Zeste encodes a sequence-specific transcription factor that activates the Ultrabithorax promoter in vitro

Mark D. Biggin; Sharon Bickel; Mark Benson; Vincenzo Pirrotta; Robert Tjian

doi:10.1016/0092-8674(88)90089-X

Zeste encodes a sequence-specific transcription factor that activates the Ultrabithorax promoter in vitro

Mark D. Biggin, Sharon Bickel, Mark Benson, Vincenzo Pirrotta, Robert Tjian

Research output: Contribution to journal › Article › peer-review

96 Scopus citations

Abstract

Zeste is a Drosophila regulatory gene that is required for transvection at the bithorax complex. Here we find that purified zeste protein binds to multiple sites just 5′ of the initiation site of Ubx RNA. Zeste protein purified from Drosophila cells or from E. coli expressing the zeste gene activates Ubx transcription in vitro. This activation is dependent on the presence of zeste protein binding sites, as it is not observed with a Ubx promoter lacking these sites or with an Adh promoter. These results suggest that transvection involves regulatory elements that act at the level of transcriptional initiation and may be mechanistically similar to activation of transcription by enhancer elements, except that transvection occurs across paired chromosomes. These findings are consistent with the hypothesis that zeste may play a more important role in the normal regulation of Ubx and its other target genes than current genetic evidence implies.

Original language	English (US)
Pages (from-to)	713-722
Number of pages	10
Journal	Cell
Volume	53
Issue number	5
DOIs	https://doi.org/10.1016/0092-8674(88)90089-X
State	Published - Jun 3 1988
Externally published	Yes

All Science Journal Classification (ASJC) codes

General Biochemistry, Genetics and Molecular Biology

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10.1016/0092-8674(88)90089-X

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title = "Zeste encodes a sequence-specific transcription factor that activates the Ultrabithorax promoter in vitro",

abstract = "Zeste is a Drosophila regulatory gene that is required for transvection at the bithorax complex. Here we find that purified zeste protein binds to multiple sites just 5′ of the initiation site of Ubx RNA. Zeste protein purified from Drosophila cells or from E. coli expressing the zeste gene activates Ubx transcription in vitro. This activation is dependent on the presence of zeste protein binding sites, as it is not observed with a Ubx promoter lacking these sites or with an Adh promoter. These results suggest that transvection involves regulatory elements that act at the level of transcriptional initiation and may be mechanistically similar to activation of transcription by enhancer elements, except that transvection occurs across paired chromosomes. These findings are consistent with the hypothesis that zeste may play a more important role in the normal regulation of Ubx and its other target genes than current genetic evidence implies.",

author = "Biggin, {Mark D.} and Sharon Bickel and Mark Benson and Vincenzo Pirrotta and Robert Tjian",

note = "Funding Information: {\textquoteleft}We are grateful to Bruce England for generously supplying Kc cell protein fractions and advice. We thank Al Courey, Michael Jantzen, Richard Carthew, Steve Bell, Trevor Williams, and Jim Kadonaga for helpful comments on the manuscript. This work is funded in part by grants from the National Institutes of Health (NIH) and the National Science Foundation (NSF) to Ft. T. and from the NIH to V. f? M. D. B. is supported by a Science and Engineering Research Council/NATO fellowship, S. B. by an NSF fellowship, and M. B. by the MSTP The costs of publication of this article were defrayed in part by the payment of page charges. This article must therefore be hereby marked “advertisement” in accordance with 18 U.S.C. Section 1734 solely to indicate this fact.",

year = "1988",

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doi = "10.1016/0092-8674(88)90089-X",

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AU - Biggin, Mark D.

AU - Bickel, Sharon

AU - Benson, Mark

AU - Pirrotta, Vincenzo

AU - Tjian, Robert

N1 - Funding Information: ‘We are grateful to Bruce England for generously supplying Kc cell protein fractions and advice. We thank Al Courey, Michael Jantzen, Richard Carthew, Steve Bell, Trevor Williams, and Jim Kadonaga for helpful comments on the manuscript. This work is funded in part by grants from the National Institutes of Health (NIH) and the National Science Foundation (NSF) to Ft. T. and from the NIH to V. f? M. D. B. is supported by a Science and Engineering Research Council/NATO fellowship, S. B. by an NSF fellowship, and M. B. by the MSTP The costs of publication of this article were defrayed in part by the payment of page charges. This article must therefore be hereby marked “advertisement” in accordance with 18 U.S.C. Section 1734 solely to indicate this fact.

PY - 1988/6/3

Y1 - 1988/6/3

N2 - Zeste is a Drosophila regulatory gene that is required for transvection at the bithorax complex. Here we find that purified zeste protein binds to multiple sites just 5′ of the initiation site of Ubx RNA. Zeste protein purified from Drosophila cells or from E. coli expressing the zeste gene activates Ubx transcription in vitro. This activation is dependent on the presence of zeste protein binding sites, as it is not observed with a Ubx promoter lacking these sites or with an Adh promoter. These results suggest that transvection involves regulatory elements that act at the level of transcriptional initiation and may be mechanistically similar to activation of transcription by enhancer elements, except that transvection occurs across paired chromosomes. These findings are consistent with the hypothesis that zeste may play a more important role in the normal regulation of Ubx and its other target genes than current genetic evidence implies.

AB - Zeste is a Drosophila regulatory gene that is required for transvection at the bithorax complex. Here we find that purified zeste protein binds to multiple sites just 5′ of the initiation site of Ubx RNA. Zeste protein purified from Drosophila cells or from E. coli expressing the zeste gene activates Ubx transcription in vitro. This activation is dependent on the presence of zeste protein binding sites, as it is not observed with a Ubx promoter lacking these sites or with an Adh promoter. These results suggest that transvection involves regulatory elements that act at the level of transcriptional initiation and may be mechanistically similar to activation of transcription by enhancer elements, except that transvection occurs across paired chromosomes. These findings are consistent with the hypothesis that zeste may play a more important role in the normal regulation of Ubx and its other target genes than current genetic evidence implies.

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Zeste encodes a sequence-specific transcription factor that activates the Ultrabithorax promoter in vitro

Abstract

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