The role of transcription factor PU.I in the activity of the intronic enhancer of the eosinophil-derived neurotoxin (RNS2) gene

Thamar B. Van Dijk; Eric Caldenhoven; Jan A M Raaijmakers; Jan Willem J Lammers; Leo Koenderman; Rolf P. De Groot

The role of transcription factor PU.I in the activity of the intronic enhancer of the eosinophil-derived neurotoxin (RNS2) gene

Thamar B. Van Dijk, Eric Caldenhoven, Jan A M Raaijmakers, Jan Willem J Lammers, Leo Koenderman, Rolf P. De Groot^*

^*Corresponding author for this work

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

35 Citations (Scopus)

Abstract

Eosinophil-derived neurotoxin (EDN) found in the granules of human eosinophils is a cationic ribonuclease toxin. Expression of the EDN gene (RNS2) in eosinophils is dependent on proximal promoter sequences in combination with an enhancer located in the first intron. We further define here the active region of the intron using transfections in differentiated eosinophilic HL60 cells. We show that a region containing a tandem PU.I binding site is important for intronic enhancer activity. This region binds multiple forms of transcription factor PU.I as judged by gel-shift analysis and DNA affinity precipitation. Importantly, introducing point mutations in the PU.I site drastically reduces the intronic enhancer activity, showing the importance of PU.I for expression of EDN in cells of the eosinophilic lineage.

Original language	English
Pages (from-to)	2126-2132
Number of pages	7
Journal	Blood
Volume	91
Issue number	6
Publication status	Published - 15 Mar 1998

Cite this

@article{569c8d08c5084c64abb3ae7eda5c4899,

title = "The role of transcription factor PU.I in the activity of the intronic enhancer of the eosinophil-derived neurotoxin (RNS2) gene",

abstract = "Eosinophil-derived neurotoxin (EDN) found in the granules of human eosinophils is a cationic ribonuclease toxin. Expression of the EDN gene (RNS2) in eosinophils is dependent on proximal promoter sequences in combination with an enhancer located in the first intron. We further define here the active region of the intron using transfections in differentiated eosinophilic HL60 cells. We show that a region containing a tandem PU.I binding site is important for intronic enhancer activity. This region binds multiple forms of transcription factor PU.I as judged by gel-shift analysis and DNA affinity precipitation. Importantly, introducing point mutations in the PU.I site drastically reduces the intronic enhancer activity, showing the importance of PU.I for expression of EDN in cells of the eosinophilic lineage.",

author = "{Van Dijk}, {Thamar B.} and Eric Caldenhoven and Raaijmakers, {Jan A M} and Lammers, {Jan Willem J} and Leo Koenderman and {De Groot}, {Rolf P.}",

year = "1998",

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T1 - The role of transcription factor PU.I in the activity of the intronic enhancer of the eosinophil-derived neurotoxin (RNS2) gene

AU - Van Dijk, Thamar B.

AU - Caldenhoven, Eric

AU - Raaijmakers, Jan A M

AU - Lammers, Jan Willem J

AU - Koenderman, Leo

AU - De Groot, Rolf P.

PY - 1998/3/15

Y1 - 1998/3/15

N2 - Eosinophil-derived neurotoxin (EDN) found in the granules of human eosinophils is a cationic ribonuclease toxin. Expression of the EDN gene (RNS2) in eosinophils is dependent on proximal promoter sequences in combination with an enhancer located in the first intron. We further define here the active region of the intron using transfections in differentiated eosinophilic HL60 cells. We show that a region containing a tandem PU.I binding site is important for intronic enhancer activity. This region binds multiple forms of transcription factor PU.I as judged by gel-shift analysis and DNA affinity precipitation. Importantly, introducing point mutations in the PU.I site drastically reduces the intronic enhancer activity, showing the importance of PU.I for expression of EDN in cells of the eosinophilic lineage.

AB - Eosinophil-derived neurotoxin (EDN) found in the granules of human eosinophils is a cationic ribonuclease toxin. Expression of the EDN gene (RNS2) in eosinophils is dependent on proximal promoter sequences in combination with an enhancer located in the first intron. We further define here the active region of the intron using transfections in differentiated eosinophilic HL60 cells. We show that a region containing a tandem PU.I binding site is important for intronic enhancer activity. This region binds multiple forms of transcription factor PU.I as judged by gel-shift analysis and DNA affinity precipitation. Importantly, introducing point mutations in the PU.I site drastically reduces the intronic enhancer activity, showing the importance of PU.I for expression of EDN in cells of the eosinophilic lineage.

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AN - SCOPUS:0032520934

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JF - Blood

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The role of transcription factor PU.I in the activity of the intronic enhancer of the eosinophil-derived neurotoxin (RNS2) gene

Abstract

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