pS2 Gene Expression in HepG2 cells: Complex Regulation through Crosstalk between the Estrogen Receptor α, an Estrogen-Responsive Element, and the Activator Protein 1 Response Element
The pS2 promoter is complex with binding sites for a number of protein factors that may participate in modulating its activity. The pS2 gene was transcriptionally activated by estrogens in HepG2 cells transformed (HepER3) to express the estrogen receptor α (ERα). The phorbol ester phorbol 12-myris...
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| Veröffentlicht in: | Molecular pharmacology 2002-06, Vol.61 (6), p.1273 |
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| creator | Tomas Barkhem Lars-Arne Haldosén Jan-à ke Gustafsson Stefan Nilsson |
| description | The pS2 promoter is complex with binding sites for a number of protein factors that may participate in modulating its activity.
The pS2 gene was transcriptionally activated by estrogens in HepG2 cells transformed (HepER3) to express the estrogen receptor α
(ERα). The phorbol ester phorbol 12-myristate 13-acetate (PMA) stimulated pS2 expression in both HepER3 and the parental,
nonâER-expressing HepG2 cells, although its activity was substantially less in HepG2 cells. The use of selective protein kinase
inhibitors suggested that the MAPK pathway contributes substantially to estrogen stimulation of the pS2 promoter. The activator
protein 1 (AP1) site at â332 to â338 in the pS2 promoter had a dominant role in the response to both estrogens and PMA, although
the estrogen response element at â393 to â405 was essential to mediate the response to estrogen. The potentiation of pS2 promoter
activity by the AP1 motif in response to estrogen was dependent on the ligand binding domain of ERα. Furthermore, the presence
of an intact AP1 element in the pS2 promoter sustained suppression of pS2 promoter activity by an LXXLL peptide. In summary,
the data suggest that the effect of estrogen is mediated through a cross-talk between the estrogen-responsive element and
the AP1 response element and that ERα plays a crucial role in mediating the effect of both estrogen and PMA. |
| doi_str_mv | 10.1124/mol.61.6.1273 |
| format | Article |
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ke Gustafsson ; Stefan Nilsson</creator><creatorcontrib>Tomas Barkhem ; Lars-Arne Haldosén ; Jan-Ã
ke Gustafsson ; Stefan Nilsson</creatorcontrib><description>The pS2 promoter is complex with binding sites for a number of protein factors that may participate in modulating its activity.
The pS2 gene was transcriptionally activated by estrogens in HepG2 cells transformed (HepER3) to express the estrogen receptor α
(ERα). The phorbol ester phorbol 12-myristate 13-acetate (PMA) stimulated pS2 expression in both HepER3 and the parental,
nonâER-expressing HepG2 cells, although its activity was substantially less in HepG2 cells. The use of selective protein kinase
inhibitors suggested that the MAPK pathway contributes substantially to estrogen stimulation of the pS2 promoter. The activator
protein 1 (AP1) site at â332 to â338 in the pS2 promoter had a dominant role in the response to both estrogens and PMA, although
the estrogen response element at â393 to â405 was essential to mediate the response to estrogen. The potentiation of pS2 promoter
activity by the AP1 motif in response to estrogen was dependent on the ligand binding domain of ERα. Furthermore, the presence
of an intact AP1 element in the pS2 promoter sustained suppression of pS2 promoter activity by an LXXLL peptide. In summary,
the data suggest that the effect of estrogen is mediated through a cross-talk between the estrogen-responsive element and
the AP1 response element and that ERα plays a crucial role in mediating the effect of both estrogen and PMA.</description><identifier>ISSN: 0026-895X</identifier><identifier>EISSN: 1521-0111</identifier><identifier>DOI: 10.1124/mol.61.6.1273</identifier><identifier>PMID: 12021387</identifier><language>eng</language><publisher>American Society for Pharmacology and Experimental Therapeutics</publisher><ispartof>Molecular pharmacology, 2002-06, Vol.61 (6), p.1273</ispartof><lds50>peer_reviewed</lds50><woscitedreferencessubscribed>false</woscitedreferencessubscribed></display><links><openurl>$$Topenurl_article</openurl><openurlfulltext>$$Topenurlfull_article</openurlfulltext><thumbnail>$$Tsyndetics_thumb_exl</thumbnail><link.rule.ids>314,780,784,27924,27925</link.rule.ids></links><search><creatorcontrib>Tomas Barkhem</creatorcontrib><creatorcontrib>Lars-Arne Haldosén</creatorcontrib><creatorcontrib>Jan-Ã
ke Gustafsson</creatorcontrib><creatorcontrib>Stefan Nilsson</creatorcontrib><title>pS2 Gene Expression in HepG2 cells: Complex Regulation through Crosstalk between the Estrogen Receptor α, an Estrogen-Responsive Element, and the Activator Protein 1 Response Element</title><title>Molecular pharmacology</title><description>The pS2 promoter is complex with binding sites for a number of protein factors that may participate in modulating its activity.
The pS2 gene was transcriptionally activated by estrogens in HepG2 cells transformed (HepER3) to express the estrogen receptor α
(ERα). The phorbol ester phorbol 12-myristate 13-acetate (PMA) stimulated pS2 expression in both HepER3 and the parental,
nonâER-expressing HepG2 cells, although its activity was substantially less in HepG2 cells. The use of selective protein kinase
inhibitors suggested that the MAPK pathway contributes substantially to estrogen stimulation of the pS2 promoter. The activator
protein 1 (AP1) site at â332 to â338 in the pS2 promoter had a dominant role in the response to both estrogens and PMA, although
the estrogen response element at â393 to â405 was essential to mediate the response to estrogen. The potentiation of pS2 promoter
activity by the AP1 motif in response to estrogen was dependent on the ligand binding domain of ERα. Furthermore, the presence
of an intact AP1 element in the pS2 promoter sustained suppression of pS2 promoter activity by an LXXLL peptide. In summary,
the data suggest that the effect of estrogen is mediated through a cross-talk between the estrogen-responsive element and
the AP1 response element and that ERα plays a crucial role in mediating the effect of both estrogen and PMA.</description><issn>0026-895X</issn><issn>1521-0111</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2002</creationdate><recordtype>article</recordtype><sourceid/><recordid>eNqNkD1PwzAQhi0EouFjZPfERILPadLAhqrSjigwsEUmHInBsS3b_eBP8F8YWeGPkaCqM9Pp9Dzv6fQScgYsAeDjy86oJIckT4BP0j0SQcYhZgCwTyLGeB4XV9njiBx5_8oYjLOCHZIRcMYhLSYR-bL3nM5RI51trEPvpdFUarpAO-e0RqX8NZ2azirc0BKbpRJhUELrzLJp6dQZ74NQb_QJwxpxIP0tH5xp-qXEGm0wjv58fH9eUKF3KC7RW6O9XPW6wg51GPjzX_6mDnIlhtydMwH7f4Bu_Z19Qg5ehPJ4up3H5Px29jBdxK1s2rV0WNlWuE7URpnmvcqhyquho_Tf4i_I83De</recordid><startdate>20020601</startdate><enddate>20020601</enddate><creator>Tomas Barkhem</creator><creator>Lars-Arne Haldosén</creator><creator>Jan-Ã
ke Gustafsson</creator><creator>Stefan Nilsson</creator><general>American Society for Pharmacology and Experimental Therapeutics</general><scope/></search><sort><creationdate>20020601</creationdate><title>pS2 Gene Expression in HepG2 cells: Complex Regulation through Crosstalk between the Estrogen Receptor α, an Estrogen-Responsive Element, and the Activator Protein 1 Response Element</title><author>Tomas Barkhem ; Lars-Arne Haldosén ; Jan-Ã
ke Gustafsson ; Stefan Nilsson</author></sort><facets><frbrtype>5</frbrtype><frbrgroupid>cdi_FETCH-highwire_pharmacology_61_6_12733</frbrgroupid><rsrctype>articles</rsrctype><prefilter>articles</prefilter><language>eng</language><creationdate>2002</creationdate><toplevel>peer_reviewed</toplevel><toplevel>online_resources</toplevel><creatorcontrib>Tomas Barkhem</creatorcontrib><creatorcontrib>Lars-Arne Haldosén</creatorcontrib><creatorcontrib>Jan-Ã
ke Gustafsson</creatorcontrib><creatorcontrib>Stefan Nilsson</creatorcontrib><jtitle>Molecular pharmacology</jtitle></facets><delivery><delcategory>Remote Search Resource</delcategory><fulltext>fulltext</fulltext></delivery><addata><au>Tomas Barkhem</au><au>Lars-Arne Haldosén</au><au>Jan-Ã
ke Gustafsson</au><au>Stefan Nilsson</au><format>journal</format><genre>article</genre><ristype>JOUR</ristype><atitle>pS2 Gene Expression in HepG2 cells: Complex Regulation through Crosstalk between the Estrogen Receptor α, an Estrogen-Responsive Element, and the Activator Protein 1 Response Element</atitle><jtitle>Molecular pharmacology</jtitle><date>2002-06-01</date><risdate>2002</risdate><volume>61</volume><issue>6</issue><spage>1273</spage><pages>1273-</pages><issn>0026-895X</issn><eissn>1521-0111</eissn><abstract>The pS2 promoter is complex with binding sites for a number of protein factors that may participate in modulating its activity.
The pS2 gene was transcriptionally activated by estrogens in HepG2 cells transformed (HepER3) to express the estrogen receptor α
(ERα). The phorbol ester phorbol 12-myristate 13-acetate (PMA) stimulated pS2 expression in both HepER3 and the parental,
nonâER-expressing HepG2 cells, although its activity was substantially less in HepG2 cells. The use of selective protein kinase
inhibitors suggested that the MAPK pathway contributes substantially to estrogen stimulation of the pS2 promoter. The activator
protein 1 (AP1) site at â332 to â338 in the pS2 promoter had a dominant role in the response to both estrogens and PMA, although
the estrogen response element at â393 to â405 was essential to mediate the response to estrogen. The potentiation of pS2 promoter
activity by the AP1 motif in response to estrogen was dependent on the ligand binding domain of ERα. Furthermore, the presence
of an intact AP1 element in the pS2 promoter sustained suppression of pS2 promoter activity by an LXXLL peptide. In summary,
the data suggest that the effect of estrogen is mediated through a cross-talk between the estrogen-responsive element and
the AP1 response element and that ERα plays a crucial role in mediating the effect of both estrogen and PMA.</abstract><pub>American Society for Pharmacology and Experimental Therapeutics</pub><pmid>12021387</pmid><doi>10.1124/mol.61.6.1273</doi></addata></record> |
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| title | pS2 Gene Expression in HepG2 cells: Complex Regulation through Crosstalk between the Estrogen Receptor α, an Estrogen-Responsive Element, and the Activator Protein 1 Response Element |
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