmediated transcription in vivo, while the initially described 110 kDa isoform behaves as a transcriptional activator (Majello et al, 1994). In the present study, we observed that all three isoforms of Sp3 are present in PC12 cells and speci®cally associate with the NGF-responsive region of the p21 promoter in both NGF-treated and exponentially-growing PC12 cells.…”

Section: Cooperation Of P300 and Sp1 In Cell Cycle Arrest During DI Ementioning

confidence: 99%

Cooperation of Sp1 and p300 in the induction of the CDK inhibitor p21WAF1/CIP1 during NGF-mediated neuronal differentiation

et al. 1999

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Addition of nerve growth factor (NGF) to PC12 cells promotes neuronal di erentiation while inhibiting cell proliferation. In order to understand how NGF exerts its antimitogenic e ect during di erentiation, we have studied the mechanism by which this factor activates the promoter of the CDK inhibitor p21 WAF1/CIP1 . The minimal region of the p21 promoter required for the NGF-induction was mapped to a contiguous stretch of 10 bp located 83 bases upstream of the transcription initiation site. This GC-rich region was shown to interact speci®cally with the transcription factor Sp1 and the related protein Sp3, in either exponentiallygrowing or NGF-treated PC12 cells. The addition of NGF resulted in an accumulation of the transcriptional co-activator p300 in complexes associated with the NGF-responsive region. Transcriptional activity of Sp1, Sp3 and p300 was speci®cally induced by NGF in a Gal4-fusion assay, indicating that induction of p21 during neuronal di erentiation may involve regulation of the activity of these factors by NGF. Furthermore, p300 was able to act as a co-activator for Sp1-mediated transcriptional activation in PC12 cells, suggesting that p300 and Sp1 may cooperate in activating p21 transcription during the withdrawal of neuronal precursors from the cell cycle. This hypothesis is supported by experiments showing that p300 and Sp1 form complexes in PC12 cells.

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“…Sp2, Sp3 and Sp4 are Sp1-related proteins. These proteins, like Sp1, are ubiquitously expressed, are glutamine-and serine/threonine-rich, and have similar DNA-binding speci®city, but display di erential e ects on the gene regulation (Hagen et al, 1992Kingsley and Winoto, 1992;Majello et al, 1994;Dennig et al, 1995). Among these, Sp1 is a highly studied factor and is known to activate many GC-box-containing viral and cellular promoters Tjian, 1983a,b, 1985;Gidoni et al, 1985).…”

Section: Introductionmentioning

confidence: 99%

Kinetic analysis of Sp1-mediated transcriptional activation of the human DNA polymerase β promoter

Narayan

Wilson

2000

Oncogene

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In the present studies, we have examined the e ect of Sp1 on the activation of the human DNA polymerase b (b-pol), a TATA-less promoter. A HeLa cell nuclear extract (NE) based in vitro runo transcription system of core b-pol promoter human DNA (pbP8) three-step kinetic model of transcription initiation were used to describe the kinetic e ect of Sp1. The results showed that distal Sp1-binding sites in the core b-pol promoter are important for transcriptional activation of the pbP8 promoter. A detailed kinetic analysis showed that Sp1 stimulates the activity of the pbP8 promoter through distal Sp1-binding sites by increasing the amount of recruitment, instead of stimulating the apparent rate of RP c assembly (k 1 ). There was no signi®cant e ect of Sp1 on the apparent rate of open complex (RP o ) formation (k 2 ) or on the apparent rate of promoter clearance (k 3 ) of the pbP8 promoter. These studies de®ne the kinetic mechanisms by which Sp1 may regulate the rate of transcript formation of the pbP8 promoter, and these results may have implications for Sp1 regulation of TATA-less promoters. Oncogene (2000) 19, 4729 ± 4735.

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Different members of the Sp1 multigene family exert opposite transcritional regulation of the long terminal repeat of HIV-1

Cited by 237 publications

References 31 publications

Overlapping Sp1 and AP2 binding sites in a promoter element of the lens-specific MIP gene

Overlapping Sp1 and AP2 binding sites in a promoter element of the lens-specific MIP gene

Cooperation of Sp1 and p300 in the induction of the CDK inhibitor p21WAF1/CIP1 during NGF-mediated neuronal differentiation

Kinetic analysis of Sp1-mediated transcriptional activation of the human DNA polymerase β promoter

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